The meiotic LINC complex component KASH5 is an activating adaptor for cytoplasmic dynein

Kirsten E. L. Garner, A. Salter, C. K. Lau, M. Gurusaran, Cécile Villemant, Elizabeth P. Granger, G. McNee, P. Woodman, O. Davies, B. Burke, V. Allan
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引用次数: 5

Abstract

Cytoplasmic dynein-driven movement of chromosomes during prophase I of mammalian meiosis is essential for synapsis and genetic exchange. Dynein connects to chromosome telomeres via KASH5 and SUN1 or SUN2, which together span the nuclear envelope. Here, we show that KASH5 promotes dynein motility in vitro, and cytosolic KASH5 inhibits dynein’s interphase functions. KASH5 interacts with either dynein light intermediate chain (DYNC1LI1 or DYNC1LI2) via a conserved helix in the LIC C-terminal, and this region is also needed for dynein’s recruitment to other cellular membranes. KASH5’s N-terminal EF-hands are essential, as the interaction with dynein is disrupted by mutation of key calcium-binding residues, although it is not regulated by cellular calcium levels. Dynein can be recruited to KASH5 at the nuclear envelope independently of dynactin, while LIS1 is essential for dynactin incorporation into the KASH5-dynein complex. Altogether, we show that the trans-membrane protein KASH5 is an activating adaptor for dynein, and shed light on the hierarchy of assembly of KASH5-dynein-dynactin complexes.
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减数分裂LINC复合体成分KASH5是细胞质动力蛋白的激活适配器
哺乳动物减数分裂前I期细胞质动力蛋白驱动的染色体运动对突触和遗传交换至关重要。动力蛋白通过KASH5和SUN1或SUN2连接染色体端粒,它们一起跨越核膜。在这里,我们发现KASH5在体外促进动力蛋白的运动,而细胞质KASH5抑制动力蛋白的间期功能。KASH5通过LIC c末端的保守螺旋与动力蛋白轻中间链(DYNC1LI1或DYNC1LI2)相互作用,并且该区域也是动力蛋白募集到其他细胞膜所需的区域。KASH5的n端ef -手是必不可少的,因为与动力蛋白的相互作用被关键钙结合残基的突变破坏,尽管它不受细胞钙水平的调节。Dynein可以独立于dynactin在核包膜处被募集到KASH5,而LIS1对于dynactin并入KASH5- Dynein复合体至关重要。总之,我们证明了跨膜蛋白KASH5是动力蛋白的激活适配器,并阐明了KASH5-动力蛋白-动力蛋白复合物的组装层次。
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