| Literature DB >> 27884807 |
Eduard V Bocharov1, Konstantin S Mineev2, Konstantin V Pavlov3, Sergey A Akimov4, Andrey S Kuznetsov2, Roman G Efremov5, Alexander S Arseniev6.
Abstract
Interaction between transmembrane helices often determines biological activity of membrane proteins. Bitopic proteins, a broad subclass of membrane proteins, form dimers containing two membrane-spanning helices. Some aspects of their structure-function relationship cannot be fully understood without considering the protein-lipid interaction, which can determine the protein conformational ensemble. Experimental and computer modeling data concerning transmembrane parts of bitopic proteins are reviewed in the present paper. They highlight the importance of lipid-protein interactions and resolve certain paradoxes in the behavior of such proteins. Besides, some properties of membrane organization provided a clue to understanding of allosteric interactions between distant parts of proteins. Interactions of these kinds appear to underlie a signaling mechanism, which could be widely employed in the functioning of many membrane proteins. Treatment of membrane proteins as parts of integrated fine-tuned proteolipid system promises new insights into biological function mechanisms and approaches to drug design. This article is part of a Special Issue entitled: Lipid order/lipid defects and lipid-control of protein activity edited by Dirk Schneider.Entities:
Keywords: bitopic membrane protein; lipid density fluctuations; protein-lipid and protein-protein interactions; receptor tyrosine kinase; signal transduction; transmembrane domain
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Year: 2016 PMID: 27884807 DOI: 10.1016/j.bbamem.2016.10.024
Source DB: PubMed Journal: Biochim Biophys Acta Biomembr ISSN: 0005-2736 Impact factor: 3.747