A role for BYN-1/bystin in cellular uptake and clearance of residual bodies in the Caenorhabditis elegans germline.

IF 3.7 2区生物学 Q1 DEVELOPMENTAL BIOLOGY

Development Pub Date : 2024-10-01 Epub Date: 2024-10-08 DOI:10.1242/dev.202694

Hyemin Min, Emily L Spaulding, Catherine S Sharp, Pankaj Garg, Esther Jeon, Lyn S Miranda Portillo, Noah A Lind, Dustin L Updike

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引用次数: 0

Abstract

GLH/Vasa/DDX4 helicases are core germ-granule proteins that promote germline development and fertility. A yeast-two-hybrid screen using Caenorhabditis elegans GLH-1 as bait identified BYN-1, the homolog of human bystin/BYSL. In humans, bystin promotes cell adhesion and invasion in gliomas, and, with its binding partner trophinin, triggers embryonic implantation into the uterine wall. C. elegans embryos do not implant and lack a homolog of trophinin, but both trophinin and GLH-1 contain unique decapeptide phenylalanine-glycine (FG)-repeat domains. In germ cells, we find endogenous BYN-1 in the nucleolus, partitioned away from cytoplasmic germ granules. However, BYN-1 enters the cytoplasm during spermatogenesis to colocalize with GLH-1. Both proteins become deposited in residual bodies (RBs), which are then engulfed and cleared by the somatic gonad. We show that BYN-1 acts upstream of CED-1 to drive RB engulfment, and that removal of the FG-repeat domains from GLH-1 and GLH-2 can partially phenocopy byn-1 defects in RB clearance. These results point to an evolutionarily conserved pathway whereby cellular uptake is triggered by the cytoplasmic mobilization of bystin/BYN-1 to interact with proteins harboring FG-repeats.

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BYN-1/bystin在秀丽隐杆线虫生殖系细胞摄取和清除残留体中的作用

GLH/Vasa/DDX4螺旋酶是生殖细胞的核心蛋白，能促进生殖细胞的发育和生育能力。以草履虫 GLH-1 为诱饵进行的酵母双杂交筛选发现了人类 bystin/BYSL 的同源物 BYN-1。在人类中，bystin 能促进胶质瘤的细胞粘附和侵袭，并与其结合伙伴 trophinin 一起引发胚胎植入子宫壁。秀丽隐杆线虫胚胎不着床，也缺乏trophinin的同源物，但trophinin和GLH-1都含有独特的十肽苯丙氨酸-甘氨酸（FG）重复结构域。在生殖细胞中，我们发现内源性 BYN-1 位于核仁中，与细胞质中的生殖颗粒分离。不过，在精子发生过程中，BYN-1 会进入细胞质与 GLH-1 共定位。这两种蛋白质都沉积在残留体（RB）中，然后被体细胞性腺吞噬和清除。我们发现 BYN-1 作用于 CED-1 的上游以驱动 RB 吞噬，而且从 GLH-1 和 GLH-2 中去除 FG 重复结构域可以部分表征 byn-1 在 RB 清除中的缺陷。这些结果表明了一种进化保守的途径，即通过细胞质动员 bystin/BYN-1 与携带 FG 重复的蛋白质相互作用来触发细胞吞噬。

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来源期刊

Development 生物-发育生物学

CiteScore

6.70

自引率

4.30%

发文量

433

审稿时长

3 months

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