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Myofibril diameter is set by a finely tuned mechanism of protein oligomerization in Drosophila

机译:肌纤维直径由果蝇中的蛋白质低聚的细固机制设定

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摘要

Myofibrils are huge cytoskeletal assemblies embedded in the cytosol of muscle cells. They consist of arrays of sarcomeres, the smallest contractile unit of muscles. Within a muscle type, myofibril diameter is highly invariant and contributes to its physiological properties, yet little is known about the underlying mechanisms setting myofibril diameter. Here we show that the PDZ and LIM domain protein Zasp, a structural component of Z-discs, mediates Z-disc and thereby myofibril growth through protein oligomerization. Oligomerization is induced by an interaction of its ZM domain with LIM domains. Oligomerization is terminated upon upregulation of shorter Zasp isoforms which lack LIM domains at later developmental stages. The balance between these two isoforms, which we call growing and blocking isoforms sets the stereotyped diameter of myofibrils. If blocking isoforms dominate, myofibrils become smaller. If growing isoforms dominate, myofibrils and Z-discs enlarge, eventually resulting in large pathological aggregates that disrupt muscle function.
机译:肌纤维是嵌入肌细胞细胞细胞细胞瘤的巨大细胞骨骼组件。它们由SARCOMERES阵列组成,肌肉最小的收缩单位。在肌肉型内,肌纤维直径是高度不变的,有助于其生理特性,但是关于设置肌纤维直径的潜在机制很少。在这里,我们表明PDZ和LIM结构域蛋白ZASP,Z盘状的结构组分,介导Z盘,从而通过蛋白质寡聚化肌原纤维生长。通过其ZM域与氧域域的相互作用诱导寡聚化。在缺少血清域以后的发育阶段的缺少肢体域的上调时终止寡聚化。这两种同种型之间的平衡,我们称之为生长和阻断同种型,设定了肌原纤维的陈规定型直径。如果阻断同种型占主导地位,肌原纤维将变小。如果种植同种型占主导地位,肌纤维和Z盘子放大,最终导致破坏肌肉功能的大病理聚集体。

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