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肌球蛋白重链样蛋白在果蝇成肌细胞融合过程中定位于细胞接触部位,并在体外与 Rolling pebbles 7 相互作用。

Myosin heavy chain-like localizes at cell contact sites during Drosophila myoblast fusion and interacts in vitro with Rolling pebbles 7.

机构信息

Developmental Biology, Department of Biology, Philipps-Universität Marburg, Karl-von-Frisch-Strasse 8, 35037 Marburg, Germany.

出版信息

Exp Cell Res. 2013 Feb 15;319(4):402-16. doi: 10.1016/j.yexcr.2012.12.005. Epub 2012 Dec 13.

Abstract

Besides representing the sarcomeric thick filaments, myosins are involved in many cellular transport and motility processes. Myosin heavy chains are grouped into 18 classes. Here we show that in Drosophila, the unconventional group XVIII myosin heavy chain-like (Mhcl) is transcribed in the mesoderm of embryos, most prominently in founder cells (FCs). An ectopically expressed GFP-tagged Mhcl localizes in the growing muscle at cell-cell contacts towards the attached fusion competent myoblast (FCM). We further show that Mhcl interacts in vitro with the essential fusion protein Rolling pebbles 7 (Rols7), which is part of a protein complex established at cell contact sites (Fusion-restricted Myogenic-Adhesive Structure or FuRMAS). Here, branched F-actin is likely needed to widen the fusion pore and to integrate the myoblast into the growing muscle. We show that the localization of Mhcl is dependent on the presence of Rols7, and we postulate that Mhcl acts at the FuRMAS as an actin motor protein. We further show that Mhcl deficient embryos develop a wild-type musculature. We thus propose that Mhcl functions redundantly to other myosin heavy chains in myoblasts. Lastly, we found that the protein is detectable adjacent to the sarcomeric Z-discs, suggesting an additional function in mature muscles.

摘要

除了代表肌球蛋白粗丝外,肌球蛋白还参与许多细胞运输和运动过程。肌球蛋白重链分为 18 类。在这里,我们表明在果蝇中,非典型的第 XVIII 组肌球蛋白重链样(Mhcl)在胚胎的中胚层中被转录,在创始细胞(FC)中最为明显。异位表达的 GFP 标记的 Mhcl 定位于细胞-细胞接触处的生长肌肉中,朝向附着的融合有能力的成肌细胞(FCM)。我们进一步表明,Mhcl 在体外与必需的融合蛋白 Rolling pebbles 7(Rols7)相互作用,后者是在细胞接触位点建立的蛋白质复合物的一部分(融合受限的肌原性粘着结构或 FuRMAS)。在这里,分支的 F-肌动蛋白可能需要扩大融合孔,并将成肌细胞整合到生长的肌肉中。我们表明 Mhcl 的定位依赖于 Rols7 的存在,并且我们推测 Mhcl 在 FuRMAS 中作为肌球蛋白重链的肌动蛋白马达蛋白发挥作用。我们进一步表明,缺乏 Mhcl 的胚胎发育出野生型肌肉。因此,我们提出 Mhcl 在成肌细胞中与其他肌球蛋白重链具有冗余功能。最后,我们发现该蛋白可检测到肌节 Z 盘附近,表明在成熟肌肉中具有额外的功能。

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