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A Single Common Portal for Clathrin-mediated Endocytosis of Distinct Cargo Governed by Cargo-selective Adaptors

机译:网格选择蛋白介导的不同货物的网格蛋白介导的内吞作用的单个共同门户。

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摘要

Sorting of transmembrane cargo into clathrin-coated vesicles requires endocytic adaptors, yet RNA interference (RNAi)-mediated gene silencing of the AP-2 adaptor complex only disrupts internalization of a subset of clathrin-dependent cargo. This suggests alternate clathrin-associated sorting proteins participate in cargo capture at the cell surface, and a provocative recent proposal is that discrete endocytic cargo are sorted into compositionally and functionally distinct clathrin coats. We show here that the FXNPXY-type internalization signal within cytosolic domain of the LDL receptor is recognized redundantly by two phosphotyrosine-binding domain proteins, Dab2 and ARH; diminishing both proteins by RNAi leads to conspicuous LDL receptor accumulation at the cell surface. AP-2–dependent uptake of transferrin ensues relatively normally in the absence of Dab2 and ARH, clearly revealing delegation of sorting operations at the bud site. AP-2, Dab2, ARH, transferrin, and LDL receptors are all present within the vast majority of clathrin structures at the surface, challenging the general existence of specialized clathrin coats for segregated internalization of constitutively internalized cargo. However, Dab2 expression is exceptionally low in hepatocytes, likely accounting for the pathological hypercholesterolemia that accompanies ARH loss.
机译:将跨膜货物分选到网格蛋白包被的囊泡中需要胞吞衔接子,但RNA干扰(RNAi)介导的AP-2衔接子复合物的基因沉默只会破坏一部分网格蛋白依赖性货物的内在化。这表明替代网格蛋白相关的分选蛋白参与细胞表面的货物捕获,并且最近的一项提议是将离散的内吞货物分类为组成和功能各异的网格蛋白涂层。我们在这里显示LDL受体的胞质域内的FXNPXY型内在信号被两个磷酸酪氨酸结合域蛋白Dab2和ARH多余地识别。通过RNAi减少这两种蛋白质会导致LDL受体在细胞表面明显聚集。在没有Dab2和ARH的情况下,相对于AP-2依赖性的转铁蛋白的吸收相对正常,这清楚地揭示了芽部位分选操作的授权。 AP-2,Dab2,ARH,转铁蛋白和LDL受体全部存在于表面的绝大多数网格蛋白结构中,这对用于组成型内部化货物的单独内部化的专用网格蛋白涂层的普遍存在提出了挑战。但是,Dab2在肝细胞中的表达异常低,这可能解释了伴随ARH丢失的病理性高胆固醇血症。

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