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Eteplirsen

February 01, 2023

Eteplirsen (brand name Exondys 51) is a medication to treat, but not cure, some types of Duchenne muscular dystrophy (DMD), caused by a specific mutation. Eteplirsen only targets specific mutations and can be used to treat about 14% of DMD cases.[1][2] Eteplirsen is a form of antisense therapy.

Eteplirsen
Clinical data
Trade namesExondys 51
Other namesAVI-4658
License data
Routes of
administration		Intravenous infusion
Drug classAntisense oligonucleotide
ATC code
Legal status
Legal status
Identifiers
  • (P-deoxy-P-(dimethylamino))(2',3'-dideoxy-2',3'-imino-2',3'-seco)(2'a→5')(C-m5U-C-C-A-A-C-A-m5U-C-A-A-G-G-A-A-G-A-m5U-G-G-C-A-m5U-m5U-m5U-C-m5U-A-G),5'-(P-(4-((2-(2-(2-hydroxyethoxy)ethoxy)ethoxy)carbonyl)-1-piperazinyl)-N,N-dimethylphosphonamidate) RNA
CAS Number
  • 1173755-55-9
DrugBank
  • DB06014
ChemSpider
  • 34983391
UNII
  • AIW6036FAS
KEGG
  • D09900
ChEMBL
  • ChEMBL2108278
Chemical and physical data
FormulaC364H569N177O122P30
Molar mass10305.886 g·mol−1
  • Cc1cn(c(=O)[nH]c1=O)[C@H]2CN(C[C@H](O2)COP(=O)(N3C[C@H](O[C@H](C3)n4ccc(nc4=O)N)COP(=O)(N5CCN(CC5)C(=O)OCCOCCOCCO)N(C)C)N(C)C)P(=O)(N(C)C)OC[C@@H]6CN(C[C@@H](O6)n7ccc(nc7=O)N)P(=O)(N(C)C)OC[C@@H]8CN(C[C@@H](O8)n9ccc(nc9=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1ccc(nc1=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1ccc(nc1=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1nc([nH]c2=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1nc([nH]c2=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1nc([nH]c2=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1nc([nH]c2=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1nc([nH]c2=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1ccc(nc1=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1ccc(nc1=O)N)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cc(c(=O)[nH]c1=O)C)P(=O)(N(C)C)OC[C@@H]1CN(C[C@@H](O1)n1cnc2c1ncnc2N)P(=O)(N(C)C)OC[C@@H]1CNC[C@@H](O1)n1cnc2c1nc([nH]c2=O)N
  • InChI=1S/C364H569N177O122P30/c1-215-94-519(357(563)444-331(215)543)267-137-490(108-230(642-267)167-612-667(574,454(14)15)483-101-223(635-260(130-483)512-75-68-252(365)425-350(512)556)160-605-664(571,451(8)9)482-84-82-481(83-85-482)364(570)603-91-90-602-89-88-601-87-86-542)673(580,460(26)27)607-162-225-103-484(131-261(637-225)513-76-69-253(366)426-351(513)557)666(573,453(12)13)606-161-224-102-486(133-263(636-224)515-78-71-255(368)428-353(515)559)669(576,456(18)19)621-176-240-118-502(149-279(652-240)532-204-414-294-310(377)394-194-404-320(294)532)684(591,471(48)49)625-179-242-120-498(145-275(654-242)528-200-410-290-306(373)390-190-400-316(290)528)680(587,467(40)41)610-165-228-106-488(135-265(640-228)517-80-73-257(370)430-355(517)561)671(578,458(22)23)619-174-238-116-499(146-276(650-238)529-201-411-291-307(374)391-191-401-317(291)529)681(588,468(42)43)616-171-234-112-492(139-269(646-234)521-96-217(3)333(545)446-359(521)565)675(582,462(30)31)609-164-227-105-487(134-264(639-227)516-79-72-256(369)429-354(516)560)670(577,457(20)21)622-177-241-119-503(150-280(653-241)533-205-415-295-311(378)395-195-405-321(295)533)685(592,472(50)51)626-180-243-122-506(153-282(655-243)535-207-417-297-313(380)397-197-407-323(297)535)688(595,475(56)57)631-186-249-128-511(158-288(661-249)541-214-424-304-330(541)437-349(387)443-343(304)555)693(600,480(66)67)633-188-251-129-509(156-287(663-251)540-213-423-303-329(540)436-348(386)442-342(303)554)691(598,478(62)63)629-183-246-124-504(151-281(658-246)534-206-416-296-312(379)396-196-406-322(296)534)686(593,473(52)53)627-181-244-123-505(152-283(656-244)536-208-418-298-314(381)398-198-408-324(298)536)687(594,474(54)55)630-185-248-127-508(155-286(660-248)539-212-422-302-328(539)435-347(385)441-341(302)553)690(597,477(60)61)628-182-245-121-501(148-278(657-245)531-203-413-293-309(376)393-193-403-319(293)531)683(590,470(46)47)618-173-236-114-496(143-273(648-236)525-100-221(7)337(549)450-363(525)569)679(586,466(38)39)624-184-247-125-510(157-285(659-247)538-211-421-301-327(538)434-346(384)440-340(301)552)692(599,479(64)65)632-187-250-126-507(154-284(662-250)537-210-420-300-326(537)433-345(383)439-339(300)551)689(596,476(58)59)611-166-229-107-489(136-266(641-229)518-81-74-258(371)431-356(518)562)672(579,459(24)25)620-175-239-117-500(147-277(651-239)530-202-412-292-308(375)392-192-402-318(292)530)682(589,469(44)45)617-172-235-113-494(141-271(647-235)523-98-219(5)335(547)448-361(523)567)677(584,464(34)35)615-170-233-111-493(140-270(645-233)522-97-218(4)334(546)447-360(522)566)676(583,463(32)33)614-169-232-110-491(138-268(644-232)520-95-216(2)332(544)445-358(520)564)674(581,461(28)29)608-163-226-104-485(132-262(638-226)514-77-70-254(367)427-352(514)558)668(575,455(16)17)613-168-231-109-495(142-272(643-231)524-99-220(6)336(548)449-362(524)568)678(585,465(36)37)623-178-237-115-497(144-274(649-237)527-199-409-289-305(372)389-189-399-315(289)527)665(572,452(10)11)604-159-222-92-388-93-259(634-222)526-209-419-299-325(526)432-344(382)438-338(299)550/h68-81,94-100,189-214,222-251,259-288,388,542H,82-93,101-188H2,1-67H3,(H2,365,425,556)(H2,366,426,557)(H2,367,427,558)(H2,368,428,559)(H2,369,429,560)(H2,370,430,561)(H2,371,431,562)(H2,372,389,399)(H2,373,390,400)(H2,374,391,401)(H2,375,392,402)(H2,376,393,403)(H2,377,394,404)(H2,378,395,405)(H2,379,396,406)(H2,380,397,407)(H2,381,398,408)(H,444,543,563)(H,445,544,564)(H,446,545,565)(H,447,546,566)(H,448,547,567)(H,449,548,568)(H,450,549,569)(H3,382,432,438,550)(H3,383,433,439,551)(H3,384,434,440,552)(H3,385,435,441,553)(H3,386,436,442,554)(H3,387,437,443,555)/t222-,223-,224-,225-,226-,227-,228-,229-,230-,231-,232-,233-,234-,235-,236-,237-,238-,239-,240-,241-,242-,243-,244-,245-,246-,247-,248-,249-,250-,251-,259+,260+,261+,262+,263+,264+,265+,266+,267+,268+,269+,270+,271+,272+,273+,274+,275+,276+,277+,278+,279+,280+,281+,282+,283+,284+,285+,286+,287+,288+,664?,665?,666?,667?,668?,669?,670?,671?,672?,673?,674?,675?,676?,677?,678?,679?,680?,681?,682?,683?,684?,685?,686?,687?,688?,689?

Eteplirsen was developed by Steve Wilton, Sue Fletcher and colleagues at the University of Western Australia and commercialized by Sarepta Therapeutics.[3] After a controversial debate surrounding the drug's efficacy, during which two FDA review panel members resigned in protest, eteplirsen received accelerated approval from the US Food and Drug administration in late 2016.[4][5] The Committee for Medicinal Products for Human Use (CHMP) of the European Medicines Agency (EMA) refused to authorize the use of eteplirsen.[6]

Adverse effects

The following adverse events were observed in at least 10% of people who received eteplirsen in trials: vomiting, contusion, excoriation, arthralgia, rash, catheter site pain, and upper respiratory tract infection.[7]

Mechanism of action

Duchenne muscular dystrophy is caused when a mutation in the DMD gene changes the DMD mRNA so that it no longer codes for functional dystrophin protein, usually due to a nonsense mutation that introduces a premature stop codon into the mRNA.[citation needed] If an exon with an appropriate number of bases lies near the mutation, by removing the defective exon the downstream reading frame can be corrected and production of partially functional dystrophin can be restored.[citation needed] This is the general strategy used for designing exon-skipping oligos for DMD; as there are 79 exons transcribed in the longest splice form of the dystrophin transcript, many different oligos are needed to address the range of mutations present in the population of people with DMD.[citation needed]

Eteplirsen is a morpholino antisense oligomer which triggers excision of exon 51 during pre-mRNA splicing of the dystrophin RNA transcript. Skipping exon 51 changes the downstream reading frame of dystrophin;[8] giving eteplirsen to a healthy person would result in production of dystrophin mRNA which would not code for functional dystrophin protein but, for DMD patients with particular nonsense mutations, giving eteplirsen can restore the reading frame of the dystrophin mRNA and result in production of functional (although modified by having an internal deletion consisting of both the patient's original defect, as well as the therapeutically skipped exon) dystrophin.[9] Eteplirsen is given by intravenous infusion for systemic treatment of DMD.

Exon skipping is induced by eteplirsen, a charge-neutral, phosphorodiamidate morpholino oligomer (PMO) that selectively binds to exon 51 of dystrophin pre-mRNA, restoring the phase of the reading frame and enabling production of functional, but internally edited, dystrophin.[10] The uncharged nature of the PMO helps make it resistant to biological degradation.[11] This modified dystrophin protein produced by eteplirsen may cause a less severe form of dystrophinopathy, much like Becker muscular dystrophy. Eteplirsen's proposed mechanism of action is to bind to dystrophin pre-mRNA and alter the exon splicing of the RNA so that more almost full-length dystrophin is made. By increasing the quantity of an abnormal, but potentially functional, dystrophin protein, the objective is to slow or prevent the progression of DMD.[10][12]

Nature and sequence of oligo and target

Eteplirsen is a morpholino phosphorodiamidate antisense oligomer.

CTCCAACATCAAGGAAGATGGCATTTCTAG (sequence source: US FDA ETEPLIRSEN BRIEFING DOCUMENT NDA 206488[10]),
30-mer,
20% G,
43% CG,
Predicted Tm: 88.9 °C at 10 μM oligo.

Oligo complement CTAGAAATGCCATCTTCCTTGATGTTGGAG

DMD-001 Exon 51, ENST00000357033.8 in Ensembl.org, RNA target site marked. Given that the target site is within an exon, this is likely blocking binding of an exonic splice enhancer protein and so altering splicing by interfering with splice regulation. CTCCTACTCAGACTGTTACTCTGGTGACACAACCTGTGGTTACTAAGGAAACTGCCATCT CCAAA[CTAGAAATGCCATCTTCCTTGATGTTGGAG]GTACCTGCTCTGGCAGATTTCAACC GGGCTTGGACAGAACTTACCGACTGGCTTTCTCTGCTTGATCAAGTTATAAAATCACAGA GGGTGATGGTGGGTGACCTTGAGGATATCAACGAGATGATCATCAAGCAGAAG

Pharmacokinetics

Following single or multiple intravenous infusions, the majority of drug elimination occurred within 24 hours of intravenous administration. Elimination half-life of eteplirsen was 3 to 4 hours.[7]

History

New Drug Applications (NDA) for eteplirsen and a similar drug drisapersen were filed with the US Food and Drug Administration (FDA) in August 2015.[13] The Prescription Drug User Fee Act (PDUFA) goal dates for these were December 27, 2015 for drisapersen and February 26, 2016, for eteplirsen. Following FDA rejection of drisapersen, the agency announced a three-month time extension for its review of eteplirsen. The FDA panel decision was controversial because the FDA staff and the panel used a stricter standard of evidence than Sarepta and patient groups used. The FDA panel said that it was required by law to apply the standard of "substantial evidence" of effectiveness. This required randomized, controlled trials showing effectiveness of a meaningful clinical outcome, such as the ability to function in daily life. Sarepta and patient groups wanted to use the standard of historical controls, personal testimonies, and the presence of altered dystrophin in the body. On April 25, 2016, the Advisory Committee Panel voted against approval;.[14] However, in June 2016, FDA requested for additional data from Sarepta to confirm findings of dystrophin production by eteplirsen. Janet Woodcock, director of the FDA's Center for Drug Evaluation and Research, overruled the panel, and FDA Commissioner Robert Califf deferred to her decision. Eterplirsen received accelerated approval on September 19, 2016.[15]

The European Medicines Agency reviewed the molecule in 2018, and refused to approve it.[6][16]

Following the approval of eteplirsen, two other drugs of a similar kind, golodirsen and viltolarsen received provisional approval from the FDA for the treatment of people with a confirmed mutation of the dystrophin gene that is amenable to exon 53 skipping[17][18] as well as casimersen for exon 45 skipping.[19]

Society and culture

Economics

The US list price of eteplirsen is US$300,000 per year of treatment. The Institute for Clinical and Economic Review has found the drug not cost effective at the list price when the cost of one Quality-adjusted life year (QALY) was equal to US$150,000.[20]

References

  1. ^ Scoto M, Finkel R, Mercuri E, Muntoni F (August 2018). "Genetic therapies for inherited neuromuscular disorders". The Lancet. Child & Adolescent Health. 2 (8): 600–609. doi:10.1016/S2352-4642(18)30140-8. PMID 30119719. S2CID 52032568.
  2. ^ Lim KR, Maruyama R, Yokota T (2017). "Eteplirsen in the treatment of Duchenne muscular dystrophy". Drug Design, Development and Therapy. 11: 533–545. doi:10.2147/DDDT.S97635. PMC 5338848. PMID 28280301. Eteplirsen is applicable for approximately 14% of patients with DMDmutations
  3. ^ "Perron and UWA to reap $70 million windfall". Retrieved 16 November 2021.
  4. ^ "FDA grants accelerated approval to first drug for Duchenne muscular dystrophy". Press Announcements. U.S. Food & Drug Administration. September 19, 2016. Retrieved September 19, 2016.
  5. ^ "Railroading at the FDA". Nature Biotechnology. 34 (11): 1078. November 2016. doi:10.1038/nbt.3733. PMID 27824847.
  6. ^ a b "Exondys EPAR". European Medicines Agency (EMA). Retrieved 13 August 2020.
  7. ^ a b "Eteplirsen - prescribing information" (PDF). FDA. September 2016.
  8. ^ Anthony K, Feng L, Arechavala-Gomeza V, Guglieri M, Straub V, Bushby K, et al. (October 2012). "Exon skipping quantification by quantitative reverse-transcription polymerase chain reaction in Duchenne muscular dystrophy patients treated with the antisense oligomer eteplirsen". Human Gene Therapy Methods. 23 (5): 336–45. doi:10.1089/hgtb.2012.117. PMID 23075107.
  9. ^ Moulton HM, Moulton JD (December 2010). "Morpholinos and their peptide conjugates: therapeutic promise and challenge for Duchenne muscular dystrophy". Biochimica et Biophysica Acta (BBA) - Biomembranes. 1798 (12): 2296–303. doi:10.1016/j.bbamem.2010.02.012. PMID 20170628.
  10. ^ a b c "Eteplirsen" (PDF). FDA Briefing Document. 25 April 2016.
  11. ^ Kole R, Leppert BJ (July 2012). "Targeting mRNA splicing as a potential treatment for Duchenne muscular dystrophy". Discovery Medicine. 14 (74): 59–69. PMID 22846203.
  12. ^ Mendell JR, Rodino-Klapac LR, Sahenk Z, Roush K, Bird L, Lowes LP, et al. (November 2013). "Eteplirsen for the treatment of Duchenne muscular dystrophy". Annals of Neurology. 74 (5): 637–47. doi:10.1002/ana.23982. PMID 23907995. S2CID 24359589.
  13. ^ . Rare Disease Report. Archived from the original on 2015-08-28. Retrieved 2015-08-28.
  14. ^ Pollack, Andrew (2016-04-25). "Advisers to F.D.A. Vote Against Duchenne Muscular Dystrophy Drug". The New York Times.
  15. ^ Column: To appease a patient lobby, did the FDA approve a $300,000 drug that doesn't work? Michael Hiltzik, Los Angeles Times, October 28, 2016
  16. ^ "Going Its Own Way, European Regulators Reject Sarepta's Exondys 51 for DMD". BioSpace. Retrieved 2019-12-14.
  17. ^ Anwar S, Yokota T (August 2020). "Golodirsen for Duchenne muscular dystrophy". Drugs of Today. 56 (8): 491–504. doi:10.1358/dot.2020.56.8.3159186. PMID 33025945. S2CID 222183389.
  18. ^ Dhillon S (Jul 2020). "Viltolarsen: first approval". Drugs. 80 (10): 1027–1031. doi:10.1007/s40265-020-01339-3. PMID 32519222. S2CID 219542850.
  19. ^ "FDA Approves Targeted Treatment for Rare Duchenne Muscular Dystrophy Mutation". Food and Drug Administration. 25 February 2021.
  20. ^ "ICER sees current DMD therapies as too pricey, but notes data limitations". BioPharma Dive. Retrieved 2019-12-14.

External links

  • "Eteplirsen". Drug Information Portal. U.S. National Library of Medicine.

February 01, 2023
eteplirsen, brand, name, exondys, medication, treat, cure, some, types, duchenne, muscular, dystrophy, caused, specific, mutation, only, targets, specific, mutations, used, treat, about, cases, form, antisense, therapy, clinical, datatrade, namesexondys, 51oth. Eteplirsen brand name Exondys 51 is a medication to treat but not cure some types of Duchenne muscular dystrophy DMD caused by a specific mutation Eteplirsen only targets specific mutations and can be used to treat about 14 of DMD cases 1 2 Eteplirsen is a form of antisense therapy EteplirsenClinical dataTrade namesExondys 51Other namesAVI 4658License dataUS DailyMed EteplirsenRoutes ofadministrationIntravenous infusionDrug classAntisense oligonucleotideATC codeM09AX06 WHO Legal statusLegal statusUS onlyIdentifiersIUPAC name P deoxy P dimethylamino 2 3 dideoxy 2 3 imino 2 3 seco 2 a 5 C m5U C C A A C A m5U C A A G G A A G A m5U G G C A m5U m5U m5U C m5U A G 5 P 4 2 2 2 hydroxyethoxy ethoxy ethoxy carbonyl 1 piperazinyl N N dimethylphosphonamidate RNACAS Number1173755 55 9DrugBankDB06014ChemSpider34983391UNIIAIW6036FASKEGGD09900ChEMBLChEMBL2108278Chemical and physical dataFormulaC 364H 569N 177O 122P 30Molar mass10305 886 g mol 1SMILES Cc1cn c O nH c1 O C H 2CN C C H O2 COP O N3C C H O C H C3 n4ccc nc4 O N COP O N5CCN CC5 C O OCCOCCOCCO N C C N C C P O N C C OC C H 6CN C C H O6 n7ccc nc7 O N P O N C C OC C H 8CN C C H O8 n9ccc nc9 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1ccc nc1 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1ccc nc1 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cnc2c1nc nH c2 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1nc nH c2 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cnc2c1nc nH c2 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1cnc2c1nc nH c2 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1nc nH c2 O N P O N C C OC C H 1CN C C H O1 n1ccc nc1 O N P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1ccc nc1 O N P O N C C OC C H 1CN C C H O1 n1cc c O nH c1 O C P O N C C OC C H 1CN C C H O1 n1cnc2c1ncnc2N P O N C C OC C H 1CNC C H O1 n1cnc2c1nc nH c2 O NInChI InChI 1S C364H569N177O122P30 c1 215 94 519 357 563 444 331 215 543 267 137 490 108 230 642 267 167 612 667 574 454 14 15 483 101 223 635 260 130 483 512 75 68 252 365 425 350 512 556 160 605 664 571 451 8 9 482 84 82 481 83 85 482 364 570 603 91 90 602 89 88 601 87 86 542 673 580 460 26 27 607 162 225 103 484 131 261 637 225 513 76 69 253 366 426 351 513 557 666 573 453 12 13 606 161 224 102 486 133 263 636 224 515 78 71 255 368 428 353 515 559 669 576 456 18 19 621 176 240 118 502 149 279 652 240 532 204 414 294 310 377 394 194 404 320 294 532 684 591 471 48 49 625 179 242 120 498 145 275 654 242 528 200 410 290 306 373 390 190 400 316 290 528 680 587 467 40 41 610 165 228 106 488 135 265 640 228 517 80 73 257 370 430 355 517 561 671 578 458 22 23 619 174 238 116 499 146 276 650 238 529 201 411 291 307 374 391 191 401 317 291 529 681 588 468 42 43 616 171 234 112 492 139 269 646 234 521 96 217 3 333 545 446 359 521 565 675 582 462 30 31 609 164 227 105 487 134 264 639 227 516 79 72 256 369 429 354 516 560 670 577 457 20 21 622 177 241 119 503 150 280 653 241 533 205 415 295 311 378 395 195 405 321 295 533 685 592 472 50 51 626 180 243 122 506 153 282 655 243 535 207 417 297 313 380 397 197 407 323 297 535 688 595 475 56 57 631 186 249 128 511 158 288 661 249 541 214 424 304 330 541 437 349 387 443 343 304 555 693 600 480 66 67 633 188 251 129 509 156 287 663 251 540 213 423 303 329 540 436 348 386 442 342 303 554 691 598 478 62 63 629 183 246 124 504 151 281 658 246 534 206 416 296 312 379 396 196 406 322 296 534 686 593 473 52 53 627 181 244 123 505 152 283 656 244 536 208 418 298 314 381 398 198 408 324 298 536 687 594 474 54 55 630 185 248 127 508 155 286 660 248 539 212 422 302 328 539 435 347 385 441 341 302 553 690 597 477 60 61 628 182 245 121 501 148 278 657 245 531 203 413 293 309 376 393 193 403 319 293 531 683 590 470 46 47 618 173 236 114 496 143 273 648 236 525 100 221 7 337 549 450 363 525 569 679 586 466 38 39 624 184 247 125 510 157 285 659 247 538 211 421 301 327 538 434 346 384 440 340 301 552 692 599 479 64 65 632 187 250 126 507 154 284 662 250 537 210 420 300 326 537 433 345 383 439 339 300 551 689 596 476 58 59 611 166 229 107 489 136 266 641 229 518 81 74 258 371 431 356 518 562 672 579 459 24 25 620 175 239 117 500 147 277 651 239 530 202 412 292 308 375 392 192 402 318 292 530 682 589 469 44 45 617 172 235 113 494 141 271 647 235 523 98 219 5 335 547 448 361 523 567 677 584 464 34 35 615 170 233 111 493 140 270 645 233 522 97 218 4 334 546 447 360 522 566 676 583 463 32 33 614 169 232 110 491 138 268 644 232 520 95 216 2 332 544 445 358 520 564 674 581 461 28 29 608 163 226 104 485 132 262 638 226 514 77 70 254 367 427 352 514 558 668 575 455 16 17 613 168 231 109 495 142 272 643 231 524 99 220 6 336 548 449 362 524 568 678 585 465 36 37 623 178 237 115 497 144 274 649 237 527 199 409 289 305 372 389 189 399 315 289 527 665 572 452 10 11 604 159 222 92 388 93 259 634 222 526 209 419 299 325 526 432 344 382 438 338 299 550 h68 81 94 100 189 214 222 251 259 288 388 542H 82 93 101 188H2 1 67H3 H2 365 425 556 H2 366 426 557 H2 367 427 558 H2 368 428 559 H2 369 429 560 H2 370 430 561 H2 371 431 562 H2 372 389 399 H2 373 390 400 H2 374 391 401 H2 375 392 402 H2 376 393 403 H2 377 394 404 H2 378 395 405 H2 379 396 406 H2 380 397 407 H2 381 398 408 H 444 543 563 H 445 544 564 H 446 545 565 H 447 546 566 H 448 547 567 H 449 548 568 H 450 549 569 H3 382 432 438 550 H3 383 433 439 551 H3 384 434 440 552 H3 385 435 441 553 H3 386 436 442 554 H3 387 437 443 555 t222 223 224 225 226 227 228 229 230 231 232 233 234 235 236 237 238 239 240 241 242 243 244 245 246 247 248 249 250 251 259 260 261 262 263 264 265 266 267 268 269 270 271 272 273 274 275 276 277 278 279 280 281 282 283 284 285 286 287 288 664 665 666 667 668 669 670 671 672 673 674 675 676 677 678 679 680 681 682 683 684 685 686 687 688 689 Eteplirsen was developed by Steve Wilton Sue Fletcher and colleagues at the University of Western Australia and commercialized by Sarepta Therapeutics 3 After a controversial debate surrounding the drug s efficacy during which two FDA review panel members resigned in protest eteplirsen received accelerated approval from the US Food and Drug administration in late 2016 4 5 The Committee for Medicinal Products for Human Use CHMP of the European Medicines Agency EMA refused to authorize the use of eteplirsen 6 Contents 1 Adverse effects 2 Mechanism of action 2 1 Nature and sequence of oligo and target 3 Pharmacokinetics 4 History 5 Society and culture 5 1 Economics 6 References 7 External linksAdverse effects EditThe following adverse events were observed in at least 10 of people who received eteplirsen in trials vomiting contusion excoriation arthralgia rash catheter site pain and upper respiratory tract infection 7 Mechanism of action EditDuchenne muscular dystrophy is caused when a mutation in the DMD gene changes the DMD mRNA so that it no longer codes for functional dystrophin protein usually due to a nonsense mutation that introduces a premature stop codon into the mRNA citation needed If an exon with an appropriate number of bases lies near the mutation by removing the defective exon the downstream reading frame can be corrected and production of partially functional dystrophin can be restored citation needed This is the general strategy used for designing exon skipping oligos for DMD as there are 79 exons transcribed in the longest splice form of the dystrophin transcript many different oligos are needed to address the range of mutations present in the population of people with DMD citation needed Eteplirsen is a morpholino antisense oligomer which triggers excision of exon 51 during pre mRNA splicing of the dystrophin RNA transcript Skipping exon 51 changes the downstream reading frame of dystrophin 8 giving eteplirsen to a healthy person would result in production of dystrophin mRNA which would not code for functional dystrophin protein but for DMD patients with particular nonsense mutations giving eteplirsen can restore the reading frame of the dystrophin mRNA and result in production of functional although modified by having an internal deletion consisting of both the patient s original defect as well as the therapeutically skipped exon dystrophin 9 Eteplirsen is given by intravenous infusion for systemic treatment of DMD Exon skipping is induced by eteplirsen a charge neutral phosphorodiamidate morpholino oligomer PMO that selectively binds to exon 51 of dystrophin pre mRNA restoring the phase of the reading frame and enabling production of functional but internally edited dystrophin 10 The uncharged nature of the PMO helps make it resistant to biological degradation 11 This modified dystrophin protein produced by eteplirsen may cause a less severe form of dystrophinopathy much like Becker muscular dystrophy Eteplirsen s proposed mechanism of action is to bind to dystrophin pre mRNA and alter the exon splicing of the RNA so that more almost full length dystrophin is made By increasing the quantity of an abnormal but potentially functional dystrophin protein the objective is to slow or prevent the progression of DMD 10 12 Nature and sequence of oligo and target Edit Eteplirsen is a morpholino phosphorodiamidate antisense oligomer CTCCAACATCAAGGAAGATGGCATTTCTAG sequence source US FDA ETEPLIRSEN BRIEFING DOCUMENT NDA 206488 10 30 mer 20 G 43 CG Predicted Tm 88 9 C at 10 mM oligo Oligo complement CTAGAAATGCCATCTTCCTTGATGTTGGAGDMD 001 Exon 51 ENST00000357033 8 in Ensembl org RNA target site marked Given that the target site is within an exon this is likely blocking binding of an exonic splice enhancer protein and so altering splicing by interfering with splice regulation CTCCTACTCAGACTGTTACTCTGGTGACACAACCTGTGGTTACTAAGGAAACTGCCATCT CCAAA CTAGAAATGCCATCTTCCTTGATGTTGGAG GTACCTGCTCTGGCAGATTTCAACC GGGCTTGGACAGAACTTACCGACTGGCTTTCTCTGCTTGATCAAGTTATAAAATCACAGA GGGTGATGGTGGGTGACCTTGAGGATATCAACGAGATGATCATCAAGCAGAAGPharmacokinetics EditFollowing single or multiple intravenous infusions the majority of drug elimination occurred within 24 hours of intravenous administration Elimination half life of eteplirsen was 3 to 4 hours 7 History EditNew Drug Applications NDA for eteplirsen and a similar drug drisapersen were filed with the US Food and Drug Administration FDA in August 2015 13 The Prescription Drug User Fee Act PDUFA goal dates for these were December 27 2015 for drisapersen and February 26 2016 for eteplirsen Following FDA rejection of drisapersen the agency announced a three month time extension for its review of eteplirsen The FDA panel decision was controversial because the FDA staff and the panel used a stricter standard of evidence than Sarepta and patient groups used The FDA panel said that it was required by law to apply the standard of substantial evidence of effectiveness This required randomized controlled trials showing effectiveness of a meaningful clinical outcome such as the ability to function in daily life Sarepta and patient groups wanted to use the standard of historical controls personal testimonies and the presence of altered dystrophin in the body On April 25 2016 the Advisory Committee Panel voted against approval 14 However in June 2016 FDA requested for additional data from Sarepta to confirm findings of dystrophin production by eteplirsen Janet Woodcock director of the FDA s Center for Drug Evaluation and Research overruled the panel and FDA Commissioner Robert Califf deferred to her decision Eterplirsen received accelerated approval on September 19 2016 15 The European Medicines Agency reviewed the molecule in 2018 and refused to approve it 6 16 Following the approval of eteplirsen two other drugs of a similar kind golodirsen and viltolarsen received provisional approval from the FDA for the treatment of people with a confirmed mutation of the dystrophin gene that is amenable to exon 53 skipping 17 18 as well as casimersen for exon 45 skipping 19 Society and culture EditEconomics Edit The US list price of eteplirsen is US 300 000 per year of treatment The Institute for Clinical and Economic Review has found the drug not cost effective at the list price when the cost of one Quality adjusted life year QALY was equal to US 150 000 20 References Edit Scoto M Finkel R Mercuri E Muntoni F August 2018 Genetic therapies for inherited neuromuscular disorders The Lancet Child amp Adolescent Health 2 8 600 609 doi 10 1016 S2352 4642 18 30140 8 PMID 30119719 S2CID 52032568 Lim KR Maruyama R Yokota T 2017 Eteplirsen in the treatment of Duchenne muscular dystrophy Drug Design Development and Therapy 11 533 545 doi 10 2147 DDDT S97635 PMC 5338848 PMID 28280301 Eteplirsen is applicable for approximately 14 of patients with DMDmutations Perron and UWA to reap 70 million windfall Retrieved 16 November 2021 FDA grants accelerated approval to first drug for Duchenne muscular dystrophy Press Announcements U S Food amp Drug Administration September 19 2016 Retrieved September 19 2016 Railroading at the FDA Nature Biotechnology 34 11 1078 November 2016 doi 10 1038 nbt 3733 PMID 27824847 a b Exondys EPAR European Medicines Agency EMA Retrieved 13 August 2020 a b Eteplirsen prescribing information PDF FDA September 2016 Anthony K Feng L Arechavala Gomeza V Guglieri M Straub V Bushby K et al October 2012 Exon skipping quantification by quantitative reverse transcription polymerase chain reaction in Duchenne muscular dystrophy patients treated with the antisense oligomer eteplirsen Human Gene Therapy Methods 23 5 336 45 doi 10 1089 hgtb 2012 117 PMID 23075107 Moulton HM Moulton JD December 2010 Morpholinos and their peptide conjugates therapeutic promise and challenge for Duchenne muscular dystrophy Biochimica et Biophysica Acta BBA Biomembranes 1798 12 2296 303 doi 10 1016 j bbamem 2010 02 012 PMID 20170628 a b c Eteplirsen PDF FDA Briefing Document 25 April 2016 Kole R Leppert BJ July 2012 Targeting mRNA splicing as a potential treatment for Duchenne muscular dystrophy Discovery Medicine 14 74 59 69 PMID 22846203 Mendell JR Rodino Klapac LR Sahenk Z Roush K Bird L Lowes LP et al November 2013 Eteplirsen for the treatment of Duchenne muscular dystrophy Annals of Neurology 74 5 637 47 doi 10 1002 ana 23982 PMID 23907995 S2CID 24359589 FDA Accepts Sarepta s NDA for Eteplirsen Rare Disease Report Archived from the original on 2015 08 28 Retrieved 2015 08 28 Pollack Andrew 2016 04 25 Advisers to F D A Vote Against Duchenne Muscular Dystrophy Drug The New York Times Column To appease a patient lobby did the FDA approve a 300 000 drug that doesn t work Michael Hiltzik Los Angeles Times October 28 2016 Going Its Own Way European Regulators Reject Sarepta s Exondys 51 for DMD BioSpace Retrieved 2019 12 14 Anwar S Yokota T August 2020 Golodirsen for Duchenne muscular dystrophy Drugs of Today 56 8 491 504 doi 10 1358 dot 2020 56 8 3159186 PMID 33025945 S2CID 222183389 Dhillon S Jul 2020 Viltolarsen first approval Drugs 80 10 1027 1031 doi 10 1007 s40265 020 01339 3 PMID 32519222 S2CID 219542850 FDA Approves Targeted Treatment for Rare Duchenne Muscular Dystrophy Mutation Food and Drug Administration 25 February 2021 ICER sees current DMD therapies as too pricey but notes data limitations BioPharma Dive Retrieved 2019 12 14 External links Edit Eteplirsen Drug Information Portal U S National Library of Medicine Portal Medicine Retrieved from https en wikipedia org w index php title Eteplirsen amp oldid 1131890842, wikipedia, wiki, book, books, library,

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