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Wikipedia

Gene therapy

February 26, 2023

Gene therapy is a medical field which focuses on the genetic modification of cells to produce a therapeutic effect[1] or the treatment of disease by repairing or reconstructing defective genetic material.[2] The first attempt at modifying human DNA was performed in 1980, by Martin Cline, but the first successful nuclear gene transfer in humans, approved by the National Institutes of Health, was performed in May 1989.[3] The first therapeutic use of gene transfer as well as the first direct insertion of human DNA into the nuclear genome was performed by French Anderson in a trial starting in September 1990. It is thought to be able to cure many genetic disorders or treat them over time.

Between 1989 and December 2018, over 2,900 clinical trials were conducted, with more than half of them in phase I.[4] In 2003, Gendicine became the first gene therapy to receive regulatory approval. Since that time, further gene therapy drugs were approved, such as Glybera (2012), Strimvelis (2016), Kymriah (2017), Luxturna (2017), Onpattro (2018), Zolgensma (2019), Abecma (2021), Adstiladrin, Roctavian and Hemgenix (all 2022). Most of these approaches utilize adeno-associated viruses (AAVs) and lentiviruses for performing gene insertions, in vivo and ex vivo, respectively. AAVs are characterized by stabilizing the viral capsid, lower immunogenicity, ability to transduce both dividing and nondividing cells, the potential to integrate site specifically and to achieve long-term expression in the in-vivo treatment.[5] ASO / siRNA approaches such as those conducted by Alnylam and Ionis Pharmaceuticals require non-viral delivery systems, and utilize alternative mechanisms for trafficking to liver cells by way of GalNAc transporters.

Not all medical procedures that introduce alterations to a patient's genetic makeup can be considered gene therapy. Bone marrow transplantation and organ transplants in general have been found to introduce foreign DNA into patients.[6]

Background

Gene therapy was conceptualized in 1972, by authors who urged caution before commencing human gene therapy studies.

The first attempt, an unsuccessful one, at gene therapy (as well as the first case of medical transfer of foreign genes into humans not counting organ transplantation) was performed by Martin Cline on 10 July 1980.[7][8] Cline claimed that one of the genes in his patients was active six months later, though he never published this data or had it verified[9] and even if he is correct, it's unlikely it produced any significant beneficial effects treating beta thalassemia.[medical citation needed]

After extensive research on animals throughout the 1980s and a 1989 bacterial gene tagging trial on humans, the first gene therapy widely accepted as a success was demonstrated in a trial that started on 14 September 1990, when Ashanthi DeSilva was treated for ADA-SCID.[10]

The first somatic treatment that produced a permanent genetic change was initiated in 1993.[11] The goal was to cure malignant brain tumors by using recombinant DNA to transfer a gene making the tumor cells sensitive to a drug that in turn would cause the tumor cells to die.[12]

The polymers are either translated into proteins, interfere with target gene expression, or possibly correct genetic mutations. The most common form uses DNA that encodes a functional, therapeutic gene to replace a mutated gene. The polymer molecule is packaged within a "vector", which carries the molecule inside cells.[medical citation needed]

Early clinical failures led to dismissals of gene therapy. Clinical successes since 2006 regained researchers' attention, although as of 2014, it was still largely an experimental technique.[13] These include treatment of retinal diseases Leber's congenital amaurosis[14][15][16][17] and choroideremia,[18] X-linked SCID,[19] ADA-SCID,[20][21] adrenoleukodystrophy,[22] chronic lymphocytic leukemia (CLL),[23] acute lymphocytic leukemia (ALL),[24] multiple myeloma,[25] haemophilia,[21] and Parkinson's disease.[26] Between 2013 and April 2014, US companies invested over $600 million in the field.[27]

The first commercial gene therapy, Gendicine, was approved in China in 2003, for the treatment of certain cancers.[28] In 2011, Neovasculgen was registered in Russia as the first-in-class gene-therapy drug for treatment of peripheral artery disease, including critical limb ischemia.[29] In 2012, Glybera, a treatment for a rare inherited disorder, lipoprotein lipase deficiency, became the first treatment to be approved for clinical use in either Europe or the United States after its endorsement by the European Commission.[13][30]

Following early advances in genetic engineering of bacteria, cells, and small animals, scientists started considering how to apply it to medicine. Two main approaches were considered – replacing or disrupting defective genes.[31] Scientists focused on diseases caused by single-gene defects, such as cystic fibrosis, haemophilia, muscular dystrophy, thalassemia, and sickle cell anemia. Glybera treats one such disease, caused by a defect in lipoprotein lipase.[30]

DNA must be administered, reach the damaged cells, enter the cell and either express or disrupt a protein.[32] Multiple delivery techniques have been explored. The initial approach incorporated DNA into an engineered virus to deliver the DNA into a chromosome.[33][34] Naked DNA approaches have also been explored, especially in the context of vaccine development.[35]

Generally, efforts focused on administering a gene that causes a needed protein to be expressed. More recently, increased understanding of nuclease function has led to more direct DNA editing, using techniques such as zinc finger nucleases and CRISPR. The vector incorporates genes into chromosomes. The expressed nucleases then knock out and replace genes in the chromosome. As of 2014 these approaches involve removing cells from patients, editing a chromosome and returning the transformed cells to patients.[36]

Gene editing is a potential approach to alter the human genome to treat genetic diseases,[37] viral diseases,[38] and cancer.[39][40] As of 2020 these approaches are being studied in clinical trials.[41][42]

Classification

Breadth of definition

In 1986, a meeting at the Institute Of Medicine defined gene therapy as the addition or replacement of a gene in a targeted cell type. In the same year, the FDA announced that it had jurisdiction over approving "gene therapy" without defining the term. The FDA added a very broad definition in 1993 of any treatment that would ‘modify or manipulate the expression of genetic material or to alter the biological properties of living cells’. In 2018 this was narrowed to ‘products that mediate their effects by transcription or translation of transferred genetic material or by specifically altering host (human) genetic sequences’.[43]

Writing in 2018, in the Journal of Law and the Biosciences, Sherkow et al argued for a narrower definition of gene therapy than the FDA's in light of new technology that would consist of any treatment that intentionally and permanently modified a cell's genome, with the definition of genome including episomes outside the nucleus but excluding changes due to episomes that are lost over time. This definition would also exclude introducing cells that did not derive from a patient themselves, but include ex vivo approaches, and would not depend on the vector used.[43]

During the COVID-19 pandemic, some academics insisted that the MRNA vaccines for COVID were not gene therapy to prevent the spread of incorrect information that the vaccine could alter DNA, other academics maintained that the vaccines were a gene therapy because they introduced genetic material into a cell.[44] Fact-checkers, such as Full Fact,[45] Reuters,[46] PolitiFact,[47] and FactCheck.org[48] said that calling the vaccines a gene therapy was incorrect. Podcast host Joe Rogan was criticized for calling MRNA vaccines gene therapy as was British politician Andrew Bridgen, with fact checker Full Fact calling for Bridgen to be removed from the conservative party for this and other statements.[49][50]

Genes present or added

Gene therapy encapsulates many forms of adding different nucleic acids to a cell. Gene augmentation adds a new protein coding gene to a cell. One form of gene augmentiation is gene replacement therapy, a treatment for monogenic recessive disorders where a single gene is not functional an additional functional gene is added. For diseases caused by multiple genes or a dominant gene gene silencing or gene editing approaches are more appropriate but gene addition, a form of gene augmentation where new gene is added, may improve a cells function despite other without modifying the genes that cause a disorder.[51]: 117 

Cell types

Gene therapy may be classified into two types by the type of cell it affects: somatic cell and germlie gene therapy.

In somatic cell gene therapy (SCGT), the therapeutic genes are transferred into any cell other than a gamete, germ cell, gametocyte, or undifferentiated stem cell. Any such modifications affect the individual patient only, and are not inherited by offspring. Somatic gene therapy represents mainstream basic and clinical research, in which therapeutic DNA (either integrated in the genome or as an external episome or plasmid) is used to treat disease.[52] Over 600 clinical trials utilizing SCGT are underway[when?] in the US. Most focus on severe genetic disorders, including immunodeficiencies, haemophilia, thalassaemia, and cystic fibrosis. Such single gene disorders are good candidates for somatic cell therapy. The complete correction of a genetic disorder or the replacement of multiple genes is not yet possible. Only a few of the trials are in the advanced stages.[53][needs update]

In germline gene therapy (GGT), germ cells (sperm or egg cells) are modified by the introduction of functional genes into their genomes. Modifying a germ cell causes all the organism's cells to contain the modified gene. The change is therefore heritable and passed on to later generations. Australia, Canada, Germany, Israel, Switzerland, and the Netherlands[54] prohibit GGT for application in human beings, for technical and ethical reasons, including insufficient knowledge about possible risks to future generations[54] and higher risks versus SCGT.[55] The US has no federal controls specifically addressing human genetic modification (beyond FDA regulations for therapies in general).[54][56][57][58]

In vivo versus ex vivo therapies

 

In in vivo gene therapy, a vector (typically, a virus) is introduced to the patient, which then achieves the desired biological effect by passing the genetic material (e.g. for a missing protein) into the patient's cells. In ex vivo gene therapies, such as CAR-T therapeutics, the patient's own cells (autologous) or healthy donor cells (allogeneic) are modified outside the body (hence, ex vivo) using a vector to express a particular protein, such as a chimeric antigen receptor.[59]

In vivo gene therapy is seen as simpler, since it does not require the harvesting of mitotic cells. However, ex vivo gene therapies are better tolerated and less associated with severe immune responses.[60] The death of Jesse Gelsinger in a trial of an adenovirus-vectored treatment for ornithine transcarbamylase deficiency due to a systemic inflammatory reaction led to a temporary halt on gene therapy trials across the United States.[61] As of 2021, in vivo and ex vivo therapeutics are both seen as safe.[62]

Gene editing

 
A duplex of crRNA and tracrRNA acts as guide RNA to introduce a specifically located gene modification based on the RNA 5' upstream of the crRNA. Cas9 binds the tracrRNA and needs a DNA binding sequence (5'NGG3'), which is called protospacer adjacent motif (PAM). After binding, Cas9 introduces a DNA double strand break, which is then followed by gene modification via homologous recombination (HDR) or non-homologous end joining (NHEJ).

The concept of gene therapy is to fix a genetic problem at its source. If, for instance, a mutation in a certain gene causes the production of a dysfunctional protein resulting (usually recessively) in an inherited disease, gene therapy could be used to deliver a copy of this gene that does not contain the deleterious mutation and thereby produces a functional protein. This strategy is referred to as gene replacement therapy and is employed to treat inherited retinal diseases.[14][63]

While the concept of gene replacement therapy is mostly suitable for recessive diseases, novel strategies have been suggested that are capable of also treating conditions with a dominant pattern of inheritance.

  • The introduction of CRISPR gene editing has opened new doors for its application and utilization in gene therapy, as instead of pure replacement of a gene, it enables correction of the particular genetic defect.[37] Solutions to medical hurdles, such as the eradication of latent human immunodeficiency virus (HIV) reservoirs and correction of the mutation that causes sickle cell disease, may be available as a therapeutic option in the future.[64][65][66]
  • Prosthetic gene therapy aims to enable cells of the body to take over functions they physiologically do not carry out. One example is the so-called vision restoration gene therapy, that aims to restore vision in patients with end-stage retinal diseases.[67][68] In end-stage retinal diseases, the photoreceptors, as the primary light sensitive cells of the retina are irreversibly lost. By the means of prosthetic gene therapy light sensitive proteins are delivered into the remaining cells of the retina, to render them light sensitive and thereby enable them to signal visual information towards the brain.G

Vectors

Main article: Vectors in gene therapy

The delivery of DNA into cells can be accomplished by multiple methods. The two major classes are recombinant viruses (sometimes called biological nanoparticles or viral vectors) and naked DNA or DNA complexes (non-viral methods).[69]

Viruses

Main article: Viral vector
 
Gene therapy using an adenovirus vector. In some cases, the adenovirus will insert the new gene into a cell. If the treatment is successful, the new gene will make a functional protein to treat a disease.

In order to replicate, viruses introduce their genetic material into the host cell, tricking the host's cellular machinery into using it as blueprints for viral proteins.[51]: 39  Retroviruses go a stage further by having their genetic material copied into the nuclear genome of the host cell. Scientists exploit this by substituting partt of a virus's genetic material with therapeutic DNA or RNA.[51]: 40  [70] Like the genetic material (DNA or RNA) in viruses, therapeutic genetic material can be designed to simply serve as a temporary blueprint that degrades naturally, as in a non-integrative vectors, or to enter the host's nucleus becoming a permanent part of the host's nuclear DNA in infected cells.[51]: 50 

A number of viruses have been used for human gene therapy, including retroviruses such as lentivirus, adenoviruses, herpes simplex, vaccinia, and adeno-associated virus.[4]

Adenovirus viral vectors (Ad) temporarily modify a cell's genetic expression with genetic material that is not integrated into the host cell's DNA.[71]: 5  As of 2017, such vectors were used in 20% of trials for gene therapy.[70]: 10  Adenovirus vectors are mostly used in cancer treatments and novel genetic vaccines such as the Ebola vaccine, vaccines used in clinical trials for HIV and SARS-CoV-2, or cancer vaccines.[71]: 5 

Lentiviral vectors based on lentivirus, a retrovirus, can modify a cell's nuclear genome to permanently express a gene, although vectors can be modify to prevent integration.[51]: 40,50  Retroviruses were used in 18% of trials before 2018.[70]: 10 

Adeno-associated virus (AAV) is a virus that is incapable of transmission between cells unless the cell is infected by another virus, a helper virus. Adenovirus and the herpes viruses act as helper viruses for AAV. AAV persists within the cell outside of the cell's nuclear genome for an extended period of time through the formation of concatemers mostly organized as episomes.[72]: 4  Genetic material from AAV vectors is integrated into the host cell's nuclear genome at a low frequency and likely mediated by the DNA-modifying enzymes of the host cell.[73]: 2647  Animal models suggest that integration of AAV genetic material into the host cell's nuclear genome may cause hepatocellular carcinoma, a form of liver cancer.[73]

Non-viral

Non-viral vectors for gene therapy[74] present certain advantages over viral methods, such as large scale production and low host immunogenicity. However, non-viral methods initially produced lower levels of transfection and gene expression, and thus lower therapeutic efficacy. Newer technologies offer promise of solving these problems, with the advent of increased cell-specific targeting and subcellular trafficking control.

Methods for non-viral gene therapy include the injection of naked DNA, electroporation, the gene gun, sonoporation, magnetofection, the use of oligonucleotides, lipoplexes, dendrimers, and inorganic nanoparticles.

More recent approaches, such as those performed by companies such as Ligandal, offer the possibility of creating cell-specific targeting technologies for a variety of gene therapy modalities, including RNA, DNA and gene editing tools such as CRISPR. Other companies, such as Arbutus Biopharma and Arcturus Therapeutics, offer non-viral, non-cell-targeted approaches that mainly exhibit liver trophism. In more recent years, startups such as Sixfold Bio, GenEdit, and Spotlight Therapeutics have begun to solve the non-viral gene delivery problem. Non-viral techniques offer the possibility of repeat dosing and greater tailorability of genetic payloads, which in the future will be more likely to take over viral-based delivery systems.

Companies such as Editas Medicine, Intellia Therapeutics, CRISPR Therapeutics, Casebia, Cellectis, Precision Biosciences, bluebird bio, and Sangamo have developed non-viral gene editing techniques, however frequently still use viruses for delivering gene insertion material following genomic cleavage by guided nucleases. These companies focus on gene editing, and still face major delivery hurdles.

BioNTech, Moderna Therapeutics and CureVac focus on delivery of mRNA payloads, which are necessarily non-viral delivery problems.

Alnylam, Dicerna Pharmaceuticals, and Ionis Pharmaceuticals focus on delivery of siRNA (antisense oligonucleotides) for gene suppression, which also necessitate non-viral delivery systems.

In academic contexts, a number of laboratories are working on delivery of PEGylated particles, which form serum protein coronas and chiefly exhibit LDL receptor mediated uptake in cells in vivo.[75]

Treatment

Cancer

 
Suicide gene therapy graphic used to treat cancer

There have been attempts to treat cancer using gene therapy. As of 2017, 65% of gene therapy trials were for cancer treatment.[70]: 7 

Adenovirus vectors are useful for some cancer gene therapies because adenovirus can transiently insert genetic material into a cell without permanently altering the cell's nuclear genome. These vectors can be used to cause antigens to be added to cancers causing an immune response, or hinder angiogenesis by expressing certain proteins.[76]: 5  An Adenovirus vector is used in the commercial products Gendicine and Oncorine.[76]: 10  Another commercial product, Rexin G, uses a retrovirus-based vector and selectively binds to receptors that are more expressed in tumors.[76]: 10 

One approach, suicide gene therapy, works by introducing genes encoding enzymes that will cause a cancer cell to die. Another approach is the use oncolytic viruses, such as Oncorine,[77]: 165  which are viruses that selectively reproduce in cancerous cells leaving other cells unaffected.[78]: 6 [79]: 280 

MRNA has been suggested as a non-viral vector for cancer gene therapy that would temporarily change a cancer cells function to create antigens or kill the cells, resulting in several trials.[80]

Genetic diseases

Gene therapy approaches to replace a faulty gene with a healthy gene have been proposed and are being studied for treating some genetic diseases. As of 2017, 11.1% of gene therapy clinical trials targeted monogentic genetic diseases.[70]: 9 

Diseases such as sickle cell disease that are caused by autosomal recessive disorders for which a person's normal phenotype or cell function may be restored in cells that have the disease by a normal copy of the gene that is mutated, may be a good candidate for gene therapy treatment.[81][82] The risks and benefits related to gene therapy for sickle cell disease are not known.[82]

Gene therapy has been use in the eye. The eye is especially suitable for adeno-associated virus vectors. Luxturna is an approved gene therapy to treat Leber's hereditary optic neuropathy.[83]: 1354  Glybera, a treatment for pancreatitis caused by a genetic condition, and Zolgensma for the treatment of spinal muscular atrophy both use an adeno-associated virus vector.[73]: 2647 

Infectious diseases

As of 2017, 7% of genetic therapy trials targetted infectious diseases. 69.2% of trials targetted HIV, 11% hepatitis B or C, and 7.1% malaria.[70]

List of gene therapies for treatment of disease

See also: List of gene therapies

Some genetic therapies have been approved by the U.S. Food and Drug Administration (FDA), the European Medicines Agency (EMA), and for use in Russia and China.

List of approved gene therapies for the treatment of disease
INN Brand name Type Manufacturer Target FDA approved EMA authorized
alipogene tiparvovec Glybera In vivo Chiesi Farmaceutici lipoprotein lipase deficiency No Withdrawn
atidarsagene autotemcel Libmeldy

(Arylsulfatase A gene encoding autologous CD34+ cells)

Ex vitro Orchard Therapeutics metachromatic leukodystrophy No 17 December 2020[84]
autologous CD34+ Strimvelis adenosine deaminase deficiency (ADA-SCID) 26 May 2016
axicabtagene ciloleucel Yescarta large B-cell lymphoma 18 October 2017 23 August 2018
betibeglogene autotemcel Zynteglo beta thalassemia 17 August 2022[85] 29 May 2019
brexucabtagene autoleucel Tecartus Ex vitro Kite Pharma mantle cell lymphoma and acute lymphoblastic leukemia 24 July 2020[86][87] 14 December 2020[88]
cambiogenplasmid Neovasculgen vascular endothelial growth factor peripheral artery disease
elivaldogene autotemcel Skysona cerebral adrenoleukodystrophy 16 July 2021
gendicine head and neck squamous cell carcinoma
idecabtagene vicleucel Abecma Ex vivo Celgene multiple myeloma 26 March 2021[89] No
lisocabtagene maraleucel Breyanzi Ex vivo Juno Therapeutics B-cell lymphoma 5 February 2021[90] No
nadofaragene firadenovec Adstiladrin Ferring Pharmaceuticals high-risk Bacillus Calmette-Guérin (BCG)-unresponsive non-muscle-invasive bladder cancer (NMIBC) with carcinoma in situ (CIS) Yes[91] No
onasemnogene abeparvovec Zolgensma In vivo Novartis Gene Therapies Spinal muscular atrophy Type I 24 May 2019[92] 26 March 2020[93]
talimogene laherparepvec Imlygic In vivo Amgen melanoma 27 October 2015[94] 16 December 2015[95]
tisagenlecleucel Kymriah B cell lymphoblastic leukemia 22 August 2018
valoctocogene roxaparvovec Roctavian BioMarin International Limited hemophilia A August 2022[96][97][98]
voretigene neparvovec Luxturna In vivo Spark Therapeutics biallelic RPE65 mutation associated Leber congenital amaurosis 18 December 2017[99] 22 November 2018[100]

Adverse effects, contraindications and hurdles for use

Some of the unsolved problems include:

  • Short-lived nature – Before gene therapy can become a permanent cure for a condition, the therapeutic DNA introduced into target cells must remain functional and the cells containing the therapeutic DNA must be stable. Problems with integrating therapeutic DNA into the nuclear genome and the rapidly dividing nature of many cells prevent it from achieving long-term benefits. Patients require multiple treatments.
  • Immune response – Any time a foreign object is introduced into human tissues, the immune system is stimulated to attack the invader. Stimulating the immune system in a way that reduces gene therapy effectiveness is possible. The immune system's enhanced response to viruses that it has seen before reduces the effectiveness to repeated treatments.
  • Problems with viral vectors – Viral vectors carry the risks of toxicity, inflammatory responses, and gene control and targeting issues.
  • Multigene disorders – Some commonly occurring disorders, such as heart disease, high blood pressure, Alzheimer's disease, arthritis, and diabetes, are affected by variations in multiple genes, which complicate gene therapy.
  • Some therapies may breach the Weismann barrier (between soma and germ-line) protecting the testes, potentially modifying the germline, falling afoul of regulations in countries that prohibit the latter practice.[101]
  • Insertional mutagenesis – If the DNA is integrated in a sensitive spot in the genome, for example in a tumor suppressor gene, the therapy could induce a tumor. This has occurred in clinical trials for X-linked severe combined immunodeficiency (X-SCID) patients, in which hematopoietic stem cells were transduced with a corrective transgene using a retrovirus, and this led to the development of T cell leukemia in 3 of 20 patients.[102][103] One possible solution is to add a functional tumor suppressor gene to the DNA to be integrated. This may be problematic since the longer the DNA is, the harder it is to integrate into cell genomes.[104] CRISPR technology allows researchers to make much more precise genome changes at exact locations.[105]
  • Cost – Alipogene tiparvovec or Glybera, for example, at a cost of $1.6 million per patient, was reported in 2013, to be the world's most expensive drug.[106][107]

Deaths

Three patients' deaths have been reported in gene therapy trials, putting the field under close scrutiny. The first was that of Jesse Gelsinger, who died in 1999, because of immune rejection response.[108][109] One X-SCID patient died of leukemia in 2003.[10] In 2007, a rheumatoid arthritis patient died from an infection; the subsequent investigation concluded that the death was not related to gene therapy.[110]

Regulations

Regulations covering genetic modification are part of general guidelines about human-involved biomedical research.[citation needed] There are no international treaties which are legally binding in this area, but there are recommendations for national laws from various bodies.[citation needed]

The Helsinki Declaration (Ethical Principles for Medical Research Involving Human Subjects) was amended by the World Medical Association's General Assembly in 2008. This document provides principles physicians and researchers must consider when involving humans as research subjects. The Statement on Gene Therapy Research initiated by the Human Genome Organization (HUGO) in 2001, provides a legal baseline for all countries. HUGO's document emphasizes human freedom and adherence to human rights, and offers recommendations for somatic gene therapy, including the importance of recognizing public concerns about such research.[111]

United States

No federal legislation lays out protocols or restrictions about human genetic engineering. This subject is governed by overlapping regulations from local and federal agencies, including the Department of Health and Human Services, the FDA and NIH's Recombinant DNA Advisory Committee. Researchers seeking federal funds for an investigational new drug application, (commonly the case for somatic human genetic engineering,) must obey international and federal guidelines for the protection of human subjects.[112]

NIH serves as the main gene therapy regulator for federally funded research. Privately funded research is advised to follow these regulations. NIH provides funding for research that develops or enhances genetic engineering techniques and to evaluate the ethics and quality in current research. The NIH maintains a mandatory registry of human genetic engineering research protocols that includes all federally funded projects.[113]

An NIH advisory committee published a set of guidelines on gene manipulation.[114] The guidelines discuss lab safety as well as human test subjects and various experimental types that involve genetic changes. Several sections specifically pertain to human genetic engineering, including Section III-C-1. This section describes required review processes and other aspects when seeking approval to begin clinical research involving genetic transfer into a human patient.[115] The protocol for a gene therapy clinical trial must be approved by the NIH's Recombinant DNA Advisory Committee prior to any clinical trial beginning; this is different from any other kind of clinical trial.[114]

As with other kinds of drugs, the FDA regulates the quality and safety of gene therapy products and supervises how these products are used clinically. Therapeutic alteration of the human genome falls under the same regulatory requirements as any other medical treatment. Research involving human subjects, such as clinical trials, must be reviewed and approved by the FDA and an Institutional Review Board.[116][117]

Gene doping

Main article: Gene doping

Athletes may adopt gene therapy technologies to improve their performance.[118] Gene doping is not known to occur, but multiple gene therapies may have such effects. Kayser et al. argue that gene doping could level the playing field if all athletes receive equal access. Critics claim that any therapeutic intervention for non-therapeutic/enhancement purposes compromises the ethical foundations of medicine and sports.[119]

Genetic enhancement

Further information: Human genetic enhancement
See also: Human germline engineering and Assisted reproductive technology

Genetic engineering could be used to cure diseases, but also to change physical appearance, metabolism, and even improve physical capabilities and mental faculties such as memory and intelligence. Ethical claims about germline engineering include beliefs that every fetus has a right to remain genetically unmodified, that parents hold the right to genetically modify their offspring, and that every child has the right to be born free of preventable diseases.[120][121][122] For parents, genetic engineering could be seen as another child enhancement technique to add to diet, exercise, education, training, cosmetics, and plastic surgery.[123][124] Another theorist claims that moral concerns limit but do not prohibit germline engineering.[125]

A recent issue of the journal Bioethics was devoted to moral issues surrounding germline genetic engineering in people.[126]

Possible regulatory schemes include a complete ban, provision to everyone, or professional self-regulation. The American Medical Association's Council on Ethical and Judicial Affairs stated that "genetic interventions to enhance traits should be considered permissible only in severely restricted situations: (1) clear and meaningful benefits to the fetus or child; (2) no trade-off with other characteristics or traits; and (3) equal access to the genetic technology, irrespective of income or other socioeconomic characteristics."[127]

As early in the history of biotechnology as 1990, there have been scientists opposed to attempts to modify the human germline using these new tools,[128] and such concerns have continued as technology progressed.[129][130] With the advent of new techniques like CRISPR, in March 2015 a group of scientists urged a worldwide moratorium on clinical use of gene editing technologies to edit the human genome in a way that can be inherited.[131][132][133][134] In April 2015, researchers sparked controversy when they reported results of basic research to edit the DNA of non-viable human embryos using CRISPR.[135][136] A committee of the American National Academy of Sciences and National Academy of Medicine gave qualified support to human genome editing in 2017[137][138] once answers have been found to safety and efficiency problems "but only for serious conditions under stringent oversight."[139]

History

1970s and earlier

In 1972, Friedmann and Roblin authored a paper in Science titled "Gene therapy for human genetic disease?".[140] Rogers (1970) was cited for proposing that exogenous good DNA be used to replace the defective DNA in those with genetic defects.[141]

1980s

In 1984, a retrovirus vector system was designed that could efficiently insert foreign genes into mammalian chromosomes.[142]

1990s

The first approved gene therapy clinical research in the US took place on 14 September 1990, at the National Institutes of Health (NIH), under the direction of William French Anderson.[143] Four-year-old Ashanti DeSilva received treatment for a genetic defect that left her with adenosine deaminase deficiency (ADA-SCID), a severe immune system deficiency. The defective gene of the patient's blood cells was replaced by the functional variant. Ashanti's immune system was partially restored by the therapy. Production of the missing enzyme was temporarily stimulated, but the new cells with functional genes were not generated. She led a normal life only with the regular injections performed every two months. The effects were successful, but temporary.[144]

Cancer gene therapy was introduced in 1992/93 (Trojan et al. 1993).[145] The treatment of glioblastoma multiforme, the malignant brain tumor whose outcome is always fatal, was done using a vector expressing antisense IGF-I RNA (clinical trial approved by NIH protocol no.1602 24 November 1993,[146] and by the FDA in 1994). This therapy also represents the beginning of cancer immunogene therapy, a treatment which proves to be effective due to the anti-tumor mechanism of IGF-I antisense, which is related to strong immune and apoptotic phenomena.

In 1992, Claudio Bordignon, working at the Vita-Salute San Raffaele University, performed the first gene therapy procedure using hematopoietic stem cells as vectors to deliver genes intended to correct hereditary diseases.[147] In 2002, this work led to the publication of the first successful gene therapy treatment for ADA-SCID. The success of a multi-center trial for treating children with SCID (severe combined immune deficiency or "bubble boy" disease) from 2000 and 2002, was questioned when two of the ten children treated at the trial's Paris center developed a leukemia-like condition. Clinical trials were halted temporarily in 2002, but resumed after regulatory review of the protocol in the US, the United Kingdom, France, Italy, and Germany.[148]

In 1993, Andrew Gobea was born with SCID following prenatal genetic screening. Blood was removed from his mother's placenta and umbilical cord immediately after birth, to acquire stem cells. The allele that codes for adenosine deaminase (ADA) was obtained and inserted into a retrovirus. Retroviruses and stem cells were mixed, after which the viruses inserted the gene into the stem cell chromosomes. Stem cells containing the working ADA gene were injected into Andrew's blood. Injections of the ADA enzyme were also given weekly. For four years T cells (white blood cells), produced by stem cells, made ADA enzymes using the ADA gene. After four years more treatment was needed.[149]

Jesse Gelsinger's death in 1999 impeded gene therapy research in the US.[150][151] As a result, the FDA suspended several clinical trials pending the reevaluation of ethical and procedural practices.[152]

2000s

The modified gene therapy strategy of antisense IGF-I RNA (NIH n˚ 1602)[146] using antisense / triple helix anti-IGF-I approach was registered in 2002, by Wiley gene therapy clinical trial - n˚ 635 and 636. The approach has shown promising results in the treatment of six different malignant tumors: glioblastoma, cancers of liver, colon, prostate, uterus, and ovary (Collaborative NATO Science Programme on Gene Therapy USA, France, Poland n˚ LST 980517 conducted by J. Trojan) (Trojan et al., 2012). This anti-gene antisense/triple helix therapy has proven to be efficient, due to the mechanism stopping simultaneously IGF-I expression on translation and transcription levels, strengthening anti-tumor immune and apoptotic phenomena.

2002

Sickle cell disease can be treated in mice.[153] The mice – which have essentially the same defect that causes human cases – used a viral vector to induce production of fetal hemoglobin (HbF), which normally ceases to be produced shortly after birth. In humans, the use of hydroxyurea to stimulate the production of HbF temporarily alleviates sickle cell symptoms. The researchers demonstrated this treatment to be a more permanent means to increase therapeutic HbF production.[154]

A new gene therapy approach repaired errors in messenger RNA derived from defective genes. This technique has the potential to treat thalassaemia, cystic fibrosis and some cancers.[155]

Researchers created liposomes 25 nanometers across that can carry therapeutic DNA through pores in the nuclear membrane.[156]

2003

In 2003, a research team inserted genes into the brain for the first time. They used liposomes coated in a polymer called polyethylene glycol, which unlike viral vectors, are small enough to cross the blood–brain barrier.[157]

Short pieces of double-stranded RNA (short, interfering RNAs or siRNAs) are used by cells to degrade RNA of a particular sequence. If a siRNA is designed to match the RNA copied from a faulty gene, then the abnormal protein product of that gene will not be produced.[158]

Gendicine is a cancer gene therapy that delivers the tumor suppressor gene p53 using an engineered adenovirus. In 2003, it was approved in China for the treatment of head and neck squamous cell carcinoma.[28]

2006

In March, researchers announced the successful use of gene therapy to treat two adult patients for X-linked chronic granulomatous disease, a disease which affects myeloid cells and damages the immune system. The study is the first to show that gene therapy can treat the myeloid system.[159]

In May, a team reported a way to prevent the immune system from rejecting a newly delivered gene.[160] Similar to organ transplantation, gene therapy has been plagued by this problem. The immune system normally recognizes the new gene as foreign and rejects the cells carrying it. The research utilized a newly uncovered network of genes regulated by molecules known as microRNAs. This natural function selectively obscured their therapeutic gene in immune system cells and protected it from discovery. Mice infected with the gene containing an immune-cell microRNA target sequence did not reject the gene.

In August, scientists successfully treated metastatic melanoma in two patients using killer T cells genetically retargeted to attack the cancer cells.[161]

In November, researchers reported on the use of VRX496, a gene-based immunotherapy for the treatment of HIV that uses a lentiviral vector to deliver an antisense gene against the HIV envelope. In a phase I clinical trial, five subjects with chronic HIV infection who had failed to respond to at least two antiretroviral regimens were treated. A single intravenous infusion of autologous CD4 T cells genetically modified with VRX496 was well tolerated. All patients had stable or decreased viral load; four of the five patients had stable or increased CD4 T cell counts. All five patients had stable or increased immune response to HIV antigens and other pathogens. This was the first evaluation of a lentiviral vector administered in a US human clinical trial.[162][163]

2007

In May, researchers announced the first gene therapy trial for inherited retinal disease. The first operation was carried out on a 23-year-old British male, Robert Johnson, in early 2007.[164]

2008

Main article: Gene therapy of the human retina

Leber's congenital amaurosis is an inherited blinding disease caused by mutations in the RPE65 gene. The results of a small clinical trial in children were published in April.[14] Delivery of recombinant adeno-associated virus (AAV) carrying RPE65 yielded positive results. In May, two more groups reported positive results in independent clinical trials using gene therapy to treat the condition. In all three clinical trials, patients recovered functional vision without apparent side-effects.[14][15][16][17]

2009

In September researchers were able to give trichromatic vision to squirrel monkeys.[165] In November 2009, researchers halted a fatal genetic disorder called adrenoleukodystrophy in two children using a lentivirus vector to deliver a functioning version of ABCD1, the gene that is mutated in the disorder.[166]

2010s

2010

An April paper reported that gene therapy addressed achromatopsia (color blindness) in dogs by targeting cone photoreceptors. Cone function and day vision were restored for at least 33 months in two young specimens. The therapy was less efficient for older dogs.[167]

In September it was announced that an 18-year-old male patient in France with beta thalassemia major had been successfully treated.[168] Beta thalassemia major is an inherited blood disease in which beta haemoglobin is missing and patients are dependent on regular lifelong blood transfusions.[169] The technique used a lentiviral vector to transduce the human β-globin gene into purified blood and marrow cells obtained from the patient in June 2007.[170] The patient's haemoglobin levels were stable at 9 to 10 g/dL. About a third of the hemoglobin contained the form introduced by the viral vector and blood transfusions were not needed.[170][171] Further clinical trials were planned.[172] Bone marrow transplants are the only cure for thalassemia, but 75% of patients do not find a matching donor.[171]

Cancer immunogene therapy using modified antigene, antisense/triple helix approach was introduced in South America in 2010/11 in La Sabana University, Bogota (Ethical Committee 14 December 2010, no P-004-10). Considering the ethical aspect of gene diagnostic and gene therapy targeting IGF-I, the IGF-I expressing tumors i.e. lung and epidermis cancers were treated (Trojan et al. 2016).[173][174]

2011

In 2007 and 2008, a man (Timothy Ray Brown) was cured of HIV by repeated hematopoietic stem cell transplantation (see also allogeneic stem cell transplantation, allogeneic bone marrow transplantation, allotransplantation) with double-delta-32 mutation which disables the CCR5 receptor. This cure was accepted by the medical community in 2011.[175] It required complete ablation of existing bone marrow, which is very debilitating.[176]

In August two of three subjects of a pilot study were confirmed to have been cured from chronic lymphocytic leukemia (CLL). The therapy used genetically modified T cells to attack cells that expressed the CD19 protein to fight the disease.[23] In 2013, the researchers announced that 26 of 59 patients had achieved complete remission and the original patient had remained tumor-free.[177]

Human HGF plasmid DNA therapy of cardiomyocytes is being examined as a potential treatment for coronary artery disease as well as treatment for the damage that occurs to the heart after myocardial infarction.[178][179]

In 2011, Neovasculgen was registered in Russia as the first-in-class gene-therapy drug for treatment of peripheral artery disease, including critical limb ischemia; it delivers the gene encoding for VEGF.[29] Neovasculogen is a plasmid encoding the CMV promoter and the 165 amino acid form of VEGF.[180][181]

2012

The FDA approved Phase I clinical trials on thalassemia major patients in the US for 10 participants in July.[182] The study was expected to continue until 2015.[172]

In July 2012, the European Medicines Agency recommended approval of a gene therapy treatment for the first time in either Europe or the United States. The treatment used Alipogene tiparvovec (Glybera) to compensate for lipoprotein lipase deficiency, which can cause severe pancreatitis.[183] The recommendation was endorsed by the European Commission in November 2012,[13][30][184][185] and commercial rollout began in late 2014.[186] Alipogene tiparvovec was expected to cost around $1.6 million per treatment in 2012,[187] revised to $1 million in 2015,[188] making it the most expensive medicine in the world at the time.[189] As of 2016, only the patients treated in clinical trials and a patient who paid the full price for treatment have received the drug.[190]

In December 2012, it was reported that 10 of 13 patients with multiple myeloma were in remission "or very close to it" three months after being injected with a treatment involving genetically engineered T cells to target proteins NY-ESO-1 and LAGE-1, which exist only on cancerous myeloma cells.[25]

2013

In March researchers reported that three of five adult subjects who had acute lymphocytic leukemia (ALL) had been in remission for five months to two years after being treated with genetically modified T cells which attacked cells with CD19 genes on their surface, i.e. all B cells, cancerous or not. The researchers believed that the patients' immune systems would make normal T cells and B cells after a couple of months. They were also given bone marrow. One patient relapsed and died and one died of a blood clot unrelated to the disease.[24]

Following encouraging Phase I trials, in April, researchers announced they were starting Phase II clinical trials (called CUPID2 and SERCA-LVAD) on 250 patients[191] at several hospitals to combat heart disease. The therapy was designed to increase the levels of SERCA2, a protein in heart muscles, improving muscle function.[192] The U.S. Food and Drug Administration (FDA) granted this a breakthrough therapy designation to accelerate the trial and approval process.[193] In 2016, it was reported that no improvement was found from the CUPID 2 trial.[194]

In July researchers reported promising results for six children with two severe hereditary diseases had been treated with a partially deactivated lentivirus to replace a faulty gene and after 7–32 months. Three of the children had metachromatic leukodystrophy, which causes children to lose cognitive and motor skills.[195] The other children had Wiskott–Aldrich syndrome, which leaves them to open to infection, autoimmune diseases, and cancer.[196] Follow up trials with gene therapy on another six children with Wiskott–Aldrich syndrome were also reported as promising.[197][198]

In October researchers reported that two children born with adenosine deaminase severe combined immunodeficiency disease (ADA-SCID) had been treated with genetically engineered stem cells 18 months previously and that their immune systems were showing signs of full recovery. Another three children were making progress.[21] In 2014, a further 18 children with ADA-SCID were cured by gene therapy.[199] ADA-SCID children have no functioning immune system and are sometimes known as "bubble children".[21]

Also in October researchers reported that they had treated six people with haemophilia in early 2011 using an adeno-associated virus. Over two years later all six were producing clotting factor.[21][200]

2014

In January researchers reported that six choroideremia patients had been treated with adeno-associated virus with a copy of REP1. Over a six-month to two-year period all had improved their sight.[63][201] By 2016, 32 patients had been treated with positive results and researchers were hopeful the treatment would be long-lasting.[18] Choroideremia is an inherited genetic eye disease with no approved treatment, leading to loss of sight.

In March researchers reported that 12 HIV patients had been treated since 2009 in a trial with a genetically engineered virus with a rare mutation (CCR5 deficiency) known to protect against HIV with promising results.[202][203]

Clinical trials of gene therapy for sickle cell disease were started in 2014.[204][205]

In February LentiGlobin BB305, a gene therapy treatment undergoing clinical trials for treatment of beta thalassemia gained FDA "breakthrough" status after several patients were able to forgo the frequent blood transfusions usually required to treat the disease.[206]

In March researchers delivered a recombinant gene encoding a broadly neutralizing antibody into monkeys infected with simian HIV; the monkeys' cells produced the antibody, which cleared them of HIV. The technique is named immunoprophylaxis by gene transfer (IGT). Animal tests for antibodies to ebola, malaria, influenza, and hepatitis were underway.[207][208]

In March, scientists, including an inventor of CRISPR, Jennifer Doudna, urged a worldwide moratorium on germline gene therapy, writing "scientists should avoid even attempting, in lax jurisdictions, germline genome modification for clinical application in humans" until the full implications "are discussed among scientific and governmental organizations".[131][132][133][134]

In December, scientists of major world academies called for a moratorium on inheritable human genome edits, including those related to CRISPR-Cas9 technologies[209] but that basic research including embryo gene editing should continue.[210]

2015

Researchers successfully treated a boy with epidermolysis bullosa using skin grafts grown from his own skin cells, genetically altered to repair the mutation that caused his disease.[211]

In November, researchers announced that they had treated a baby girl, Layla Richards, with an experimental treatment using donor T cells genetically engineered using TALEN to attack cancer cells. One year after the treatment she was still free of her cancer (a highly aggressive form of acute lymphoblastic leukaemia [ALL]).[212] Children with highly aggressive ALL normally have a very poor prognosis and Layla's disease had been regarded as terminal before the treatment.[213][214]

2016

In April the Committee for Medicinal Products for Human Use of the European Medicines Agency endorsed a gene therapy treatment called Strimvelis[215][216] and the European Commission approved it in June.[217] This treats children born with adenosine deaminase deficiency and who have no functioning immune system. This was the second gene therapy treatment to be approved in Europe.[218]

In October, Chinese scientists reported they had started a trial to genetically modify T cells from 10 adult patients with lung cancer and reinject the modified T cells back into their bodies to attack the cancer cells. The T cells had the PD-1 protein (which stops or slows the immune response) removed using CRISPR-Cas9.[219][220]

A 2016 Cochrane systematic review looking at data from four trials on topical cystic fibrosis transmembrane conductance regulator (CFTR) gene therapy does not support its clinical use as a mist inhaled into the lungs to treat cystic fibrosis patients with lung infections. One of the four trials did find weak evidence that liposome-based CFTR gene transfer therapy may lead to a small respiratory improvement for people with CF. This weak evidence is not enough to make a clinical recommendation for routine CFTR gene therapy.[221]

2017

In February Kite Pharma announced results from a clinical trial of CAR-T cells in around a hundred people with advanced non-Hodgkin lymphoma.[222]

In March, French scientists reported on clinical research of gene therapy to treat sickle cell disease.[223]

In August, the FDA approved tisagenlecleucel for acute lymphoblastic leukemia.[224] Tisagenlecleucel is an adoptive cell transfer therapy for B-cell acute lymphoblastic leukemia; T cells from a person with cancer are removed, genetically engineered to make a specific T-cell receptor (a chimeric T cell receptor, or "CAR-T") that reacts to the cancer, and are administered back to the person. The T cells are engineered to target a protein called CD19 that is common on B cells. This is the first form of gene therapy to be approved in the United States. In October, a similar therapy called axicabtagene ciloleucel was approved for non-Hodgkin lymphoma.[225]

In October, biophysicist and biohacker Josiah Zayner claimed to have performed the very first in-vivo human genome editing in the form of a self-administered therapy.[226][227]

On 13 November, medical scientists working with Sangamo Therapeutics, headquartered in Richmond, California, announced the first ever in-body human gene editing therapy.[228][229] The treatment, designed to permanently insert a healthy version of the flawed gene that causes Hunter syndrome, was given to 44-year-old Brian Madeux and is part of the world's first study to permanently edit DNA inside the human body.[230] The success of the gene insertion was later confirmed.[231][232] Clinical trials by Sangamo involving gene editing using zinc finger nuclease (ZFN) are ongoing.[233]

In December the results of using an adeno-associated virus with blood clotting factor VIII to treat nine haemophilia A patients were published. Six of the seven patients on the high dose regime increased the level of the blood clotting VIII to normal levels. The low and medium dose regimes had no effect on the patient's blood clotting levels.[234][235]

In December, the FDA approved Luxturna, the first in vivo gene therapy, for the treatment of blindness due to Leber's congenital amaurosis.[236] The price of this treatment is US$850,000 for both eyes.[237][238]

2019

In May, the FDA approved onasemnogene abeparvovec (Zolgensma) for treating spinal muscular atrophy in children under two years of age. The list price of Zolgensma was set at US$2.125 million per dose, making it the most expensive drug ever.[239]

In May, the EMA approved betibeglogene autotemcel (Zynteglo) for treating beta thalassemia for people twelve years of age and older.[240][241]

In July, Allergan and Editas Medicine announced phase I/II clinical trial of AGN-151587 for the treatment of Leber congenital amaurosis 10.[242] This is the first study of a CRISPR-based in vivo human gene editing therapy, where the editing takes place inside the human body.[243] The first injection of the CRISPR-Cas System was confirmed in March 2020.[244]

2020s

2020

In May, onasemnogene abeparvovec (Zolgensma) was approved by the European Union for the treatment of spinal muscular atrophy in people who either have clinical symptoms of SMA type 1 or who have no more than three copies of the SMN2 gene, irrespective of body weight or age.[245]

In August, Audentes Therapeutics reported that three out of 17 children with X-linked myotubular myopathy participating the clinical trial of a AAV8-based gene therapy treatment AT132 have died. It was suggested that the treatment, whose dosage is based on body weight, exerts a disproportionately toxic effect on heavier patients, since the three patients who died were heavier than the others.[246][247] The trial has been put on clinical hold.[248]

On 15 October, the Committee for Medicinal Products for Human Use (CHMP) of the European Medicines Agency (EMA) adopted a positive opinion, recommending the granting of a marketing authorisation for the medicinal product Libmeldy (autologous CD34+ cell enriched population that contains hematopoietic stem and progenitor cells transduced ex vivo using a lentiviral vector encoding the human arylsulfatase A gene), a gene therapy for the treatment of children with the "late infantile" (LI) or "early juvenile" (EJ) forms of metachromatic leukodystrophy (MLD).[249] The active substance of Libmeldy consists of the child's own stem cells which have been modified to contain working copies of the ARSA gene.[249] When the modified cells are injected back into the patient as a one-time infusion, the cells are expected to start producing the ARSA enzyme that breaks down the build-up of sulfatides in the nerve cells and other cells of the patient's body.[250] Libmeldy was approved for medical use in the EU in December 2020.[251]

On 15 October, Lysogene, a French biotechnological company, reported the death of a patient in who has received LYS-SAF302, an experimental gene therapy treatment for mucopolysaccharidosis type IIIA (Sanfilippo syndrome type A).[252]

2021

In May, a new method using an altered version of the HIV virus as a lentivirus vector was reported in the treatment of 50 children with ADA-SCID obtaining positive results in 48 of them,[253][254][255] this method is expected to be safer than retroviruses vectors commonly used in previous studies of SCID where the development of leukemia was usually observed[256] and had already been used in 2019, but in a smaller group with X-SCID.[257][258][259][260]

In June a clinical trial on six patients affected with transthyretin amyloidosis reported a reduction the concentration of missfolded transthretin (TTR) protein in serum through CRISPR-based inactivation of the TTR gene in liver cells observing mean reductions of 52% and 87% among the lower and higher dose groups.This was done in vivo without taking cells out of the patient to edit them and reinfuse them later.[261][262][263]

In July results of a small gene therapy phase I study was published reporting observation of dopamine restoration on seven patients between 4 and 9 years old affected by aromatic L-amino acid decarboxylase deficiency (AADC deficiency).[264][265][266]

2022

In February, the first ever gene therapy for Tay–Sachs disease was announced, it uses an adeno-associated virus to deliver the correct instruction for the HEXA gene on brain cells which causes the disease. Only two children were part of a compassionate trial presenting improvements over the natural course of the disease and no vector-related adverse events.[267][268][269]

In May, eladocagene exuparvovec is recommended for approval by the European Commission.[270][271]

In July results of a gene therapy candidate for haemophilia B called FLT180 were announced, it works using an adeno-associated virus (AAV) to restore the clotting factor IX (FIX) protein, normal levels of the protein were observed with low doses of the therapy but immunosuppression was necessitated to decrease the risk of vector-related immune responses.[272][273][274]

In December, a 13-year girl that had been diagnosed with T-cell acute lymphoblastic leukaemia was successfully treated at Great Ormond Street Hospital (GOSH) in the first documented use of therapeutic gene editing for this purpose, after undergoing six months of an experimental treatment, where all attempts of other treatments failed. The procedure included reprogramming a healthy T-cell to destroy the cancerous T-cells to first rid her of leukaemia, and then rebuilding her immune system using healthy immune cells.[275] The GOSH team used BASE editing and had previously treated a case of acute lymphoblastic leukaemia in 2015 using TALENs.[214]

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Further reading

  • "Gene Therapy: An Overview of Approved and Pipeline Technologies" (PDF). CADTH (171). March 2018. (PDF) from the original on 19 October 2018.
February 26, 2023
gene, therapy, medical, field, which, focuses, genetic, modification, cells, produce, therapeutic, effect, treatment, disease, repairing, reconstructing, defective, genetic, material, first, attempt, modifying, human, performed, 1980, martin, cline, first, suc. Gene therapy is a medical field which focuses on the genetic modification of cells to produce a therapeutic effect 1 or the treatment of disease by repairing or reconstructing defective genetic material 2 The first attempt at modifying human DNA was performed in 1980 by Martin Cline but the first successful nuclear gene transfer in humans approved by the National Institutes of Health was performed in May 1989 3 The first therapeutic use of gene transfer as well as the first direct insertion of human DNA into the nuclear genome was performed by French Anderson in a trial starting in September 1990 It is thought to be able to cure many genetic disorders or treat them over time Between 1989 and December 2018 over 2 900 clinical trials were conducted with more than half of them in phase I 4 In 2003 Gendicine became the first gene therapy to receive regulatory approval Since that time further gene therapy drugs were approved such as Glybera 2012 Strimvelis 2016 Kymriah 2017 Luxturna 2017 Onpattro 2018 Zolgensma 2019 Abecma 2021 Adstiladrin Roctavian and Hemgenix all 2022 Most of these approaches utilize adeno associated viruses AAVs and lentiviruses for performing gene insertions in vivo and ex vivo respectively AAVs are characterized by stabilizing the viral capsid lower immunogenicity ability to transduce both dividing and nondividing cells the potential to integrate site specifically and to achieve long term expression in the in vivo treatment 5 ASO siRNA approaches such as those conducted by Alnylam and Ionis Pharmaceuticals require non viral delivery systems and utilize alternative mechanisms for trafficking to liver cells by way of GalNAc transporters Not all medical procedures that introduce alterations to a patient s genetic makeup can be considered gene therapy Bone marrow transplantation and organ transplants in general have been found to introduce foreign DNA into patients 6 Contents 1 Background 2 Classification 2 1 Breadth of definition 2 2 Genes present or added 2 3 Cell types 2 4 In vivo versus ex vivo therapies 2 5 Gene editing 3 Vectors 3 1 Viruses 3 2 Non viral 4 Treatment 4 1 Cancer 4 2 Genetic diseases 4 3 Infectious diseases 4 4 List of gene therapies for treatment of disease 5 Adverse effects contraindications and hurdles for use 5 1 Deaths 6 Regulations 6 1 United States 7 Gene doping 8 Genetic enhancement 9 History 9 1 1970s and earlier 9 2 1980s 9 3 1990s 9 4 2000s 9 4 1 2002 9 4 2 2003 9 4 3 2006 9 4 4 2007 9 4 5 2008 9 4 6 2009 9 5 2010s 9 5 1 2010 9 5 2 2011 9 5 3 2012 9 5 4 2013 9 5 5 2014 9 5 6 2015 9 5 7 2016 9 5 8 2017 9 5 9 2019 9 6 2020s 9 6 1 2020 9 6 2 2021 9 6 3 2022 10 References 11 Further reading 12 External linksBackground EditGene therapy was conceptualized in 1972 by authors who urged caution before commencing human gene therapy studies The first attempt an unsuccessful one at gene therapy as well as the first case of medical transfer of foreign genes into humans not counting organ transplantation was performed by Martin Cline on 10 July 1980 7 8 Cline claimed that one of the genes in his patients was active six months later though he never published this data or had it verified 9 and even if he is correct it s unlikely it produced any significant beneficial effects treating beta thalassemia medical citation needed After extensive research on animals throughout the 1980s and a 1989 bacterial gene tagging trial on humans the first gene therapy widely accepted as a success was demonstrated in a trial that started on 14 September 1990 when Ashanthi DeSilva was treated for ADA SCID 10 The first somatic treatment that produced a permanent genetic change was initiated in 1993 11 The goal was to cure malignant brain tumors by using recombinant DNA to transfer a gene making the tumor cells sensitive to a drug that in turn would cause the tumor cells to die 12 The polymers are either translated into proteins interfere with target gene expression or possibly correct genetic mutations The most common form uses DNA that encodes a functional therapeutic gene to replace a mutated gene The polymer molecule is packaged within a vector which carries the molecule inside cells medical citation needed Early clinical failures led to dismissals of gene therapy Clinical successes since 2006 regained researchers attention although as of 2014 update it was still largely an experimental technique 13 These include treatment of retinal diseases Leber s congenital amaurosis 14 15 16 17 and choroideremia 18 X linked SCID 19 ADA SCID 20 21 adrenoleukodystrophy 22 chronic lymphocytic leukemia CLL 23 acute lymphocytic leukemia ALL 24 multiple myeloma 25 haemophilia 21 and Parkinson s disease 26 Between 2013 and April 2014 US companies invested over 600 million in the field 27 The first commercial gene therapy Gendicine was approved in China in 2003 for the treatment of certain cancers 28 In 2011 Neovasculgen was registered in Russia as the first in class gene therapy drug for treatment of peripheral artery disease including critical limb ischemia 29 In 2012 Glybera a treatment for a rare inherited disorder lipoprotein lipase deficiency became the first treatment to be approved for clinical use in either Europe or the United States after its endorsement by the European Commission 13 30 Following early advances in genetic engineering of bacteria cells and small animals scientists started considering how to apply it to medicine Two main approaches were considered replacing or disrupting defective genes 31 Scientists focused on diseases caused by single gene defects such as cystic fibrosis haemophilia muscular dystrophy thalassemia and sickle cell anemia Glybera treats one such disease caused by a defect in lipoprotein lipase 30 DNA must be administered reach the damaged cells enter the cell and either express or disrupt a protein 32 Multiple delivery techniques have been explored The initial approach incorporated DNA into an engineered virus to deliver the DNA into a chromosome 33 34 Naked DNA approaches have also been explored especially in the context of vaccine development 35 Generally efforts focused on administering a gene that causes a needed protein to be expressed More recently increased understanding of nuclease function has led to more direct DNA editing using techniques such as zinc finger nucleases and CRISPR The vector incorporates genes into chromosomes The expressed nucleases then knock out and replace genes in the chromosome As of 2014 update these approaches involve removing cells from patients editing a chromosome and returning the transformed cells to patients 36 Gene editing is a potential approach to alter the human genome to treat genetic diseases 37 viral diseases 38 and cancer 39 40 As of 2020 update these approaches are being studied in clinical trials 41 42 Classification EditBreadth of definition Edit In 1986 a meeting at the Institute Of Medicine defined gene therapy as the addition or replacement of a gene in a targeted cell type In the same year the FDA announced that it had jurisdiction over approving gene therapy without defining the term The FDA added a very broad definition in 1993 of any treatment that would modify or manipulate the expression of genetic material or to alter the biological properties of living cells In 2018 this was narrowed to products that mediate their effects by transcription or translation of transferred genetic material or by specifically altering host human genetic sequences 43 Writing in 2018 in the Journal of Law and the Biosciences Sherkow et al argued for a narrower definition of gene therapy than the FDA s in light of new technology that would consist of any treatment that intentionally and permanently modified a cell s genome with the definition of genome including episomes outside the nucleus but excluding changes due to episomes that are lost over time This definition would also exclude introducing cells that did not derive from a patient themselves but include ex vivo approaches and would not depend on the vector used 43 During the COVID 19 pandemic some academics insisted that the MRNA vaccines for COVID were not gene therapy to prevent the spread of incorrect information that the vaccine could alter DNA other academics maintained that the vaccines were a gene therapy because they introduced genetic material into a cell 44 Fact checkers such as Full Fact 45 Reuters 46 PolitiFact 47 and FactCheck org 48 said that calling the vaccines a gene therapy was incorrect Podcast host Joe Rogan was criticized for calling MRNA vaccines gene therapy as was British politician Andrew Bridgen with fact checker Full Fact calling for Bridgen to be removed from the conservative party for this and other statements 49 50 Genes present or added Edit Gene therapy encapsulates many forms of adding different nucleic acids to a cell Gene augmentation adds a new protein coding gene to a cell One form of gene augmentiation is gene replacement therapy a treatment for monogenic recessive disorders where a single gene is not functional an additional functional gene is added For diseases caused by multiple genes or a dominant gene gene silencing or gene editing approaches are more appropriate but gene addition a form of gene augmentation where new gene is added may improve a cells function despite other without modifying the genes that cause a disorder 51 117 Cell types Edit Gene therapy may be classified into two types by the type of cell it affects somatic cell and germlie gene therapy In somatic cell gene therapy SCGT the therapeutic genes are transferred into any cell other than a gamete germ cell gametocyte or undifferentiated stem cell Any such modifications affect the individual patient only and are not inherited by offspring Somatic gene therapy represents mainstream basic and clinical research in which therapeutic DNA either integrated in the genome or as an external episome or plasmid is used to treat disease 52 Over 600 clinical trials utilizing SCGT are underway when in the US Most focus on severe genetic disorders including immunodeficiencies haemophilia thalassaemia and cystic fibrosis Such single gene disorders are good candidates for somatic cell therapy The complete correction of a genetic disorder or the replacement of multiple genes is not yet possible Only a few of the trials are in the advanced stages 53 needs update In germline gene therapy GGT germ cells sperm or egg cells are modified by the introduction of functional genes into their genomes Modifying a germ cell causes all the organism s cells to contain the modified gene The change is therefore heritable and passed on to later generations Australia Canada Germany Israel Switzerland and the Netherlands 54 prohibit GGT for application in human beings for technical and ethical reasons including insufficient knowledge about possible risks to future generations 54 and higher risks versus SCGT 55 The US has no federal controls specifically addressing human genetic modification beyond FDA regulations for therapies in general 54 56 57 58 In vivo versus ex vivo therapies Edit In in vivo gene therapy a vector typically a virus is introduced to the patient which then achieves the desired biological effect by passing the genetic material e g for a missing protein into the patient s cells In ex vivo gene therapies such as CAR T therapeutics the patient s own cells autologous or healthy donor cells allogeneic are modified outside the body hence ex vivo using a vector to express a particular protein such as a chimeric antigen receptor 59 In vivo gene therapy is seen as simpler since it does not require the harvesting of mitotic cells However ex vivo gene therapies are better tolerated and less associated with severe immune responses 60 The death of Jesse Gelsinger in a trial of an adenovirus vectored treatment for ornithine transcarbamylase deficiency due to a systemic inflammatory reaction led to a temporary halt on gene therapy trials across the United States 61 As of 2021 update in vivo and ex vivo therapeutics are both seen as safe 62 Gene editing Edit A duplex of crRNA and tracrRNA acts as guide RNA to introduce a specifically located gene modification based on the RNA 5 upstream of the crRNA Cas9 binds the tracrRNA and needs a DNA binding sequence 5 NGG3 which is called protospacer adjacent motif PAM After binding Cas9 introduces a DNA double strand break which is then followed by gene modification via homologous recombination HDR or non homologous end joining NHEJ The concept of gene therapy is to fix a genetic problem at its source If for instance a mutation in a certain gene causes the production of a dysfunctional protein resulting usually recessively in an inherited disease gene therapy could be used to deliver a copy of this gene that does not contain the deleterious mutation and thereby produces a functional protein This strategy is referred to as gene replacement therapy and is employed to treat inherited retinal diseases 14 63 While the concept of gene replacement therapy is mostly suitable for recessive diseases novel strategies have been suggested that are capable of also treating conditions with a dominant pattern of inheritance The introduction of CRISPR gene editing has opened new doors for its application and utilization in gene therapy as instead of pure replacement of a gene it enables correction of the particular genetic defect 37 Solutions to medical hurdles such as the eradication of latent human immunodeficiency virus HIV reservoirs and correction of the mutation that causes sickle cell disease may be available as a therapeutic option in the future 64 65 66 Prosthetic gene therapy aims to enable cells of the body to take over functions they physiologically do not carry out One example is the so called vision restoration gene therapy that aims to restore vision in patients with end stage retinal diseases 67 68 In end stage retinal diseases the photoreceptors as the primary light sensitive cells of the retina are irreversibly lost By the means of prosthetic gene therapy light sensitive proteins are delivered into the remaining cells of the retina to render them light sensitive and thereby enable them to signal visual information towards the brain GVectors EditMain article Vectors in gene therapy The delivery of DNA into cells can be accomplished by multiple methods The two major classes are recombinant viruses sometimes called biological nanoparticles or viral vectors and naked DNA or DNA complexes non viral methods 69 Viruses Edit Main article Viral vector Gene therapy using an adenovirus vector In some cases the adenovirus will insert the new gene into a cell If the treatment is successful the new gene will make a functional protein to treat a disease In order to replicate viruses introduce their genetic material into the host cell tricking the host s cellular machinery into using it as blueprints for viral proteins 51 39 Retroviruses go a stage further by having their genetic material copied into the nuclear genome of the host cell Scientists exploit this by substituting partt of a virus s genetic material with therapeutic DNA or RNA 51 40 70 Like the genetic material DNA or RNA in viruses therapeutic genetic material can be designed to simply serve as a temporary blueprint that degrades naturally as in a non integrative vectors or to enter the host s nucleus becoming a permanent part of the host s nuclear DNA in infected cells 51 50 A number of viruses have been used for human gene therapy including retroviruses such as lentivirus adenoviruses herpes simplex vaccinia and adeno associated virus 4 Adenovirus viral vectors Ad temporarily modify a cell s genetic expression with genetic material that is not integrated into the host cell s DNA 71 5 As of 2017 such vectors were used in 20 of trials for gene therapy 70 10 Adenovirus vectors are mostly used in cancer treatments and novel genetic vaccines such as the Ebola vaccine vaccines used in clinical trials for HIV and SARS CoV 2 or cancer vaccines 71 5 Lentiviral vectors based on lentivirus a retrovirus can modify a cell s nuclear genome to permanently express a gene although vectors can be modify to prevent integration 51 40 50 Retroviruses were used in 18 of trials before 2018 70 10 Adeno associated virus AAV is a virus that is incapable of transmission between cells unless the cell is infected by another virus a helper virus Adenovirus and the herpes viruses act as helper viruses for AAV AAV persists within the cell outside of the cell s nuclear genome for an extended period of time through the formation of concatemers mostly organized as episomes 72 4 Genetic material from AAV vectors is integrated into the host cell s nuclear genome at a low frequency and likely mediated by the DNA modifying enzymes of the host cell 73 2647 Animal models suggest that integration of AAV genetic material into the host cell s nuclear genome may cause hepatocellular carcinoma a form of liver cancer 73 Non viral Edit This section needs additional citations for verification Please help improve this article by adding citations to reliable sources Unsourced material may be challenged and removed April 2021 Learn how and when to remove this template message Non viral vectors for gene therapy 74 present certain advantages over viral methods such as large scale production and low host immunogenicity However non viral methods initially produced lower levels of transfection and gene expression and thus lower therapeutic efficacy Newer technologies offer promise of solving these problems with the advent of increased cell specific targeting and subcellular trafficking control Methods for non viral gene therapy include the injection of naked DNA electroporation the gene gun sonoporation magnetofection the use of oligonucleotides lipoplexes dendrimers and inorganic nanoparticles More recent approaches such as those performed by companies such as Ligandal offer the possibility of creating cell specific targeting technologies for a variety of gene therapy modalities including RNA DNA and gene editing tools such as CRISPR Other companies such as Arbutus Biopharma and Arcturus Therapeutics offer non viral non cell targeted approaches that mainly exhibit liver trophism In more recent years startups such as Sixfold Bio GenEdit and Spotlight Therapeutics have begun to solve the non viral gene delivery problem Non viral techniques offer the possibility of repeat dosing and greater tailorability of genetic payloads which in the future will be more likely to take over viral based delivery systems Companies such as Editas Medicine Intellia Therapeutics CRISPR Therapeutics Casebia Cellectis Precision Biosciences bluebird bio and Sangamo have developed non viral gene editing techniques however frequently still use viruses for delivering gene insertion material following genomic cleavage by guided nucleases These companies focus on gene editing and still face major delivery hurdles BioNTech Moderna Therapeutics and CureVac focus on delivery of mRNA payloads which are necessarily non viral delivery problems Alnylam Dicerna Pharmaceuticals and Ionis Pharmaceuticals focus on delivery of siRNA antisense oligonucleotides for gene suppression which also necessitate non viral delivery systems In academic contexts a number of laboratories are working on delivery of PEGylated particles which form serum protein coronas and chiefly exhibit LDL receptor mediated uptake in cells in vivo 75 Treatment EditCancer Edit Suicide gene therapy graphic used to treat cancer There have been attempts to treat cancer using gene therapy As of 2017 65 of gene therapy trials were for cancer treatment 70 7 Adenovirus vectors are useful for some cancer gene therapies because adenovirus can transiently insert genetic material into a cell without permanently altering the cell s nuclear genome These vectors can be used to cause antigens to be added to cancers causing an immune response or hinder angiogenesis by expressing certain proteins 76 5 An Adenovirus vector is used in the commercial products Gendicine and Oncorine 76 10 Another commercial product Rexin G uses a retrovirus based vector and selectively binds to receptors that are more expressed in tumors 76 10 One approach suicide gene therapy works by introducing genes encoding enzymes that will cause a cancer cell to die Another approach is the use oncolytic viruses such as Oncorine 77 165 which are viruses that selectively reproduce in cancerous cells leaving other cells unaffected 78 6 79 280 MRNA has been suggested as a non viral vector for cancer gene therapy that would temporarily change a cancer cells function to create antigens or kill the cells resulting in several trials 80 Genetic diseases Edit Gene therapy approaches to replace a faulty gene with a healthy gene have been proposed and are being studied for treating some genetic diseases As of 2017 11 1 of gene therapy clinical trials targeted monogentic genetic diseases 70 9 Diseases such as sickle cell disease that are caused by autosomal recessive disorders for which a person s normal phenotype or cell function may be restored in cells that have the disease by a normal copy of the gene that is mutated may be a good candidate for gene therapy treatment 81 82 The risks and benefits related to gene therapy for sickle cell disease are not known 82 Gene therapy has been use in the eye The eye is especially suitable for adeno associated virus vectors Luxturna is an approved gene therapy to treat Leber s hereditary optic neuropathy 83 1354 Glybera a treatment for pancreatitis caused by a genetic condition and Zolgensma for the treatment of spinal muscular atrophy both use an adeno associated virus vector 73 2647 Infectious diseases Edit As of 2017 7 of genetic therapy trials targetted infectious diseases 69 2 of trials targetted HIV 11 hepatitis B or C and 7 1 malaria 70 List of gene therapies for treatment of disease Edit See also List of gene therapies Some genetic therapies have been approved by the U S Food and Drug Administration FDA the European Medicines Agency EMA and for use in Russia and China List of approved gene therapies for the treatment of disease INN Brand name Type Manufacturer Target FDA approved EMA authorizedalipogene tiparvovec Glybera In vivo Chiesi Farmaceutici lipoprotein lipase deficiency No Withdrawnatidarsagene autotemcel Libmeldy Arylsulfatase A gene encoding autologous CD34 cells Ex vitro Orchard Therapeutics metachromatic leukodystrophy No 17 December 2020 84 autologous CD34 Strimvelis adenosine deaminase deficiency ADA SCID 26 May 2016axicabtagene ciloleucel Yescarta large B cell lymphoma 18 October 2017 23 August 2018betibeglogene autotemcel Zynteglo beta thalassemia 17 August 2022 85 29 May 2019brexucabtagene autoleucel Tecartus Ex vitro Kite Pharma mantle cell lymphoma and acute lymphoblastic leukemia 24 July 2020 86 87 14 December 2020 88 cambiogenplasmid Neovasculgen vascular endothelial growth factor peripheral artery diseaseelivaldogene autotemcel Skysona cerebral adrenoleukodystrophy 16 July 2021gendicine head and neck squamous cell carcinomaidecabtagene vicleucel Abecma Ex vivo Celgene multiple myeloma 26 March 2021 89 Nolisocabtagene maraleucel Breyanzi Ex vivo Juno Therapeutics B cell lymphoma 5 February 2021 90 Nonadofaragene firadenovec Adstiladrin Ferring Pharmaceuticals high risk Bacillus Calmette Guerin BCG unresponsive non muscle invasive bladder cancer NMIBC with carcinoma in situ CIS Yes 91 Noonasemnogene abeparvovec Zolgensma In vivo Novartis Gene Therapies Spinal muscular atrophy Type I 24 May 2019 92 26 March 2020 93 talimogene laherparepvec Imlygic In vivo Amgen melanoma 27 October 2015 94 16 December 2015 95 tisagenlecleucel Kymriah B cell lymphoblastic leukemia 22 August 2018valoctocogene roxaparvovec Roctavian BioMarin International Limited hemophilia A August 2022 96 97 98 voretigene neparvovec Luxturna In vivo Spark Therapeutics biallelic RPE65 mutation associated Leber congenital amaurosis 18 December 2017 99 22 November 2018 100 Adverse effects contraindications and hurdles for use EditSome of the unsolved problems include Short lived nature Before gene therapy can become a permanent cure for a condition the therapeutic DNA introduced into target cells must remain functional and the cells containing the therapeutic DNA must be stable Problems with integrating therapeutic DNA into the nuclear genome and the rapidly dividing nature of many cells prevent it from achieving long term benefits Patients require multiple treatments Immune response Any time a foreign object is introduced into human tissues the immune system is stimulated to attack the invader Stimulating the immune system in a way that reduces gene therapy effectiveness is possible The immune system s enhanced response to viruses that it has seen before reduces the effectiveness to repeated treatments Problems with viral vectors Viral vectors carry the risks of toxicity inflammatory responses and gene control and targeting issues Multigene disorders Some commonly occurring disorders such as heart disease high blood pressure Alzheimer s disease arthritis and diabetes are affected by variations in multiple genes which complicate gene therapy Some therapies may breach the Weismann barrier between soma and germ line protecting the testes potentially modifying the germline falling afoul of regulations in countries that prohibit the latter practice 101 Insertional mutagenesis If the DNA is integrated in a sensitive spot in the genome for example in a tumor suppressor gene the therapy could induce a tumor This has occurred in clinical trials for X linked severe combined immunodeficiency X SCID patients in which hematopoietic stem cells were transduced with a corrective transgene using a retrovirus and this led to the development of T cell leukemia in 3 of 20 patients 102 103 One possible solution is to add a functional tumor suppressor gene to the DNA to be integrated This may be problematic since the longer the DNA is the harder it is to integrate into cell genomes 104 CRISPR technology allows researchers to make much more precise genome changes at exact locations 105 Cost Alipogene tiparvovec or Glybera for example at a cost of 1 6 million per patient was reported in 2013 to be the world s most expensive drug 106 107 Deaths Edit Three patients deaths have been reported in gene therapy trials putting the field under close scrutiny The first was that of Jesse Gelsinger who died in 1999 because of immune rejection response 108 109 One X SCID patient died of leukemia in 2003 10 In 2007 a rheumatoid arthritis patient died from an infection the subsequent investigation concluded that the death was not related to gene therapy 110 Regulations EditRegulations covering genetic modification are part of general guidelines about human involved biomedical research citation needed There are no international treaties which are legally binding in this area but there are recommendations for national laws from various bodies citation needed The Helsinki Declaration Ethical Principles for Medical Research Involving Human Subjects was amended by the World Medical Association s General Assembly in 2008 This document provides principles physicians and researchers must consider when involving humans as research subjects The Statement on Gene Therapy Research initiated by the Human Genome Organization HUGO in 2001 provides a legal baseline for all countries HUGO s document emphasizes human freedom and adherence to human rights and offers recommendations for somatic gene therapy including the importance of recognizing public concerns about such research 111 United States Edit No federal legislation lays out protocols or restrictions about human genetic engineering This subject is governed by overlapping regulations from local and federal agencies including the Department of Health and Human Services the FDA and NIH s Recombinant DNA Advisory Committee Researchers seeking federal funds for an investigational new drug application commonly the case for somatic human genetic engineering must obey international and federal guidelines for the protection of human subjects 112 NIH serves as the main gene therapy regulator for federally funded research Privately funded research is advised to follow these regulations NIH provides funding for research that develops or enhances genetic engineering techniques and to evaluate the ethics and quality in current research The NIH maintains a mandatory registry of human genetic engineering research protocols that includes all federally funded projects 113 An NIH advisory committee published a set of guidelines on gene manipulation 114 The guidelines discuss lab safety as well as human test subjects and various experimental types that involve genetic changes Several sections specifically pertain to human genetic engineering including Section III C 1 This section describes required review processes and other aspects when seeking approval to begin clinical research involving genetic transfer into a human patient 115 The protocol for a gene therapy clinical trial must be approved by the NIH s Recombinant DNA Advisory Committee prior to any clinical trial beginning this is different from any other kind of clinical trial 114 As with other kinds of drugs the FDA regulates the quality and safety of gene therapy products and supervises how these products are used clinically Therapeutic alteration of the human genome falls under the same regulatory requirements as any other medical treatment Research involving human subjects such as clinical trials must be reviewed and approved by the FDA and an Institutional Review Board 116 117 Gene doping EditMain article Gene doping Athletes may adopt gene therapy technologies to improve their performance 118 Gene doping is not known to occur but multiple gene therapies may have such effects Kayser et al argue that gene doping could level the playing field if all athletes receive equal access Critics claim that any therapeutic intervention for non therapeutic enhancement purposes compromises the ethical foundations of medicine and sports 119 Genetic enhancement EditFurther information Human genetic enhancement See also Human germline engineering and Assisted reproductive technology Genetic engineering could be used to cure diseases but also to change physical appearance metabolism and even improve physical capabilities and mental faculties such as memory and intelligence Ethical claims about germline engineering include beliefs that every fetus has a right to remain genetically unmodified that parents hold the right to genetically modify their offspring and that every child has the right to be born free of preventable diseases 120 121 122 For parents genetic engineering could be seen as another child enhancement technique to add to diet exercise education training cosmetics and plastic surgery 123 124 Another theorist claims that moral concerns limit but do not prohibit germline engineering 125 A recent issue of the journal Bioethics was devoted to moral issues surrounding germline genetic engineering in people 126 Possible regulatory schemes include a complete ban provision to everyone or professional self regulation The American Medical Association s Council on Ethical and Judicial Affairs stated that genetic interventions to enhance traits should be considered permissible only in severely restricted situations 1 clear and meaningful benefits to the fetus or child 2 no trade off with other characteristics or traits and 3 equal access to the genetic technology irrespective of income or other socioeconomic characteristics 127 As early in the history of biotechnology as 1990 there have been scientists opposed to attempts to modify the human germline using these new tools 128 and such concerns have continued as technology progressed 129 130 With the advent of new techniques like CRISPR in March 2015 a group of scientists urged a worldwide moratorium on clinical use of gene editing technologies to edit the human genome in a way that can be inherited 131 132 133 134 In April 2015 researchers sparked controversy when they reported results of basic research to edit the DNA of non viable human embryos using CRISPR 135 136 A committee of the American National Academy of Sciences and National Academy of Medicine gave qualified support to human genome editing in 2017 137 138 once answers have been found to safety and efficiency problems but only for serious conditions under stringent oversight 139 History EditThis section may be too long and excessively detailed Please consider summarizing the material November 2018 1970s and earlier Edit In 1972 Friedmann and Roblin authored a paper in Science titled Gene therapy for human genetic disease 140 Rogers 1970 was cited for proposing that exogenous good DNA be used to replace the defective DNA in those with genetic defects 141 1980s Edit In 1984 a retrovirus vector system was designed that could efficiently insert foreign genes into mammalian chromosomes 142 1990s Edit The first approved gene therapy clinical research in the US took place on 14 September 1990 at the National Institutes of Health NIH under the direction of William French Anderson 143 Four year old Ashanti DeSilva received treatment for a genetic defect that left her with adenosine deaminase deficiency ADA SCID a severe immune system deficiency The defective gene of the patient s blood cells was replaced by the functional variant Ashanti s immune system was partially restored by the therapy Production of the missing enzyme was temporarily stimulated but the new cells with functional genes were not generated She led a normal life only with the regular injections performed every two months The effects were successful but temporary 144 Cancer gene therapy was introduced in 1992 93 Trojan et al 1993 145 The treatment of glioblastoma multiforme the malignant brain tumor whose outcome is always fatal was done using a vector expressing antisense IGF I RNA clinical trial approved by NIH protocol no 1602 24 November 1993 146 and by the FDA in 1994 This therapy also represents the beginning of cancer immunogene therapy a treatment which proves to be effective due to the anti tumor mechanism of IGF I antisense which is related to strong immune and apoptotic phenomena In 1992 Claudio Bordignon working at the Vita Salute San Raffaele University performed the first gene therapy procedure using hematopoietic stem cells as vectors to deliver genes intended to correct hereditary diseases 147 In 2002 this work led to the publication of the first successful gene therapy treatment for ADA SCID The success of a multi center trial for treating children with SCID severe combined immune deficiency or bubble boy disease from 2000 and 2002 was questioned when two of the ten children treated at the trial s Paris center developed a leukemia like condition Clinical trials were halted temporarily in 2002 but resumed after regulatory review of the protocol in the US the United Kingdom France Italy and Germany 148 In 1993 Andrew Gobea was born with SCID following prenatal genetic screening Blood was removed from his mother s placenta and umbilical cord immediately after birth to acquire stem cells The allele that codes for adenosine deaminase ADA was obtained and inserted into a retrovirus Retroviruses and stem cells were mixed after which the viruses inserted the gene into the stem cell chromosomes Stem cells containing the working ADA gene were injected into Andrew s blood Injections of the ADA enzyme were also given weekly For four years T cells white blood cells produced by stem cells made ADA enzymes using the ADA gene After four years more treatment was needed 149 Jesse Gelsinger s death in 1999 impeded gene therapy research in the US 150 151 As a result the FDA suspended several clinical trials pending the reevaluation of ethical and procedural practices 152 2000s Edit The modified gene therapy strategy of antisense IGF I RNA NIH n 1602 146 using antisense triple helix anti IGF I approach was registered in 2002 by Wiley gene therapy clinical trial n 635 and 636 The approach has shown promising results in the treatment of six different malignant tumors glioblastoma cancers of liver colon prostate uterus and ovary Collaborative NATO Science Programme on Gene Therapy USA France Poland n LST 980517 conducted by J Trojan Trojan et al 2012 This anti gene antisense triple helix therapy has proven to be efficient due to the mechanism stopping simultaneously IGF I expression on translation and transcription levels strengthening anti tumor immune and apoptotic phenomena 2002 Edit Sickle cell disease can be treated in mice 153 The mice which have essentially the same defect that causes human cases used a viral vector to induce production of fetal hemoglobin HbF which normally ceases to be produced shortly after birth In humans the use of hydroxyurea to stimulate the production of HbF temporarily alleviates sickle cell symptoms The researchers demonstrated this treatment to be a more permanent means to increase therapeutic HbF production 154 A new gene therapy approach repaired errors in messenger RNA derived from defective genes This technique has the potential to treat thalassaemia cystic fibrosis and some cancers 155 Researchers created liposomes 25 nanometers across that can carry therapeutic DNA through pores in the nuclear membrane 156 2003 Edit In 2003 a research team inserted genes into the brain for the first time They used liposomes coated in a polymer called polyethylene glycol which unlike viral vectors are small enough to cross the blood brain barrier 157 Short pieces of double stranded RNA short interfering RNAs or siRNAs are used by cells to degrade RNA of a particular sequence If a siRNA is designed to match the RNA copied from a faulty gene then the abnormal protein product of that gene will not be produced 158 Gendicine is a cancer gene therapy that delivers the tumor suppressor gene p53 using an engineered adenovirus In 2003 it was approved in China for the treatment of head and neck squamous cell carcinoma 28 2006 Edit In March researchers announced the successful use of gene therapy to treat two adult patients for X linked chronic granulomatous disease a disease which affects myeloid cells and damages the immune system The study is the first to show that gene therapy can treat the myeloid system 159 In May a team reported a way to prevent the immune system from rejecting a newly delivered gene 160 Similar to organ transplantation gene therapy has been plagued by this problem The immune system normally recognizes the new gene as foreign and rejects the cells carrying it The research utilized a newly uncovered network of genes regulated by molecules known as microRNAs This natural function selectively obscured their therapeutic gene in immune system cells and protected it from discovery Mice infected with the gene containing an immune cell microRNA target sequence did not reject the gene In August scientists successfully treated metastatic melanoma in two patients using killer T cells genetically retargeted to attack the cancer cells 161 In November researchers reported on the use of VRX496 a gene based immunotherapy for the treatment of HIV that uses a lentiviral vector to deliver an antisense gene against the HIV envelope In a phase I clinical trial five subjects with chronic HIV infection who had failed to respond to at least two antiretroviral regimens were treated A single intravenous infusion of autologous CD4 T cells genetically modified with VRX496 was well tolerated All patients had stable or decreased viral load four of the five patients had stable or increased CD4 T cell counts All five patients had stable or increased immune response to HIV antigens and other pathogens This was the first evaluation of a lentiviral vector administered in a US human clinical trial 162 163 2007 Edit In May researchers announced the first gene therapy trial for inherited retinal disease The first operation was carried out on a 23 year old British male Robert Johnson in early 2007 164 2008 Edit Main article Gene therapy of the human retina Leber s congenital amaurosis is an inherited blinding disease caused by mutations in the RPE65 gene The results of a small clinical trial in children were published in April 14 Delivery of recombinant adeno associated virus AAV carrying RPE65 yielded positive results In May two more groups reported positive results in independent clinical trials using gene therapy to treat the condition In all three clinical trials patients recovered functional vision without apparent side effects 14 15 16 17 2009 Edit In September researchers were able to give trichromatic vision to squirrel monkeys 165 In November 2009 researchers halted a fatal genetic disorder called adrenoleukodystrophy in two children using a lentivirus vector to deliver a functioning version of ABCD1 the gene that is mutated in the disorder 166 2010s Edit 2010 Edit An April paper reported that gene therapy addressed achromatopsia color blindness in dogs by targeting cone photoreceptors Cone function and day vision were restored for at least 33 months in two young specimens The therapy was less efficient for older dogs 167 In September it was announced that an 18 year old male patient in France with beta thalassemia major had been successfully treated 168 Beta thalassemia major is an inherited blood disease in which beta haemoglobin is missing and patients are dependent on regular lifelong blood transfusions 169 The technique used a lentiviral vector to transduce the human b globin gene into purified blood and marrow cells obtained from the patient in June 2007 170 The patient s haemoglobin levels were stable at 9 to 10 g dL About a third of the hemoglobin contained the form introduced by the viral vector and blood transfusions were not needed 170 171 Further clinical trials were planned 172 Bone marrow transplants are the only cure for thalassemia but 75 of patients do not find a matching donor 171 Cancer immunogene therapy using modified antigene antisense triple helix approach was introduced in South America in 2010 11 in La Sabana University Bogota Ethical Committee 14 December 2010 no P 004 10 Considering the ethical aspect of gene diagnostic and gene therapy targeting IGF I the IGF I expressing tumors i e lung and epidermis cancers were treated Trojan et al 2016 173 174 2011 Edit In 2007 and 2008 a man Timothy Ray Brown was cured of HIV by repeated hematopoietic stem cell transplantation see also allogeneic stem cell transplantation allogeneic bone marrow transplantation allotransplantation with double delta 32 mutation which disables the CCR5 receptor This cure was accepted by the medical community in 2011 175 It required complete ablation of existing bone marrow which is very debilitating 176 In August two of three subjects of a pilot study were confirmed to have been cured from chronic lymphocytic leukemia CLL The therapy used genetically modified T cells to attack cells that expressed the CD19 protein to fight the disease 23 In 2013 the researchers announced that 26 of 59 patients had achieved complete remission and the original patient had remained tumor free 177 Human HGF plasmid DNA therapy of cardiomyocytes is being examined as a potential treatment for coronary artery disease as well as treatment for the damage that occurs to the heart after myocardial infarction 178 179 In 2011 Neovasculgen was registered in Russia as the first in class gene therapy drug for treatment of peripheral artery disease including critical limb ischemia it delivers the gene encoding for VEGF 29 Neovasculogen is a plasmid encoding the CMV promoter and the 165 amino acid form of VEGF 180 181 2012 Edit The FDA approved Phase I clinical trials on thalassemia major patients in the US for 10 participants in July 182 The study was expected to continue until 2015 172 In July 2012 the European Medicines Agency recommended approval of a gene therapy treatment for the first time in either Europe or the United States The treatment used Alipogene tiparvovec Glybera to compensate for lipoprotein lipase deficiency which can cause severe pancreatitis 183 The recommendation was endorsed by the European Commission in November 2012 13 30 184 185 and commercial rollout began in late 2014 186 Alipogene tiparvovec was expected to cost around 1 6 million per treatment in 2012 187 revised to 1 million in 2015 188 making it the most expensive medicine in the world at the time 189 As of 2016 update only the patients treated in clinical trials and a patient who paid the full price for treatment have received the drug 190 In December 2012 it was reported that 10 of 13 patients with multiple myeloma were in remission or very close to it three months after being injected with a treatment involving genetically engineered T cells to target proteins NY ESO 1 and LAGE 1 which exist only on cancerous myeloma cells 25 2013 Edit In March researchers reported that three of five adult subjects who had acute lymphocytic leukemia ALL had been in remission for five months to two years after being treated with genetically modified T cells which attacked cells with CD19 genes on their surface i e all B cells cancerous or not The researchers believed that the patients immune systems would make normal T cells and B cells after a couple of months They were also given bone marrow One patient relapsed and died and one died of a blood clot unrelated to the disease 24 Following encouraging Phase I trials in April researchers announced they were starting Phase II clinical trials called CUPID2 and SERCA LVAD on 250 patients 191 at several hospitals to combat heart disease The therapy was designed to increase the levels of SERCA2 a protein in heart muscles improving muscle function 192 The U S Food and Drug Administration FDA granted this a breakthrough therapy designation to accelerate the trial and approval process 193 In 2016 it was reported that no improvement was found from the CUPID 2 trial 194 In July researchers reported promising results for six children with two severe hereditary diseases had been treated with a partially deactivated lentivirus to replace a faulty gene and after 7 32 months Three of the children had metachromatic leukodystrophy which causes children to lose cognitive and motor skills 195 The other children had Wiskott Aldrich syndrome which leaves them to open to infection autoimmune diseases and cancer 196 Follow up trials with gene therapy on another six children with Wiskott Aldrich syndrome were also reported as promising 197 198 In October researchers reported that two children born with adenosine deaminase severe combined immunodeficiency disease ADA SCID had been treated with genetically engineered stem cells 18 months previously and that their immune systems were showing signs of full recovery Another three children were making progress 21 In 2014 a further 18 children with ADA SCID were cured by gene therapy 199 ADA SCID children have no functioning immune system and are sometimes known as bubble children 21 Also in October researchers reported that they had treated six people with haemophilia in early 2011 using an adeno associated virus Over two years later all six were producing clotting factor 21 200 2014 Edit In January researchers reported that six choroideremia patients had been treated with adeno associated virus with a copy of REP1 Over a six month to two year period all had improved their sight 63 201 By 2016 32 patients had been treated with positive results and researchers were hopeful the treatment would be long lasting 18 Choroideremia is an inherited genetic eye disease with no approved treatment leading to loss of sight In March researchers reported that 12 HIV patients had been treated since 2009 in a trial with a genetically engineered virus with a rare mutation CCR5 deficiency known to protect against HIV with promising results 202 203 Clinical trials of gene therapy for sickle cell disease were started in 2014 204 205 In February LentiGlobin BB305 a gene therapy treatment undergoing clinical trials for treatment of beta thalassemia gained FDA breakthrough status after several patients were able to forgo the frequent blood transfusions usually required to treat the disease 206 In March researchers delivered a recombinant gene encoding a broadly neutralizing antibody into monkeys infected with simian HIV the monkeys cells produced the antibody which cleared them of HIV The technique is named immunoprophylaxis by gene transfer IGT Animal tests for antibodies to ebola malaria influenza and hepatitis were underway 207 208 In March scientists including an inventor of CRISPR Jennifer Doudna urged a worldwide moratorium on germline gene therapy writing scientists should avoid even attempting in lax jurisdictions germline genome modification for clinical application in humans until the full implications are discussed among scientific and governmental organizations 131 132 133 134 In December scientists of major world academies called for a moratorium on inheritable human genome edits including those related to CRISPR Cas9 technologies 209 but that basic research including embryo gene editing should continue 210 2015 Edit Researchers successfully treated a boy with epidermolysis bullosa using skin grafts grown from his own skin cells genetically altered to repair the mutation that caused his disease 211 In November researchers announced that they had treated a baby girl Layla Richards with an experimental treatment using donor T cells genetically engineered using TALEN to attack cancer cells One year after the treatment she was still free of her cancer a highly aggressive form of acute lymphoblastic leukaemia ALL 212 Children with highly aggressive ALL normally have a very poor prognosis and Layla s disease had been regarded as terminal before the treatment 213 214 2016 Edit In April the Committee for Medicinal Products for Human Use of the European Medicines Agency endorsed a gene therapy treatment called Strimvelis 215 216 and the European Commission approved it in June 217 This treats children born with adenosine deaminase deficiency and who have no functioning immune system This was the second gene therapy treatment to be approved in Europe 218 In October Chinese scientists reported they had started a trial to genetically modify T cells from 10 adult patients with lung cancer and reinject the modified T cells back into their bodies to attack the cancer cells The T cells had the PD 1 protein which stops or slows the immune response removed using CRISPR Cas9 219 220 A 2016 Cochrane systematic review looking at data from four trials on topical cystic fibrosis transmembrane conductance regulator CFTR gene therapy does not support its clinical use as a mist inhaled into the lungs to treat cystic fibrosis patients with lung infections One of the four trials did find weak evidence that liposome based CFTR gene transfer therapy may lead to a small respiratory improvement for people with CF This weak evidence is not enough to make a clinical recommendation for routine CFTR gene therapy 221 2017 Edit In February Kite Pharma announced results from a clinical trial of CAR T cells in around a hundred people with advanced non Hodgkin lymphoma 222 In March French scientists reported on clinical research of gene therapy to treat sickle cell disease 223 In August the FDA approved tisagenlecleucel for acute lymphoblastic leukemia 224 Tisagenlecleucel is an adoptive cell transfer therapy for B cell acute lymphoblastic leukemia T cells from a person with cancer are removed genetically engineered to make a specific T cell receptor a chimeric T cell receptor or CAR T that reacts to the cancer and are administered back to the person The T cells are engineered to target a protein called CD19 that is common on B cells This is the first form of gene therapy to be approved in the United States In October a similar therapy called axicabtagene ciloleucel was approved for non Hodgkin lymphoma 225 In October biophysicist and biohacker Josiah Zayner claimed to have performed the very first in vivo human genome editing in the form of a self administered therapy 226 227 On 13 November medical scientists working with Sangamo Therapeutics headquartered in Richmond California announced the first ever in body human gene editing therapy 228 229 The treatment designed to permanently insert a healthy version of the flawed gene that causes Hunter syndrome was given to 44 year old Brian Madeux and is part of the world s first study to permanently edit DNA inside the human body 230 The success of the gene insertion was later confirmed 231 232 Clinical trials by Sangamo involving gene editing using zinc finger nuclease ZFN are ongoing 233 In December the results of using an adeno associated virus with blood clotting factor VIII to treat nine haemophilia A patients were published Six of the seven patients on the high dose regime increased the level of the blood clotting VIII to normal levels The low and medium dose regimes had no effect on the patient s blood clotting levels 234 235 In December the FDA approved Luxturna the first in vivo gene therapy for the treatment of blindness due to Leber s congenital amaurosis 236 The price of this treatment is US 850 000 for both eyes 237 238 2019 Edit In May the FDA approved onasemnogene abeparvovec Zolgensma for treating spinal muscular atrophy in children under two years of age The list price of Zolgensma was set at US 2 125 million per dose making it the most expensive drug ever 239 In May the EMA approved betibeglogene autotemcel Zynteglo for treating beta thalassemia for people twelve years of age and older 240 241 In July Allergan and Editas Medicine announced phase I II clinical trial of AGN 151587 for the treatment of Leber congenital amaurosis 10 242 This is the first study of a CRISPR based in vivo human gene editing therapy where the editing takes place inside the human body 243 The first injection of the CRISPR Cas System was confirmed in March 2020 244 2020s Edit 2020 Edit In May onasemnogene abeparvovec Zolgensma was approved by the European Union for the treatment of spinal muscular atrophy in people who either have clinical symptoms of SMA type 1 or who have no more than three copies of the SMN2 gene irrespective of body weight or age 245 In August Audentes Therapeutics reported that three out of 17 children with X linked myotubular myopathy participating the clinical trial of a AAV8 based gene therapy treatment AT132 have died It was suggested that the treatment whose dosage is based on body weight exerts a disproportionately toxic effect on heavier patients since the three patients who died were heavier than the others 246 247 The trial has been put on clinical hold 248 On 15 October the Committee for Medicinal Products for Human Use CHMP of the European Medicines Agency EMA adopted a positive opinion recommending the granting of a marketing authorisation for the medicinal product Libmeldy autologous CD34 cell enriched population that contains hematopoietic stem and progenitor cells transduced ex vivo using a lentiviral vector encoding the human arylsulfatase A gene a gene therapy for the treatment of children with the late infantile LI or early juvenile EJ forms of metachromatic leukodystrophy MLD 249 The active substance of Libmeldy consists of the child s own stem cells which have been modified to contain working copies of the ARSA gene 249 When the modified cells are injected back into the patient as a one time infusion the cells are expected to start producing the ARSA enzyme that breaks down the build up of sulfatides in the nerve cells and other cells of the patient s body 250 Libmeldy was approved for medical use in the EU in December 2020 251 On 15 October Lysogene a French biotechnological company reported the death of a patient in who has received LYS SAF302 an experimental gene therapy treatment for mucopolysaccharidosis type IIIA Sanfilippo syndrome type A 252 2021 Edit In May a new method using an altered version of the HIV virus as a lentivirus vector was reported in the treatment of 50 children with ADA SCID obtaining positive results in 48 of them 253 254 255 this method is expected to be safer than retroviruses vectors commonly used in previous studies of SCID where the development of leukemia was usually observed 256 and had already been used in 2019 but in a smaller group with X SCID 257 258 259 260 In June a clinical trial on six patients affected with transthyretin amyloidosis reported a reduction the concentration of missfolded transthretin TTR protein in serum through CRISPR based inactivation of the TTR gene in liver cells observing mean reductions of 52 and 87 among the lower and higher dose groups This was done in vivo without taking cells out of the patient to edit them and reinfuse them later 261 262 263 In July results of a small gene therapy phase I study was published reporting observation of dopamine restoration on seven patients between 4 and 9 years old affected by aromatic L amino acid decarboxylase deficiency AADC deficiency 264 265 266 2022 Edit In February the first ever gene therapy for Tay Sachs disease was announced it uses an adeno associated virus to deliver the correct instruction for the HEXA gene on brain cells which causes the disease Only two children were part of a compassionate trial presenting improvements over the natural course of the disease and no vector related adverse events 267 268 269 In May eladocagene exuparvovec is recommended for approval by the European Commission 270 271 In July results of a gene therapy candidate for haemophilia B called FLT180 were announced it works using an adeno associated virus AAV to restore the clotting factor IX FIX protein normal levels of the protein were observed with low doses of the therapy but immunosuppression was necessitated to decrease the risk of vector related immune responses 272 273 274 In December a 13 year girl that had been diagnosed with T cell acute lymphoblastic leukaemia was successfully treated at Great Ormond Street Hospital GOSH in the first documented use of therapeutic gene editing for this purpose after undergoing six months of an experimental treatment where all attempts of other treatments failed The procedure included reprogramming a healthy T cell to destroy the cancerous T cells to first rid her of leukaemia and then rebuilding her immune system using healthy immune cells 275 The GOSH team used BASE editing and had previously treated a case of acute lymphoblastic leukaemia in 2015 using TALENs 214 References Edit Kaji EH Leiden JM February 2001 Gene and stem cell therapies 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