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CSPP Is a Ciliary Protein Interacting with Nephrocystin 8 and Required for Cilia Formation

机译:CSPP是一种与Nerorocystin 8相互作用的睫状蛋白,是纤毛形成所必需的

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We described previously the cell cycle- and microtubule-related functions of two splice isoforms of the centrosome spindle pole-associated protein (CSPP and CSPP-L). Here, we show that endogenous CSPP isoforms not only localize to centrosomes and the midbody in cycling cells but also extend to the cilia axoneme in postmitotic resting cells. They are required for ciliogenesis in hTERT-RPE1 cells in vitro and are expressed in ciliated renal, retinal, and respiratory cells in vivo. We report that CSPP isoforms require their common C-terminal domain to interact with Nephrocystin 8 (NPHP8/RPGRIP1L) and to form a ternary complex with NPHP8 and NPHP4. We find CSPP-L to be required for the efficient localization of NPHP8 but not NPHP4 to the basal body. The ciliogenesis defect in hTERT-RPE1 cells is, however, not mediated through loss of NPHP8. Similar to the effects of ectopical expression of CSPP-L, cilia length increased in NPHP8-depleted cells. Our results thus suggest that CSPP proteins may be involved in further cytoskeletal organization of the basal body and its primary cilium. To conclude, we have identified a novel, nonmitotic function of CSPP proteins placing them into a ciliary protein network crucial for normal renal and retinal tissue architecture and physiology.
机译:我们先前描述了中心体纺锤体极相关蛋白(CSPP和CSPP-L)的两个剪接同工型的细胞周期和微管相关功能。在这里,我们显示内源性CSPP亚型不仅位于循环细胞中的中心体和中体,而且还延伸至有丝分裂后静息细胞中的纤毛轴突。它们是hTERT-RPE1细胞体外纤毛形成所必需的,并在体内纤毛的肾,视网膜和呼吸道细胞中表达。我们报告CSPP亚型需要其共同的C末端域与Nephrocystin 8(NPHP8 / RPGRIP1L)相互作用,并与NPHP8和NPHP4形成三元复合物。我们发现CSPP-L是NPHP8高效定位所必需的,而不是NPHP4到基体的有效定位。然而,hTERT-RPE1细胞的纤毛发生缺陷不是通过NPHP8的丢失来介导的。与异位表达CSPP-L的效果相似,在NPHP8缺失的细胞中,纤毛长度增加。因此,我们的结果表明CSPP蛋白可能参与了基体及其初级纤毛的进一步细胞骨架组织。总而言之,我们确定了CSPP蛋白的新型非有丝分裂功能,将其置于对正常肾和视网膜组织结构和生理至关重要的睫状蛋白网络中。

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