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首页> 外文期刊>Cell structure and function >Diphosphorylated MRLC is Required for Organization of Stress Fibers in Interphase Cells and the Contractile Ring in Dividing Cells
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Diphosphorylated MRLC is Required for Organization of Stress Fibers in Interphase Cells and the Contractile Ring in Dividing Cells

机译:在相间细胞中应力纤维的组织和在分隔细胞中的收缩环的组织需要二磷酸化的MRLC

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References(25) Cited-By(39) Activity of nonmuscle myosin II is regulated by phosphorylation of its regulatory light chain (MRLC). Phosphoryration of MRLC at both Thr18 and Ser19 (diphosphorylation) results in higher MgATPase activity and in promotion of the assembly of myosin II filaments than does that of MRLC at Ser19 (monophosphorylation) in vitro. To determine the roles of the diphosphorylated MRLC in vivo, we transfected three kinds of MRLC mutants, unphosphorylated, monophosphorylated and diphosphorylated forms (MRLC2T18AS19A, substitution of both Ser19 and Thr18 by Ala; MRLC2T18AS19D, Ser19 by Asp and Thr18 by Ala; and MRLC2T18DS19D, both Ser19 and Thr18 by Asp, respectively), into HeLa cells. Cells overexpressing the mutant MRLC2T18DS19D contained a larger number of actin filament bundles than did those overexpressing the mutant MRLC2 T18AS19D. Moreover, cells overexpressing the nonphosphorylatable mutant MRLC2T18AS19A showed a decrease in the number of actin filament bundles. Taken together, our data suggest that diphosphorylation of MRLC plays an important role in regulating actin filament assembly and reorganization in nonmuscle cells.
机译:参考文献(25)By-By(39)非肌肉肌球蛋白II的活性受其调节轻链(MRLC)磷酸化的调节。与MRLC在Ser19(单磷酸化)相比,Thr18和Ser19上的MRLC磷酸化(二磷酸化)可导致更高的MgATPase活性,并促进肌球蛋白II细丝的组装。为了确定二磷酸化MRLC在体内的作用,我们转染了三种MRLC突变体,即未磷酸化,单磷酸化和二磷酸化形式(MRLC2T18AS19A,Ala取代Ser19和Thr18; Ala取代MRLC2T18AS19D,Asp19取代Ser19,Ala取代Thr18取代Ser19,Mla2T18D Ser19和Thr18分别通过Asp)转移到HeLa细胞中。与过表达突变MRLC2 T18AS19D的细胞相比,过表达突变MRLC2T18DS19D的细胞包含更多的肌动蛋白丝束。此外,过表达不可磷酸化突变体MRLC2T18AS19A的细胞显示肌动蛋白丝束的数量减少。综上所述,我们的数据表明,MRLC的二磷酸化在调节肌动蛋白丝组装和非肌肉细胞的重组中起着重要作用。

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