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果蝇肽类激素咽侧体抑制素A和利尿激素31在后肠中部呈现互补梯度分布,它们拮抗调节肠衰老和成虫寿命。

Drosophila Peptide Hormones Allatostatin A and Diuretic Hormone 31 Exhibiting Complementary Gradient Distribution in Posterior Midgut Antagonistically Regulate Midgut Senescence and Adult Lifespan.

作者信息

Takeda Koji, Okumura Takashi, Terahata Mayu, Yamaguchi Mio, Taniguchi Kiichiro, Adachi-Yamada Takashi

机构信息

1 Graduate Course in Life Science, Graduate School of Science, Gakushuin University, 1-5-1 Mejiro, Toshima-ku, Tokyo 171-8588, Japan.

2 Department of Life Science, Faculty of Science, Gakushuin University, 1-5-1 Mejiro, Toshima-ku, Tokyo 171-8588, Japan.

出版信息

Zoolog Sci. 2018 Feb;35(1):75-85. doi: 10.2108/zs160210.

DOI:10.2108/zs160210
PMID:29417892
Abstract

Enteroendocrine cells (EEs) are evolutionarily conserved gastrointestinal secretory cells that show scattered distribution in the intestinal epithelium. These cells classified into several subtypes based on the hormones they produce in both mammals and insects. In the fruit fly Drosophila, it has been suggested that nearly equal numbers of two subtypes of EEs (Allatostatin A: AstA and Diuretic hormone 31 : Dh31) are alternately produced from the intestinal stem cells in the posterior midgut. However, we found that these two subtypes are not always present in this manner, but are rather distributed in a complementary frequency gradient along the posterior midgut. We show that midgut-preferential RNA knockdown of the peptide hormones AstA or Dh31 respectively results in decreased or increased adult lifespan. This effect on longevity is apparently correlated with the midgut senescence phenotypes as a result of direct hormone action through both hormone receptors expressed in the enteroblasts or other midgut cell types. However, gut senescence does not appear to be the direct cause for longevity regulation, as knockdown of both hormone receptors did not affect adult lifespan. Furthermore, these senescence phenotypes appear to be independent of insulin signaling and manifest in an organ-specific manner. These results indicate that the two intestinal secretory peptides antagonistically regulate adult lifespan and intestinal senescence through multiple pathways, irrespective of insulin, which implicates a complementary gradient distribution of each of the hormone-producing EEs, consistent with local requirements for cell activity along the posterior midgut.

摘要

肠内分泌细胞(EEs)是在进化上保守的胃肠道分泌细胞,分散分布于肠上皮中。在哺乳动物和昆虫中,这些细胞根据其产生的激素被分为几个亚型。在果蝇中,有人提出后肠中部的肠干细胞交替产生数量近乎相等的两种EE亚型(抑咽侧体素A:AstA和利尿激素31:Dh31)。然而,我们发现这两种亚型并非总是以这种方式存在,而是沿后肠中部以互补的频率梯度分布。我们表明,分别对肽激素AstA或Dh31进行中肠优先RNA敲低会导致成年果蝇寿命缩短或延长。这种对寿命的影响显然与中肠衰老表型相关,这是由于激素通过成肠细胞或其他中肠细胞类型中表达的激素受体直接作用的结果。然而,肠道衰老似乎不是寿命调节的直接原因,因为敲低两种激素受体均不影响成年果蝇的寿命。此外,这些衰老表型似乎独立于胰岛素信号传导,并以器官特异性方式表现出来。这些结果表明,这两种肠道分泌肽通过多种途径拮抗调节成年果蝇的寿命和肠道衰老,与胰岛素无关,这意味着产生激素的每种EEs呈互补梯度分布,这与后肠中部对细胞活性的局部需求一致。

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