Craige Branch, Salazar Gloria, Faundez Victor
Graduate Program in Biochemistry, Cell, and Developmental Biology, Emory University, Atlanta, GA 30322, USA.
Mol Biol Cell. 2008 Apr;19(4):1415-26. doi: 10.1091/mbc.e07-12-1239. Epub 2008 Feb 6.
The adaptor complex 3 (AP-3) targets membrane proteins from endosomes to lysosomes, lysosome-related organelles and synaptic vesicles. Phosphatidylinositol-4-kinase type II alpha (PI4KIIalpha) is one of several proteins possessing catalytic domains that regulate AP-3-dependent sorting. Here we present evidence that PI4KIIalpha uniquely behaves both as a membrane protein cargo as well as an enzymatic regulator of adaptor function. In fact, AP-3 and PI4KIIalpha form a complex that requires a dileucine-sorting motif present in PI4KIIalpha. Mutagenesis of either the PI4KIIalpha-sorting motif or its kinase-active site indicates that both are necessary to interact with AP-3 and properly localize PI4KIIalpha to LAMP-1-positive endosomes. Similarly, both the kinase activity and the sorting signal present in PI4KIIalpha are necessary to rescue endosomal PI4KIIalpha siRNA-induced mutant phenotypes. We propose a mechanism whereby adaptors use canonical sorting motifs to selectively recruit a regulatory enzymatic activity to restricted membrane domains.
衔接蛋白复合物3(AP-3)将内体中的膜蛋白靶向运输至溶酶体、溶酶体相关细胞器和突触小泡。II型磷脂酰肌醇-4-激酶α(PI4KIIα)是几种具有催化结构域、调节AP-3依赖性分选的蛋白质之一。在此我们提供证据表明,PI4KIIα既作为膜蛋白货物,又作为衔接蛋白功能的酶调节剂,具有独特的行为。事实上,AP-3和PI4KIIα形成一个复合物,该复合物需要PI4KIIα中存在的双亮氨酸分选基序。对PI4KIIα分选基序或其激酶活性位点进行诱变表明,两者对于与AP-3相互作用以及将PI4KIIα正确定位到LAMP-1阳性内体都是必需的。同样,PI4KIIα中存在的激酶活性和分选信号对于挽救内体PI4KIIα siRNA诱导的突变表型都是必需的。我们提出一种机制,即衔接蛋白利用经典分选基序将调节酶活性选择性地招募到受限的膜结构域。
