Alantolactone Attenuates Renal Fibrosis via Inhibition of Transforming Growth Factor β/Smad3 Signaling Pathway.

IF 6.8 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetes & Metabolism Journal Pub Date : 2024-01-01 Epub Date: 2024-01-03 DOI:10.4093/dmj.2022.0231

Kyeong-Min Lee, Yeo Jin Hwang, Gwon-Soo Jung

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引用次数: 0

Abstract

Backgruound: Renal fibrosis is characterized by the accumulation of extracellular matrix proteins and interstitial fibrosis. Alantolactone is known to exert anticancer, anti-inflammatory, antimicrobial and antifungal effects; however, its effects on renal fibrosis remains unknown. Here, we investigated whether alantolactone attenuates renal fibrosis in mice unilateral ureteral obstruction (UUO) and evaluated the effect of alantolactone on transforming growth factor (TGF) signaling pathway in renal cells.

Methods: To evaluate the therapeutic effect of alantolactone, cell counting kit-8 (CCK-8) assay, histological staining, Western blot analysis, and real-time quantitative polymerase chain reaction were performed in UUO kidneys in vivo and in TGF-β-treated renal cells in vitro.

Results: Alantolactone (0.25 to 4 µM) did not affect the viability of renal cells. Mice orally administered 5 mg/kg of alantolactone daily for 15 days did not show mortality or liver toxicity. Alantolactone decreased UUO-induced blood urea nitrogen and serum creatinine levels. In addition, it significantly alleviated renal tubulointerstitial damage and fibrosis and decreased collagen type I, fibronectin, and α-smooth muscle actin (α-SMA) expression in UUO kidneys. In NRK-49F cells, alantolactone inhibited TGF-βstimulated expression of fibronectin, collagen type I, plasminogen activator inhibitor-1 (PAI-1), and α-SMA. In HK-2 cells, alantolactone inhibited TGF-β-stimulated expression of collagen type I and PAI-1. Alantolactone inhibited UUO-induced phosphorylation of Smad3 in UUO kidneys. In addition, it not only decreased TGF-β secretion but also Smad3 phosphorylation and translocation to nucleus in both kidney cell lines.

Conclusion: Alantolactone improves renal fibrosis by inhibiting the TGF-β/Smad3 signaling pathway in obstructive nephropathy. Thus, alantolactone is a potential therapeutic agent for chronic kidney disease.

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金刚烷内酯通过抑制转化生长因子β/Smad3信号通路减轻肾脏纤维化

背景：肾脏纤维化的特征是细胞外基质蛋白的积累和间质纤维化。已知金刚烷内酯具有抗癌、抗炎、抗菌和抗真菌作用，但其对肾脏纤维化的影响尚不清楚。在此，我们研究了金刚烷内酯是否能减轻小鼠单侧输尿管梗阻（UUO）的肾脏纤维化，并评估了金刚烷内酯对肾脏细胞中转化生长因子（TGF）信号通路的影响：为了评估金刚烷内酯的治疗效果，对体内UUO肾脏和体外TGF-β处理的肾细胞进行了细胞计数试剂盒-8（CCK-8）检测、组织学染色、Western印迹分析和实时定量聚合酶链反应：结果：金刚烷内酯（0.25 至 4 µM）不影响肾细胞的活力。小鼠连续 15 天每天口服 5 毫克/千克的金刚烷内酯，没有出现死亡或肝脏毒性。金刚烷内酯可降低 UUO 诱导的血尿素氮和血清肌酐水平。此外，它还能明显减轻 UUO 肾小管间质损伤和纤维化，降低 I 型胶原、纤连蛋白和 α 平滑肌肌动蛋白（α-SMA）的表达。在 NRK-49F 细胞中，金刚烷内酯抑制了 TGF-β 刺激的纤维粘连蛋白、I 型胶原、纤溶酶原激活剂抑制剂-1（PAI-1）和 α-SMA 的表达。在 HK-2 细胞中，金刚烷内酯抑制了 TGF-β 刺激的 I 型胶原和 PAI-1 的表达。金刚烷内酯抑制了 UUO 诱导的 Smad3 在 UUO 肾脏中的磷酸化。此外，它不仅减少了 TGF-β 的分泌，还减少了两种肾细胞系中 Smad3 的磷酸化和向细胞核的转位：结论：金刚烷内酯可通过抑制阻塞性肾病的 TGF-β/Smad3 信号通路改善肾脏纤维化。因此，金刚烷内酯是一种治疗慢性肾病的潜在药物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Diabetes & Metabolism Journal Medicine-Endocrinology, Diabetes and Metabolism

CiteScore

10.40

自引率

6.80%

发文量

审稿时长

52 weeks

期刊介绍： The aims of the Diabetes & Metabolism Journal are to contribute to the cure of and education about diabetes mellitus, and the advancement of diabetology through the sharing of scientific information on the latest developments in diabetology among members of the Korean Diabetes Association and other international societies. The Journal publishes articles on basic and clinical studies, focusing on areas such as metabolism, epidemiology, pathogenesis, complications, and treatments relevant to diabetes mellitus. It also publishes articles covering obesity and cardiovascular disease. Articles on translational research and timely issues including ubiquitous care or new technology in the management of diabetes and metabolic disorders are welcome. In addition, genome research, meta-analysis, and randomized controlled studies are welcome for publication. The editorial board invites articles from international research or clinical study groups. Publication is determined by the editors and peer reviewers, who are experts in their specific fields of diabetology.

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