Leibniz-Institut für Molekulare Pharmakologie and Max-Delbrück-Centrum für Molekulare Medizin, Robert-Rössle-Strasse 10, D-13125 Berlin, Germany.
J Biol Chem. 2010 Jun 4;285(23):17595-603. doi: 10.1074/jbc.M110.115600. Epub 2010 Mar 29.
Inactivation of the mainly endosomal 2Cl(-)/H(+)-exchanger ClC-5 severely impairs endocytosis in renal proximal tubules and underlies the human kidney stone disorder Dent's disease. In heterologous expression systems, interaction of the E3 ubiquitin ligases WWP2 and Nedd4-2 with a "PY-motif" in the cytoplasmic C terminus of ClC-5 stimulates its internalization from the plasma membrane and may influence receptor-mediated endocytosis. We asked whether this interaction is relevant in vivo and generated mice in which the PY-motif was destroyed by a point mutation. Unlike ClC-5 knock-out mice, these knock-in mice displayed neither low molecular weight proteinuria nor hyperphosphaturia, and both receptor-mediated and fluid-phase endocytosis were normal. The abundances and localizations of the endocytic receptor megalin and of the Na(+)-coupled phosphate transporter NaPi-2a (Npt2) were not changed, either. To explore whether the discrepancy in results from heterologous expression studies might be due to heteromerization of ClC-5 with ClC-3 or ClC-4 in vivo, we studied knock-in mice additionally deleted for those related transporters. Disruption of neither ClC-3 nor ClC-4 led to proteinuria or impaired proximal tubular endocytosis by itself, nor in combination with the PY-mutant of ClC-5. Endocytosis of cells lacking ClC-5 was not impaired further when ClC-3 or ClC-4 was additionally deleted. We conclude that ClC-5 is unique among CLC proteins in being crucial for proximal tubular endocytosis and that PY-motif-dependent ubiquitylation of ClC-5 is dispensable for this role.
主要位于内体的 2Cl(-)/H(+)交换体 ClC-5 的失活严重损害了肾脏近端小管的内吞作用,并导致了人类肾结石疾病 Dent 病。在异源表达系统中,E3 泛素连接酶 WWP2 和 Nedd4-2 与 ClC-5 细胞质 C 末端的“PY 基序”相互作用,刺激其从质膜内化,并可能影响受体介导的内吞作用。我们想知道这种相互作用在体内是否相关,并生成了一个点突变破坏了 PY 基序的 ClC-5 敲入小鼠。与 ClC-5 敲除小鼠不同,这些敲入小鼠既没有出现低分子量蛋白尿,也没有出现高磷酸盐尿,并且受体介导的和液相等内吞作用均正常。内吞作用受体 megalin 和 Na(+)-偶联磷酸盐转运体 NaPi-2a (Npt2) 的丰度和定位也没有改变。为了探讨异源表达研究中的结果差异是否可能是由于 ClC-5 与 ClC-3 或 ClC-4 在体内异源二聚化所致,我们还研究了另外敲除这些相关转运体的敲入小鼠。ClC-3 或 ClC-4 的缺失本身既不会导致蛋白尿,也不会损害近端肾小管的内吞作用,也不会与 ClC-5 的 PY 突变体结合。当另外缺失 ClC-5 时,缺乏 ClC-3 或 ClC-4 的细胞的内吞作用没有进一步受损。我们得出结论,ClC-5 在 CLC 蛋白中是独特的,对于近端肾小管的内吞作用至关重要,而 ClC-5 的 PY 基序依赖性泛素化对于这一作用是可有可无的。