Division of Nephrology, Department of Medicine, University of Maryland School of Medicine, Baltimore, MD, USA.
Laboratory of Clinical Investigation, National Institute on Aging, National Institutes of Health, Baltimore, MD, USA.
Nat Commun. 2023 Oct 16;14(1):6513. doi: 10.1038/s41467-023-42196-4.
Fibrocystin/Polyductin (FPC), encoded by PKHD1, is associated with autosomal recessive polycystic kidney disease (ARPKD), yet its precise role in cystogenesis remains unclear. Here we show that FPC undergoes complex proteolytic processing in developing kidneys, generating three soluble C-terminal fragments (ICDs). Notably, ICD, contains a novel mitochondrial targeting sequence at its N-terminus, facilitating its translocation into mitochondria. This enhances mitochondrial respiration in renal epithelial cells, partially restoring impaired mitochondrial function caused by FPC loss. FPC inactivation leads to abnormal ultrastructural morphology of mitochondria in kidney tubules without cyst formation. Moreover, FPC inactivation significantly exacerbates renal cystogenesis and triggers severe pancreatic cystogenesis in a Pkd1 mouse mutant Pkd1 in which cleavage of Pkd1-encoded Polycystin-1 at the GPCR Proteolysis Site is blocked. Deleting ICD enhances renal cystogenesis without inducing pancreatic cysts in Pkd1 mice. These findings reveal a direct link between FPC and a mitochondrial pathway through ICD cleavage, crucial for cystogenesis mechanisms.
纤维多囊蛋白/多囊蛋白(FPC)由 PKHD1 编码,与常染色体隐性多囊肾病(ARPKD)相关,但它在囊泡形成中的确切作用仍不清楚。在这里,我们发现 FPC 在发育中的肾脏中经历复杂的蛋白水解加工,生成三个可溶性 C 端片段(ICD)。值得注意的是,ICD 在其 N 端包含一个新的线粒体靶向序列,促进其向线粒体易位。这增强了肾上皮细胞中的线粒体呼吸,部分恢复了由 FPC 缺失引起的受损线粒体功能。FPC 失活导致肾脏小管中线粒体的超微结构形态异常,而没有囊泡形成。此外,FPC 失活显著加剧了肾囊肿的发生,并在 Pkd1 突变鼠 Pkd1 中触发严重的胰腺囊肿发生,其中 Pkd1 编码的多囊蛋白-1 在 GPCR 蛋白水解位点的切割被阻断。在 Pkd1 小鼠中删除 ICD 增强了肾囊肿的发生,但没有诱导胰腺囊肿。这些发现揭示了 FPC 与通过 ICD 切割的线粒体途径之间的直接联系,这对囊泡形成机制至关重要。
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