Sulfation of minoxidil by human liver phenol sulfotransferase

硫酸化 硫转移酶 化学 米诺地尔 脱氢表雄酮 羟类固醇 胞浆 生物化学 基质(水族馆) 内分泌学 内科学 生物 激素 雄激素 医学 生态学 脱氢酶
作者
Charles N. Falany,Elizabeth A. Kerl
出处
期刊:Biochemical Pharmacology [Elsevier BV]
卷期号:40 (5): 1027-1032 被引量:70
标识
DOI:10.1016/0006-2952(90)90489-8
摘要

The N,O-sulfate of minoxidil (Mnx) is the active agent in producing the vasodilation and the hair-growth stimulating responses observed with Mnx treatment. In this report, Mnx sulfation activity was assayed in cytosol prepared from several normal human livers, and Mnx sulfation was shown to correlate significantly with the activity of the phenol-sulfating form of phenol sulfotransferase (P-PST) activity in the same livers. No correlation was observed between Mnx sulfation and the dopamine or dehydroepiandrosterone (DHEA) sulfotransferase activities present in human liver. Mnx sulfation also copurified with P-PST activity during the purification of P-PST from human liver. During the purification procedure, Mnx and p-nitrophenol sulfotransferase (P-PST) activities were resolved from the dopamine and DHEA sulfation activities catalyzed by the monoamine-sulfating form of phenol sulfotransferase (M-PST) and DHEA sulfotransferase respectively. Also, purified DHEA sulfotransferase was not capable of sulfating Mnx, and no data were obtained to indicate that Mnx is a substrate for M-PST. p-Nitrophenol, a substrate for P-PST, was demonstrated to be a competitive inhibitor of Mnx sulfation catalyzed by purified P-PST when Mnx was the variable substrate. These results indicate that Mnx is sulfated and, therefore, bioactivated by P-PST in human liver.

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