Signaling pathways regulating Dictyostelium myosin II

被引:0
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作者
Marc A. De La Roche
Janet L. Smith
Venkaiah Betapudi
Thomas T. Egelhoff
Graham P. Côté
机构
[1] Queen's University,Department of Biochemistry, Botterell Hall
[2] Boston Biomedical Research Institute,Department of Physiology and Biophysics
[3] Case Western Reserve School of Medicine,undefined
关键词
Actin Filament; Myosin Heavy Chain; Myosin Light Chain; Contractile Force; Myosin Light Chain Kinase;
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摘要
Dictyostelium myosin II is a conventional, two-headed myosin that consists of two copies each of a myosin heavy chain (MHC), an essential light chain (ELC) and a regulatory light chain (RLC). The MHC is comprised of an amino-terminal motor domain, a neck region that binds the RLC and ELC and a carboxyl-terminal α-helical coiled-coil tail. Electrostatic interactions between the tail domains mediate the self-assembly of myosin II into bipolar filaments that are capable of interacting with actin filaments to generate a contractile force. In this review we discuss the regulation of Dictyostelium myosin II by a myosin light chain kinase (MLCK-A) that phosphorylates the RLC and increases motor activity and by MHC kinases (MHCKs) that phosphorylate the tail and prevent filament assembly. Dictyostelium may express as many as four MHCKs (MHCK A–D) consisting of an atypical α-kinase catalytic domain and a carboxyl-terminal WD repeat domain that targets myosin II filaments. A previously reported MHCK, termed MHC-PKC, now seems more likely to be a diacylglycerol kinase (DgkA). The relationship of the MHCKs to the larger family of α-kinases is discussed and key features of the structure of the α-kinase catalytic domain are reviewed. Potential upstream regulators of myosin II are described, including DgkA, cGMP, cAMP and PAKa, a target for Rac GTPases. Recent results point to a complex network of signaling pathways responsible for controling the activity and localization of myosin II in the cell.
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页码:703 / 718
页数:15
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