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细胞骨架蛋白合成的空间组织

Spatial organization of the synthesis of cytoskeletal proteins.

作者信息

Fulton A B

机构信息

Department of Biochemistry, University of Iowa, City 52242.

出版信息

J Cell Biochem. 1993 Jun;52(2):148-52. doi: 10.1002/jcb.240520206.

DOI:10.1002/jcb.240520206
PMID:8366132
Abstract

The cytoskeleton of most cells is complex and spatially diverse. The mRNAs for some cytoskeletal proteins are localized, suggesting that synthesis of these proteins may occur at sites appropriate for function or assembly. mRNA concentrations were first observed for several oocyte and embryonic mRNAs. Some insight has been gained into the mechanisms that help to position these mRNAs. More surprising to some, many cytoskeletal mRNAs are also localized. Among them are mRNAs for actin, tubulin, intermediate filaments, and a variety of associated proteins. Different mRNAs in the same cell can be located in different places; the same mRNA can be located in different places; the same mRNA can be located differently at different times of development. For example, we observed vimentin mRNA in developing chicken muscle cultures by fluorescent in situ hybridization. We found that vimentin mRNA takes on a variety of positions during myogenesis, ending up located with its cognate protein at costameres. This last pattern is significant because it is too finely structured to have a function in the soluble phase and probably reflects cotranslational assembly of this particular protein. Analogies can be made between oocyte or embryonic positions (animal/vegetal poles, oocyte cortex, and interior) and somatic cell positions (anterior/posterior and cell cortex/cell center). These analogies may point to conserved mechanisms for moving and retaining mRNA. Localization of cytoskeletal synthesis, through the mRNA or by other means, may prove as important for assembling and maintaining differentiated cytoskeletal structures and somatic cells as mRNA location is for organizing the embryo. Mechanisms that permit mRNA localization are likely to be conserved.

摘要

大多数细胞的细胞骨架复杂且在空间上具有多样性。一些细胞骨架蛋白的信使核糖核酸(mRNA)是定位的,这表明这些蛋白质的合成可能发生在适合其功能或组装的位点。最初在几种卵母细胞和胚胎mRNA中观察到了mRNA浓度。对于帮助定位这些mRNA的机制已经有了一些了解。令一些人更惊讶的是,许多细胞骨架mRNA也是定位的。其中包括肌动蛋白、微管蛋白、中间丝以及多种相关蛋白的mRNA。同一细胞中的不同mRNA可以位于不同位置;相同的mRNA在不同发育阶段也可以位于不同位置。例如,我们通过荧光原位杂交在发育中的鸡肌肉培养物中观察到波形蛋白mRNA。我们发现波形蛋白mRNA在肌生成过程中呈现出多种位置,最终与其同源蛋白一起位于肌小节。最后这种模式很重要,因为它的结构过于精细,在可溶性相中无法发挥功能,可能反映了这种特定蛋白质的共翻译组装。卵母细胞或胚胎的位置(动物/植物极、卵母细胞皮质和内部)与体细胞的位置(前/后以及细胞皮质/细胞中心)之间可以进行类比。这些类比可能指向了用于移动和保留mRNA的保守机制。通过mRNA或其他方式进行细胞骨架合成的定位,对于组装和维持分化的细胞骨架结构以及体细胞可能与mRNA定位对于胚胎组织一样重要。允许mRNA定位的机制很可能是保守的。

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