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利用 IR-LEGO 单细胞基因诱导系统分析秀丽隐杆线虫中 semaphorin-plexin 相互作用的镶嵌基因表达。

Mosaic gene expression analysis of semaphorin-plexin interactions in Caenorhabditis elegans using the IR-LEGO single-cell gene induction system.

机构信息

Division of Biological Science, Graduate School of Science, Nagoya University, Nagoya, Aichi, Japan.

Laboratory for Biothermology, National Institute of Basic Biology, Okazaki, Aichi, Japan.

出版信息

Dev Growth Differ. 2022 Jun;64(5):230-242. doi: 10.1111/dgd.12793. Epub 2022 Jun 15.

Abstract

Genetic mosaic analysis is a powerful means of addressing the sites of gene action in multicellular organisms. In conventional genetic analysis, the generation of desired mosaic patterns is difficult to control due to the randomness of generating the genetic mosaic which often renders the analysis laborious and time consuming. The infrared laser-evoked gene operator (IR-LEGO) microscope system facilitates genetic mosaic analysis by enabling gene induction in targeted single cells in a living organism. However, the level of gene induction is not controllable due to the usage of a heat-shock promoter. Here, we applied IR-LEGO to examine the cell-cell interactions mediated by semaphoring-plexin signaling in Caenorhabditis elegans by inducing wild-type semaphorin/plexin in single cells within the population of mutant cells lacking the relevant proteins. We found that the cell contact-dependent termination of the extension of vulval precursor cells is elicited by the forward signaling mediated by the semaphorin receptor, PLX-1, but not by the reverse signaling via the transmembrane semaphorin, SMP-1. By utilizing Cre/loxP recombination coupled with the IR-LEGO system to induce SMP-1 at a physiological level, we found that SMP-1 interacts with PLX-1 only in trans upon contact between vulval precursor cells. In contrast, when overexpressed, SMP-1 exhibits the ability to cis-interact with PLX-1 on a single cell. These results indicate that mosaic analysis with IR-LEGO, especially when combined with an in vivo recombination system, efficiently complements conventional methods.

摘要

遗传嵌合体分析是一种研究多细胞生物中基因作用位点的有力手段。在传统的遗传分析中,由于产生遗传嵌合体的随机性,难以控制所需的嵌合图案的生成,这往往使得分析既费力又耗时。红外激光诱发基因操作器(IR-LEGO)显微镜系统通过在生物体的靶向单细胞中诱导基因,促进遗传嵌合体分析。然而,由于使用热休克启动子,基因诱导的水平是不可控的。在这里,我们应用 IR-LEGO 通过在缺乏相关蛋白的突变细胞群体中单细胞中诱导野生型信号素/神经丛蛋白,来研究半通道-神经丛信号在秀丽隐杆线虫中的细胞-细胞相互作用。我们发现,半通道受体 PLX-1 介导的正向信号而不是跨膜信号素 SMP-1 的反向信号引发了 vulval 前体细胞延伸的细胞接触依赖性终止。通过利用 Cre/loxP 重组结合 IR-LEGO 系统在生理水平上诱导 SMP-1,我们发现 SMP-1 仅在 vulval 前体细胞接触时通过 trans 相互作用与 PLX-1 相互作用。相比之下,当过度表达时,SMP-1 表现出在单个细胞上 cis 相互作用与 PLX-1 的能力。这些结果表明,IR-LEGO 的嵌合体分析,特别是与体内重组系统相结合,有效地补充了传统方法。

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