纤维性多囊性肝肾疾病模型中的小分子纤维激酶抑制剂。

Prani Paka, Brian Huang, Bin Duan, Jing-Song Li, Ping Zhou, Latha Paka, Michael A Yamin, Scott L Friedman, Itzhak D Goldberg, Prakash Narayan
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引用次数: 2

摘要

目的:探讨新型血小板源性生长因子受体和血管内皮生长因子受体双激酶抑制剂ANG3070在多囊肾病-先天性肝纤维化模型中的作用。方法:在6周龄时,将PCK大鼠随机分为对照组和ANG3070组,持续4周。在10周时,收集24 h尿液和左肾,继续给药4周。14周取24 h尿液,处死大鼠,取肝、右肾进行组织学评价。在Western blot研究中,PCK大鼠用载药或ANG3070处理7 d,并在最后一次处理后约30分钟后处死。结果:与野生型队列相比,PCK肾脏(Vehicle队列)的肾脏和肝脏质量、肝肾囊体积、肝肾纤维化和肝肾损伤生物标志物显著增加。与PCK- vehicle队列相比,ANG3070干预PCK大鼠的肾脏重量降低,肾囊体积减小,肾羟脯氨酸总量减少,表明租期间质纤维化明显减少。ANG3070治疗还减轻了几种肾损伤标志物,包括尿中性粒细胞明胶酶相关脂钙素、肾损伤分子-1、胱抑素C和白细胞介素-18水平。此外,与PCK-Vehicle队列相比,该治疗降低了肾功能的关键指标,包括蛋白尿、蛋白尿和血清尿素氮、肌酐,并显著改善了肾功能。与PCK-Vehicle队列相比,ANG3070治疗还显著减少了肝肿大、肝病变和肝纤维化,并减轻了肝功能障碍。结论:这些结果表明ANG3070具有减缓疾病的潜力,可能成为纤维多囊病患者肝肾移植的桥梁。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A small molecule fibrokinase inhibitor in a model of fibropolycystic hepatorenal disease.

A small molecule fibrokinase inhibitor in a model of fibropolycystic hepatorenal disease.

A small molecule fibrokinase inhibitor in a model of fibropolycystic hepatorenal disease.

A small molecule fibrokinase inhibitor in a model of fibropolycystic hepatorenal disease.

Aim: To evaluate the novel platelet-derived growth factor receptor and vascular endothelial growth factor receptor dual kinase inhibitor ANG3070 in a polycystic kidney disease-congenital hepatic fibrosis model.

Methods: At 6 wk of age, PCK rats were randomized to vehicle or ANG3070 for 4 wk. At 10 wk, 24 h urine and left kidneys were collected and rats were continued on treatment for 4 wk. At 14 wk, 24 h urine was collected, rats were sacrificed, and liver and right kidneys were collected for histological evaluation. For Western blot studies, PCK rats were treated with vehicle or ANG3070 for 7 d and sacrificed approximately 30 min after the last treatments.

Results: Compared to the wild-type cohort, the PCK kidney (Vehicle cohort) exhibited a marked increase in kidney and liver mass, hepato-renal cystic volume, hepato-renal fibrosis and hepato-renal injury biomarkers. Intervention with ANG3070 in PCK rats decreased kidney weight, reduced renal cystic volume and reduced total kidney hydroxyproline, indicating significantly reduced rental interstitial fibrosis compared to the PCK-Vehicle cohort. ANG3070 treatment also mitigated several markers of kidney injury, including urinary neutrophil gelatinase-associated lipocalin, kidney injury molecule-1, cystatin C and interleukin-18 levels. In addition, this treatment attenuated key indices of renal dysfunction, including proteinuria, albuminuria and serum blood urea nitrogen and creatinine, and significantly improved renal function compared to the PCK-Vehicle cohort. ANG3070 treatment also significantly decreased liver enlargement, hepatic lesions, and liver fibrosis, and mitigated liver dysfunction compared to the PCK-Vehicle cohort.

Conclusion: These results suggest that ANG3070 has the potential to slow disease, and may serve as a bridge toward hepato-renal transplantation in patients with fibropolycystic disease.

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