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Proteins of the endoplasmic-reticulum-associated degradation pathway: domain detection and function prediction.

机译:内质网相关降解途径的蛋白质:结构域检测和功能预测。

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摘要

Sequence database searches, using iterative-profile and Hidden-Markov-model approaches, were used to detect hitherto-undetected homologues of proteins that regulate the endoplasmic reticulum (ER)-associated degradation pathway. The translocon-associated subunit Sec63p (Sec=secretory) was shown to contain a domain of unknown function found twice in several Brr2p-like RNA helicases (Brr2=bad response to refrigeration 2). Additionally, Cue1p (Cue=coupling of ubiquitin conjugation to ER degradation), a yeast protein that recruits the ubiquitin-conjugating (UBC) enzyme Ubc7p to an ER-associated complex, was found to be one of a large family of putative scaffolding-domain-containing proteins that include the autocrine motility factor receptor and fungal Vps9p (Vps=vacuolar protein sorting). Two other yeast translocon-associated molecules, Sec72p and Hrd3p (Hrd=3-hydroxy-3-methylglutaryl-CoA reductase degradation), were shown to contain multiple tetratricopeptide-repeat-like sequences. From this observation it is suggested that Sec72p associates with a heat-shock protein, Hsp70, in a manner analogous to that known for Hop (Hsp70/Hsp90 organizing protein). Finally, the luminal portion of Ire1p (Ire=high inositol-requiring), thought to convey the sensing function of this transmembrane kinase and endoribonuclease, was shown to contain repeats similar to those in beta-propeller proteins. This finding hints at the mechanism by which Ire1p may sense extended unfolded proteins at the expense of compact folded molecules.
机译:序列数据库搜索,使用迭代模式和Hidden-Markov模型方法,用于检测调节内质网(ER)相关降解途径的蛋白质的迄今未检测到的同源物。显示与转运蛋白相关的亚基Sec63p(Sec =分泌)包含一个未知功能域,该功能域在几种Brr2p-like RNA解旋酶中两次发现(Brr2 =对冷藏反应差2)。此外,发现将提示泛素结合(UBC)酶Ubc7p结合至ER相关复合物的酵母蛋白Cue1p(泛素结合与ER降解的偶联)是推定支架结构域的一大家族包含自分泌运动因子受体和真菌Vps9p的蛋白质(Vps =卵泡蛋白分选)。 Sec72p和Hrd3p(Hrd = 3-羟基-3-甲基戊二酰辅酶A还原酶降解)是另外两个与酵母错位相关的分子,它们包含多个四肽重复序列。根据该观察结果,暗示Sec72p以与Hop(Hsp70 / Hsp90组织蛋白)相似的方式与热休克蛋白Hsp70缔合。最后,Ire1p的管腔部分(Ire =要求高肌醇)被认为传达了这种跨膜激酶和核糖核酸内切酶的传感功能,显示其包含与β-螺旋桨蛋白相似的重复序列。这一发现暗示了Ire1p可能以牺牲紧密折叠分子为代价来感知延伸的未折叠蛋白的机制。

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