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Constitutively active ESCRT-II suppresses the MVB-sorting phenotype of ESCRT-0 and ESCRT-I mutants

机译:组成性活性ESCRT-II抑制ESCRT-0和ESCRT-I突变体的MVB分选表型

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The endosomal sorting complex required for transport (ESCRT) protein complexes function at the endosome in the formation of intraluminal vesicles (ILVs) containing cargo proteins destined for the vacuolar/lysosomal lumen. The early ESCRTs (ESCRT-0 and -I) are likely involved in cargo sorting, whereas ESCRT-III and Vps4 function to sever the neck of the forming ILVs. ESCRT-II links these functions by initiating ESCRT-III formation in an ESCRT-I-regulated manner. We identify a constitutively active mutant of ESCRT-II that partially suppresses the phenotype of an ESCRT-I or ESCRT-0 deletion strain, suggesting that these early ESCRTs are not essential and have redundant functions. However, the ESCRT-III/Vps4 system alone is not sufficient for ILV formation but requires cargo sorting mediated by one of the early ESCRTs.
机译:运输所需的内体分选复合物(ESCRT)蛋白复合物在腔内囊泡(ILV)的形成中在内体起作用,腔内囊泡(ILV)包含运往液泡/溶酶体腔的货物蛋白。早期的ESCRT(ESCRT-0和-I)可能参与了货物分拣,而ESCRT-III和Vps4的作用是切断形成的ILV的颈部。 ESCRT-II通过以ESCRT-I调节的方式启动ESCRT-III的形成来链接这些功能。我们确定了一种组成性活性的ESCRT-II突变体,该突变体部分抑制了ESCRT-I或ESCRT-0缺失菌株的表型,表明这些早期的ESCRTs不是必需的,并且具有多余的功能。但是,仅ESCRT-III / Vps4系统不足以形成ILV,但需要由早期ESCRT之一介导的货物分拣。

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