瘙痒/ AIP4通过形成K29连接的多聚泛素链介导Deltex降解。
Itch/AIP4 mediates Deltex degradation through the formation of K29-linked polyubiquitin chains.
作者信息
Chastagner Patricia, Israël Alain, Brou Christel
机构信息
Unité de Signalisation Moléculaire et Activation Cellulaire, URA 2582, CNRS, Institut Pasteur, 25 rue du Dr Roux, 75724 Paris cedex 15, France.
出版信息
EMBO Rep. 2006 Nov;7(11):1147-53. doi: 10.1038/sj.embor.7400822. Epub 2006 Oct 6.
Abstract
Deltex (DTX) and AIP4 are the human orthologues of the Drosophila deltex and Suppressor of deltex, which have been genetically described as being antagonistically involved in the Notch signalling pathway. Both genes encode E3 ubiquitin ligases of the RING (Really interesting new gene)-H2 and HECT (Homologous to E6AP carboxyl terminus) families, respectively. In an attempt to understand the molecular basis of their genetic interactions, we studied the relationship between DTX and AIP4 in the absence of activation of the Notch pathway. We show here that both molecules interact and partially colocalize to endocytic vesicles, and that AIP4 targets DTX for lysosomal degradation. Furthermore, AIP4-generated polyubiquitin chains are mainly conjugated through lysine 29 of ubiquitin in vivo, indicating a link between this type of chain and lysosomal degradation.
摘要
Deltex(DTX)和AIP4分别是果蝇deltex和deltex抑制因子在人类中的同源物,在遗传学上已被描述为在Notch信号通路中发挥拮抗作用。这两个基因分别编码RING(真有趣的新基因)-H2家族和HECT(与E6AP羧基末端同源)家族的E3泛素连接酶。为了理解它们遗传相互作用的分子基础,我们在未激活Notch通路的情况下研究了DTX和AIP4之间的关系。我们在此表明,这两种分子相互作用并部分共定位于内吞小泡,并且AIP4将DTX靶向溶酶体降解。此外,AIP4生成的多聚泛素链在体内主要通过泛素的赖氨酸29进行共轭,表明这种类型的链与溶酶体降解之间存在联系。
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