Department of Medicine, Pulmonary, Allergy, and Critical Care Division, University of Pennsylvania, Philadelphia, PA, USA.
J Lipid Res. 2011 Aug;52(8):1471-82. doi: 10.1194/jlr.M013284. Epub 2011 May 17.
The ATP binding cassette, class A (ABCA) proteins are homologous polytopic transmembrane transporters that function as lipid pumps at distinct subcellular sites in a variety of cells. Located within the N terminus of these transporters, there exists a highly conserved xLxxKN motif of unknown function. To define its role, human ABCA3 was employed as a primary model representing ABCA transporters, while mouse ABCA1 was utilized to support major findings. Transfection studies showed colocalization of both transporters with surfactant protein C (SP-C), a marker peptide for successful protein targeting to lysosomal-like organelles. In contrast, alanine mutation of xLxxKN resulted in endoplasmic reticulum retention. As proof of principle, swapping xLxxKN for the known lysosomal targeting motif of SP-C resulted in post-Golgi targeting of the SP-C chimera. However, these products failed to reach their terminal processing compartments, suggesting that the xLxxKN motif only serves as a Golgi exit signal. We propose a model whereby an N-terminal signal sequence, xLxxKN, directs ABCA transporters to a post-Golgi vesicular sorting station where additional signals may be required for selective delivery of individual transporters to final subcellular destinations.
ATP 结合盒式蛋白,A 类(ABCA)蛋白是同源的多跨膜转运蛋白,在多种细胞的不同亚细胞部位作为脂质泵发挥作用。这些转运蛋白的 N 端存在一个高度保守的 xLxxKN 模体,但其功能未知。为了确定其作用,我们用人 ABCA3 作为主要模型来代表 ABCA 转运蛋白,同时使用鼠 ABCA1 来支持主要发现。转染研究表明,两种转运蛋白均与表面活性蛋白 C(SP-C)共定位,SP-C 是一种标记肽,用于成功靶向溶酶体样细胞器。相反,xLxxKN 的丙氨酸突变导致内质网滞留。作为原理的证明,将 xLxxKN 替换为 SP-C 的已知溶酶体靶向基序导致 SP-C 嵌合体的高尔基体后靶向。然而,这些产物未能到达其终末加工隔室,表明 xLxxKN 模体仅作为高尔基体出口信号。我们提出了一个模型,即 N 端信号序列 xLxxKN 将 ABCA 转运蛋白引导到高尔基体后囊泡分拣站,在该分拣站,可能需要其他信号来选择性地将单个转运蛋白递送到最终的亚细胞目的地。
