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果蝇小分子热休克蛋白CryAB确保发育中肌肉的结构完整性以及正常的肌肉和心脏功能。

Drosophila small heat shock protein CryAB ensures structural integrity of developing muscles, and proper muscle and heart performance.

作者信息

Wójtowicz Inga, Jabłońska Jadwiga, Zmojdzian Monika, Taghli-Lamallem Ouarda, Renaud Yoan, Junion Guillaume, Daczewska Malgorzata, Huelsmann Sven, Jagla Krzysztof, Jagla Teresa

机构信息

GReD - INSERM U1103, CNRS UMR6293, Clermont Université, 28, place Henri Dunant, Clermont-Ferrand 63000, France Department of Animal Developmental Biology, Institute of Experimental Biology, University of Wrocław, Sienkiewicza 21, Wrocław 50-335, Poland.

Department of Animal Developmental Biology, Institute of Experimental Biology, University of Wrocław, Sienkiewicza 21, Wrocław 50-335, Poland.

出版信息

Development. 2015 Mar 1;142(5):994-1005. doi: 10.1242/dev.115352.

Abstract

Molecular chaperones, such as the small heat shock proteins (sHsps), maintain normal cellular function by controlling protein homeostasis in stress conditions. However, sHsps are not only activated in response to environmental insults, but also exert developmental and tissue-specific functions that are much less known. Here, we show that during normal development the Drosophila sHsp CryAB [L(2)efl] is specifically expressed in larval body wall muscles and accumulates at the level of Z-bands and around myonuclei. CryAB features a conserved actin-binding domain and, when attenuated, leads to clustering of myonuclei and an altered pattern of sarcomeric actin and the Z-band-associated actin crosslinker Cheerio (filamin). Our data suggest that CryAB and Cheerio form a complex essential for muscle integrity: CryAB colocalizes with Cheerio and, as revealed by mass spectrometry and co-immunoprecipitation experiments, binds to Cheerio, and the muscle-specific attenuation of cheerio leads to CryAB-like sarcomeric phenotypes. Furthermore, muscle-targeted expression of CryAB(R120G), which carries a mutation associated with desmin-related myopathy (DRM), results in an altered sarcomeric actin pattern, in affected myofibrillar integrity and in Z-band breaks, leading to reduced muscle performance and to marked cardiac arrhythmia. Taken together, we demonstrate that CryAB ensures myofibrillar integrity in Drosophila muscles during development and propose that it does so by interacting with the actin crosslinker Cheerio. The evidence that a DRM-causing mutation affects CryAB muscle function and leads to DRM-like phenotypes in the fly reveals a conserved stress-independent role of CryAB in maintaining muscle cell cytoarchitecture.

摘要

分子伴侣,如小热休克蛋白(sHsps),通过在应激条件下控制蛋白质稳态来维持正常的细胞功能。然而,sHsps不仅在应对环境损伤时被激活,还发挥着发育和组织特异性功能,而这些功能鲜为人知。在这里,我们表明在正常发育过程中,果蝇的sHsp CryAB [L(2)efl] 在幼虫体壁肌肉中特异性表达,并在Z线水平和肌核周围积累。CryAB具有一个保守的肌动蛋白结合结构域,当其功能减弱时,会导致肌核聚集以及肌节肌动蛋白和Z线相关肌动蛋白交联蛋白Cheerio(细丝蛋白)的模式改变。我们的数据表明,CryAB和Cheerio形成了一个对肌肉完整性至关重要的复合物:CryAB与Cheerio共定位,并且如质谱和免疫共沉淀实验所揭示的,与Cheerio结合,而Cheerio的肌肉特异性减弱会导致类似CryAB的肌节表型。此外,携带与结蛋白相关肌病(DRM)相关突变的CryAB(R120G) 在肌肉中的靶向表达,会导致肌节肌动蛋白模式改变、受影响的肌原纤维完整性以及Z线断裂,从而导致肌肉性能下降和明显的心律失常。综上所述,我们证明CryAB在果蝇肌肉发育过程中确保肌原纤维的完整性,并提出它是通过与肌动蛋白交联蛋白Cheerio相互作用来实现的。导致DRM的突变影响CryAB肌肉功能并在果蝇中导致类似DRM的表型,这一证据揭示了CryAB在维持肌肉细胞细胞结构方面保守的非应激依赖性作用。

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