Department of Internal Medicine.
Jared Grantham Kidney Institute.
JCI Insight. 2021 Mar 30;6(8):141299. doi: 10.1172/jci.insight.141299.
Despite the recent launch of tolvaptan, the search for safer polycystic kidney disease (PKD) drugs continues. Ciclopirox (CPX) or its olamine salt (CPX-O) is contained in a number of commercially available antifungal agents. CPX is also reported to possess anticancer activity. Several mechanisms of action have been proposed, including chelation of iron and inhibition of iron-dependent enzymes. Here, we show that CPX-O inhibited in vitro cystogenesis of primary human PKD cyst-lining epithelial cells cultured in a 3D collagen matrix. To assess the in vivo role of CPX-O, we treated PKD mice with CPX-O. CPX-O reduced the kidney-to-body weight ratios of PKD mice. The CPX-O treatment was also associated with decreased cell proliferation, decreased cystic area, and improved renal function. Ferritin levels were markedly elevated in cystic kidneys of PKD mice, and CPX-O treatment reduced renal ferritin levels. The reduction in ferritin was associated with increased ferritinophagy marker nuclear receptor coactivator 4, which reversed upon CPX-O treatment in PKD mice. Interestingly, these effects on ferritin appeared independent of iron. These data suggest that CPX-O can induce ferritin degradation via ferritinophagy, which is associated with decreased cyst growth progression in PKD mice. Most importantly these data indicate that CPX-O has the potential to treat autosomal dominant PKD.
尽管托伐普坦最近已经上市,但人们仍在继续寻找更安全的多囊肾病 (PKD) 药物。环吡酮(CPX)或其油胺盐(CPX-O)包含在许多市售的抗真菌药物中。CPX 也被报道具有抗癌活性。已经提出了几种作用机制,包括铁螯合和抑制铁依赖性酶。在这里,我们表明 CPX-O 抑制了在 3D 胶原基质中培养的原代人 PKD 囊泡衬里上皮细胞的体外囊泡发生。为了评估 CPX-O 在体内的作用,我们用 CPX-O 治疗 PKD 小鼠。CPX-O 降低了 PKD 小鼠的肾脏与体重比。CPX-O 治疗还与细胞增殖减少、囊泡面积减少和肾功能改善有关。PKD 小鼠囊泡肾脏中的铁蛋白水平显著升高,CPX-O 治疗降低了肾脏铁蛋白水平。铁蛋白水平的降低与铁蛋白自噬标志物核受体共激活物 4 的增加有关,而在 PKD 小鼠中 CPX-O 治疗后则逆转。有趣的是,这些铁蛋白的变化似乎与铁无关。这些数据表明,CPX-O 可以通过铁蛋白自噬诱导铁蛋白降解,从而与 PKD 小鼠中囊泡生长进展减少相关。最重要的是,这些数据表明 CPX-O 有可能治疗常染色体显性多囊肾病。
