Stereoselective formation of a cholesterol ester conjugate from fenvalerate by mouse microsomal carboxyesterase(s)
- 8 June 1986
- journal article
- research article
- Published by Wiley in Journal of Biochemical Toxicology
- Vol. 1 (2) , 79-93
- https://doi.org/10.1002/jbt.2570010208
Abstract
In accordance with in vivo findings, of the four chiral isomers of fenvalerate (S‐5602 SumicidinR, PydrinR, [RS]‐α‐cyano‐3‐phenoxybenzyl [RS]‐2‐(4‐chlorophenyl)isovalerate), only the [2R,αS]‐isomer (B‐isomer) yielded cholesteryl [2R]‐2‐(4‐chlorophenyl)isovalerate (CPIA‐cholesterol ester) in the in vitro study using several tissue homogenates of mice, rats, dogs, and monkeys. There were species differences in the extent of CPIA‐cholesterol‐ester formation, with mouse tissues showing relatively higher activity than those of other animals. The kidney, brain, and spleen of mice showed relatively higher capacities to form this ester compared to other tissues, and the enzyme activity was mainly localized in microsomal fractions. The CPIA‐cholesterol ester did not seem to be produced by three known biosynthetic pathways of endogenous cholesterol esters–acyl‐CoA:cholesterol O‐acyltransferase (ACAT),2 lecithin:cholesterol O‐acyltransferase (LCAT)3 and cholesterol esterase.4 Carboxyesterase(s) of mouse kidney microsomes solubilized by digitonin hydrolyzed only the Bα‐isomer of fenvalerate, yielding CPIA, whereas they yielded the corresponding cholesterol ester in the presence of artificial liposomes containing cholesterol. Thus, it appears that the stereoselective formation of the CPIA‐cholesterol ester results from the stereoselective formation of the CPIA‐carboxyesterase complex only from the Bα‐isomer, which subsequently undergoes cleavage by cholesterol to yield the CPIA‐cholesterol ester.Keywords
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