Literature DB >> 24998673

Structural characteristics of the nonallosteric human cytosolic malic enzyme.

Ju-Yi Hsieh1, Shao-Yu Li1, Meng-Chun Chen1, Pai-Chun Yang1, Hui-Yi Chen2, Nei-Li Chan3, Jyung-Hurng Liu4, Hui-Chih Hung5.   

Abstract

Human cytosolic NADP(+)-dependent malic enzyme (c-NADP-ME) is neither a cooperative nor an allosteric enzyme, whereas mitochondrial NAD(P)(+)-dependent malic enzyme (m-NAD(P)-ME) is allosterically activated by fumarate. This study examines the molecular basis for the different allosteric properties and quaternary structural stability of m-NAD(P)-ME and c-NADP-ME. Multiple residues corresponding to the fumarate-binding site were mutated in human c-NADP-ME to correspond to those found in human m-NAD(P)-ME. Additionally, the crystal structure of the apo (ligand-free) human c-NADP-ME conformation was determined. Kinetic studies indicated no significant difference between the wild-type and mutant enzymes in Km,NADP, Km,malate, and kcat. A chimeric enzyme, [51-105]_c-NADP-ME, was designed to include the putative fumarate-binding site of m-NAD(P)-ME at the dimer interface of c-NADP-ME; however, this chimera remained nonallosteric. In addition to fumarate activation, the quaternary structural stability of c-NADP-ME and m-NAD(P)-ME is quite different; c-NADP-ME is a stable tetramer, whereas m-NAD(P)-ME exists in equilibrium between a dimer and a tetramer. The quaternary structures for the S57K/N59E/E73K/S102D and S57K/N59E/E73K/S102D/H74K/D78P/D80E/D87G mutants of c-NADP-ME are tetrameric, whereas the K57S/E59N/K73E/D102S m-NAD(P)-ME quadruple mutant is primarily monomeric with some dimer formation. These results strongly suggest that the structural features near the fumarate-binding site and the dimer interface are highly related to the quaternary structural stability of c-NADP-ME and m-NAD(P)-ME. In this study, we attempt to delineate the structural features governing the fumarate-induced allosteric activation of malic enzyme.
Copyright © 2014 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Allosteric activation; Fumarate-binding site; Kinetics; Malic enzyme; Mutagenesis; Quaternary structural stability

Year:  2014        PMID: 24998673     DOI: 10.1016/j.bbapap.2014.06.019

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  7 in total

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3.  A small-molecule inhibitor suppresses the tumor-associated mitochondrial NAD(P)+-dependent malic enzyme (ME2) and induces cellular senescence.

Authors:  Ju-Yi Hsieh; Shao-Yu Li; Wen-Chen Tsai; Jyung-Hurng Liu; Chih-Li Lin; Guang-Yaw Liu; Hui-Chih Hung
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Authors:  Hongchao Wang; Chen Zhang; Haiqin Chen; Zhennan Gu; Jianxin Zhao; Hao Zhang; Yong Q Chen; Wei Chen
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7.  A rotary mechanism for allostery in bacterial hybrid malic enzymes.

Authors:  Christopher John Harding; Ian Thomas Cadby; Patrick Joseph Moynihan; Andrew Lee Lovering
Journal:  Nat Commun       Date:  2021-02-23       Impact factor: 14.919

  7 in total

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