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Other names | EMATE; J994; Estrone-3-O-sulfamate; 17-Oxoestra-1,3,5(10)-trien-3-yl sulfamate; 3-estra-1,3,5(10)-trien-17-one |
Routes of administration | By mouth |
Drug class | Steroid sulfatase inhibitor |
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Formula | C18H23NO4S |
Molar mass | 349.45 g·mol |
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Estrone sulfamate (EMATE; developmental code name J994), or estrone-3-O-sulfamate, is a steroid sulfatase (STS) inhibitor which has not yet been marketed. It is the C3 sulfamate ester of the estrogen estrone. Unlike other estrogen esters however, EMATE is not an effective prodrug of estrogens. A closely related compound is estradiol sulfamate (E2MATE), which is extensively metabolized into EMATE and has similar properties to it.
EMATE shows high bioavailability and undergoes little or no first-pass metabolism with oral administration. The sulfamate moiety of EMATE results in carbonic anhydrase binding which, in turn, results in EMATE being taken up into and stored in erythrocytes in the blood. Since this occurs in the hepatic portal vein, it prevents EMATE from entering the liver during the first pass with the oral route. The inhibition of STS by EMATE prevents its bioactivation into estrone and estradiol, which in turn accounts for the lack of estrogenicity of EMATE. A short initial peak of estradiol and estrone levels was observed with E2MATE at the start of treatment in humans, followed by very high and long-lasting concentrations of EMATE and estrone sulfate in erythrocytes, observations that are in accordance with STS inhibition.
EMATE is an extremely potent and irreversible inhibitor of STS. It was found to have an IC50Tooltip half-maximal inhibitory concentration of 65 pM for STS inhibition in MCF-7 cells, with an almost complete inhibition of the hydrolysis of physiological concentrations of the steroid sulfates estrone sulfate and dehydroepiandrosterone sulfate in MCF-7 cells observed at a concentration of 1 μM. At a dosage of 1 mg/kg orally or subcutaneously in rats, it effectively abolished estrone and DHEA-S sulfatase activities in all tissues assessed. It also showed a prolonged duration of action, with only a small recovery (<10%) of hepatic STS activity occurring 7 days after a single 10 mg/kg dose in rats.
Due to its ability to prevent the conversion of hormonally inactive steroid sulfates into their hormonally active forms (e.g., estrone sulfate into estrone), STS inhibitors like EMATE have potential applications in the treatment of estrogen-dependent conditions like estrogen receptor-positive breast cancer and endometriosis. However, estrogenicity was paradoxically observed with EMATE in rodents, and this resulted in clinical development of the compound not being pursued. However, E2MATE was investigated as an estradiol prodrug with improved oral pharmacokinetics and little or no first-pass hepatic impact in humans, but was found to completely lack estrogenic effects. Following this, E2MATE was repurposed as an STS inhibitor, and is now under development for the treatment of endometriosis.
See also
References
- ^ Elger W, Barth A, Hedden A, Reddersen G, Ritter P, Schneider B, et al. (2001). "Estrogen sulfamates: a new approach to oral estrogen therapy". Reproduction, Fertility, and Development. 13 (4): 297–305. doi:10.1071/rd01029. PMID 11800168.
- ^ Thomas MP, Potter BV (September 2015). "Estrogen O-sulfamates and their analogues: Clinical steroid sulfatase inhibitors with broad potential". The Journal of Steroid Biochemistry and Molecular Biology. 153: 160–169. doi:10.1016/j.jsbmb.2015.03.012. PMID 25843211. S2CID 24116740.
- ^ Elger W, Schwarz S, Hedden A, Reddersen G, Schneider B (December 1995). "Sulfamates of various estrogens are prodrugs with increased systemic and reduced hepatic estrogenicity at oral application". The Journal of Steroid Biochemistry and Molecular Biology. 55 (3–4): 395–403. doi:10.1016/0960-0760(95)00214-6. PMID 8541236. S2CID 31312.
- ^ Elger W, Wyrwa R, Ahmed G, Meece F, Nair HB, Santhamma B, et al. (January 2017). "Estradiol prodrugs (EP) for efficient oral estrogen treatment and abolished effects on estrogen modulated liver functions". The Journal of Steroid Biochemistry and Molecular Biology. 165 (Pt B): 305–311. doi:10.1016/j.jsbmb.2016.07.008. PMID 27449818. S2CID 26650319.
- ^ Reed MJ, Purohit A (6 December 2012). "Pharmacology of Inhibition of Estrogen-Metabolizing Enzymes". In Oettel M, Schillinger E (eds.). Estrogens and Antiestrogens II: Pharmacology and Clinical Application of Estrogens and Antiestrogen. Springer Science & Business Media. pp. 233–239. ISBN 978-3-642-60107-1.
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