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Changes in organelle position and epithelial architecture associated with loss of CrebA

机译:与CrebA丢失相关的细胞器位置和上皮结构变化

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Drosophila CrebA facilitates high-level secretion by transcriptional upregulation of the protein components of the core secretory machinery. In CrebA mutant embryos, both salivary gland (SG) morphology and epidermal cuticle secretion are abnormal, phenotypes similar to those observed with mutations in core secretory pathway component genes. Here, we examine the cellular defects associated with CrebA loss in the SG epithelium. Apically localized secretory vesicles are smaller and less abundant, consistent with overall reductions in secretion. Unexpectedly, global mislocalization of cellular organelles and excess membrane accumulation in the septate junctions (SJs) are also observed. Whereas mutations in core secretory pathway genes lead to organelle localization defects similar to those of CrebA mutants, they have no effect on SJ-associated membrane. Mutations in tetraspanin genes, which are normally repressed by CrebA, have mild defects in SJ morphology that are rescued by simultaneous CrebA loss. Correspondingly, removal of several tetraspanins gives partial rescue of the CrebA SJ phenotype, supporting a role for tetraspanins in SJ organization.
机译:果蝇CrebA通过转录上调核心分泌机制的蛋白质成分来促进高水平分泌。在CrebA突变体胚胎中,唾液腺(SG)形态和表皮角质层分泌均异常,其表型类似于在核心分泌途径成分基因中观察到的表型。在这里,我们检查与SG上皮细胞CrebA丢失相关的细胞缺陷。根尖上局部的分泌囊泡更小和更少,与分泌的总体减少一致。出乎意料的是,还观察到细胞器的整体错位和在分隔连接处(SJs)中过多的膜堆积。尽管核心分泌途径基因中的突变导致类似于CrebA突变体的细胞器定位缺陷,但它们对SJ相关膜没有影响。通常由CrebA抑制的四跨素基因突变在SJ形态上具有轻度缺陷,可通过同时CrebA丢失来挽救。相应地,去除几种四跨膜蛋白可部分拯救CrebA SJ表型,从而支持四跨膜蛋白在SJ组织中的作用。

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