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Wikipedia

Bremelanotide

August 25, 2023

Bremelanotide, sold under the brand name Vyleesi, is a medication used to treat low sexual desire in women.[2] Specifically it is used for low sexual desire which occurs before menopause and is not due to medical problems, psychiatric problems, or problems within the relationship.[3][4][2] It is given by an injection just under the skin of the thigh or abdomen.[2][4]

Bremelanotide
Clinical data
Pronunciation/ˌbrɛmɪˈlænətd/ (listen)
Trade namesVyleesi
Other namesPT-141; Rekynda, bremelanotide acetate (USAN US)
AHFS/Drugs.comMonograph
MedlinePlusa619054
License data
Routes of
administration		Subcutaneous[1]
Drug classCentral nervous system agent
ATC code
Legal status
Legal status
Pharmacokinetic data
BioavailabilitySC: ~100%[1]
Protein binding21%[1]
MetabolismHydrolysis of peptide bonds[1]
Elimination half-life2.7 hours[1]
ExcretionUrine: 64.8%
Feces: 22.8%
Identifiers
  • (3S,6S,9R,12S,15S,23S)-15-[(N-Acetyl-L-norleucyl)amino]-9-benzyl-6-{3-[(diaminomethylidene)amino]propyl}-12-(1H-imidazol-5-ylmethyl)-3-(1H-indol-3-ylmethyl)-2,5,8,11,14,17-hexaoxo-1,4,7,10,13,18-hexaazacyclotricosane-23-carboxylic acid
CAS Number
  • 189691-06-3 Y
PubChem CID
  • 9941379
DrugBank
  • DB11653 Y
ChemSpider
  • 8116997 Y
UNII
  • 6Y24O4F92S
KEGG
  • D06569 Y
ChEMBL
  • ChEMBL2070241 Y
CompTox Dashboard (EPA)
  • DTXSID40893711
Chemical and physical data
FormulaC50H68N14O10
Molar mass1025.182 g·mol−1
3D model (JSmol)
  • Interactive image
  • O=C(C)N[C@@H](CCCC)C(N[C@@H]1C(N[C@@H](CC2=CNC=N2)C(N[C@H](CC3=CC=CC=C3)C(N[C@@H](CCC/N=C(N)\N)C(N[C@@H](CC4=CNC5C=CC=CC45)C(N[C@@H](CCCCNC(C1)=O)C(O)=O)=O)=O)=O)=O)=O)=O
  • InChI=1S/C50H68N14O10/c1-3-4-16-35(58-29(2)65)43(67)64-41-25-42(66)54-20-11-10-18-37(49(73)74)60-46(70)39(23-31-26-56-34-17-9-8-15-33(31)34)62-44(68)36(19-12-21-55-50(51)52)59-45(69)38(22-30-13-6-5-7-14-30)61-47(71)40(63-48(41)72)24-32-27-53-28-57-32/h5-9,13-15,17,26-28,35-41,56H,3-4,10-12,16,18-25H2,1-2H3,(H,53,57)(H,54,66)(H,58,65)(H,59,69)(H,60,70)(H,61,71)(H,62,68)(H,63,72)(H,64,67)(H,73,74)(H4,51,52,55)/t35-,36-,37-,38+,39-,40-,41-/m0/s1 Y
  • Key:FFHBJDQSGDNCIV-MFVUMRCOSA-N Y
  (verify)

Common side effects include nausea, pain at the site of injection, and headache.[2] It may also cause a temporary increase in blood pressure and decrease in heart rate after each dose, and darkening of the gums, face, and breasts.[4] The medication is a peptide and acts by activating the melanocortin receptors.[1][5]

Bremelanotide was approved for medical use in the United States in 2019.[2] It was developed by Palatin Technologies.[6] The U.S. Food and Drug Administration (FDA) considers it to be a first-in-class medication.[7]

Medical uses

Bremelanotide is used for the treatment of generalized hypoactive sexual desire disorder (HSDD) in premenopausal women.[3][8] Specifically it is only recommended in those who have the condition without an underlying cause, such as medical, psychiatric, or relationship problems.[3][2]

It should be used at least 45 minutes before anticipated sexual activity.[3] Only one dose per 24 hours or no more than eight doses per month is recommended.[3] It should be stopped after eight weeks if there is no improvement in sexual desire and associated distress.[3]

Contraindications

Due to its effects on blood pressure (generally a transient increase in systolic blood pressure by 6 mmHg, and diastolic blood pressure by 3 mmHg), bremelanotide is considered contraindicated in people with uncontrolled high blood pressure or cardiovascular disease.[1] As long as bremelanotide is not used more than once in one day, it is not expected to cause more severe increases in blood pressure.[1]

Side effects

The most frequently encountered side effect of bremelanotide is nausea (40.0%), which may be intolerable to some people.[1] The use of anti-nausea medications (e.g. ondansetron) prior to administration of bremelanotide may help to reduce the nausea.[1] Other side effects may include flushing (20.3%), injection site reactions (13.2%), headache (11.3%), vomiting (4.8%), cough (3.3%), fatigue (3.2%), hot flushes (2.7%), paresthesia (2.6%), dizziness (2.2%), and nasal congestion (2.1%).[1][9][10] Discoloration of the skin, specifically hyperpigmentation, may occur—especially if bremelanotide is used more than eight times in one month.[1] The discoloration may not resolve upon stopping use of bremelanotide, and may occur on the face, gums, or breasts.[1] Experiments in animals, even at high doses, failed to find any negative consequence of bremelanotide on fertility.[1]

Side effects of bremelanotide in phase 3 clinical trials
Side effect Placebo (n = 620) Bremelanotide 1.75 mg (n = 627)
n % n %
Nausea 8 1.3 251 40.0
Flushing 2 0.3 127 20.3
Headache 12 1.9 71 11.3
Injection site reaction 3 0.5 34 5.4
Vomiting 1 0.2 30 4.8
Cough 8 1.3 21 3.3
Fatigue 3 0.5 20 3.2
Injection site erythema 1 0.2 18 2.9
Hot flush 1 0.2 17 2.7
Paresthesia 0 0.0 16 2.6
Dizziness 3 0.5 14 2.2
Injection site pruritus 1 0.2 13 2.1
Abdominal pain 4 0.6 12 1.9
Myalgia 1 0.2 11 1.8
Summary: Side effects of bremelanotide with a ≥1% incidence in a combined analysis of two phase 3, double-blind, placebo controlled-clinical trials evaluating safety and efficacy at a daily dosage of 1.75 mg. Nausea was very common and occurred after a median time of 30 minutes for a median duration of 2.4 hours. "Across both studies, seven patients who received bremelanotide reported 10 treatment-emergent serious adverse events, and three patients who received placebo reported four treatment-emergent serious adverse events." Most side effects were reported to be transient and were "mild or moderate in intensity". Bremelanotide had a "favourable" safety profile. Sources: See template.

Interactions

Bremelanotide does not meaningfully interact with alcohol, unlike flibanserin (for which the interaction with alcohol is a major barrier to its use).[11][12] However, bremelanotide does interact with certain medications that people take by mouth. By slowing gastric motility, bremelanotide is thought to reduce the oral absorption (bioavailability) of certain medications, such as naltrexone and indomethacin.[1]

Pharmacology

Pharmacodynamics

Bremelanotide is a non-selective agonist of the melanocortin receptors, MC1 through MC5 (with the exception of MC2, the receptor of ACTH), but acting primarily as an MC3 and MC4 receptor agonist.[13][9][5]

Pharmacokinetics

The bioavailability of bremelanotide with subcutaneous injection is about 100%.[1] Following a subcutaneous injection of bremelanotide, maximal levels occur after about one hour, with a range of 0.5 to 1.0 hours.[1] The plasma protein binding of bremelanotide is 21%.[1] Bremelanotide is metabolized via hydrolysis of its peptide bonds.[1] The elimination half-life of bremelanotide is 2.7 hours, with a range of 1.9 to 4.0 hours.[1] Bremelanotide is excreted 64.8% in urine and 22.8% in feces.[1]

Chemistry

Bremelanotide is a cyclic heptapeptide lactam analogue of α-melanocyte-stimulating hormone (α-MSH).[10] It has the amino acid sequence Ac-Nle-cyclo[Asp-His-D-Phe-Arg-Trp-Lys]-OH,[14] and is also known as cyclo-Ac-[Nle4,Asp5,D-Phe7,Lys10]α-MSH-(4-10) (a substitutional name). Bremelanotide is an active metabolite of melanotan II that lacks the C-terminal amide group.[15]

Aside from melanotan II and endogenous melanocyte-stimulating hormones like α-MSH, other peptide analogues of the same family as bremelanotide include afamelanotide (NDP-α-MSH), modimelanotide, and setmelanotide.

History

Studies in the early 1960s showed that administration of α-MSH caused sexual arousal in rats, sparking interest in α-MSH. In the 1980s, scientists at University of Arizona began developing α-MSH and analogs as potential sunless tanning agents. They synthesized and tested several analogs, including peptides they subsequently named, melanotan-I and melanotan II.[13][15]

Very early in the process one of the scientists, Mac Hadley,[15] who was conducting experiments on himself with the peptide melanotan II, injected himself with twice the dose he intended and experienced an eight-hour erection, along with nausea and vomiting.[13]

To pursue the tanning agent, melanotan-I was licensed by Competitive Technologies, a technology transfer company operating on behalf of University of Arizona, to an Australian startup called Epitan,[16][17] which changed its name to Clinuvel in 2006.[18]

To pursue the sexual dysfunction agent, melanotan II was licensed by Competitive Technologies to Palatin Technologies.[15] Palatin ceased development of melanotan-II in 2000, and synthesized, patented, and began to develop bremelanotide, a likely metabolite of melanotan-II that differs from melanotan-II in that it has a hydroxyl group where melanotan-II has an amide.[13][19] Competitive Technologies sued Palatin for breach of contract and to try to claim ownership of bremelanotide;[19] the parties settled in 2008, with Palatin retaining rights to bremelanotide, returning rights to melanotan-II to Competitive Technologies, and paying $800,000.[20]

In August 2004, Palatin signed an agreement with King Pharmaceuticals to co-develop bremelanotide in the US and jointly license it outside the US; King paid Palatin $20M upfront.[21]

Palatin conducted Phase II trials of intranasal bremelanotide in both female sexual dysfunction (FSD) and male erectile dysfunction (ED) but these trials were halted by the FDA in 2007, due to increased blood pressure in clinical trial subjects; Palatin stopped development of the intranasal formulation in 2008.[22][9][23] Four trials were conducted in ED, the last being a Phase IIb published in 2008.[23] King terminated the co-development agreement shortly after the FDA halted the trials.[24]

The drug was then reformulated to be delivered by injection and trials continued in FSD. A phase II dose-finding trial in FSD in which the drug was administered 45 minutes before sex showed promise at the highest dose and only transient signs of high blood pressure; two Phase III trials were launched at the end of 2014.[5][10] Palatin launched the Phase III trials with bremelanotide administered via an autoinjector.[25]

In 2014, Palatin licensed European rights to bremelanotide to Gedeon Richter Plc. for around $10 million, and Palatin received a milestone payment of around $3 million when it started the Phase III trials in the US. In September 2016, Palatin and Gedeon RIchter terminated that agreement.[25]

In November 2016, Palatin announced results of the Phase III trials, and shortly thereafter began seeking a partner to complete development in the US.[26] In January 2017, Palatin and AMAG Pharmaceuticals agreed that AMAG exclusively would complete development and market bremelanotide in North America and the two would work together to license it in other territories; AMAG agreed to pay $60 million upfront, up to $80 million in regulatory milestones, up to $300 million in sales milestones, and tiered royalties ranging from high single digit to low double digit percentages.[27]

A New Drug Application of bremelanotide for female sexual dysfunction was accepted by the U.S. Food and Drug Administration (FDA) in June 2018, with a Prescription Drug User Fee Act (PDUFA) goal date set for 23 March 2019.[28] It was approved for use in the United States in June 2019.[3][29][30]

References

  1. ^ a b c d e f g h i j k l m n o p q r s t u "Vyleesi- bremelanotide injection". DailyMed. 10 September 2019. Retrieved 20 November 2019.
  2. ^ a b c d e f "Bremelanotide Acetate Monograph for Professionals". Drugs.com. Retrieved 24 October 2019.
  3. ^ a b c d e f g "FDA approves new treatment for hypoactive sexual desire disorder in premenopausal women". U.S. Food and Drug Administration (FDA) (Press release). 21 June 2019. from the original on 20 November 2019. Retrieved 24 October 2019.  This article incorporates text from this source, which is in the public domain.
  4. ^ a b c "Drug Trials Snapshots: Vyleesi". U.S. Food and Drug Administration (FDA). 12 July 2019. from the original on 20 November 2019. Retrieved 20 November 2019.  This article incorporates text from this source, which is in the public domain.
  5. ^ a b c Kingsberg SA, Clayton AH, Pfaus JG (November 2015). "The Female Sexual Response: Current Models, Neurobiological Underpinnings and Agents Currently Approved or Under Investigation for the Treatment of Hypoactive Sexual Desire Disorder". CNS Drugs. 29 (11): 915–33. doi:10.1007/s40263-015-0288-1. PMID 26519340. S2CID 7437096.
  6. ^ "Bremelanotide". AdisInsight. Retrieved 6 April 2017.
  7. ^ "New Drug Therapy Approvals 2019". U.S. Food and Drug Administration. 31 December 2019. Retrieved 15 September 2020.
  8. ^ Frellick M. "FDA Approves New Libido-Boosting Drug for Premenopausal Women". Medscape. WebMD LLC. Retrieved 22 June 2019.
  9. ^ a b c Gelman F, Atrio J (January 2017). "Flibanserin for hypoactive sexual desire disorder: place in therapy". Therapeutic Advances in Chronic Disease. 8 (1): 16–25. doi:10.1177/2040622316679933. PMC 5298357. PMID 28203348.
  10. ^ a b c Belkin ZR, Krapf JM, Goldstein AT (February 2015). "Drugs in early clinical development for the treatment of female sexual dysfunction". Expert Opinion on Investigational Drugs. 24 (2): 159–67. doi:10.1517/13543784.2015.978283. PMID 25376023. S2CID 207477620.
  11. ^ Garde D (20 June 2019). "Experimental drug for women revives an intense debate on sexual desire". STAT. Retrieved 23 June 2019.
  12. ^ Clayton AH, Kingsberg SA, Goldstein I (June 2018). "Evaluation and Management of Hypoactive Sexual Desire Disorder". Sexual Medicine. 6 (2): 59–74. doi:10.1016/j.esxm.2018.01.004. PMC 5960024. PMID 29523488.
  13. ^ a b c d King SH, Mayorov AV, Balse-Srinivasan P, Hruby VJ, Vanderah TW, Wessells H (2007). "Melanocortin receptors, melanotropic peptides and penile erection". Current Topics in Medicinal Chemistry. 7 (11): 1098–1106. doi:10.2174/1568026610707011111. PMC 2694735. PMID 17584130.
  14. ^ "Proposed INN List 95" (PDF). WHO Drug Information. 20 (2): 124. 2006.
  15. ^ a b c d Hadley ME (October 2005). "Discovery that a melanocortin regulates sexual functions in male and female humans". Peptides. 26 (10): 1687–9. doi:10.1016/j.peptides.2005.01.023. PMID 15996790. S2CID 22559801.
  16. ^ "EpiTan focuses on Melanotan, a potential blockbuster". The Pharma Letter. 1 November 2004.
  17. ^ Hadley ME, Dorr RT (April 2006). "Melanocortin peptide therapeutics: historical milestones, clinical studies and commercialization". Peptides. 27 (4): 921–30. doi:10.1016/j.peptides.2005.01.029. PMID 16412534. S2CID 21025287.
  18. ^ "Epitan changes name to Clinuvel, announces new clinical program". LabOnline. 27 February 2006.
  19. ^ a b (Press release). Palatin Technologies. 12 September 2007. Archived from the original on 7 April 2017. Retrieved 6 April 2017.
  20. ^ (Press release). Palatin Technologies. 22 January 2008. Archived from the original on 6 April 2017. Retrieved 6 April 2017.
  21. ^ "Form 10-K for the year ended June 30, 2004". Palatin via SEC EDGAR. 13 September 2004.
  22. ^ Lodise NM (April 2013). "Hypoactive sexual desire disorder in women: treatment options beyond testosterone and approaches to communicating with patients on sexual health". Pharmacotherapy. 33 (4): 411–21. doi:10.1002/phar.1209. PMID 23553810. S2CID 206357650.
  23. ^ a b Ückert S, Bannowsky A, Albrecht K, Kuczyk MA (November 2014). "Melanocortin receptor agonists in the treatment of male and female sexual dysfunctions: results from basic research and clinical studies". Expert Opinion on Investigational Drugs. 23 (11): 1477–83. doi:10.1517/13543784.2014.934805. PMID 25096243. S2CID 22665242.
  24. ^ Nagle M (10 September 2007). "Erectile dysfunction drug deemed a flop". Outsourcing Pharma.
  25. ^ a b "Palatin 10K for the fiscal year ended June 30, 2015". Palatin via SEC EDGAR. 18 September 2015.
  26. ^ "Female Viagra: Drugmaker Palatin Is Looking for a Buyer". Fortune. Reuters. 2 November 2016.
  27. ^ "AMAG Pharma closes deal for North America rights to Rekynda". The Pharma Letter. 2 February 2017.
  28. ^ "Press release: FDA Accepts Bremelanotide NDA for Treatment of Hypoactive Sexual Desire Disorder". MD Magazine. Retrieved 27 June 2018.
  29. ^ Nedelman M (21 June 2019). "FDA approves new drug for women with low sexual desire disorder". CNN. Retrieved 23 June 2019.
  30. ^ Cha AE, McGinley L (21 June 2019). "A new 'female Viagra' approved by FDA despite skepticism". The Washington Post. Retrieved 21 June 2019.

External links

  • "Bremelanotide Acetate". Drug Information Portal. U.S. National Library of Medicine.
  • "Drug Approval Package: Vyleesi". U.S. Food and Drug Administration (FDA).

August 25, 2023
bremelanotide, sold, under, brand, name, vyleesi, medication, used, treat, sexual, desire, women, specifically, used, sexual, desire, which, occurs, before, menopause, medical, problems, psychiatric, problems, problems, within, relationship, given, injection, . Bremelanotide sold under the brand name Vyleesi is a medication used to treat low sexual desire in women 2 Specifically it is used for low sexual desire which occurs before menopause and is not due to medical problems psychiatric problems or problems within the relationship 3 4 2 It is given by an injection just under the skin of the thigh or abdomen 2 4 BremelanotideClinical dataPronunciation ˌ b r ɛ m ɪ ˈ l ae n e t aɪ d listen Trade namesVyleesiOther namesPT 141 Rekynda bremelanotide acetate USAN US AHFS Drugs comMonographMedlinePlusa619054License dataUS DailyMed BremelanotideRoutes ofadministrationSubcutaneous 1 Drug classCentral nervous system agentATC codeG02CX05 WHO Legal statusLegal statusUS onlyPharmacokinetic dataBioavailabilitySC 100 1 Protein binding21 1 MetabolismHydrolysis of peptide bonds 1 Elimination half life2 7 hours 1 ExcretionUrine 64 8 Feces 22 8 IdentifiersIUPAC name 3S 6S 9R 12S 15S 23S 15 N Acetyl L norleucyl amino 9 benzyl 6 3 diaminomethylidene amino propyl 12 1H imidazol 5 ylmethyl 3 1H indol 3 ylmethyl 2 5 8 11 14 17 hexaoxo 1 4 7 10 13 18 hexaazacyclotricosane 23 carboxylic acidCAS Number189691 06 3 YPubChem CID9941379DrugBankDB11653 YChemSpider8116997 YUNII6Y24O4F92SKEGGD06569 YChEMBLChEMBL2070241 YCompTox Dashboard EPA DTXSID40893711Chemical and physical dataFormulaC 50H 68N 14O 10Molar mass1025 182 g mol 13D model JSmol Interactive imageSMILES O C C N C H CCCC C N C H 1C N C H CC2 CNC N2 C N C H CC3 CC CC C3 C N C H CCC N C N N C N C H CC4 CNC5C CC CC45 C N C H CCCCNC C1 O C O O O O O O O OInChI InChI 1S C50H68N14O10 c1 3 4 16 35 58 29 2 65 43 67 64 41 25 42 66 54 20 11 10 18 37 49 73 74 60 46 70 39 23 31 26 56 34 17 9 8 15 33 31 34 62 44 68 36 19 12 21 55 50 51 52 59 45 69 38 22 30 13 6 5 7 14 30 61 47 71 40 63 48 41 72 24 32 27 53 28 57 32 h5 9 13 15 17 26 28 35 41 56H 3 4 10 12 16 18 25H2 1 2H3 H 53 57 H 54 66 H 58 65 H 59 69 H 60 70 H 61 71 H 62 68 H 63 72 H 64 67 H 73 74 H4 51 52 55 t35 36 37 38 39 40 41 m0 s1 YKey FFHBJDQSGDNCIV MFVUMRCOSA N Y verify Common side effects include nausea pain at the site of injection and headache 2 It may also cause a temporary increase in blood pressure and decrease in heart rate after each dose and darkening of the gums face and breasts 4 The medication is a peptide and acts by activating the melanocortin receptors 1 5 Bremelanotide was approved for medical use in the United States in 2019 2 It was developed by Palatin Technologies 6 The U S Food and Drug Administration FDA considers it to be a first in class medication 7 Contents 1 Medical uses 2 Contraindications 3 Side effects 4 Interactions 5 Pharmacology 5 1 Pharmacodynamics 5 2 Pharmacokinetics 6 Chemistry 7 History 8 References 9 External linksMedical uses EditBremelanotide is used for the treatment of generalized hypoactive sexual desire disorder HSDD in premenopausal women 3 8 Specifically it is only recommended in those who have the condition without an underlying cause such as medical psychiatric or relationship problems 3 2 It should be used at least 45 minutes before anticipated sexual activity 3 Only one dose per 24 hours or no more than eight doses per month is recommended 3 It should be stopped after eight weeks if there is no improvement in sexual desire and associated distress 3 Contraindications EditDue to its effects on blood pressure generally a transient increase in systolic blood pressure by 6 mmHg and diastolic blood pressure by 3 mmHg bremelanotide is considered contraindicated in people with uncontrolled high blood pressure or cardiovascular disease 1 As long as bremelanotide is not used more than once in one day it is not expected to cause more severe increases in blood pressure 1 Side effects EditThe most frequently encountered side effect of bremelanotide is nausea 40 0 which may be intolerable to some people 1 The use of anti nausea medications e g ondansetron prior to administration of bremelanotide may help to reduce the nausea 1 Other side effects may include flushing 20 3 injection site reactions 13 2 headache 11 3 vomiting 4 8 cough 3 3 fatigue 3 2 hot flushes 2 7 paresthesia 2 6 dizziness 2 2 and nasal congestion 2 1 1 9 10 Discoloration of the skin specifically hyperpigmentation may occur especially if bremelanotide is used more than eight times in one month 1 The discoloration may not resolve upon stopping use of bremelanotide and may occur on the face gums or breasts 1 Experiments in animals even at high doses failed to find any negative consequence of bremelanotide on fertility 1 vte Side effects of bremelanotide in phase 3 clinical trials Side effect Placebo n 620 Bremelanotide 1 75 mg n 627 n n Nausea 8 1 3 251 40 0Flushing 2 0 3 127 20 3Headache 12 1 9 71 11 3Injection site reaction 3 0 5 34 5 4Vomiting 1 0 2 30 4 8Cough 8 1 3 21 3 3Fatigue 3 0 5 20 3 2Injection site erythema 1 0 2 18 2 9Hot flush 1 0 2 17 2 7Paresthesia 0 0 0 16 2 6Dizziness 3 0 5 14 2 2Injection site pruritus 1 0 2 13 2 1Abdominal pain 4 0 6 12 1 9Myalgia 1 0 2 11 1 8Summary Side effects of bremelanotide with a 1 incidence in a combined analysis of two phase 3 double blind placebo controlled clinical trials evaluating safety and efficacy at a daily dosage of 1 75 mg Nausea was very common and occurred after a median time of 30 minutes for a median duration of 2 4 hours Across both studies seven patients who received bremelanotide reported 10 treatment emergent serious adverse events and three patients who received placebo reported four treatment emergent serious adverse events Most side effects were reported to be transient and were mild or moderate in intensity Bremelanotide had a favourable safety profile Sources See template Interactions EditBremelanotide does not meaningfully interact with alcohol unlike flibanserin for which the interaction with alcohol is a major barrier to its use 11 12 However bremelanotide does interact with certain medications that people take by mouth By slowing gastric motility bremelanotide is thought to reduce the oral absorption bioavailability of certain medications such as naltrexone and indomethacin 1 Pharmacology EditPharmacodynamics Edit Bremelanotide is a non selective agonist of the melanocortin receptors MC1 through MC5 with the exception of MC2 the receptor of ACTH but acting primarily as an MC3 and MC4 receptor agonist 13 9 5 Pharmacokinetics Edit The bioavailability of bremelanotide with subcutaneous injection is about 100 1 Following a subcutaneous injection of bremelanotide maximal levels occur after about one hour with a range of 0 5 to 1 0 hours 1 The plasma protein binding of bremelanotide is 21 1 Bremelanotide is metabolized via hydrolysis of its peptide bonds 1 The elimination half life of bremelanotide is 2 7 hours with a range of 1 9 to 4 0 hours 1 Bremelanotide is excreted 64 8 in urine and 22 8 in feces 1 Chemistry EditBremelanotide is a cyclic heptapeptide lactam analogue of a melanocyte stimulating hormone a MSH 10 It has the amino acid sequence Ac Nle cyclo Asp His D Phe Arg Trp Lys OH 14 and is also known as cyclo Ac Nle4 Asp5 D Phe7 Lys10 a MSH 4 10 a substitutional name Bremelanotide is an active metabolite of melanotan II that lacks the C terminal amide group 15 Aside from melanotan II and endogenous melanocyte stimulating hormones like a MSH other peptide analogues of the same family as bremelanotide include afamelanotide NDP a MSH modimelanotide and setmelanotide History EditStudies in the early 1960s showed that administration of a MSH caused sexual arousal in rats sparking interest in a MSH In the 1980s scientists at University of Arizona began developing a MSH and analogs as potential sunless tanning agents They synthesized and tested several analogs including peptides they subsequently named melanotan I and melanotan II 13 15 Very early in the process one of the scientists Mac Hadley 15 who was conducting experiments on himself with the peptide melanotan II injected himself with twice the dose he intended and experienced an eight hour erection along with nausea and vomiting 13 To pursue the tanning agent melanotan I was licensed by Competitive Technologies a technology transfer company operating on behalf of University of Arizona to an Australian startup called Epitan 16 17 which changed its name to Clinuvel in 2006 18 To pursue the sexual dysfunction agent melanotan II was licensed by Competitive Technologies to Palatin Technologies 15 Palatin ceased development of melanotan II in 2000 and synthesized patented and began to develop bremelanotide a likely metabolite of melanotan II that differs from melanotan II in that it has a hydroxyl group where melanotan II has an amide 13 19 Competitive Technologies sued Palatin for breach of contract and to try to claim ownership of bremelanotide 19 the parties settled in 2008 with Palatin retaining rights to bremelanotide returning rights to melanotan II to Competitive Technologies and paying 800 000 20 In August 2004 Palatin signed an agreement with King Pharmaceuticals to co develop bremelanotide in the US and jointly license it outside the US King paid Palatin 20M upfront 21 Palatin conducted Phase II trials of intranasal bremelanotide in both female sexual dysfunction FSD and male erectile dysfunction ED but these trials were halted by the FDA in 2007 due to increased blood pressure in clinical trial subjects Palatin stopped development of the intranasal formulation in 2008 22 9 23 Four trials were conducted in ED the last being a Phase IIb published in 2008 23 King terminated the co development agreement shortly after the FDA halted the trials 24 The drug was then reformulated to be delivered by injection and trials continued in FSD A phase II dose finding trial in FSD in which the drug was administered 45 minutes before sex showed promise at the highest dose and only transient signs of high blood pressure two Phase III trials were launched at the end of 2014 5 10 Palatin launched the Phase III trials with bremelanotide administered via an autoinjector 25 In 2014 Palatin licensed European rights to bremelanotide to Gedeon Richter Plc for around 10 million and Palatin received a milestone payment of around 3 million when it started the Phase III trials in the US In September 2016 Palatin and Gedeon RIchter terminated that agreement 25 In November 2016 Palatin announced results of the Phase III trials and shortly thereafter began seeking a partner to complete development in the US 26 In January 2017 Palatin and AMAG Pharmaceuticals agreed that AMAG exclusively would complete development and market bremelanotide in North America and the two would work together to license it in other territories AMAG agreed to pay 60 million upfront up to 80 million in regulatory milestones up to 300 million in sales milestones and tiered royalties ranging from high single digit to low double digit percentages 27 A New Drug Application of bremelanotide for female sexual dysfunction was accepted by the U S Food and Drug Administration FDA in June 2018 with a Prescription Drug User Fee Act PDUFA goal date set for 23 March 2019 28 It was approved for use in the United States in June 2019 3 29 30 References Edit a b c d e f g h i j k l m n o p q r s t u Vyleesi bremelanotide injection DailyMed 10 September 2019 Retrieved 20 November 2019 a b c d e f Bremelanotide Acetate Monograph for Professionals Drugs com Retrieved 24 October 2019 a b c d e f g FDA approves new treatment for hypoactive sexual desire disorder in premenopausal women U S Food and Drug Administration FDA Press release 21 June 2019 Archived from the original on 20 November 2019 Retrieved 24 October 2019 This article incorporates text from this source which is in the public domain a b c Drug Trials Snapshots Vyleesi U S Food and Drug Administration FDA 12 July 2019 Archived from the original on 20 November 2019 Retrieved 20 November 2019 This article incorporates text from this source which is in the public domain a b c Kingsberg SA Clayton AH Pfaus JG November 2015 The Female Sexual Response Current Models Neurobiological Underpinnings and Agents Currently Approved or Under Investigation for the Treatment of Hypoactive Sexual Desire Disorder CNS Drugs 29 11 915 33 doi 10 1007 s40263 015 0288 1 PMID 26519340 S2CID 7437096 Bremelanotide AdisInsight Retrieved 6 April 2017 New Drug Therapy Approvals 2019 U S Food and Drug Administration 31 December 2019 Retrieved 15 September 2020 Frellick M FDA Approves New Libido Boosting Drug for Premenopausal Women Medscape WebMD LLC Retrieved 22 June 2019 a b c Gelman F Atrio J January 2017 Flibanserin for hypoactive sexual desire disorder place in therapy Therapeutic Advances in Chronic Disease 8 1 16 25 doi 10 1177 2040622316679933 PMC 5298357 PMID 28203348 a b c Belkin ZR Krapf JM Goldstein AT February 2015 Drugs in early clinical development for the treatment of female sexual dysfunction Expert Opinion on Investigational Drugs 24 2 159 67 doi 10 1517 13543784 2015 978283 PMID 25376023 S2CID 207477620 Garde D 20 June 2019 Experimental drug for women revives an intense debate on sexual desire STAT Retrieved 23 June 2019 Clayton AH Kingsberg SA Goldstein I June 2018 Evaluation and Management of Hypoactive Sexual Desire Disorder Sexual Medicine 6 2 59 74 doi 10 1016 j esxm 2018 01 004 PMC 5960024 PMID 29523488 a b c d King SH Mayorov AV Balse Srinivasan P Hruby VJ Vanderah TW Wessells H 2007 Melanocortin receptors melanotropic peptides and penile erection Current Topics in Medicinal Chemistry 7 11 1098 1106 doi 10 2174 1568026610707011111 PMC 2694735 PMID 17584130 Proposed INN List 95 PDF WHO Drug Information 20 2 124 2006 a b c d Hadley ME October 2005 Discovery that a melanocortin regulates sexual functions in male and female humans Peptides 26 10 1687 9 doi 10 1016 j peptides 2005 01 023 PMID 15996790 S2CID 22559801 EpiTan focuses on Melanotan a potential blockbuster The Pharma Letter 1 November 2004 Hadley ME Dorr RT April 2006 Melanocortin peptide therapeutics historical milestones clinical studies and commercialization Peptides 27 4 921 30 doi 10 1016 j peptides 2005 01 029 PMID 16412534 S2CID 21025287 Epitan changes name to Clinuvel announces new clinical program LabOnline 27 February 2006 a b Palatin Technologies Refutes Competitive Technologies Contention of Material Breach Press release Palatin Technologies 12 September 2007 Archived from the original on 7 April 2017 Retrieved 6 April 2017 Palatin Technologies Announces Litigation Settlement With Competitive Technologies Press release Palatin Technologies 22 January 2008 Archived from the original on 6 April 2017 Retrieved 6 April 2017 Form 10 K for the year ended June 30 2004 Palatin via SEC EDGAR 13 September 2004 Lodise NM April 2013 Hypoactive sexual desire disorder in women treatment options beyond testosterone and approaches to communicating with patients on sexual health Pharmacotherapy 33 4 411 21 doi 10 1002 phar 1209 PMID 23553810 S2CID 206357650 a b Uckert S Bannowsky A Albrecht K Kuczyk MA November 2014 Melanocortin receptor agonists in the treatment of male and female sexual dysfunctions results from basic research and clinical studies Expert Opinion on Investigational Drugs 23 11 1477 83 doi 10 1517 13543784 2014 934805 PMID 25096243 S2CID 22665242 Nagle M 10 September 2007 Erectile dysfunction drug deemed a flop Outsourcing Pharma a b Palatin 10K for the fiscal year ended June 30 2015 Palatin via SEC EDGAR 18 September 2015 Female Viagra Drugmaker Palatin Is Looking for a Buyer Fortune Reuters 2 November 2016 AMAG Pharma closes deal for North America rights to Rekynda The Pharma Letter 2 February 2017 Press release FDA Accepts Bremelanotide NDA for Treatment of Hypoactive Sexual Desire Disorder MD Magazine Retrieved 27 June 2018 Nedelman M 21 June 2019 FDA approves new drug for women with low sexual desire disorder CNN Retrieved 23 June 2019 Cha AE McGinley L 21 June 2019 A new female Viagra approved by FDA despite skepticism The Washington Post Retrieved 21 June 2019 External links Edit Bremelanotide Acetate Drug Information Portal U S National Library of Medicine Drug Approval Package Vyleesi U S Food and Drug Administration FDA Portal Medicine Retrieved from https en wikipedia org w index php title Bremelanotide amp oldid 1139396802, wikipedia, wiki, book, books, library,

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