Department of Biochemistry and Molecular Biology, Clark H Smith Brain Tumour Centre, Southern Alberta Cancer Research Institute, University of Calgary, Calgary, AB, Canada T2N 4N1.
Proc Natl Acad Sci U S A. 2012 Jan 24;109(4):1139-44. doi: 10.1073/pnas.1113311109. Epub 2012 Jan 6.
The target-of-rapamycin pathway couples nutrient availability with tissue and organismal growth in metazoans. The key effectors underlying this growth are, however, unclear. Here we show that Maf1, a repressor of RNA polymerase III-dependent tRNA transcription, is an important mediator of nutrient-dependent growth in Drosophila. We find nutrients promote tRNA synthesis during larval development by inhibiting Maf1. Genetic inhibition of Maf1 accelerates development and increases body size. These phenotypes are due to a non-cell-autonomous effect of Maf1 inhibition in the fat body, the main larval endocrine organ. Inhibiting Maf1 in the fat body increases growth by promoting the expression of brain-derived insulin-like peptides and consequently enhanced systemic insulin signaling. Remarkably, the effects of Maf1 inhibition are reproduced in flies carrying one extra copy of the initiator methionine tRNA, tRNA(i)(Met). These findings suggest the stimulation of tRNA(i)(Met) synthesis via inhibition of dMaf1 is limiting for nutrition-dependent growth during development.
雷帕霉素靶蛋白(mTOR)途径将营养物质的可用性与后生动物组织和机体的生长联系起来。然而,这种生长的关键效应物尚不清楚。本文中,作者发现 RNA 聚合酶 III 依赖性 tRNA 转录的抑制剂 Maf1 是果蝇中营养物质依赖性生长的重要介质。作者发现,营养物质通过抑制 Maf1 促进幼虫发育过程中的 tRNA 合成。遗传抑制 Maf1 可加速发育并增加体型。这些表型是由于脂肪体中非细胞自主抑制 Maf1 的作用,脂肪体是主要的幼虫内分泌器官。抑制脂肪体中的 Maf1 通过促进脑衍生胰岛素样肽的表达来促进生长,从而增强全身胰岛素信号。值得注意的是,在携带起始甲硫氨酸 tRNA(tRNA(i)(Met))一个额外拷贝的果蝇中,抑制 Maf1 的作用得到了重现。这些发现表明,通过抑制 dMaf1 刺激 tRNA(i)(Met)的合成可能是发育过程中营养物质依赖性生长的限制因素。
