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Modification of CETP function by changing its substrate preference: a new paradigm for CETP drug design.

J. Lipid Res.. 2015; 
MortonRichard E,IzemLahou
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Gene Synthesis 1) and single amino acid mutants (Q199A, R201S, H232A, M433A, D442G, and R451Q) were synthesized (GenScript, Piscataway, NJ), subcloned into pCDNA3, and sequence verifi ed ( 10 ). Get A Quote

摘要

We previously determined that hamster cholesteryl ester transfer protein (CETP), unlike human CETP, promotes a novel one-way transfer of TG from VLDL to HDL, causing HDL to gain lipid. We hypothesize that this nonreciprocal lipid transfer activity arises from the usually high TG/cholesteryl ester (CE) substrate preference of hamster CETP. Consistent with this, we report here that ∼25% of the total lipid transfer promoted by the human Q199A CETP mutant, which prefers TG as substrate, is nonreciprocal transfer. Other human CETP mutants with TG/CE substrate preferences higher or lower than wild-type also possess nonreciprocal lipid transfer activity. Mutants with high TG/CE substrate preference promo... More

关键词

TP2 Fab fragment,cholesteryl ester transfer protein,nonreciprocal lipid tran