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Genetic disorder

March 28, 2023

For a non-technical introduction to the topic, see Introduction to genetics. For a list of genetic disorders, see List of genetic disorders.

A genetic disorder is a health problem caused by one or more abnormalities in the genome. It can be caused by a mutation in a single gene (monogenic) or multiple genes (polygenic) or by a chromosomal abnormality. Although polygenic disorders are the most common, the term is mostly used when discussing disorders with a single genetic cause, either in a gene or chromosome.[1][2] The mutation responsible can occur spontaneously before embryonic development (a de novo mutation), or it can be inherited from two parents who are carriers of a faulty gene (autosomal recessive inheritance) or from a parent with the disorder (autosomal dominant inheritance). When the genetic disorder is inherited from one or both parents, it is also classified as a hereditary disease. Some disorders are caused by a mutation on the X chromosome and have X-linked inheritance. Very few disorders are inherited on the Y chromosome or mitochondrial DNA (due to their size).[3]

Genetic disorder
A boy with Down syndrome, one of the most common genetic disorders
SpecialtyMedical genetics
Diagram featuring examples of a disease located on each chromosome

There are well over 6,000 known genetic disorders,[4] and new genetic disorders are constantly being described in medical literature.[5] More than 600 genetic disorders are treatable.[6] Around 1 in 50 people are affected by a known single-gene disorder, while around 1 in 263 are affected by a chromosomal disorder.[7] Around 65% of people have some kind of health problem as a result of congenital genetic mutations.[7] Due to the significantly large number of genetic disorders, approximately 1 in 21 people are affected by a genetic disorder classified as "rare" (usually defined as affecting less than 1 in 2,000 people). Most genetic disorders are rare in themselves.[5][8]

Genetic disorders are present before birth, and some genetic disorders produce birth defects, but birth defects can also be developmental rather than hereditary. The opposite of a hereditary disease is an acquired disease. Most cancers, although they involve genetic mutations to a small proportion of cells in the body, are acquired diseases. Some cancer syndromes, however, such as BRCA mutations, are hereditary genetic disorders.[9]

Single-gene

Prevalence of some single-gene disorders[10]
Disorder prevalence (approximate)
Autosomal dominant
Familial hypercholesterolemia 1 in 500[11]
Myotonic dystrophy type 1 1 in 2,100[12]
Neurofibromatosis type I 1 in 2,500[13]
Hereditary spherocytosis 1 in 5,000
Marfan syndrome 1 in 4,000[14]
Huntington's disease 1 in 15,000[15]
Autosomal recessive
Sickle cell anaemia 1 in 625[16]
Cystic fibrosis 1 in 2,000
Tay–Sachs disease 1 in 3,000
Phenylketonuria 1 in 12,000
Autosomal recessive polycystic kidney disease 1 in 20,000[17]
Mucopolysaccharidoses 1 in 25,000
Lysosomal acid lipase deficiency 1 in 40,000
Glycogen storage diseases 1 in 50,000
Galactosemia 1 in 57,000
X-linked
Duchenne muscular dystrophy 1 in 5,000
Hemophilia 1 in 10,000
Values are for liveborn infants
See also: Oligogenic inheritance and Polygenic inheritance

A single-gene disorder (or monogenic disorder) is the result of a single mutated gene. Single-gene disorders can be passed on to subsequent generations in several ways. Genomic imprinting and uniparental disomy, however, may affect inheritance patterns. The divisions between recessive and dominant types are not "hard and fast", although the divisions between autosomal and X-linked types are (since the latter types are distinguished purely based on the chromosomal location of the gene). For example, the common form of dwarfism, achondroplasia, is typically considered a dominant disorder, but children with two genes for achondroplasia have a severe and usually lethal skeletal disorder, one that achondroplasics could be considered carriers for. Sickle cell anemia is also considered a recessive condition, but heterozygous carriers have increased resistance to malaria in early childhood, which could be described as a related dominant condition.[18] When a couple where one partner or both are affected or carriers of a single-gene disorder wish to have a child, they can do so through in vitro fertilization, which enables preimplantation genetic diagnosis to occur to check whether the embryo has the genetic disorder.[19]

Most congenital metabolic disorders known as inborn errors of metabolism result from single-gene defects. Many such single-gene defects can decrease the fitness of affected people and are therefore present in the population in lower frequencies compared to what would be expected based on simple probabilistic calculations.[20]

Autosomal dominant

Main article: Autosomal dominant § Autosomal dominant gene

Only one mutated copy of the gene will be necessary for a person to be affected by an autosomal dominant disorder. Each affected person usually has one affected parent.[21]: 57  The chance a child will inherit the mutated gene is 50%. Autosomal dominant conditions sometimes have reduced penetrance, which means although only one mutated copy is needed, not all individuals who inherit that mutation go on to develop the disease. Examples of this type of disorder are Huntington's disease,[21]: 58  neurofibromatosis type 1, neurofibromatosis type 2, Marfan syndrome, hereditary nonpolyposis colorectal cancer, hereditary multiple exostoses (a highly penetrant autosomal dominant disorder), tuberous sclerosis, Von Willebrand disease, and acute intermittent porphyria. Birth defects are also called congenital anomalies.[citation needed]

Autosomal recessive

Main article: Autosomal dominant § Autosomal recessive allele

Two copies of the gene must be mutated for a person to be affected by an autosomal recessive disorder. An affected person usually has unaffected parents who each carry a single copy of the mutated gene and are referred to as genetic carriers. Each parent with a defective gene normally do not have symptoms.[22] Two unaffected people who each carry one copy of the mutated gene have a 25% risk with each pregnancy of having a child affected by the disorder. Examples of this type of disorder are albinism, medium-chain acyl-CoA dehydrogenase deficiency, cystic fibrosis, sickle cell disease, Tay–Sachs disease, Niemann–Pick disease, spinal muscular atrophy, and Roberts syndrome. Certain other phenotypes, such as wet versus dry earwax, are also determined in an autosomal recessive fashion.[23][24] Some autosomal recessive disorders are common because, in the past, carrying one of the faulty genes led to a slight protection against an infectious disease or toxin such as tuberculosis or malaria.[25] Such disorders include cystic fibrosis,[26] sickle cell disease,[27] phenylketonuria[28] and thalassaemia.[29]

  •  

    Hereditary defects in enzymes are generally inherited in an autosomal fashion because there are more non-X chromosomes than X-chromosomes, and a recessive fashion because the enzymes from the unaffected genes are generally sufficient to prevent symptoms in carriers.

  •  

    On the other hand, hereditary defects in structural proteins (such as osteogenesis imperfecta, Marfan's syndrome and many Ehlers–Danlos syndromes) are generally autosomal dominant, because it is enough that some components are defective to make the whole structure dysfunctional. This is a dominant-negative process, wherein a mutated gene product adversely affects the non-mutated gene product within the same cell.

X-linked dominant

 
Schematic karyogram showing an overview of the human genome. It shows annotated bands and sub-bands as used in the nomenclature of genetic disorders. It shows 22 homologous chromosomes, both the female (XX) and male (XY) versions of the sex chromosome (bottom right), as well as the mitochondrial genome (to scale at bottom left)[citation needed].
Further information: Karyotype
Main article: X-linked dominant

X-linked dominant disorders are caused by mutations in genes on the X chromosome. Only a few disorders have this inheritance pattern, with a prime example being X-linked hypophosphatemic rickets. Males and females are both affected in these disorders, with males typically being more severely affected than females. Some X-linked dominant conditions, such as Rett syndrome, incontinentia pigmenti type 2, and Aicardi syndrome, are usually fatal in males either in utero or shortly after birth, and are therefore predominantly seen in females. Exceptions to this finding are extremely rare cases in which boys with Klinefelter syndrome (44+xxy) also inherit an X-linked dominant condition and exhibit symptoms more similar to those of a female in terms of disease severity. The chance of passing on an X-linked dominant disorder differs between men and women. The sons of a man with an X-linked dominant disorder will all be unaffected (since they receive their father's Y chromosome), but his daughters will all inherit the condition. A woman with an X-linked dominant disorder has a 50% chance of having an affected fetus with each pregnancy, although in cases such as incontinentia pigmenti, only female offspring are generally viable.

X-linked recessive

Main article: X-linked recessive inheritance

X-linked recessive conditions are also caused by mutations in genes on the X chromosome. Males are much more frequently affected than females, because they only have the one X chromosome necessary for the condition to present. The chance of passing on the disorder differs between men and women. The sons of a man with an X-linked recessive disorder will not be affected (since they receive their father's Y chromosome), but his daughters will be carriers of one copy of the mutated gene. A woman who is a carrier of an X-linked recessive disorder (XRXr) has a 50% chance of having sons who are affected and a 50% chance of having daughters who are carriers of one copy of the mutated gene. X-linked recessive conditions include the serious diseases hemophilia A, Duchenne muscular dystrophy, and Lesch–Nyhan syndrome, as well as common and less serious conditions such as male pattern baldness and red–green color blindness. X-linked recessive conditions can sometimes manifest in females due to skewed X-inactivation or monosomy X (Turner syndrome).[citation needed]

Y-linked

Main article: Y linkage

Y-linked disorders are caused by mutations on the Y chromosome. These conditions may only be transmitted from the heterogametic sex (e.g. male humans) to offspring of the same sex. More simply, this means that Y-linked disorders in humans can only be passed from men to their sons; females can never be affected because they do not possess Y-allosomes.[citation needed]

Y-linked disorders are exceedingly rare but the most well-known examples typically cause infertility. Reproduction in such conditions is only possible through the circumvention of infertility by medical intervention.

Mitochondrial

Main articles: Mitochondrial disease and Mitochondrial DNA

This type of inheritance, also known as maternal inheritance, is the rarest and applies to the 13 genes encoded by mitochondrial DNA. Because only egg cells contribute mitochondria to the developing embryo, only mothers (who are affected) can pass on mitochondrial DNA conditions to their children. An example of this type of disorder is Leber's hereditary optic neuropathy.[citation needed]

It is important to stress that the vast majority of mitochondrial diseases (particularly when symptoms develop in early life) are actually caused by a nuclear gene defect, as the mitochondria are mostly developed by non-mitochondrial DNA. These diseases most often follow autosomal recessive inheritance.[30]

Multifactorial disorder

Main article: Multifactorial disease

Genetic disorders may also be complex, multifactorial, or polygenic, meaning they are likely associated with the effects of multiple genes in combination with lifestyles and environmental factors. Multifactorial disorders include heart disease and diabetes. Although complex disorders often cluster in families, they do not have a clear-cut pattern of inheritance. This makes it difficult to determine a person's risk of inheriting or passing on these disorders. Complex disorders are also difficult to study and treat because the specific factors that cause most of these disorders have not yet been identified. Studies that aim to identify the cause of complex disorders can use several methodological approaches to determine genotypephenotype associations. One method, the genotype-first approach, starts by identifying genetic variants within patients and then determining the associated clinical manifestations. This is opposed to the more traditional phenotype-first approach, and may identify causal factors that have previously been obscured by clinical heterogeneity, penetrance, and expressivity.[citation needed]

On a pedigree, polygenic diseases do tend to "run in families", but the inheritance does not fit simple patterns as with Mendelian diseases. This does not mean that the genes cannot eventually be located and studied. There is also a strong environmental component to many of them (e.g., blood pressure). Other factors include:

Chromosomal disorder

See also: Chromosome abnormality
 
Chromosomes in Down syndrome, the most common human condition due to aneuploidy. There are three chromosomes 21 (in the last row).

A chromosomal disorder is a missing, extra, or irregular portion of chromosomal DNA. It can be from an atypical number of chromosomes or a structural abnormality in one or more chromosomes. An example of these disorders is trisomy 21 (Down syndrome), in which there is an extra copy of chromosome 21.[citation needed]

Diagnosis

Due to the wide range of genetic disorders that are known, diagnosis is widely varied and dependent of the disorder. Most genetic disorders are diagnosed pre-birth, at birth, or during early childhood however some, such as Huntington's disease, can escape detection until the patient is well into adulthood.[citation needed]

The basic aspects of a genetic disorder rests on the inheritance of genetic material. With an in depth family history, it is possible to anticipate possible disorders in children which direct medical professionals to specific tests depending on the disorder and allow parents the chance to prepare for potential lifestyle changes, anticipate the possibility of stillbirth, or contemplate termination.[31] Prenatal diagnosis can detect the presence of characteristic abnormalities in fetal development through ultrasound, or detect the presence of characteristic substances via invasive procedures which involve inserting probes or needles into the uterus such as in amniocentesis.[32]

Prognosis

Not all genetic disorders directly result in death; however, there are no known cures for genetic disorders. Many genetic disorders affect stages of development, such as Down syndrome, while others result in purely physical symptoms such as muscular dystrophy. Other disorders, such as Huntington's disease, show no signs until adulthood. During the active time of a genetic disorder, patients mostly rely on maintaining or slowing the degradation of quality of life and maintain patient autonomy. This includes physical therapy and pain management.

Treatment

 
From personal genomics to gene therapy
See also: Gene therapy

The treatment of genetic disorders is an ongoing battle, with over 1,800 gene therapy clinical trials having been completed, are ongoing, or have been approved worldwide.[33] Despite this, most treatment options revolve around treating the symptoms of the disorders in an attempt to improve patient quality of life.

Gene therapy refers to a form of treatment where a healthy gene is introduced to a patient. This should alleviate the defect caused by a faulty gene or slow the progression of the disease. A major obstacle has been the delivery of genes to the appropriate cell, tissue, and organ affected by the disorder. Researchers have investigated how they can introduce a gene into the potentially trillions of cells that carry the defective copy. Finding an answer to this has been a roadblock between understanding the genetic disorder and correcting the genetic disorder.[34]

Epidemiology

Around 1 in 50 people are affected by a known single-gene disorder, while around 1 in 263 are affected by a chromosomal disorder.[7] Around 65% of people have some kind of health problem as a result of congenital genetic mutations.[7] Due to the significantly large number of genetic disorders, approximately 1 in 21 people are affected by a genetic disorder classified as "rare" (usually defined as affecting less than 1 in 2,000 people). Most genetic disorders are rare in themselves.[5][8] There are well over 6,000 known genetic disorders,[4] and new genetic disorders are constantly being described in medical literature.[5]

History

The earliest known genetic condition in a hominid was in the fossil species Paranthropus robustus, with over a third of individuals displaying amelogenesis imperfecta.[35]

See also

References

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  17. ^ Swanson, Kate (2021-09-07). "Autosomal recessive polycystic kidney disease". American Journal of Obstetrics and Gynecology. Elsevier BV. 225 (5): B7–B8. doi:10.1016/j.ajog.2021.06.038. ISSN 0002-9378. PMID 34507795. S2CID 237480065.
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  32. ^ . Harvard Medical School. Archived from the original on 2008-05-16. Retrieved 2008-07-15.
  33. ^ Ginn, Samantha L.; Alexander, Ian E.; Edelstein, Michael L.; Abedi, Mohammad R.; Wixon, Jo (February 2013). "Gene therapy clinical trials worldwide to 2012 – an update". The Journal of Gene Medicine. 15 (2): 65–77. doi:10.1002/jgm.2698. PMID 23355455. S2CID 37123019.
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  35. ^ Towle, Ian; Irish, Joel D. (April 2019). "A probable genetic origin for pitting enamel hypoplasia on the molars of Paranthropus robustus" (PDF). Journal of Human Evolution. 129: 54–61. doi:10.1016/j.jhevol.2019.01.002. PMID 30904040. S2CID 85502058.

External links

  • Public Health Genomics at CDC
  • OMIM — Online Mendelian Inheritance in Man, a catalog of human genes and genetic disorders
  • Office of Rare Diseases (ORD), National Institutes of Health (NIH)
  • CDC’s National Center on Birth Defects and Developmental Disabilities
  • Global Genes Project, Genetic and Rare Diseases Organization
  • List of Genetic Disorders - Genome.gov

March 28, 2023
genetic, disorder, technical, introduction, topic, introduction, genetics, list, genetic, disorders, list, genetic, disorders, genetic, disorder, health, problem, caused, more, abnormalities, genome, caused, mutation, single, gene, monogenic, multiple, genes, . For a non technical introduction to the topic see Introduction to genetics For a list of genetic disorders see List of genetic disorders A genetic disorder is a health problem caused by one or more abnormalities in the genome It can be caused by a mutation in a single gene monogenic or multiple genes polygenic or by a chromosomal abnormality Although polygenic disorders are the most common the term is mostly used when discussing disorders with a single genetic cause either in a gene or chromosome 1 2 The mutation responsible can occur spontaneously before embryonic development a de novo mutation or it can be inherited from two parents who are carriers of a faulty gene autosomal recessive inheritance or from a parent with the disorder autosomal dominant inheritance When the genetic disorder is inherited from one or both parents it is also classified as a hereditary disease Some disorders are caused by a mutation on the X chromosome and have X linked inheritance Very few disorders are inherited on the Y chromosome or mitochondrial DNA due to their size 3 Genetic disorderA boy with Down syndrome one of the most common genetic disordersSpecialtyMedical geneticsDiagram featuring examples of a disease located on each chromosome There are well over 6 000 known genetic disorders 4 and new genetic disorders are constantly being described in medical literature 5 More than 600 genetic disorders are treatable 6 Around 1 in 50 people are affected by a known single gene disorder while around 1 in 263 are affected by a chromosomal disorder 7 Around 65 of people have some kind of health problem as a result of congenital genetic mutations 7 Due to the significantly large number of genetic disorders approximately 1 in 21 people are affected by a genetic disorder classified as rare usually defined as affecting less than 1 in 2 000 people Most genetic disorders are rare in themselves 5 8 Genetic disorders are present before birth and some genetic disorders produce birth defects but birth defects can also be developmental rather than hereditary The opposite of a hereditary disease is an acquired disease Most cancers although they involve genetic mutations to a small proportion of cells in the body are acquired diseases Some cancer syndromes however such as BRCA mutations are hereditary genetic disorders 9 Contents 1 Single gene 1 1 Autosomal dominant 1 2 Autosomal recessive 1 3 X linked dominant 1 4 X linked recessive 1 5 Y linked 1 6 Mitochondrial 2 Multifactorial disorder 3 Chromosomal disorder 4 Diagnosis 5 Prognosis 6 Treatment 7 Epidemiology 8 History 9 See also 10 References 11 External linksSingle gene EditPrevalence of some single gene disorders 10 Disorder prevalence approximate Autosomal dominantFamilial hypercholesterolemia 1 in 500 11 Myotonic dystrophy type 1 1 in 2 100 12 Neurofibromatosis type I 1 in 2 500 13 Hereditary spherocytosis 1 in 5 000Marfan syndrome 1 in 4 000 14 Huntington s disease 1 in 15 000 15 Autosomal recessiveSickle cell anaemia 1 in 625 16 Cystic fibrosis 1 in 2 000Tay Sachs disease 1 in 3 000Phenylketonuria 1 in 12 000Autosomal recessive polycystic kidney disease 1 in 20 000 17 Mucopolysaccharidoses 1 in 25 000Lysosomal acid lipase deficiency 1 in 40 000Glycogen storage diseases 1 in 50 000Galactosemia 1 in 57 000X linkedDuchenne muscular dystrophy 1 in 5 000Hemophilia 1 in 10 000Values are for liveborn infantsSee also Oligogenic inheritance and Polygenic inheritance A single gene disorder or monogenic disorder is the result of a single mutated gene Single gene disorders can be passed on to subsequent generations in several ways Genomic imprinting and uniparental disomy however may affect inheritance patterns The divisions between recessive and dominant types are not hard and fast although the divisions between autosomal and X linked types are since the latter types are distinguished purely based on the chromosomal location of the gene For example the common form of dwarfism achondroplasia is typically considered a dominant disorder but children with two genes for achondroplasia have a severe and usually lethal skeletal disorder one that achondroplasics could be considered carriers for Sickle cell anemia is also considered a recessive condition but heterozygous carriers have increased resistance to malaria in early childhood which could be described as a related dominant condition 18 When a couple where one partner or both are affected or carriers of a single gene disorder wish to have a child they can do so through in vitro fertilization which enables preimplantation genetic diagnosis to occur to check whether the embryo has the genetic disorder 19 Most congenital metabolic disorders known as inborn errors of metabolism result from single gene defects Many such single gene defects can decrease the fitness of affected people and are therefore present in the population in lower frequencies compared to what would be expected based on simple probabilistic calculations 20 Autosomal dominant Edit Main article Autosomal dominant Autosomal dominant gene Only one mutated copy of the gene will be necessary for a person to be affected by an autosomal dominant disorder Each affected person usually has one affected parent 21 57 The chance a child will inherit the mutated gene is 50 Autosomal dominant conditions sometimes have reduced penetrance which means although only one mutated copy is needed not all individuals who inherit that mutation go on to develop the disease Examples of this type of disorder are Huntington s disease 21 58 neurofibromatosis type 1 neurofibromatosis type 2 Marfan syndrome hereditary nonpolyposis colorectal cancer hereditary multiple exostoses a highly penetrant autosomal dominant disorder tuberous sclerosis Von Willebrand disease and acute intermittent porphyria Birth defects are also called congenital anomalies citation needed Autosomal recessive Edit Main article Autosomal dominant Autosomal recessive allele Two copies of the gene must be mutated for a person to be affected by an autosomal recessive disorder An affected person usually has unaffected parents who each carry a single copy of the mutated gene and are referred to as genetic carriers Each parent with a defective gene normally do not have symptoms 22 Two unaffected people who each carry one copy of the mutated gene have a 25 risk with each pregnancy of having a child affected by the disorder Examples of this type of disorder are albinism medium chain acyl CoA dehydrogenase deficiency cystic fibrosis sickle cell disease Tay Sachs disease Niemann Pick disease spinal muscular atrophy and Roberts syndrome Certain other phenotypes such as wet versus dry earwax are also determined in an autosomal recessive fashion 23 24 Some autosomal recessive disorders are common because in the past carrying one of the faulty genes led to a slight protection against an infectious disease or toxin such as tuberculosis or malaria 25 Such disorders include cystic fibrosis 26 sickle cell disease 27 phenylketonuria 28 and thalassaemia 29 Hereditary defects in enzymes are generally inherited in an autosomal fashion because there are more non X chromosomes than X chromosomes and a recessive fashion because the enzymes from the unaffected genes are generally sufficient to prevent symptoms in carriers On the other hand hereditary defects in structural proteins such as osteogenesis imperfecta Marfan s syndrome and many Ehlers Danlos syndromes are generally autosomal dominant because it is enough that some components are defective to make the whole structure dysfunctional This is a dominant negative process wherein a mutated gene product adversely affects the non mutated gene product within the same cell X linked dominant Edit Schematic karyogram showing an overview of the human genome It shows annotated bands and sub bands as used in the nomenclature of genetic disorders It shows 22 homologous chromosomes both the female XX and male XY versions of the sex chromosome bottom right as well as the mitochondrial genome to scale at bottom left citation needed Further information Karyotype Main article X linked dominant X linked dominant disorders are caused by mutations in genes on the X chromosome Only a few disorders have this inheritance pattern with a prime example being X linked hypophosphatemic rickets Males and females are both affected in these disorders with males typically being more severely affected than females Some X linked dominant conditions such as Rett syndrome incontinentia pigmenti type 2 and Aicardi syndrome are usually fatal in males either in utero or shortly after birth and are therefore predominantly seen in females Exceptions to this finding are extremely rare cases in which boys with Klinefelter syndrome 44 xxy also inherit an X linked dominant condition and exhibit symptoms more similar to those of a female in terms of disease severity The chance of passing on an X linked dominant disorder differs between men and women The sons of a man with an X linked dominant disorder will all be unaffected since they receive their father s Y chromosome but his daughters will all inherit the condition A woman with an X linked dominant disorder has a 50 chance of having an affected fetus with each pregnancy although in cases such as incontinentia pigmenti only female offspring are generally viable X linked recessive Edit Main article X linked recessive inheritance X linked recessive conditions are also caused by mutations in genes on the X chromosome Males are much more frequently affected than females because they only have the one X chromosome necessary for the condition to present The chance of passing on the disorder differs between men and women The sons of a man with an X linked recessive disorder will not be affected since they receive their father s Y chromosome but his daughters will be carriers of one copy of the mutated gene A woman who is a carrier of an X linked recessive disorder XRXr has a 50 chance of having sons who are affected and a 50 chance of having daughters who are carriers of one copy of the mutated gene X linked recessive conditions include the serious diseases hemophilia A Duchenne muscular dystrophy and Lesch Nyhan syndrome as well as common and less serious conditions such as male pattern baldness and red green color blindness X linked recessive conditions can sometimes manifest in females due to skewed X inactivation or monosomy X Turner syndrome citation needed Y linked Edit Main article Y linkage Y linked disorders are caused by mutations on the Y chromosome These conditions may only be transmitted from the heterogametic sex e g male humans to offspring of the same sex More simply this means that Y linked disorders in humans can only be passed from men to their sons females can never be affected because they do not possess Y allosomes citation needed Y linked disorders are exceedingly rare but the most well known examples typically cause infertility Reproduction in such conditions is only possible through the circumvention of infertility by medical intervention Mitochondrial Edit Main articles Mitochondrial disease and Mitochondrial DNA This type of inheritance also known as maternal inheritance is the rarest and applies to the 13 genes encoded by mitochondrial DNA Because only egg cells contribute mitochondria to the developing embryo only mothers who are affected can pass on mitochondrial DNA conditions to their children An example of this type of disorder is Leber s hereditary optic neuropathy citation needed It is important to stress that the vast majority of mitochondrial diseases particularly when symptoms develop in early life are actually caused by a nuclear gene defect as the mitochondria are mostly developed by non mitochondrial DNA These diseases most often follow autosomal recessive inheritance 30 Multifactorial disorder EditMain article Multifactorial disease Genetic disorders may also be complex multifactorial or polygenic meaning they are likely associated with the effects of multiple genes in combination with lifestyles and environmental factors Multifactorial disorders include heart disease and diabetes Although complex disorders often cluster in families they do not have a clear cut pattern of inheritance This makes it difficult to determine a person s risk of inheriting or passing on these disorders Complex disorders are also difficult to study and treat because the specific factors that cause most of these disorders have not yet been identified Studies that aim to identify the cause of complex disorders can use several methodological approaches to determine genotype phenotype associations One method the genotype first approach starts by identifying genetic variants within patients and then determining the associated clinical manifestations This is opposed to the more traditional phenotype first approach and may identify causal factors that have previously been obscured by clinical heterogeneity penetrance and expressivity citation needed On a pedigree polygenic diseases do tend to run in families but the inheritance does not fit simple patterns as with Mendelian diseases This does not mean that the genes cannot eventually be located and studied There is also a strong environmental component to many of them e g blood pressure Other factors include asthma autoimmune diseases such as multiple sclerosis cancers ciliopathies cleft palate diabetes heart disease hypertension inflammatory bowel disease intellectual disability mood disorder obesity refractive error infertilityChromosomal disorder EditSee also Chromosome abnormality Chromosomes in Down syndrome the most common human condition due to aneuploidy There are three chromosomes 21 in the last row A chromosomal disorder is a missing extra or irregular portion of chromosomal DNA It can be from an atypical number of chromosomes or a structural abnormality in one or more chromosomes An example of these disorders is trisomy 21 Down syndrome in which there is an extra copy of chromosome 21 citation needed Diagnosis EditDue to the wide range of genetic disorders that are known diagnosis is widely varied and dependent of the disorder Most genetic disorders are diagnosed pre birth at birth or during early childhood however some such as Huntington s disease can escape detection until the patient is well into adulthood citation needed The basic aspects of a genetic disorder rests on the inheritance of genetic material With an in depth family history it is possible to anticipate possible disorders in children which direct medical professionals to specific tests depending on the disorder and allow parents the chance to prepare for potential lifestyle changes anticipate the possibility of stillbirth or contemplate termination 31 Prenatal diagnosis can detect the presence of characteristic abnormalities in fetal development through ultrasound or detect the presence of characteristic substances via invasive procedures which involve inserting probes or needles into the uterus such as in amniocentesis 32 Prognosis EditNot all genetic disorders directly result in death however there are no known cures for genetic disorders Many genetic disorders affect stages of development such as Down syndrome while others result in purely physical symptoms such as muscular dystrophy Other disorders such as Huntington s disease show no signs until adulthood During the active time of a genetic disorder patients mostly rely on maintaining or slowing the degradation of quality of life and maintain patient autonomy This includes physical therapy and pain management Treatment Edit From personal genomics to gene therapy See also Gene therapyThe treatment of genetic disorders is an ongoing battle with over 1 800 gene therapy clinical trials having been completed are ongoing or have been approved worldwide 33 Despite this most treatment options revolve around treating the symptoms of the disorders in an attempt to improve patient quality of life Gene therapy refers to a form of treatment where a healthy gene is introduced to a patient This should alleviate the defect caused by a faulty gene or slow the progression of the disease A major obstacle has been the delivery of genes to the appropriate cell tissue and organ affected by the disorder Researchers have investigated how they can introduce a gene into the potentially trillions of cells that carry the defective copy Finding an answer to this has been a roadblock between understanding the genetic disorder and correcting the genetic disorder 34 Epidemiology EditAround 1 in 50 people are affected by a known single gene disorder while around 1 in 263 are affected by a chromosomal disorder 7 Around 65 of people have some kind of health problem as a result of congenital genetic mutations 7 Due to the significantly large number of genetic disorders approximately 1 in 21 people are affected by a genetic disorder classified as rare usually defined as affecting less than 1 in 2 000 people Most genetic disorders are rare in themselves 5 8 There are well over 6 000 known genetic disorders 4 and new genetic disorders are constantly being described in medical literature 5 History EditThe earliest known genetic condition in a hominid was in the fossil species Paranthropus robustus with over a third of individuals displaying amelogenesis imperfecta 35 See also EditFINDbase the Frequency of Inherited Disorders database Genetic epidemiology List of genetic disorders Population groups in biomedicine Mendelian errorReferences Edit Genetic Disorders Learn Genetics University of Utah Lvovs D Favorova O O Favorov A V 2012 A Polygenic Approach to the Study of Polygenic Diseases Acta Naturae 4 3 59 71 doi 10 32607 20758251 2012 4 3 59 71 ISSN 2075 8251 PMC 3491892 PMID 23150804 Reference Genetics Home What are the different ways in which a genetic condition can be inherited Genetics Home Reference Retrieved 2020 01 14 a b OMIM Gene Map Statistics www omim org Retrieved 2020 01 14 a b c d Orphanet About rare diseases www orpha net Retrieved 2020 01 14 Bick David Bick Sarah L Dimmock David P Fowler Tom A Caulfield Mark J Scott Richard H March 2021 An online compendium of treatable genetic disorders American Journal of Medical Genetics Part C Seminars in Medical Genetics 187 1 48 54 doi 10 1002 ajmg c 31874 ISSN 1552 4876 PMC 7986124 PMID 33350578 a b c d Kumar Pankaj Radhakrishnan Jolly Chowdhary Maksud A Giampietro Philip F 2001 08 01 Prevalence and Patterns of Presentation of Genetic Disorders in a Pediatric Emergency Department Mayo Clinic Proceedings 76 8 777 783 doi 10 4065 76 8 777 ISSN 0025 6196 PMID 11499815 a b Jackson Maria Marks Leah May Gerhard H W Wilson Joanna B 2018 12 03 The genetic basis of disease Essays in Biochemistry 62 5 643 723 doi 10 1042 EBC20170053 ISSN 0071 1365 PMC 6279436 PMID 30509934 calculated from 1 in 17 rare disorders and 80 of rare disorders being genetic Hunt Jay D An Introduction to Cancer Genetics and Louisiana Families lsuhsc edu Archived from the original on 16 January 2020 Prevalence and incidence of rare diseases PDF Archived PDF from the original on 2008 11 18 OMIM Entry 144010 HYPERCHOLESTEROLEMIA FAMILIAL 2 FCHL2 www omim org Retrieved 2019 07 01 Johnson Nicholas E Butterfield Russell J Mayne Katie Newcomb Tara Imburgia Carina Dunn Diane Duval Brett Feldkamp Marcia L Weiss Robert B 2021 Population Based Prevalence of Myotonic Dystrophy Type 1 Using Genetic Analysis of State wide Blood Screening Program Neurology 96 7 e1045 e1053 doi 10 1212 WNL 0000000000011425 PMC 8055332 PMID 33472919 OMIM Entry 162200 NEUROFIBROMATOSIS TYPE I NF1 www omim org Retrieved 2019 07 01 Keane MG Pyeritz RE May 2008 Medical management of Marfan syndrome Circulation 117 21 2802 13 doi 10 1161 CIRCULATIONAHA 107 693523 PMID 18506019 Walker FO 2007 Huntington s disease Lancet 369 9557 218 28 221 doi 10 1016 S0140 6736 07 60111 1 PMID 17240289 S2CID 46151626 OMIM Entry 603903 SICKLE CELL ANEMIA www omim org Retrieved 2019 07 01 Swanson Kate 2021 09 07 Autosomal recessive polycystic kidney disease American Journal of Obstetrics and Gynecology Elsevier BV 225 5 B7 B8 doi 10 1016 j ajog 2021 06 038 ISSN 0002 9378 PMID 34507795 S2CID 237480065 Williams T N Obaro S K 2011 Sickle cell disease and malaria morbidity a tale with two tails Trends in Parasitology 27 7 315 320 doi 10 1016 j pt 2011 02 004 PMID 21429801 Kuliev Anver Verlinsky Yury 2005 Preimplantation diagnosis A realistic option for assisted reproduction and genetic practice Curr Opin Obstet Gynecol 17 2 179 83 doi 10 1097 01 gco 0000162189 76349 c5 PMID 15758612 S2CID 9382420 Simcikova D Heneberg P December 2019 Refinement of evolutionary medicine predictions based on clinical evidence for the manifestations of Mendelian diseases Scientific Reports 9 1 18577 Bibcode 2019NatSR 918577S doi 10 1038 s41598 019 54976 4 PMC 6901466 PMID 31819097 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint uses authors parameter link a b Griffiths Anthony J F Wessler Susan R Carroll Sean B Doebley John 2012 2 Single Gene Inheritance Introduction to Genetic Analysis 10th ed New York W H Freeman and Company ISBN 978 1 4292 2943 2 Inheritance Patterns for Single Gene Disorders learn genetics utah edu Retrieved 2019 07 01 Wade Nicholas 29 January 2006 Japanese Scientists Identify Ear Wax Gene The New York Times Yoshiura K Kinoshita A Ishida T et al March 2006 A SNP in the ABCC11 gene is the determinant of human earwax type Nat Genet 38 3 324 30 doi 10 1038 ng1733 PMID 16444273 S2CID 3201966 Mitton Jeffry B 2002 Heterozygous Advantage eLS doi 10 1038 npg els 0001760 ISBN 978 0 470 01617 6 Poolman EM Galvani AP February 2007 Evaluating candidate agents of selective pressure for cystic fibrosis Journal of the Royal Society Interface 4 12 91 8 doi 10 1098 rsif 2006 0154 PMC 2358959 PMID 17015291 Allison AC October 2009 Genetic control of resistance to human malaria Current Opinion in Immunology 21 5 499 505 doi 10 1016 j coi 2009 04 001 PMID 19442502 Woolf LI 1986 The heterozygote advantage in phenylketonuria American Journal of Human Genetics 38 5 773 5 PMC 1684820 PMID 3717163 Weatherall D J 2015 The Thalassemias Disorders of Globin Synthesis Williams Hematology 9e ed McGraw Hill Professional p 725 ISBN 9780071833011 Nussbaum Robert McInnes Roderick Willard Huntington 2007 Thompson amp Thompson Genetics in Medicine Philadelphia PA Saunders pp 144 145 146 ISBN 9781416030805 Milunsky Aubrey Milunsky Jeff M 2021 Genetic Counseling Preconception Prenatal and Perinatal Genetic Disorders and the Fetus pp 1 101 doi 10 1002 9781119676980 ch1 ISBN 978 1 119 67698 0 Diagnostic Tests Amniocentesis Harvard Medical School Archived from the original on 2008 05 16 Retrieved 2008 07 15 Ginn Samantha L Alexander Ian E Edelstein Michael L Abedi Mohammad R Wixon Jo February 2013 Gene therapy clinical trials worldwide to 2012 an update The Journal of Gene Medicine 15 2 65 77 doi 10 1002 jgm 2698 PMID 23355455 S2CID 37123019 Verma I M 22 August 2013 Gene Therapy That Works Science 341 6148 853 855 Bibcode 2013Sci 341 853V doi 10 1126 science 1242551 PMID 23970689 S2CID 206550787 Towle Ian Irish Joel D April 2019 A probable genetic origin for pitting enamel hypoplasia on the molars of Paranthropus robustus PDF Journal of Human Evolution 129 54 61 doi 10 1016 j jhevol 2019 01 002 PMID 30904040 S2CID 85502058 External links EditPublic Health Genomics at CDC OMIM Online Mendelian Inheritance in Man a catalog of human genes and genetic disorders Genetic and Rare Diseases Information Center GARD Office of Rare Diseases ORD National Institutes of Health NIH CDC s National Center on Birth Defects and Developmental Disabilities Genetic Disease Information from the Human Genome Project Global Genes Project Genetic and Rare Diseases Organization List of Genetic Disorders Genome gov Retrieved from https en wikipedia org w index php title Genetic disorder amp oldid 1144622759, wikipedia, 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