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SKIP controls lysosome positioning using a composite kinesin-1 heavy and light chain-binding domain

Journal of Cell Science, 130(22). 2018; 
Anneri Sanger, Yan Y. Yip, Thomas S. Randall, Stefano Pernigo, Roberto A. Steiner and Mark P. Dodding
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PCR Cloning and Subcloning For expression of SKIP-CSTN chimeric proteins, DNAs encoding the indicated protein sequences were synthesised by Genscript (NJ, USA) and subcloned into CB6-GFP. Get A Quote

摘要

The molecular interplay between cargo recognition and regulation of the activity of the kinesin-1 microtubule motor is not well understood. Using the lysosome adaptor SKIP as model cargo, we show that the heavy chains (KHCs), in addition to the light chains (KLCs), can recognize tryptophan-acidic binding determinants on the cargo when presented in the context of an extended KHC interacting domain. Mutational separation of KHC and KLC binding shows that both interactions are important for SKIP-kinesin-1 interaction in vitro and that KHC binding is important for lysosome transport in vivo. However, in the absence of KLCs, SKIP can only bind to KHC when autoinhibition is relieved, suggesting that the KLCs gate acc... More

关键词

kinesin-1, SKIP, lysosome positioning, microtubule transport