Literature DB >> 10617600

Sulfation of "estrogenic" alkylphenols and 17beta-estradiol by human platelet phenol sulfotransferases.

R M Harris1, R H Waring, C J Kirk, P J Hughes.   

Abstract

We have investigated the ability of alkylphenols to act as substrates and/or inhibitors of phenol sulfotransferase enzymes in human platelet cytosolic fractions. Our results indicate: (i) straight chain alkylphenols do not interact with the monoamine-sulfating phenol sulfotransferase (SULT1A3); (ii) short chain 4-n-alkylphenols (C < 8) are substrates for the phenol-sulfating enzymes (SULT1A1/2), which exhibit two activity maxima against substrates with alkyl chain lengths of C1-2 and C4-5; (iii) long chain 4-n-substituted alkylphenols (C >/= 8) are poor substrates and act as inhibitors of SULT1A1/2; (iv) human platelets contain two activities, of low and high affinity, capable of sulfating 17beta-estradiol, and 4-n-nonylphenol is a partial mixed inhibitor of the low affinity form of this activity. We conclude that by acting either as substrates or inhibitors of SULT1A1/2, alkylphenols may influence the sulfation, and hence the excretion, of estrogens and other phenol sulfotransferase substrates in humans.

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Year:  2000        PMID: 10617600     DOI: 10.1074/jbc.275.1.159

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  6 in total

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6.  Computational Analysis of Chemical Space of Natural Compounds Interacting with Sulfotransferases.

Authors:  Iglika Lessigiarska; Yunhui Peng; Ivanka Tsakovska; Petko Alov; Nathalie Lagarde; Dessislava Jereva; Bruno O Villoutreix; Arnaud B Nicot; Ilza Pajeva; Tania Pencheva; Maria A Miteva
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  6 in total

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