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Two regions of the tail are necessary for the isoform-specific functions of nonmuscle myosin IIB

机译:尾巴的两个区域对于非肌肉肌球蛋白IIB的同工型特异功能是必需的

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摘要

To function in the cell, nonmuscle myosin 11 molecules assemble into filaments through their C-terminal tails. Because myosin II isoforms most likely assemble into homo-filaments in vivo, it seems that some self-recognition mechanisms of individual myosin II isoforms should exist. Exogenous expression of myosin IIB rod fragment is thus expected to prevent the function of myosin IIB specifically. We expected to reveal some self-recognition sites of myosin IIB from the phenotype by expressing appropriate myosin IIB rod fragments. We expressed the C-terminal 305-residue rod fragment of the myosin IIB heavy chain (BRF305) in MRC-5 SV1 TG1 cells. As a result, unstable morphology was observed like MHC-IIB-/- fibroblasts. This phenotype was not observed in cells expressing BRF305 mutants: 1) with a defect in assembling, 2) lacking N-terminal 57 residues (N-57), or 3) lacking C-terminal 63 residues (C-63). A myosin IIA rod fragment ARF296 corresponding to BRF305 was not effective. However, the chimeric ARF296, in which the N-57 and C-63 of BRF305 were substituted for the corresponding regions of ARF296, acquired the ability to induce unstable morphology. We propose that the N-57 and C-63 of BRF305 are involved in self-recognition when myosin IIB molecules assemble into homo-filament.
机译:为了在细胞中发挥作用,非肌肉肌球蛋白11分子通过其C末端尾部组装成细丝。因为肌球蛋白II同工型很可能在体内组装成均丝,所以似乎应该存在一些个体肌球蛋白II同工型的自识别机制。因此预期肌球蛋白IIB杆片段的外源表达将特异性地阻止肌球蛋白IIB的功能。我们期望通过表达合适的肌球蛋白IIB杆片段从表型揭示一些肌球蛋白IIB的自我识别位点。我们在MRC-5 SV1 TG1细胞中表达了肌球蛋白IIB重链(BRF305)的C末端305残基杆片段。结果,观察到不稳定的形态,如MHC-IIB-/-成纤维细胞。在表达BRF305突变体的细胞中未观察到此表型:1)装配缺陷; 2)缺少N端57个残基(N-57),或3)缺少C端63残基(C-63)。对应于BRF305的肌球蛋白IIA杆片段ARF296无效。但是,嵌合的ARF296获得了诱导不稳定形态的能力,其中BRF305的N-57和C-63取代了ARF296的相应区域。我们建议当肌球蛋白IIB分子组装成均丝时,BRF305的N-57和C-63参与自我识别。

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