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6月27日JMCB新文上线-ABOUT E-selectin conformation (OA)

已有 2094 次阅读 2015-7-14 15:06 |个人分类:最新上线|系统分类:论文交流

E-selectin ligand complexes adopt an extended high-affinity conformation


Abstarct

E-selectin is a cell-adhesion molecule of the vascular endothelium that promotes essential leukocyte rolling in the early inflammatory response by binding to glycoproteins containing the tetrasaccharide sialyl Lewisx (sLex). Efficient leukocyte recruitment under vascular flow conditions depends on an increased lifetime of E-selectin/ligand complexes under tensile force in a so-called catch-bond binding mode. Co-crystal structures of a representative fragment of the extracellular E-selectin region with sLex and a glycomimetic antagonist thereof reveal an extended E-selectin conformation, which is identified as a high-affinity binding state of E-selectin by molecular dynamics simulations. Small-angle X-ray scattering experiments demonstrate a direct link between ligand binding and E-selectin conformational transition under static conditions in solution. This permits tracing a series of concerted structural changes connecting ligand binding to conformational stretching as the structural basis of E-selectin catch-bond-mediated leukocyte recruitment. The detailed molecular view of the binding site paves the way for the design of a new generation of selectin antagonists. This is of special interest, since their therapeutic potential was recently demonstrated with the pan-selectin antagonists GMI-1070 (Rivipansel).


J Mol Cell Biol mjv046 first published online June 27, 2015 doi:10.1093/jmcb/mjv046


Keywords: inflammation, leukocyte adhesion, E-selectin, glycomimetic antagonist, sialyl Lewisx, conformational change


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https://blog.sciencenet.cn/blog-1045694-905373.html

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