Renal-Electrolyte Division, Department of Medicine, University of Pittsburgh, Pittsburgh, PA, USA.
Traffic. 2012 Sep;13(9):1295-305. doi: 10.1111/j.1600-0854.2012.01387.x. Epub 2012 Jul 4.
Lowe syndrome is an X-linked disorder characterized by cataracts at birth, mental retardation and progressive renal malfunction that results from loss of function of the OCRL1 (oculocerebrorenal syndrome of Lowe) protein. OCRL1 is a lipid phosphatase that converts phosphatidylinositol 4,5-bisphosphate to phosphatidylinositol 4-phosphate. The renal pathogenesis of Lowe syndrome patients has been suggested to result from alterations in membrane trafficking, but this cannot fully explain the disease progression. We found that knockdown of OCRL1 in zebrafish caused developmental defects consistent with disruption of ciliary function, including body axis curvature, pericardial edema, hydrocephaly and impaired renal clearance. In addition, cilia in the proximal tubule of the zebrafish pronephric kidney were longer in ocrl morphant embryos. We also found that knockdown of OCRL1 in polarized renal epithelial cells caused elongation of the primary cilium and disrupted formation of cysts in three-dimensional cultures. Calcium release in response to ATP was blunted in OCRL1 knockdown cells, suggesting changes in signaling that could lead to altered cell function. Our results suggest a new role for OCRL1 in renal epithelial cell function that could contribute to the pathogenesis of Lowe syndrome.
Lowe 综合征是一种 X 连锁疾病,其特征为出生时即有白内障、智力障碍和进行性肾功能衰竭,这是由于 OCRL1( Lowe 眼-脑-肾综合征)蛋白功能丧失所致。OCRL1 是一种脂质磷酸酶,可将磷脂酰肌醇 4,5-二磷酸转化为磷脂酰肌醇 4-磷酸。 Lowe 综合征患者的肾脏发病机制被认为是由于膜运输的改变,但这不能完全解释疾病的进展。我们发现,在斑马鱼中敲低 OCRL1 会导致与纤毛功能障碍一致的发育缺陷,包括身体轴弯曲、心包水肿、脑积水和肾功能清除受损。此外,ocrl 突变体胚胎中斑马鱼肾前肾近端小管的纤毛更长。我们还发现,在极化的肾上皮细胞中敲低 OCRL1 会导致初级纤毛伸长,并破坏三维培养物中囊肿的形成。OCRL1 敲低细胞对 ATP 的钙释放减弱,表明信号转导的变化可能导致细胞功能改变。我们的研究结果表明 OCRL1 在肾上皮细胞功能中的新作用,可能有助于 Lowe 综合征的发病机制。
