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The sema domain
Authors:Gherardi Ermanno  Love Christopher A  Esnouf Robert M  Jones E Yvonne
Institution:MRC Centre, Hills Road, Cambridge CB2 2QH, UK. egherard@mrc-lmb.cam.ac.uk
Abstract:The sema domain was first defined from sequence by Kolodkin and colleagues in the early 1990s, and constitutes the distinctive structural and functional element of semaphorins, their plexin receptors and the receptor tyrosine kinases MET and RON, three protein families with major roles in development, tissue regeneration and cancer. Recently determined crystal structures of two semaphorins (SEMA3A and SEMA4D) and the MET receptor have shown that the sema domain consists of a highly conserved variant form of the seven-blade beta-propeller fold. The structures, however, also suggest differences between these families with respect to the mode of dimerisation and the regions of the domain involved in ligand-receptor interactions. This reflects the considerable plasticity and adaptation of the sema domain in order to meet different binding requirements, properties that may underlie the vast array of ligand-receptor specificities and functions of the semaphorin superfamily.
Keywords:Abbreviations: aa  amino acid(s)  CRD  cystine-rich domain  GPI  glycosylphosphatidylinositol  HGFl/MSP  hepatocyte growth factor-like/macrophage stimulating protein  HGF/SF  hepatocyte growth factor/scatter factor  HMM  hidden Markov model  Ig  immunoglobulin  PDB  Protein Data Bank  RTK  receptor tyrosine kinase
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