Department of Pediatrics, Feinberg School of Medicine, Northwestern University, Chicago , IL, USA.
J Lipid Res. 2011 Jul;52(7):1328-44. doi: 10.1194/jlr.M012377. Epub 2011 May 16.
Niemann-Pick disease, type C (NP-C), often associated with Niemann-Pick disease, type C1 (NPC1) mutations, is a cholesterol-storage disorder characterized by cellular lipid accumulation, neurodegeneration, and reduced steroid production. To study NPC1 function in vivo, we cloned zebrafish npc1 and analyzed its gene expression and activity by reducing Npc1 protein with morpholino (MO)-oligonucleotides. Filipin staining in npc1-morphant cells was punctate, suggesting abnormal accumulation of cholesterol. Developmentally, reducing Npc1 did not disrupt early cell fate or survival; however, early morphogenetic movements were delayed, and the actin cytoskeleton network was abnormal. MO-induced defects were rescued with ectopic expression of mouse NPC1, demonstrating functional gene conservation, and by treatments with steroids pregnenolone or dexamethasone, suggesting that reduced steroidogenesis contributed to abnormal cell movements. Cell death was found in anterior tissues of npc1 morphants at later stages, consistent with findings in mammals. Collectively, these studies show that npc1 is required early for proper cell movement and cholesterol localization and later for cell survival.
尼曼-匹克病 C 型(NP-C)常与尼曼-匹克病 C1 型(NPC1)突变相关,是一种胆固醇贮积病,其特征为细胞脂质蓄积、神经退行性变和类固醇生成减少。为了在体内研究 NPC1 的功能,我们克隆了斑马鱼 NPC1,并通过使用反义寡核苷酸(MO)降低 NPC1 蛋白的方法分析其基因表达和活性。npc1 突变体细胞中的 Filipin 染色呈点状,提示胆固醇异常蓄积。在发育过程中,降低 NPC1 并未破坏早期细胞命运或存活;然而,早期的形态发生运动被延迟,肌动蛋白细胞骨架网络异常。用外源表达的鼠 NPC1 挽救 MO 诱导的缺陷,证明了功能基因的保守性,并且用类固醇孕烯醇酮或地塞米松处理,提示类固醇生成减少导致了异常的细胞运动。在后期,npc1 突变体的前体组织中发现了细胞死亡,这与哺乳动物的发现一致。总之,这些研究表明 NPC1 早期对于适当的细胞运动和胆固醇定位,后期对于细胞存活是必需的。
