首页> 外文期刊>Cell death and differentiation >Drosophila homolog of APP-BP1 (dAPP-BP1) interacts antagonistically with APPL during Drosophila development.
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Drosophila homolog of APP-BP1 (dAPP-BP1) interacts antagonistically with APPL during Drosophila development.

机译:果蝇发展过程中,APP-BP1的果蝇同源物(dAPP-BP1)与APPL拮抗相互作用。

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摘要

beta-Amyloid precursor protein binding protein 1 (APP-BP1) was previously identified based on its binding to the carboxyl terminal of beta-amyloid precursor protein. In this report, we have discovered that a mutation of dAPP-BP1 (Drosophila ortholog of APP-BP1) hinders tissue development, causes apoptosis in imaginal disc cells, and blocks the NEDD8 conjugation pathway. We show that dAPP-BP1 specifically binds the intracellular domain of APP-like protein (APPL). The dAPP-BP1 mutation partially suppresses the abnormal macrochaete phenotype of Appl(d), while overexpression of dAPP-BP1 causes abnormal macrochaetes. When APPL is overexpressed, the normal bristle pattern in the fly thorax is disturbed and apoptosis is induced in wing imaginal discs. APPL overexpression phenotypes are enhanced by reducing the level of dAPP-BP1. APPL overexpression is shown to inhibit the NEDD8 conjugation pathway. APPL-induced apoptosis is rescued by overexpression of dAPP-BP1. Our data suggest that APPL and dAPP-BP1 interact antagonistically during Drosophila development.
机译:β-淀粉样蛋白前体蛋白结合蛋白1(APP-BP1)先前是根据其与β淀粉样蛋白前体蛋白的羧基末端结合而鉴定的。在此报告中,我们发现dAPP-BP1(果蝇直系同源果蝇APP-BP1)的突变会阻碍组织发育,导致假想椎间盘细胞凋亡,并阻断NEDD8偶联途径。我们显示,dAPP-BP1特异性结合APP样蛋白(APPL)的胞内域。 dAPP-BP1突变部分抑制了Appl(d)的异常大动物表型,而dAPP-BP1的过表达导致了异常的大动物。当APPL过表达时,the胸中的正常刷毛模式会受到干扰,并在机翼假体椎间盘中诱导凋亡。通过降低dAPP-BP1的水平可以增强APPL过表达的表型。显示APPL过表达抑制NEDD8缀合途径。 dAPP-BP1的过表达可以挽救APPL诱导的细胞凋亡。我们的数据表明果蝇发育过程中APPL和dAPP-BP1拮抗相互作用。

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