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Biophysical basis of the promiscuous binding of B-cell lymphoma protein 2 apoptotic repressor to BH3 ligands.

J Mol Recognit.. 2013-10;  26(10):501-13
Bhat V, Olenick MB, Schuchardt BJ, Mikles DC, McDonald CB, Farooq A. Department of Biochemistry & Molecular Biology, Miller School of Medicine, University of Miami, Miami, FL, 33136, USA.
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摘要

B-cell lymphoma protein 2 (Bcl2) apoptotic repressor carries out its function by virtue of its ability to bind to BH3 domains of various pro-apoptotic regulators in a highly promiscuous manner. Herein, we investigate the biophysical basis of such promiscuity of Bcl2 toward its cognate BH3 ligands. Our data show that although the BH3 ligands harboring the LXXXAD motif bind to Bcl2 with submicromolar affinity, those with the LXXX[G/S]D motif afford weak interactions. This implies that the replacement of alanine at the fourth position (A+4)-relative to the N-terminal leucine (L0) within the LXXXAD motif-to glycine/serine results in the loss of free energy of binding. Consistent with this notion, the A+4 residue wi... More

关键词

binding thermodynamics; molecular dynamics; salt dependence; structural models