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Ansuvimab

January 01, 1970

Ansuvimab, sold under the brand name Ebanga, is a monoclonal antibody medication for the treatment of Zaire ebolavirus (Ebolavirus) infection.[1][2]

Ansuvimab
Monoclonal antibody
TypeWhole antibody
SourceHuman
TargetZaire ebolavirus
Clinical data
Trade namesEbanga
Other namesAnsuvimab-zykl, mAb114
License data
Routes of
administration		Intravenous
Drug classMonoclonal antibody
ATC code
Legal status
Legal status
Identifiers
CAS Number
  • 2375952-29-5
DrugBank
  • DB16385
UNII
  • TG8IQ19NG2
KEGG
  • D11875
Chemical and physical data
FormulaC6368H9924N1724O1994S44
Molar mass143950.15 g·mol−1

The most common symptoms include fever, tachycardia (fast heart rate), diarrhea, vomiting, hypotension (low blood pressure), tachypnea (fast breathing) and chills; however, these are also common symptoms of Ebolavirus infection.[1]

Ansuvimab was approved for medical use in the United States in December 2020.[1][2][3] It is on the World Health Organization's List of Essential Medicines.[4]

Chemistry edit

The drug is composed of a single monoclonal antibody (mAb) and was initially isolated from immortalized B-cells that were obtained from a survivor of the 1995 outbreak of Ebola virus disease in Kikwit, Democratic Republic of Congo.[5] In work supported by the United States National Institutes of Health and the Defense Advanced Projects Agency, the heavy and light chain sequences of ansuvimab mAb was cloned into CHO cell lines and initial production runs were produced by Cook Phamica d.b.a. Catalent under contract of Medimmune.[6][7]

Mechanism of action edit

Neutralization edit

Ansuvimab is a monoclonal antibody therapy that is infused intravenously into patients with Ebola virus disease. Ansuvimab is a neutralizing antibody,[5] meaning it binds to a protein on the surface of Ebola virus that is required to infect cells. Specifically, ansuvimab neutralizes infection by binding to a region of the Ebola virus envelope glycoprotein that, in the absence of ansuvimab, would interact with virus's cell receptor protein, Niemann-Pick C1 (NPC1).[8][9][10] This "competition" by ansuvimab prevents Ebola virus from binding to NPC1 and "neutralizes" the virus's ability to infect the targeted cell.[8]

Effector function edit

Antibodies have antigen-binding fragment (Fab) regions and constant fragment (Fc) regions. The Neutralization of virus infection occurs when the Fab regions of antibodies binds to virus antigen(s) in a manner that blocks infection. Antibodies are also able to "kill" virus particles directly and/or kill infected cells using antibody-mediated "effector functions" such as opsonization, complement-dependent cytotoxicity, antibody-dependent cell-mediated cytotoxicity and antibody-dependent phagocytosis. These effector functions are contained in the Fc region of antibodies, but is also dependent on binding of the Fab region to antigen. Effector functions also require the use of complement proteins in serum or Fc-receptor on cell membranes. Ansuvimab has been found to be capable of killing cells by antibody-dependent cell-mediated cytotoxicity.[5] Other functional killing tests have not been performed.[citation needed]

History edit

Ansuvimab is a monoclonal antibody that is being evaluated as a treatment for Ebola virus disease.[11] Its discovery was led by the laboratory of Nancy Sullivan at the United States National Institutes of Health Vaccine Research Center and J. J. Muyembe-Tamfum from the Institut National pour la Recherche Biomedicale (INRB) in the Democratic Republic of Congo, working in collaboration with the Institute for Research in Biomedicine (IRB) (Bellinzona, Switzerland) and the United States Army Medical Research Institute of Infectious Diseases.[5][12] Ansuvimab was isolated from the blood of a survivor of the 1995 outbreak of Ebola virus disease in Kikwit, Democratic Republic of Congo roughly ten years later.[5]

In 2018, a Phase 1 clinical trial of ansuvimab was conducted by Martin Gaudinski within the Vaccine Research Center Clinical Trials Program that is led by Julie E. Ledgerwood.[7][6][13] Ansuvimab is also being evaluated during the 2018 North Kivu Ebola outbreak.[14]

Ansuvimab has also shown success with lowering the mortality rate from ~70% to about 34%. In August 2019, Congolese health authorities, the World Health Organization, and the U.S. National Institutes of Health promoted the use of ansuvimab, alongside atoltivimab/maftivimab/odesivimab, a similar Regeneron-produced monoclonal antibody treatment, over other treatments yielding higher mortality rates, after ending clinical trials during the outbreak.[15][16]

The U.S. Food and Drug Administration (FDA) approved ansuvimab based primarily on evidence from a clinical trial (Trial 1/ NCT NCT03719586) of 342 participants with Zaire ebolavirus infection.[3] The trial enrolled newborn, pediatric and adult participants (including pregnant women) with Zaire ebolavirus infection.[3] All participants received standard, supportive care for the disease.[3] In addition to the standard care, participants were randomly assigned to receive either a one-time dose of ansuvimab or one of the three other types of experimental treatments (including one as the control group).[3] The participants and the health care providers knew which treatment was being given.[3] The trial was conducted at four sites in the Democratic Republic of Congo during an outbreak that began in August 2018.[3]

Discovery edit

A 2016 paper describes the efforts of how ansuvimab was originally developed as part of research efforts led by Dr. Nancy Sullivan at the United States National Institutes of Health Vaccine Research Center and Dr. J. J. Muyembe-Tamfum from the Institut National de Recherche Biomedicale (INRB) in the Democratic Republic of Congo.[5][12] This collaborative effort also involved researchers from Institute of Biomedical Research and the United States Army Medical Research Institute of Infectious Diseases.[5][12] A survivor from the 1995 outbreak of Ebola virus disease in Kikwit, Democratic Republic of Congo donated blood to the project that began roughly ten years after they had recovered.[5] Memory B cells isolated from the survivor's blood were immortalized, cultured and screened for their ability to produce monoclonal antibodies that reacted with the glycoprotein of Ebola virus. Ansuvimab was identified from one of these cultures and the antibody heavy and light chain gene sequences were sequenced from the cells.[5] These sequences were then cloned into recombinant DNA plasmids and purified antibody protein for initial studies was produced in cells derived from HEK 293 cells.[5]

Ansuvimab and mAb100 combination edit

In an experiment described in the 2016 paper, rhesus macaques were infected with Ebola virus and treated with a combination of ansuvimab and another antibody isolated from the same subject, mAb100. Three doses of the combination were given once a day starting 1 day after the animals were infected. The control animal died and the treated animals all survived.[5]

Ansuvimab monotherapy edit

In a second experiment described in the 2016 paper, rhesus macaques were infected with Ebola virus and only treated with ansuvimab. Three doses of ansuvimab were given once a day starting 1 day or 5 days after the animals were infected. The control animals died and the treated animals all survived.[5] Unpublished data referred to in a publication of the 2018 Phase I clinical trial results of ansuvimab, reported that a single infusion of ansuvimab provided full protection of rhesus macaques and was the basis of the dosing used for human studies.[7][6]

Development edit

Ansuvimab was developed by the Vaccine Research Center with support of the United States National Institutes of Health and the Defense Advanced Projects Agency. The heavy and light chain sequences of ansuvimab mAb were cloned into CHO cell lines to enable large-scale production of antibody product for use in humans.[6][7]

Human safety testing edit

In early 2018,[11] a Phase 1 clinical trial of ansuvimab's safety, tolerability and pharmacokinetics was conducted by Dr. Martin Gaudinski within the Vaccine Research Center Clinical Trials Program that is led by Dr. Julie E. Ledgerwood.[7][6][13] The study was performed in the United States at the NIH Clinical Center and tested single dose infusions of ansuvimab infused over 30 minutes. The study showed that ansuvimab was safe, had minimal side effects and had a half-life of 24 days.[7][6]

Ridgeback Biotherapeutics edit

A license for ansuvimab was obtained by Ridgeback Biotherapeutics in 2018, from the National Institutes of Health-National Institute of Allergy and Infectious Diseases.[17] Ansuvimab was given orphan drug status in May 2019 and March 2020.[18][19][20]

Experimental use in the Democratic Republic of Congo edit

During the 2018 Équateur province Ebola outbreak, ansuvimab was requested by the Democratic Republic of Congo (DRC) Ministry of Public Health. Ansuvimab was approved for compassionate use by the World Health Organization MEURI ethical protocol and at DRC ethics board. Ansuvimab was sent along with other therapeutic agents to the outbreak sites.[21][22][13] However, the outbreak came to a conclusion before any therapeutic agents were given to patients.[13]

Approximately one month following the conclusion of the Équateur province outbreak, a distinct outbreak was noted in Kivu in the DRC (2018–20 Kivu Ebola outbreak). Once again, ansuvimab received approval for compassionate use by WHO MEURI and DRC ethic boards and has been given to many patients under these protocols.[13] In November 2018, the Pamoja Tulinde Maisha (PALM [together save lives]) open-label randomized clinical control trial was begun at multiple treatment units testing ansuvimab, atoltivimab/maftivimab/odesivimab (REGN-EB3) and remdesivir to ZMapp. Despite the difficulty of running a clinical trial in a conflict zone, investigators have enrolled 681 patients towards their goal of 725. An interim analysis by the Data Safety and Monitoring Board (DSMB) of the first 499 patient found that ansuvimab and REGN-EB3 were superior to the comparator ZMapp. Overall mortality of patients in the ZMapp and remdesivir groups were 49% and 53% compared to 34% and 29% for ansuvimab and REGN-EB3. When looking at patients who arrived early after disease symptoms appeared, survival was 89% for ansuvimab and 94% for REGN-EB3. While the study was not powered to determine whether there is any difference between REGN-EB3 and ansuvimab, the survival difference between those two therapies and ZMapp was significant. This led to the DSMB halting the study and PALM investigators dropping the remdesivir and ZMapp arms from the clinical trial. All patients in the outbreak who elect to participate in the trial will now be given either ansuvimab or REGN-EB3.[23][24][15][14]

In October 2020, the U.S. Food and Drug Administration (FDA) approved atoltivimab/maftivimab/odesivimab (Inmazeb, formerly REGN-EB3) with an indication for the treatment of infection caused by Zaire ebolavirus.[25]

References edit

  1. ^ a b c d "FDA Approves Treatment for Ebola Virus". U.S. Food and Drug Administration. 21 December 2020. Retrieved 23 December 2020.   This article incorporates text from this source, which is in the public domain.
  2. ^ a b "Ridgeback Biotherapeutics LP Announces the Approval of Ebanga for Ebola" (Press release). Ridgeback Biotherapeutics LP. 22 December 2020. Retrieved 23 December 2020 – via Business Wire.
  3. ^ a b c d e f g "Drug Trials Snapshot: Ebanga". U.S. Food and Drug Administration (FDA). 21 December 2020. Retrieved 13 January 2021.   This article incorporates text from this source, which is in the public domain.
  4. ^ World Health Organization (2023). The selection and use of essential medicines 2023: web annex A: World Health Organization model list of essential medicines: 23rd list (2023). Geneva: World Health Organization. hdl:10665/371090. WHO/MHP/HPS/EML/2023.02.
  5. ^ a b c d e f g h i j k l Corti D, Misasi J, Mulangu S, Stanley DA, Kanekiyo M, Wollen S, et al. (March 2016). "Protective monotherapy against lethal Ebola virus infection by a potently neutralizing antibody". Science. 351 (6279): 1339–42. Bibcode:2016Sci...351.1339C. doi:10.1126/science.aad5224. PMID 26917593.
  6. ^ a b c d e f Clinical trial number NCT03478891 for "Safety and Pharmacokinetics of a Human Monoclonal Antibody, VRC-EBOMAB092-00-AB (MAb114), Administered Intravenously to Healthy Adults" at ClinicalTrials.gov
  7. ^ a b c d e f Gaudinski MR, Coates EE, Novik L, Widge A, Houser KV, Burch E, et al. (March 2019). "Safety, tolerability, pharmacokinetics, and immunogenicity of the therapeutic monoclonal antibody ansuvimab targeting Ebola virus glycoprotein (VRC 608): an open-label phase 1 study". Lancet. 393 (10174): 889–898. doi:10.1016/S0140-6736(19)30036-4. PMC 6436835. PMID 30686586.
  8. ^ a b Misasi J, Gilman MS, Kanekiyo M, Gui M, Cagigi A, Mulangu S, et al. (March 2016). "Structural and molecular basis for Ebola virus neutralization by protective human antibodies". Science. 351 (6279): 1343–6. Bibcode:2016Sci...351.1343M. doi:10.1126/science.aad6117. PMC 5241105. PMID 26917592.
  9. ^ Côté M, Misasi J, Ren T, Bruchez A, Lee K, Filone CM, et al. (August 2011). "Small molecule inhibitors reveal Niemann-Pick C1 is essential for Ebola virus infection". Nature. 477 (7364): 344–8. Bibcode:2011Natur.477..344C. doi:10.1038/nature10380. PMC 3230319. PMID 21866101.
  10. ^ Carette JE, Raaben M, Wong AC, Herbert AS, Obernosterer G, Mulherkar N, et al. (August 2011). "Ebola virus entry requires the cholesterol transporter Niemann-Pick C1". Nature. 477 (7364): 340–3. Bibcode:2011Natur.477..340C. doi:10.1038/nature10348. PMC 3175325. PMID 21866103.
  11. ^ a b "NIH begins testing Ebola treatment in early-stage trial". National Institutes of Health (NIH). 2018-05-23. Retrieved 2018-10-15.
  12. ^ a b c Hayden EC (2016-02-26). "Ebola survivor's blood holds promise of new treatment". Nature. doi:10.1038/nature.2016.19440. ISSN 1476-4687. S2CID 211835755.
  13. ^ a b c d e "NIH VideoCast - CC Grand Rounds: Response to an Outbreak: Ebola Virus Monoclonal Antibody (mAb114) Rapid Clinical Development". videocast.nih.gov. 13 March 2019. Retrieved 2019-08-09.
  14. ^ a b Kingsley-Hall A. "Congo's experimental mAb114 Ebola treatment appears successful: authorities | Central Africa". www.theafricareport.com. Retrieved 2018-10-15.
  15. ^ a b McNeil DG (12 August 2019). "A Cure for Ebola? Two New Treatments Prove Highly Effective in Congo". The New York Times. Retrieved 13 August 2019.
  16. ^ Molteni M (12 August 2019). "Ebola is Now Curable. Here's How The New Treatments Work". Wired. Retrieved 13 August 2019.
  17. ^ "Ridgeback Biotherapeutics LP announces licensing of mAb114, an experimental Ebola treatment, from the National Institute of Allergy and Infectious Diseases" (Press release). Ridgeback Biotherapeutics LP. Retrieved 2019-08-17 – via PR Newswire.
  18. ^ "Ansuvimab Orphan Drug Designations and Approvals". accessdata.fda.gov. 8 May 2019. Retrieved 24 December 2020.
  19. ^ "Ansuvimab Orphan Drug Designations and Approvals". accessdata.fda.gov. 30 March 2020. Retrieved 24 December 2020.
  20. ^ "Ridgeback Biotherapeutics LP Announces Orphan Drug Designation for mAb114" (Press release). Ridgeback Biotherapeutics LP. Retrieved 2019-08-17 – via PR Newswire.
  21. ^ Check Hayden, Erika (May 2018). "Experimental drugs poised for use in Ebola outbreak". Nature. 557 (7706): 475–476. Bibcode:2018Natur.557..475C. doi:10.1038/d41586-018-05205-x. ISSN 0028-0836. PMID 29789732.
  22. ^ "WHO: Consultation on Monitored Emergency Use of Unregistered and Investigational Interventions for Ebola virus Disease" (PDF). who.int. World Health Organization. May 17, 2018. Retrieved November 2, 2021.
  23. ^ Mole B (2019-08-13). "Two Ebola drugs boost survival rates, according to early trial data". Ars Technica. Retrieved 2019-08-17.
  24. ^ "Independent monitoring board recommends early termination of Ebola therapeutics trial in DRC because of favorable results with two of four candidates". National Institutes of Health (NIH). 2019-08-12. Retrieved 2019-08-17.
  25. ^ "FDA Approves First Treatment for Ebola Virus". U.S. Food and Drug Administration (FDA) (Press release). 14 October 2020. Retrieved 14 October 2020.   This article incorporates text from this source, which is in the public domain.

External links edit

  • Clinical trial number NCT03719586 for "Investigational Therapeutics for the Treatment of People With Ebola Virus Disease" at ClinicalTrials.gov

January 01, 1970
ansuvimab, sold, under, brand, name, ebanga, monoclonal, antibody, medication, treatment, zaire, ebolavirus, ebolavirus, infection, monoclonal, antibodytypewhole, antibodysourcehumantargetzaire, ebolavirusclinical, datatrade, namesebangaother, names, zykl, mab. Ansuvimab sold under the brand name Ebanga is a monoclonal antibody medication for the treatment of Zaire ebolavirus Ebolavirus infection 1 2 AnsuvimabMonoclonal antibodyTypeWhole antibodySourceHumanTargetZaire ebolavirusClinical dataTrade namesEbangaOther namesAnsuvimab zykl mAb114License dataUS DailyMed AnsuvimabRoutes ofadministrationIntravenousDrug classMonoclonal antibodyATC codeJ06BD04 WHO Legal statusLegal statusUS only 1 IdentifiersCAS Number2375952 29 5DrugBankDB16385UNIITG8IQ19NG2KEGGD11875Chemical and physical dataFormulaC 6368H 9924N 1724O 1994S 44Molar mass143950 15 g mol 1 The most common symptoms include fever tachycardia fast heart rate diarrhea vomiting hypotension low blood pressure tachypnea fast breathing and chills however these are also common symptoms of Ebolavirus infection 1 Ansuvimab was approved for medical use in the United States in December 2020 1 2 3 It is on the World Health Organization s List of Essential Medicines 4 Contents 1 Chemistry 2 Mechanism of action 2 1 Neutralization 2 2 Effector function 3 History 3 1 Discovery 3 1 1 Ansuvimab and mAb100 combination 3 1 2 Ansuvimab monotherapy 3 2 Development 3 3 Human safety testing 3 4 Ridgeback Biotherapeutics 4 Experimental use in the Democratic Republic of Congo 5 References 6 External linksChemistry editThe drug is composed of a single monoclonal antibody mAb and was initially isolated from immortalized B cells that were obtained from a survivor of the 1995 outbreak of Ebola virus disease in Kikwit Democratic Republic of Congo 5 In work supported by the United States National Institutes of Health and the Defense Advanced Projects Agency the heavy and light chain sequences of ansuvimab mAb was cloned into CHO cell lines and initial production runs were produced by Cook Phamica d b a Catalent under contract of Medimmune 6 7 Mechanism of action editNeutralization edit Ansuvimab is a monoclonal antibody therapy that is infused intravenously into patients with Ebola virus disease Ansuvimab is a neutralizing antibody 5 meaning it binds to a protein on the surface of Ebola virus that is required to infect cells Specifically ansuvimab neutralizes infection by binding to a region of the Ebola virus envelope glycoprotein that in the absence of ansuvimab would interact with virus s cell receptor protein Niemann Pick C1 NPC1 8 9 10 This competition by ansuvimab prevents Ebola virus from binding to NPC1 and neutralizes the virus s ability to infect the targeted cell 8 Effector function edit Antibodies have antigen binding fragment Fab regions and constant fragment Fc regions The Neutralization of virus infection occurs when the Fab regions of antibodies binds to virus antigen s in a manner that blocks infection Antibodies are also able to kill virus particles directly and or kill infected cells using antibody mediated effector functions such as opsonization complement dependent cytotoxicity antibody dependent cell mediated cytotoxicity and antibody dependent phagocytosis These effector functions are contained in the Fc region of antibodies but is also dependent on binding of the Fab region to antigen Effector functions also require the use of complement proteins in serum or Fc receptor on cell membranes Ansuvimab has been found to be capable of killing cells by antibody dependent cell mediated cytotoxicity 5 Other functional killing tests have not been performed citation needed History editAnsuvimab is a monoclonal antibody that is being evaluated as a treatment for Ebola virus disease 11 Its discovery was led by the laboratory of Nancy Sullivan at the United States National Institutes of Health Vaccine Research Center and J J Muyembe Tamfum from the Institut National pour la Recherche Biomedicale INRB in the Democratic Republic of Congo working in collaboration with the Institute for Research in Biomedicine IRB Bellinzona Switzerland and the United States Army Medical Research Institute of Infectious Diseases 5 12 Ansuvimab was isolated from the blood of a survivor of the 1995 outbreak of Ebola virus disease in Kikwit Democratic Republic of Congo roughly ten years later 5 In 2018 a Phase 1 clinical trial of ansuvimab was conducted by Martin Gaudinski within the Vaccine Research Center Clinical Trials Program that is led by Julie E Ledgerwood 7 6 13 Ansuvimab is also being evaluated during the 2018 North Kivu Ebola outbreak 14 Ansuvimab has also shown success with lowering the mortality rate from 70 to about 34 In August 2019 Congolese health authorities the World Health Organization and the U S National Institutes of Health promoted the use of ansuvimab alongside atoltivimab maftivimab odesivimab a similar Regeneron produced monoclonal antibody treatment over other treatments yielding higher mortality rates after ending clinical trials during the outbreak 15 16 The U S Food and Drug Administration FDA approved ansuvimab based primarily on evidence from a clinical trial Trial 1 NCT NCT03719586 of 342 participants with Zaire ebolavirus infection 3 The trial enrolled newborn pediatric and adult participants including pregnant women with Zaire ebolavirus infection 3 All participants received standard supportive care for the disease 3 In addition to the standard care participants were randomly assigned to receive either a one time dose of ansuvimab or one of the three other types of experimental treatments including one as the control group 3 The participants and the health care providers knew which treatment was being given 3 The trial was conducted at four sites in the Democratic Republic of Congo during an outbreak that began in August 2018 3 Discovery edit A 2016 paper describes the efforts of how ansuvimab was originally developed as part of research efforts led by Dr Nancy Sullivan at the United States National Institutes of Health Vaccine Research Center and Dr J J Muyembe Tamfum from the Institut National de Recherche Biomedicale INRB in the Democratic Republic of Congo 5 12 This collaborative effort also involved researchers from Institute of Biomedical Research and the United States Army Medical Research Institute of Infectious Diseases 5 12 A survivor from the 1995 outbreak of Ebola virus disease in Kikwit Democratic Republic of Congo donated blood to the project that began roughly ten years after they had recovered 5 Memory B cells isolated from the survivor s blood were immortalized cultured and screened for their ability to produce monoclonal antibodies that reacted with the glycoprotein of Ebola virus Ansuvimab was identified from one of these cultures and the antibody heavy and light chain gene sequences were sequenced from the cells 5 These sequences were then cloned into recombinant DNA plasmids and purified antibody protein for initial studies was produced in cells derived from HEK 293 cells 5 Ansuvimab and mAb100 combination edit In an experiment described in the 2016 paper rhesus macaques were infected with Ebola virus and treated with a combination of ansuvimab and another antibody isolated from the same subject mAb100 Three doses of the combination were given once a day starting 1 day after the animals were infected The control animal died and the treated animals all survived 5 Ansuvimab monotherapy edit In a second experiment described in the 2016 paper rhesus macaques were infected with Ebola virus and only treated with ansuvimab Three doses of ansuvimab were given once a day starting 1 day or 5 days after the animals were infected The control animals died and the treated animals all survived 5 Unpublished data referred to in a publication of the 2018 Phase I clinical trial results of ansuvimab reported that a single infusion of ansuvimab provided full protection of rhesus macaques and was the basis of the dosing used for human studies 7 6 Development edit Ansuvimab was developed by the Vaccine Research Center with support of the United States National Institutes of Health and the Defense Advanced Projects Agency The heavy and light chain sequences of ansuvimab mAb were cloned into CHO cell lines to enable large scale production of antibody product for use in humans 6 7 Human safety testing edit In early 2018 11 a Phase 1 clinical trial of ansuvimab s safety tolerability and pharmacokinetics was conducted by Dr Martin Gaudinski within the Vaccine Research Center Clinical Trials Program that is led by Dr Julie E Ledgerwood 7 6 13 The study was performed in the United States at the NIH Clinical Center and tested single dose infusions of ansuvimab infused over 30 minutes The study showed that ansuvimab was safe had minimal side effects and had a half life of 24 days 7 6 Ridgeback Biotherapeutics edit A license for ansuvimab was obtained by Ridgeback Biotherapeutics in 2018 from the National Institutes of Health National Institute of Allergy and Infectious Diseases 17 Ansuvimab was given orphan drug status in May 2019 and March 2020 18 19 20 Experimental use in the Democratic Republic of Congo editDuring the 2018 Equateur province Ebola outbreak ansuvimab was requested by the Democratic Republic of Congo DRC Ministry of Public Health Ansuvimab was approved for compassionate use by the World Health Organization MEURI ethical protocol and at DRC ethics board Ansuvimab was sent along with other therapeutic agents to the outbreak sites 21 22 13 However the outbreak came to a conclusion before any therapeutic agents were given to patients 13 Approximately one month following the conclusion of the Equateur province outbreak a distinct outbreak was noted in Kivu in the DRC 2018 20 Kivu Ebola outbreak Once again ansuvimab received approval for compassionate use by WHO MEURI and DRC ethic boards and has been given to many patients under these protocols 13 In November 2018 the Pamoja Tulinde Maisha PALM together save lives open label randomized clinical control trial was begun at multiple treatment units testing ansuvimab atoltivimab maftivimab odesivimab REGN EB3 and remdesivir to ZMapp Despite the difficulty of running a clinical trial in a conflict zone investigators have enrolled 681 patients towards their goal of 725 An interim analysis by the Data Safety and Monitoring Board DSMB of the first 499 patient found that ansuvimab and REGN EB3 were superior to the comparator ZMapp Overall mortality of patients in the ZMapp and remdesivir groups were 49 and 53 compared to 34 and 29 for ansuvimab and REGN EB3 When looking at patients who arrived early after disease symptoms appeared survival was 89 for ansuvimab and 94 for REGN EB3 While the study was not powered to determine whether there is any difference between REGN EB3 and ansuvimab the survival difference between those two therapies and ZMapp was significant This led to the DSMB halting the study and PALM investigators dropping the remdesivir and ZMapp arms from the clinical trial All patients in the outbreak who elect to participate in the trial will now be given either ansuvimab or REGN EB3 23 24 15 14 In October 2020 the U S Food and Drug Administration FDA approved atoltivimab maftivimab odesivimab Inmazeb formerly REGN EB3 with an indication for the treatment of infection caused by Zaire ebolavirus 25 References edit a b c d FDA Approves Treatment for Ebola Virus U S Food and Drug Administration 21 December 2020 Retrieved 23 December 2020 nbsp This article incorporates text from this source which is in the public domain a b Ridgeback Biotherapeutics LP Announces the Approval of Ebanga for Ebola Press release Ridgeback Biotherapeutics LP 22 December 2020 Retrieved 23 December 2020 via Business Wire a b c d e f g Drug Trials Snapshot Ebanga U S Food and Drug Administration FDA 21 December 2020 Retrieved 13 January 2021 nbsp This article incorporates text from this source which is in the public domain World Health Organization 2023 The selection and use of essential medicines 2023 web annex A World Health Organization model list of essential medicines 23rd list 2023 Geneva World Health Organization hdl 10665 371090 WHO MHP HPS EML 2023 02 a b c d e f g h i j k l Corti D Misasi J Mulangu S Stanley DA Kanekiyo M Wollen S et al March 2016 Protective monotherapy against lethal Ebola virus infection by a potently neutralizing antibody Science 351 6279 1339 42 Bibcode 2016Sci 351 1339C doi 10 1126 science aad5224 PMID 26917593 a b c d e f Clinical trial number NCT03478891 for Safety and Pharmacokinetics of a Human Monoclonal Antibody VRC EBOMAB092 00 AB MAb114 Administered Intravenously to Healthy Adults at ClinicalTrials gov a b c d e f Gaudinski MR Coates EE Novik L Widge A Houser KV Burch E et al March 2019 Safety tolerability pharmacokinetics and immunogenicity of the therapeutic monoclonal antibody ansuvimab targeting Ebola virus glycoprotein VRC 608 an open label phase 1 study Lancet 393 10174 889 898 doi 10 1016 S0140 6736 19 30036 4 PMC 6436835 PMID 30686586 a b Misasi J Gilman MS Kanekiyo M Gui M Cagigi A Mulangu S et al March 2016 Structural and molecular basis for Ebola virus neutralization by protective human antibodies Science 351 6279 1343 6 Bibcode 2016Sci 351 1343M doi 10 1126 science aad6117 PMC 5241105 PMID 26917592 Cote M Misasi J Ren T Bruchez A Lee K Filone CM et al August 2011 Small molecule inhibitors reveal Niemann Pick C1 is essential for Ebola virus infection Nature 477 7364 344 8 Bibcode 2011Natur 477 344C doi 10 1038 nature10380 PMC 3230319 PMID 21866101 Carette JE Raaben M Wong AC Herbert AS Obernosterer G Mulherkar N et al August 2011 Ebola virus entry requires the cholesterol transporter Niemann Pick C1 Nature 477 7364 340 3 Bibcode 2011Natur 477 340C doi 10 1038 nature10348 PMC 3175325 PMID 21866103 a b NIH begins testing Ebola treatment in early stage trial National Institutes of Health NIH 2018 05 23 Retrieved 2018 10 15 a b c Hayden EC 2016 02 26 Ebola survivor s blood holds promise of new treatment Nature doi 10 1038 nature 2016 19440 ISSN 1476 4687 S2CID 211835755 a b c d e NIH VideoCast CC Grand Rounds Response to an Outbreak Ebola Virus Monoclonal Antibody mAb114 Rapid Clinical Development videocast nih gov 13 March 2019 Retrieved 2019 08 09 a b Kingsley Hall A Congo s experimental mAb114 Ebola treatment appears successful authorities Central Africa www theafricareport com Retrieved 2018 10 15 a b McNeil DG 12 August 2019 A Cure for Ebola Two New Treatments Prove Highly Effective in Congo The New York Times Retrieved 13 August 2019 Molteni M 12 August 2019 Ebola is Now Curable Here s How The New Treatments Work Wired Retrieved 13 August 2019 Ridgeback Biotherapeutics LP announces licensing of mAb114 an experimental Ebola treatment from the National Institute of Allergy and Infectious Diseases Press release Ridgeback Biotherapeutics LP Retrieved 2019 08 17 via PR Newswire Ansuvimab Orphan Drug Designations and Approvals accessdata fda gov 8 May 2019 Retrieved 24 December 2020 Ansuvimab Orphan Drug Designations and Approvals accessdata fda gov 30 March 2020 Retrieved 24 December 2020 Ridgeback Biotherapeutics LP Announces Orphan Drug Designation for mAb114 Press release Ridgeback Biotherapeutics LP Retrieved 2019 08 17 via PR Newswire Check Hayden Erika May 2018 Experimental drugs poised for use in Ebola outbreak Nature 557 7706 475 476 Bibcode 2018Natur 557 475C doi 10 1038 d41586 018 05205 x ISSN 0028 0836 PMID 29789732 WHO Consultation on Monitored Emergency Use of Unregistered and Investigational Interventions for Ebola virus Disease PDF who int World Health Organization May 17 2018 Retrieved November 2 2021 Mole B 2019 08 13 Two Ebola drugs boost survival rates according to early trial data Ars Technica Retrieved 2019 08 17 Independent monitoring board recommends early termination of Ebola therapeutics trial in DRC because of favorable results with two of four candidates National Institutes of Health NIH 2019 08 12 Retrieved 2019 08 17 FDA Approves First Treatment for Ebola Virus U S Food and Drug Administration FDA Press release 14 October 2020 Retrieved 14 October 2020 nbsp This article incorporates text from this source which is in the public domain External links editClinical trial number NCT03719586 for Investigational Therapeutics for the Treatment of People With Ebola Virus Disease at ClinicalTrials gov Portals nbsp Medicine nbsp Viruses Retrieved from https en wikipedia org w index php title Ansuvimab amp oldid 1211596011, wikipedia, wiki, book, books, library,

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