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Ubiquitin over-expression phenotypes and ubiquitin gene molecular misreading during aging in Drosophila melanogaster

机译:果蝇衰老过程中泛素过表达表型和泛素基因分子错读

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摘要

Molecular Misreading (MM) is the inaccurate conversion of genomic information into aberrant proteins. For example, when RNA polymerase II transcribes a GAGAG motif it synthesizes at low frequency RNA with a two-base deletion. If the deletion occurs in a coding region, translation will result in production of misframed proteins. During mammalian aging, misframed versions of human amyloid precursor protein (hApp) and ubiquitin (hUbb) accumulate in the aggregates characteristic of neurodegenerative diseases, suggesting dysfunctional degradation or clearance. Here cDNA clones encoding wild-type hUbb and the frame-shifted version hUbb+1 were expressed in transgenic Drosophila using the doxycycline-regulated system. Misframed proteins were abundantly produced, both from the transgenes and from endogenous Drosophila ubiquitin-encoding genes, and their abundance increased during aging in whole-fly extracts. Over-expression of wild-type hUbb, but not hUbb+1, was toxic during fly development. In contrast, when over-expressed specifically in adult flies, hUbb+1 caused small decreases in life span, whereas hUbb was associated with small increases, preferentially in males. The data suggest that MM occurs in Drosophila and that the resultant misframed proteins accumulate with age. MM of the ubiquitin gene can produce alternative ubiquitin gene products with different and sometimes opposing phenotypic effects.
机译:分子误读(MM)是将基因组信息不准确地转换为异常蛋白质的过程。例如,当RNA聚合酶II转录GAGAG基序时,它会以低频RNA合成并带有两个碱基的缺失。如果缺失发生在编码区,则翻译将导致产生错误构筑的蛋白质。在哺乳动物衰老过程中,人淀粉样蛋白前体蛋白(hApp)和泛素(hUbb)构图错误的版本会积聚在神经退行性疾病的特征性聚集物中,提示功能失调或清除。使用强力霉素调节系统,在转基因果蝇中表达了编码野生型hUbb和移码版本hUbb +1 的cDNA克隆。从转基因和内源果蝇泛素编码基因中,错构蛋白大量产生,并且在全蝇提取物中的衰老过程中它们的丰度增加。野生型hUbb的过度表达对果蝇的发育有毒,但hUbb +1 却没有。相反,当在成年果蝇中过度表达时,hUbb +1 会导致寿命的小幅下降,而hUbb则有小幅增长,​​尤其是雄性。数据表明,果蝇发生在果蝇中,并且随着年龄的增长,错误构图的蛋白质会积累。泛素基因的MM可以产生具有不同的,有时是相反的表型效应的替代泛素基因产物。

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