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胰岛素受体/Foxo信号与dMyc活性在肌肉生长过程中的整合调控果蝇的体型。

Integration of Insulin receptor/Foxo signaling and dMyc activity during muscle growth regulates body size in Drosophila.

作者信息

Demontis Fabio, Perrimon Norbert

机构信息

Department of Genetics, Howard Hughes Medical Institute, Harvard Medical School, 77 Avenue Louis Pasteur, Boston, MA 02115, USA.

出版信息

Development. 2009 Mar;136(6):983-93. doi: 10.1242/dev.027466. Epub 2009 Feb 11.

Abstract

Drosophila larval skeletal muscles are single, multinucleated cells of different sizes that undergo tremendous growth within a few days. The mechanisms underlying this growth in concert with overall body growth are unknown. We find that the size of individual muscles correlates with the number of nuclei per muscle cell and with increasing nuclear ploidy during development. Inhibition of Insulin receptor (InR; Insulin-like receptor) signaling in muscles autonomously reduces muscle size and systemically affects the size of other tissues, organs and indeed the entire body, most likely by regulating feeding behavior. In muscles, InR/Tor signaling, Foxo and dMyc (Diminutive) are key regulators of endoreplication, which is necessary but not sufficient to induce growth. Mechanistically, InR/Foxo signaling controls cell cycle progression by modulating dmyc expression and dMyc transcriptional activity. Thus, maximal dMyc transcriptional activity depends on InR to control muscle mass, which in turn induces a systemic behavioral response to allocate body size and proportions.

摘要

果蝇幼虫的骨骼肌是单个、多核且大小各异的细胞,在几天内会经历巨大的生长。这种与整体身体生长协同的生长机制尚不清楚。我们发现,个体肌肉的大小与每个肌细胞中的细胞核数量以及发育过程中核多倍性的增加相关。肌肉中胰岛素受体(InR;胰岛素样受体)信号的抑制会自主降低肌肉大小,并系统性地影响其他组织、器官乃至整个身体的大小,最有可能是通过调节进食行为来实现的。在肌肉中,InR/Tor信号传导、Foxo和dMyc(微小)是内复制的关键调节因子,内复制是诱导生长所必需但不充分的条件。从机制上讲,InR/Foxo信号通过调节dmyc表达和dMyc转录活性来控制细胞周期进程。因此,最大程度的dMyc转录活性依赖于InR来控制肌肉质量,而肌肉质量又会反过来引发一种系统性行为反应,以分配身体大小和比例。

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