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Different Evolutionary Trajectories of Two Insect-Specific Paralogous Proteins Involved in Stabilizing Muscle Myofibrils

机译:两种昆虫特异性副蛋白蛋白的不同进化轨迹参与稳定肌肉肌原纤维

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摘要

Alp/Enigma family members have a unique PDZ domain followed by zero to four LIM domains, and are essential for myofibril assembly across all species analyzed so far. Drosophila melanogaster has three Alp/Enigma family members, Zasp52, Zasp66, and Zasp67. Ortholog search and phylogenetic tree analysis suggest that Zasp genes have a common ancestor, and that Zasp66 and Zasp67 arose by duplication in insects. While Zasp66 has a conserved domain structure across orthologs, Zasp67 domains and lengths are highly variable. In flies, Zasp67 appears to be expressed only in indirect flight muscles, where it colocalizes with Zasp52 at Z-discs. We generated a CRISPR null mutant of Zasp67, which is viable but flightless. We can rescue all phenotypes by re-expressing a Zasp67 transgene at endogenous levels. Zasp67 mutants show extended and broken Z-discs in adult flies, indicating that the protein helps stabilize the highly regular myofibrils of indirect flight muscles. In contrast, a Zasp66 CRISPR null mutant has limited viability, but only mild indirect flight muscle defects illustrating the diverging evolutionary paths these two paralogous genes have taken since they arose by duplication.
机译:ALP / Enigma家族成员具有独特的PDZ域,然后是零至四个雷域,对于到目前为止分析的所有物种上,对于肌纤维组件至关重要。果蝇Melanogaster拥有三个Alp / Enigma系列成员,Zasp52,Zasp66和Zasp67。 Ortholog搜索和系统发育树分析表明,Zasp基因具有共同的祖先,Zasp66和Zasp67通过昆虫复制来源。虽然Zasp66具有跨越外翻的节约域结构,但Zasp67域和长度是高度变化的。在苍蝇中,Zasp67似乎仅在间接飞行肌肉中表达,在那里它在Z盘上用Zasp52结合。我们生成了Zasp67的Crisprp null突变体,这是可行但不断的。我们可以通过在内源水平重新表达Zasp67转基因来拯救所有表型。 Zasp67突变体显示成人苍蝇的延长和破碎的Z盘,表明蛋白质有助于稳定间接飞行肌肉的高度常规肌原纤维。相比之下,Zasp66 Crispr缺失突变体具有有限的活力,但只有轻度间接飞行肌缺陷,说明了这两个副潜级基因的发散进化途径,因为它们通过重复而采取了这种两种副潜级基因。

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