Dual therapy with vildagliptin and sacubitril/valsartan alleviates portal hypertension and inhibits soluble epoxide hydrolase in cirrhotic rats.

IF 5.4 3区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

World Journal of Gastroenterology Pub Date : 2025-09-07 DOI:10.3748/wjg.v31.i33.109562

Masafumi Oyama, Kosuke Kaji, Norihisa Nishimura, Junichi Hanatani, Tatsuya Nakatani, Naoki Nishimura, Akihiko Shibamoto, Shohei Asada, Yuki Tsuji, Koh Kitagawa, Shinya Sato, Tadashi Namisaki, Hitoshi Yoshiji

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引用次数: 0

Abstract

Background: Portal hypertension (PH), a major complication of cirrhosis, arises from increased intrahepatic resistance and splanchnic vasodilation. Epoxyeicosatrienoic acids (EETs) improve hepatic microcirculation, but their effects are rapidly inactivated by soluble epoxide hydrolase (sEH), an enzyme upregulated in the cirrhotic liver. Inhibiting sEH increases EET levels, reducing portal pressure and fibrosis. Dipeptidyl peptidase-4 inhibitors (DPP4-Is) and angiotensin II blockers have been reported to suppress sEH and enhance EET activity. Angiotensin receptor-neprilysin inhibitors (ARNIs) also lower portal pressure. However, the combined effect of DPP4-I and ARNI on the sEH-EET axis in PH and liver fibrosis remains uninvestigated.

Aim: To study the effects of vildagliptin, a DPP4-I and sacubitril/valsartan, an ARNI on PH and liver fibrosis in cirrhotic rats.

Methods: Two rodent models of liver cirrhosis: (1) Choline-deficient, L-amino acid-defined, high-fat diet (CDAHFD) diet-fed rats; and (2) Bile duct ligation-induced rats were treated with vildagliptin (10 mg/kg/day), sacubitril/valsartan (30 mg/kg/day), or a combination of both drugs. Hemodynamic parameters, sEH activity, EET levels, vascular remodeling, and fibrosis were assessed using enzyme-linked immunosorbent assay, quantitative real-time polymerase chain reaction, Western blotting, histology, and immunofluorescence.

Results: In CDAHFD-fed models, both DPP4-I and ARNI significantly reduced portal pressure in cirrhotic rats by decreasing intrahepatic vascular resistance without affecting systemic hemodynamics. These agents downregulated sEH expression and activity, increasing EET levels, and improved endothelial function via nitric oxide signaling enhancement. They also suppressed sinusoidal capillarization, pathological angiogenesis, and Hedgehog signaling, while restoring sinusoidal endothelial markers. Additionally, DPP4-I and ARNI attenuated liver fibrosis and stellate cell activation, reducing profibrotic gene expression. These effects were additive by the combination of both drugs. Similar effects were observed in bile duct ligation-induced PH, confirming their therapeutic potential in managing both PH and liver fibrosis through modulation of the sEH-EET pathway.

Conclusion: Combined DPP4-I with ARNI therapy ameliorates PH and fibrosis via sEH suppression and EET restoration, offering a promising treatment strategy for cirrhosis-related PH.

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维格列汀和苏比里尔/缬沙坦双重治疗可减轻肝硬化大鼠门脉高压并抑制可溶性环氧化物水解酶。

背景：门脉高压（PH）是肝硬化的主要并发症，由肝内阻力增加和内脏血管舒张引起。环氧二碳三烯酸（EETs）可改善肝脏微循环，但其作用会被可溶性环氧化物水解酶（sEH）迅速灭活，这种酶在肝硬化中表达上调。抑制sEH可增加EET水平，降低门静脉压力和纤维化。二肽基肽酶-4抑制剂（DPP4-Is）和血管紧张素II阻滞剂有抑制sEH和增强EET活性的报道。血管紧张素受体-neprilysin抑制剂（ARNIs）也能降低门静脉压力。然而，DPP4-I和ARNI对PH和肝纤维化中sEH-EET轴的联合作用尚未研究。目的：研究维格列汀（DPP4-I）和苏比里尔/缬沙坦（ARNI）对肝硬化大鼠PH和肝纤维化的影响。方法：两种肝硬化啮齿动物模型：(1)胆碱缺乏、l -氨基酸限定、高脂肪饮食（CDAHFD）喂养的大鼠；(2)胆管结扎大鼠分别给予维格列汀（10 mg/kg/天）、苏比里尔/缬沙坦（30 mg/kg/天）或两种药物联合治疗。采用酶联免疫吸附法、定量实时聚合酶链反应、Western blotting、组织学和免疫荧光法评估血液动力学参数、sEH活性、EET水平、血管重塑和纤维化。结果：在cdahfd喂养的模型中，DPP4-I和ARNI均通过降低肝内血管阻力而显著降低肝硬化大鼠的门静脉压力，而不影响全身血流动力学。这些药物下调sEH表达和活性，增加EET水平，并通过增强一氧化氮信号改善内皮功能。它们还抑制了窦状动脉毛细血管形成、病理性血管生成和Hedgehog信号，同时恢复了窦状动脉内皮标志物。此外，DPP4-I和ARNI可减轻肝纤维化和星状细胞活化，降低促纤维化基因表达。这些效果是两种药物联合作用的结果。在胆管结扎诱导的PH中观察到类似的效果，证实了它们通过调节sEH-EET途径在控制PH和肝纤维化方面的治疗潜力。结论：DPP4-I联合ARNI治疗通过抑制sEH和恢复EET改善PH和纤维化，为肝硬化相关PH提供了一种有希望的治疗策略。

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来源期刊

World Journal of Gastroenterology 医学-胃肠肝病学

CiteScore

7.80

自引率

4.70%

发文量

464

审稿时长

2.4 months

期刊介绍： The primary aims of the WJG are to improve diagnostic, therapeutic and preventive modalities and the skills of clinicians and to guide clinical practice in gastroenterology and hepatology.