Source:http://linkedlifedata.com/resource/pubmed/id/11087571
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pubmed-article:11087571 | rdf:type | pubmed:Citation | lld:pubmed |
pubmed-article:11087571 | lifeskim:mentions | umls-concept:C0014912 | lld:lifeskim |
pubmed-article:11087571 | lifeskim:mentions | umls-concept:C0052456 | lld:lifeskim |
pubmed-article:11087571 | lifeskim:mentions | umls-concept:C0038477 | lld:lifeskim |
pubmed-article:11087571 | lifeskim:mentions | umls-concept:C0243077 | lld:lifeskim |
pubmed-article:11087571 | pubmed:issue | 23 | lld:pubmed |
pubmed-article:11087571 | pubmed:dateCreated | 2000-12-4 | lld:pubmed |
pubmed-article:11087571 | pubmed:abstractText | The steroid sulfatase or steryl sulfatase is a microsomal enzyme widely distributed in human tissues that catalyzes the hydrolysis of sulfated 3-hydroxy steroids to the corresponding free active 3-hydroxy steroids. Since androgens and estrogens may be synthesized inside the cancerous cells starting from dehydroepiandrosterone sulfate (DHEAS) and estrone sulfate (E(1)S) available in blood circulation, the use of therapeutic agents that inhibit steroid sulfatase activity may be a rewarding approach to the treatment of androgeno-sensitive and estrogeno-sensitive diseases. In the present study, we report the chemical synthesis and biological evaluation of a new family of steroid sulfatase inhibitors. The inhibitors were designed by adding an alkyl, a phenyl, a benzyl, or a benzyl substituted at position 17alpha of estradiol (E(2)), a C18-steroid, and enzymatic assays were performed using the steroid sulfatase of homogenized JEG-3 cells or transfected in HEK-293 cells. We observed that a hydrophobic substituent induces powerful inhibition of steroid sulfatase while a hydrophilic one was weak. Although a hydrophobic group at the 17alpha-position increased the inhibitory activity, the steric factors contribute to the opposite effect. As exemplified by 17alpha-decyl-E(2) and 17alpha-dodecyl-E(2), a long flexible side chain prevents adequate fitting into the enzyme catalytic site, thus decreasing capacity to inhibit the steroid sulfatase activity. In the alkyl series, the best compromise between hydrophobicity and steric hindrance was obtained with the octyl group (IC(50) = 440 nM), but judicious branching of side chain could improve this further. Benzyl substituted derivatives of estradiol were better inhibitors than alkyl analogues. Among the series of 17alpha-(benzyl substituted)-E(2) derivatives studied, the 3'-bromobenzyl, 4'-tert-butylbenzyl, 4'-butylbenzyl, and 4'-benzyloxybenzyl groups provided the most potent inhibition of steroid sulfatase transformation of E(1)S into E(1) (IC(50) = 24, 28, 25, and 22 nM, respectively). As an example, the tert-butylbenzyl group increases the ability of the E(2) nucleus to inhibit the steroid sulfatase by 3000-fold, and it also inhibits similarly the steroid sulfatase transformations of both natural substrates, E(1)S and DHEAS. Interestingly, the newly reported family of steroid sulfatase inhibitors acts by a reversible mechanism of action that is different from the irreversible mechanism of the known inhibitor estrone sulfamate (EMATE). | lld:pubmed |
pubmed-article:11087571 | pubmed:language | eng | lld:pubmed |
pubmed-article:11087571 | pubmed:journal | http://linkedlifedata.com/r... | lld:pubmed |
pubmed-article:11087571 | pubmed:citationSubset | IM | lld:pubmed |
pubmed-article:11087571 | pubmed:chemical | http://linkedlifedata.com/r... | lld:pubmed |
pubmed-article:11087571 | pubmed:chemical | http://linkedlifedata.com/r... | lld:pubmed |
pubmed-article:11087571 | pubmed:chemical | http://linkedlifedata.com/r... | lld:pubmed |
pubmed-article:11087571 | pubmed:chemical | http://linkedlifedata.com/r... | lld:pubmed |
pubmed-article:11087571 | pubmed:status | MEDLINE | lld:pubmed |
pubmed-article:11087571 | pubmed:month | Nov | lld:pubmed |
pubmed-article:11087571 | pubmed:issn | 0022-2623 | lld:pubmed |
pubmed-article:11087571 | pubmed:author | pubmed-author:LachanceRR | lld:pubmed |
pubmed-article:11087571 | pubmed:author | pubmed-author:LabrieFF | lld:pubmed |
pubmed-article:11087571 | pubmed:author | pubmed-author:Luu-TheVV | lld:pubmed |
pubmed-article:11087571 | pubmed:author | pubmed-author:PoirierDD | lld:pubmed |
pubmed-article:11087571 | pubmed:author | pubmed-author:BoivinR PRP | lld:pubmed |
pubmed-article:11087571 | pubmed:issnType | lld:pubmed | |
pubmed-article:11087571 | pubmed:day | 16 | lld:pubmed |
pubmed-article:11087571 | pubmed:volume | 43 | lld:pubmed |
pubmed-article:11087571 | pubmed:owner | NLM | lld:pubmed |
pubmed-article:11087571 | pubmed:authorsComplete | Y | lld:pubmed |
pubmed-article:11087571 | pubmed:pagination | 4465-78 | lld:pubmed |
pubmed-article:11087571 | pubmed:dateRevised | 2006-11-15 | lld:pubmed |
pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
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pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
pubmed-article:11087571 | pubmed:meshHeading | pubmed-meshheading:11087571... | lld:pubmed |
pubmed-article:11087571 | pubmed:year | 2000 | lld:pubmed |
pubmed-article:11087571 | pubmed:articleTitle | Structure-activity relationships of 17alpha-derivatives of estradiol as inhibitors of steroid sulfatase. | lld:pubmed |
pubmed-article:11087571 | pubmed:affiliation | Medicinal Chemistry Division and MRC Group in Molecular Endocrinology, Oncology and Molecular Endocrinology Research Center, Laval University Medical Center (CHUL), 2705 Laurier Boulevard, Sainte-Foy, Québec G1V 4G2, Canada. | lld:pubmed |
pubmed-article:11087571 | pubmed:publicationType | Journal Article | lld:pubmed |
pubmed-article:11087571 | pubmed:publicationType | Research Support, Non-U.S. Gov't | lld:pubmed |
http://linkedlifedata.com/r... | http://linkedlifedata.com/r... | pubmed-article:11087571 | lld:chembl |