Activation of naturally occurring lecithin: Cholesterol acyltransferase mutants by a novel activator compound

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Abstract

Lecithin:cholesterol acyltransferase (LCAT) is a unique plasma enzyme able to esterify cholesterol, and it plays an important role in HDL maturation and promotion of reverse cholesterol transport. Familial LCAT deficiency (FLD; OMIM number 245900) is a rare recessive disease that results from loss-of-function mutations in the LCAT gene and has no cure. In this study, we assessed the in vitro efficacy of a novel small-molecule LCAT activator. Cholesterol esterification rate (CER) and LCAT activity were tested in plasma from six controls and five FLD homozygous carriers of various LCAT mutations at different doses of the compound (0.1, 1, and 10 mg/ml). In control plasma, the compound significantly increased both CER (P, 0.001) and LCAT activity (P = 0.007) in a dose-dependent manner. Both CER and LCAT activity increased by 4- to 5-fold, reaching maximum activation at the dose of 1 mg/ml. Interestingly, Daiichi Sankyo compound produced an increase in CER in two of the five tested LCAT mutants (Leu372-Arg and Val309-Met), while LCAT activity increased in three LCAT mutants (Arg147-Trp, Thr274-Ile and Leu372-Arg); mutant Pro254-Ser was not activated at any of the tested doses. The present findings form the basis for personalized therapeutic interventions in FLD carriers and support the potential LCAT activation in secondary LCAT defects. SIGNIFICANCE STATEMENT We characterized the pharmacology of a novel small-molecule LCAT activator in vitro on a subset of naturally occurring LCAT mutants. Our findings form the basis for personalized therapeutic interventions for familial LCAT deficiency carriers, who can face severe complications and for whom no cure exists.

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APA

Pavanello, C., Ossoli, A., Turri, M., Strazzella, A., Simonelli, S., Laurenzi, T., … Calabresi, L. (2020). Activation of naturally occurring lecithin: Cholesterol acyltransferase mutants by a novel activator compound. Journal of Pharmacology and Experimental Therapeutics, 375(3), 463–468. https://doi.org/10.1124/JPET.120.000159

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