Biochimie. 1991 Jan;73(1):77-84.

New insights into the mitochondrial carnitine palmitoyltransferase enzyme system.

McGarry JD, Sen A, Esser V, Woeltje KF, Weis B, Foster DW.

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Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas 75235.

Abstract

Dissection of the mitochondrial carnitine palmitoyltransferase (CPT) enzyme system in terms of its structure/function relationships has proved to be a formidable task. Although no one formulation has gained universal agreement we believe that the weight of evidence supports a model with the following features: a) in any given tissue CPT I and CPT II are distinct proteins; b) CPT I, unlike CPT II, is detergent labile; c) within a species CPT II is expressed body wide, whereas CPT I exists as tissue specific isoforms; d) malonyl-CoA and other CPT I inhibitors probably interact at the catalytic center of the enzyme, not with a regulatory subunit. The amino acid sequences of rat and human CPT II (deduced from cDNA clones) show them to be similar proteins (greater than 80% identity) but encoded by mRNAs of significantly different sizes. Efforts to clone and sequence the cDNA for rat liver CPT I are presently underway.

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Inter-tissue and inter-species characteristics of the mitochondrial carnitine palmitoyltransferase enzyme system. [J Biol Chem. 1990]
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Woeltje KF, Esser V, Weis BC, Cox WF, Schroeder JG, Liao ST, Foster DW, McGarry JD. J Biol Chem. 1990 Jun 25; 265(18):10714-9.
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Cited by 6 PubMed Central articles

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