Epristeride
- None
- In general: ℞ (Prescription only)
- (8S,9S,10R,13S,14S,17S)-17-(tert-butylcarbamoyl)-10,13-dimethyl-2,7,8,9,11,12,14,15,16,17-decahydro-1H-cyclopenta[a]phenanthrene-3-carboxylic acid
- 119169-78-7
- 68741
- 10625794
- 39517A04PS
- ChEMBL290823
- DTXSID9048643
- Interactive image
- CC(C)(C)NC(=O)C1CCC2C3C\C=C4\C=C(/CCC4(C)C3CCC12C)C(O)=O
- InChI=1S/C25H37NO3/c1-23(2,3)26-21(27)20-9-8-18-17-7-6-16-14-15(22(28)29)10-12-24(16,4)19(17)11-13-25(18,20)5/h6,14,17-20H,7-13H2,1-5H3,(H,26,27)(H,28,29)
- Key:VAPSMQAHNAZRKC-UHFFFAOYSA-N
Epristeride, sold under the brand names Aipuliete and Chuanliu, is a medication which is used in the treatment of enlarged prostate in China.[3][4][5] It is taken by mouth.[1]
Epristeride is a 5α-reductase inhibitor and works by decreasing the production of dihydrotestosterone (DHT), an androgen sex hormone, in certain parts of the body like the prostate gland.[6][7][8] It inhibits two of the three forms of 5α-reductase but is of relatively low efficacy and can decrease DHT levels in the blood only by about 25 to 54%.[8]
Epristeride was under development for the treatment of enlarged prostate, scalp hair loss, and acne in the United States and other countries in the 1990s but did not complete development in these countries.[6][4] Instead, it was developed and introduced for the treatment of enlarged prostate in China in 2000.[4]
Medical uses
Epristeride is used in the treatment of benign prostatic hyperplasia (BPH), otherwise known as enlarged prostate.[3][4]
Pharmacology
Pharmacodynamics
Epristeride is a selective, transition-state, non-competitive or uncompetitive, irreversible inhibitor of 5α-reductase,[6][7] and is specific to the type II isoform of the enzyme similarly to finasteride and turosteride but unlike dutasteride.[8]
Epristeride is unique in its mechanism of action relative to finasteride and dutasteride in that it binds irreversibly to 5α-reductase and results in the formation of an unproductive complex of the 5α-reductase enzyme, the substrate testosterone, and the cofactor NADPH.[8][9] For this reason, testosterone is caught in a trap, and it was initially speculated that the reciprocal increase in intraprostatic levels of testosterone seen with finasteride and dutasteride should not happen with epristeride.[8][9] However, subsequent clinical data have not supported this hypothesis.[8] Moreover, in spite of the fact that epristeride is a very potent inhibitor of 5α-reductase type II (0.18–2 nM), it has been found to reduce circulating levels of dihydrotestosterone (DHT) by only 25 to 54% following 8 days of therapy over a dosage range of 0.4 to 160 mg/day.[8] For this reason, relative to other 5α-reductase inhibitors like finasteride and dutasteride, the degree of DHT suppression with epristeride falls short of that desirable for full clinical benefit.[8]
Pharmacokinetics
The oral bioavailability of epristeride is 93%.[2] It has an elimination half-life of 26 hours.[2]
Chemistry
Epristeride, also known as 17β-(tert-butylcarbamoyl)androsta-3,5-diene-3-carboxylic acid, is a synthetic androstane steroid.
History
Epristeride was under development for the treatment of BPH, androgenic alopecia (pattern hair loss), and acne vulgaris by SmithKline Beecham (now GlaxoSmithKline) in the 1990s and reached phase III clinical trials in the United States, United Kingdom, and Japan,[6] but ultimately was never marketed in these countries.[4] Instead, epristeride was developed by Ono Pharmaceutical and introduced for the treatment of BPH in China in 2000.[4]
Society and culture
Generic names
Epristeride is the generic name of the drug and its INNTooltip International Nonproprietary Name, USANTooltip United States Adopted Name, BANTooltip British Approved Name, and JANTooltip Japanese Accepted Name.[5]
Brand names
Epristeride is marketed under the brand names Aipuliete and Chuanliu in China.[5][4]
Synthesis
![](http://upload.wikimedia.org/wikipedia/commons/thumb/2/22/Epristeride_synthesis.svg/500px-Epristeride_synthesis.svg.png)
Oxidation of the methylketone in progesterone to a carboxylic acid gives Etienic acid [302-97-6] (1). Halogenation with phosphorus tribromide converts the enone to the enol bromide and the acid to the acyl halide; mild base hydrolyzes the latter back to the free acid giving PC10474840 (2). Halogenation with oxalyl chloride and then Schotten-Baumann reaction with tertiary-butylamine then gives the corresponding amide, PC10320718 (3). An indirect process is then used to produce the intermediate 3-lithio reagent. Thus, reaction of the intermediate with ethylmagnesium chloride exchanges the halide at 3 to form the 3-organomagesium reagent and ethyl chloride. Addition of butyl lithium to the reaction mixture then leads to the corresponding lithio derivative. Reaction with carbon dioxide leads to the carbonation of the 3 position. On workup there is thus obtained the carboxylic acid epristeride.
References
- ^ a b Copeland RA, Sanderson P (2 August 2003). "Enzymes and enzyme inhibitors". In Liljefors T, Krogsgaard-Larsen P, Madsen U (eds.). Textbook of Drug Design and Discovery (Third ed.). CRC Press. pp. 400–. ISBN 978-0-203-30137-1.
- ^ a b c d Benincosa LJ, Audet PR, Lundberg D, Zariffa N, Jorkasky DK (April 1996). "Pharmacokinetics and absolute bioavailability of epristeride in healthy male subjects". Biopharmaceutics & Drug Disposition. 17 (3): 249–258. doi:10.1002/(SICI)1099-081X(199604)17:3<249::AID-BDD952>3.0.CO;2-E. PMID 8983399.
- ^ a b Morton IK, Hall JM (31 October 1999). Concise Dictionary of Pharmacological Agents: Properties and Synonyms. Springer Science & Business Media. pp. 113–. ISBN 978-0-7514-0499-9.
- ^ a b c d e f g "Epristeride". AdisInsight. Springer Nature Switzerland AG.
- ^ a b c "List of 21 Benign Prostatic Hyperplasia Medications Compared". Drugs.com.
- ^ a b c d Hedge SS (May 1998). "Epristeride SmithKline Beecham". IDrugs. 1 (1): 152–157. PMID 18465521.
- ^ a b Berthaut I, Mestayer C, Portois MC, Cussenot O, Mowszowicz I (August 1997). "Pharmacological and molecular evidence for the expression of the two steroid 5 alpha-reductase isozymes in normal and hyperplastic human prostatic cells in culture". The Prostate. 32 (3): 155–163. doi:10.1002/(SICI)1097-0045(19970801)32:3<155::AID-PROS1>3.0.CO;2-K. PMID 9254894. S2CID 19849292.
- ^ a b c d e f g h Frye SV (February 1996). "Inhibitors of 5 alpha-Reductase". Current Pharmaceutical Design. 2 (1). Bentham Science Publishers: 70–.
- ^ a b Hoffman J, Sommer A (30 January 2007). "Anti-hormome Therapy: Principles of Endocrine Therapy of Cancer". In Bradbury R (ed.). Cancer. Springer Science & Business Media. pp. 49–. ISBN 978-3-540-33120-9.
- ^ Audet, P. R., Baine, N. H., Benincosa, L. J., Holt, D. A., Wier, P. J., Rappaport, E. B., Metcalf, B. W., Levy, M. A. (1994). "Epristeride < Rec INN; USAN >". Drugs of the Future. 19 (7): 646. doi:10.1358/dof.1994.019.07.257360.
- ^ Holt, Dennis A.; Levy, Mark A.; Oh, Hye Ja; Erb, Jill M.; Heaslip, Julie I.; Brandt, Martin; Lan-Hargest, Hsuan Yin; Metcalf, Brian W. (1990). "Inhibition of steroid 5.alpha.-reductase by unsaturated 3-carboxy steroids". Journal of Medicinal Chemistry. 33 (3): 943–950. doi:10.1021/jm00165a010.
- ^ Dennis A. Holt, Mark A. Levy, Brian W. Metcalf, U.S. patent 4,910,226 (1990 to Smithkline Beckman Corporation).
- ^ Dennis A. Holt, Conrad J. Kowalski, Mark A. Levy, Brian W. Metcalf, Ann M. Tickner, U.S. patent 5,017,568 (1991 to Smithkline Beecham Corporation).
- ^ Neil Howard Baine, WO1993014106 (to SmithKline Beecham Corp).
- ^ McGuire∗, M. A., Sorenson, E., Klein, D. N., Baine, N. H. (May 1998). "Palladium and Nickel Catalyzed Hydroxycarbonylation of a Steroidal Bromodiene in the Synthesis of Episteride, a Potent 5α-Reductase Inhibitor". Synthetic Communications. 28 (9): 1611–1615. doi:10.1080/00397919808006865.
- ^ Weisheng Tian, Zheng Zhu, Qingjiang Liao, Yikang Wu (August 1998). "A practical synthesis of 3-substituted Δ3,5(6)-Steroids as new potential 5α-reductase inhibitor". Bioorganic & Medicinal Chemistry Letters. 8 (15): 1949–1952. doi:10.1016/S0960-894X(98)00339-4.
- ^ Baine, N. H., Owings, F. F., Kline, D. N., Resnick, T., Ping, L.-J., Fox, M., Mewshaw, R. E., Tickner, A. M., Kowalski, C. J. (October 1994). "Improved Syntheses of Epristeride, a Potent Human 5.alpha.-Reductase Inhibitor". The Journal of Organic Chemistry. 59 (20): 5987–5989. doi:10.1021/jo00099a031.
- ^ Shu, Arthur Y. L.; Heys, J. Richard (1994). "Synthesis of carbon-14 and tritiated steroidal 5α-reductase inhibitors". Journal of Labelled Compounds and Radiopharmaceuticals. 34 (7): 587–596. doi:10.1002/jlcr.2580340702.
External links
- Epristeride - AdisInsight
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