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斑马鱼中的靶向基因敲低揭示了胰岛素样生长因子II信号在胚胎内的不同功能。

Targeted gene knockdown in zebrafish reveals distinct intraembryonic functions for insulin-like growth factor II signaling.

作者信息

White Yvonne A R, Kyle Joshua T, Wood Antony W

机构信息

Vincent Center for Reproductive Biology, Vincent Obstetrics and Gynecology Services, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02118, USA

出版信息

Endocrinology. 2009 Sep;150(9):4366-75. doi: 10.1210/en.2009-0356. Epub 2009 May 14.

Abstract

IGF-II is the predominant IGF ligand regulating prenatal growth in all vertebrates, including humans, but its central role in placental development has confounded efforts to fully elucidate its functions within the embryo. Here we use a nonplacental model vertebrate (zebrafish) to interrogate the intraembryonic functions of IGF-II signaling. The zebrafish genome contains two coorthologs of mammalian IGF2 (igf2a, igf2b), which exhibit distinct patterns of expression during embryogenesis. Expression of igf2a mRNA is restricted to the notochord, primarily during segmentation/neurulation. By contrast, igf2b mRNA is expressed in midline tissues adjacent to the notochord, with additional sites of expression in the ventral forebrain, and the pronephros. To identify their intraembryonic functions, we suppressed the expression of each gene with morpholino oligonucleotides. Knockdown of igf2a led to defects in dorsal midline development, characterized by delayed segmentation, notochord undulations, and ventral curvature. Similarly, suppression of igf2b led to defects in dorsal midline development but also induced ectopic fusion of the nephron primordia, and defects in ventral forebrain development. Subsequent onset of severe body edema in igf2b, but not igf2a morphants, further suggested a distinct role for igf2b in development of the embryonic kidney. Simultaneous knockdown of both genes increased the severity of dorsal midline defects, confirming a conserved role for both genes in dorsal midline development. Collectively, these data provide evidence that the zebrafish orthologs of IGF2 function in dorsal midline development during segmentation/neurulation, whereas one paralog, igf2b, has evolved additional, distinct functions during subsequent organogenesis.

摘要

胰岛素样生长因子-II(IGF-II)是调节包括人类在内的所有脊椎动物产前生长的主要IGF配体,但其在胎盘发育中的核心作用使得全面阐明其在胚胎内的功能变得困难。在这里,我们使用一种非胎盘模式脊椎动物(斑马鱼)来探究IGF-II信号传导在胚胎内的功能。斑马鱼基因组包含两个与哺乳动物IGF2同源的基因(igf2a、igf2b),它们在胚胎发育过程中表现出不同的表达模式。igf2a mRNA的表达主要局限于脊索,主要在体节形成/神经胚形成期间。相比之下,igf2b mRNA在与脊索相邻的中线组织中表达,在腹侧前脑和前肾中也有额外的表达位点。为了确定它们在胚胎内的功能,我们用吗啉代寡核苷酸抑制每个基因的表达。敲低igf2a导致背侧中线发育缺陷,其特征为体节形成延迟、脊索波动和腹侧弯曲。同样,抑制igf2b也导致背侧中线发育缺陷,但也诱导了肾单位原基的异位融合以及腹侧前脑发育缺陷。igf2b而非igf2a morphants随后出现严重的身体水肿,这进一步表明igf2b在胚胎肾脏发育中具有独特作用。同时敲低这两个基因增加了背侧中线缺陷的严重程度,证实了这两个基因在背侧中线发育中具有保守作用。总体而言,这些数据提供了证据,表明IGF2的斑马鱼同源基因在体节形成/神经胚形成期间参与背侧中线发育,而其中一个旁系同源基因igf2b在随后的器官发生过程中进化出了额外的、独特的功能。

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