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早老素蛋白家族成员SPE-4定位于内质网/高尔基体衍生的细胞器,且在线虫精子发生过程中正确的细胞质分配是必需的。

The presenilin protein family member SPE-4 localizes to an ER/Golgi derived organelle and is required for proper cytoplasmic partitioning during Caenorhabditis elegans spermatogenesis.

作者信息

Arduengo P M, Appleberry O K, Chuang P, L'Hernault S W

机构信息

Graduate Program in Biochemistry, Emory University, Atlanta, Georgia 30322, USA.

出版信息

J Cell Sci. 1998 Dec 18;111 ( Pt 24):3645-54. doi: 10.1242/jcs.111.24.3645.

Abstract

During Caenorhabditis elegans spermatogenesis, asymmetric partitioning of cellular components principally occurs via ER/Golgi-derived organelles, named fibrous body-membranous organelles. In C. elegans spe-4 mutants, morphogenesis of fibrous body-membranous organelle complexes is defective and spermatogenesis arrests at an unusual cellular stage with four haploid nuclei within a common cytoplasm. The spe-4 encoded integral membrane protein is a diverged member of the presenilin family implicated in early onset Alzheimer's disease. Specific antisera were used to show that SPE-4 resides within the fibrous body-membranous organelles membranes during wild-type spermatogenesis. Several spe-4 recessive mutants were examined for SPE-4 immunoreactivity and a deletion mutant lacks detectable SPE-4 while either of two missense mutants synthesize and localize immunoreactive SPE-4 within their fibrous body-membranous organelles. One of these missense mutations is located within a motif that is common to all presenilins. spe-4 mutants were also examined for other partitioning defects and tubulin was found to accumulate in unusual deposits close to the plasma membrane. These results suggest that wild-type SPE-4 is required for proper localization of macromolecules that are subject to asymmetric partitioning during spermatogenesis.

摘要

在秀丽隐杆线虫精子发生过程中,细胞成分的不对称分配主要通过内质网/高尔基体衍生的细胞器(称为纤维体-膜性细胞器)发生。在秀丽隐杆线虫spe-4突变体中,纤维体-膜性细胞器复合体的形态发生存在缺陷,精子发生在一个不寻常的细胞阶段停滞,此时一个共同的细胞质中有四个单倍体细胞核。spe-4编码的整合膜蛋白是早发性阿尔茨海默病相关的早老素家族的一个分化成员。使用特异性抗血清显示,在野生型精子发生过程中,SPE-4存在于纤维体-膜性细胞器膜内。对几个spe-4隐性突变体进行了SPE-4免疫反应性检测,一个缺失突变体检测不到SPE-4,而两个错义突变体中的任何一个都能在其纤维体-膜性细胞器内合成并定位免疫反应性SPE-4。其中一个错义突变位于所有早老素共有的一个基序内。还对spe-4突变体进行了其他分配缺陷检测,发现微管蛋白在靠近质膜的异常沉积物中积累。这些结果表明,野生型SPE-4是精子发生过程中经历不对称分配的大分子正确定位所必需的。

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