首页> 外文期刊>Molecular cell >Asymmetric segregation of PIE-1 in C. elegans is mediated by two complementary mechanisms that act through separate PIE-1 protein domains.
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Asymmetric segregation of PIE-1 in C. elegans is mediated by two complementary mechanisms that act through separate PIE-1 protein domains.

机译:秀丽隐杆线虫中PIE-1的不对称分离是通过两个通过单独PIE-1蛋白结构域起作用的互补机制介导的。

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摘要

The CCCH finger protein PIE-1 is a regulator of germ cell fate that segregates with the germ lineage in early embryos. At each asymmetric division, PIE-1 is inherited preferentially by the germline daughter and is excluded from the somatic daughter. We show that this asymmetry is regulated at the protein level by two complementary mechanisms. The first acts before cell division to enrich PIE-1 in the cytoplasm destined for the germline daughter. The second acts after cell division to eliminate any PIE-1 left in the somatic daughter. The latter mechanism depends on PIE-1's first CCCH finger (ZF1), which targets PIE-1 for degradation in somatic blastomeres. ZF1s in two other germline proteins, POS-1 and MEX-1, are also degraded in somatic blastomeres, suggesting that localized degradation also acts on these proteins to exclude them from somatic lineages.
机译:CCCH手指蛋白PIE-1是生殖细胞命运的调节物,它与早期胚胎的生殖谱系隔离。在每个不对称分裂处,PIE-1优先由种系子代遗传,并从体细胞子代中排除。我们表明,这种不对称性在蛋白质水平上由两个互补机制调控。在细胞分裂之前,第一个作用是使PIE-1富集到种系子代的细胞质中。细胞分裂后的第二个作用是消除残留在体细胞子体中的任何PIE-1。后者的机制取决于PIE-1的第一个CCCH手指(ZF1),该手指将PIE-1定位为在卵裂球中降解。另外两个种系蛋白POS-1和MEX-1中的ZF1在体细胞卵裂球中也被降解,这表明局部降解也作用于这些蛋白,将它们排除在体细胞谱系之外。

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