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异鼠李素在培养肝细胞和模型小鼠中的抗高尿酸血症作用:甲基槲皮素作为尿酸生成抑制剂的构效关系

Anti-hyperuricemic effect of isorhamnetin in cultured hepatocytes and model mice: structure-activity relationships of methylquercetins as inhibitors of uric acid production.

作者信息

Adachi Shin-Ichi, Kondo Shinji, Sato Yusuke, Yoshizawa Fumiaki, Yagasaki Kazumi

机构信息

Center for Bioscience Research and Education, Utsunomiya University, Utsunomiya, Tochigi, 321-8505, Japan.

Faculty of Agriculture, Utsunomiya University, Utsunomiya, Tochigi, 321-8505, Japan.

出版信息

Cytotechnology. 2019 Feb;71(1):181-192. doi: 10.1007/s10616-018-0275-8. Epub 2019 Jan 2.

Abstract

Hyperuricemia is an important risk factor for gout. Isorhamnetin (3'-O-methylquercetin) is an O-methylated flavonol, which occurs in onion, almond and sea buckthorn. It is also one of the metabolites of quercetin in mammals. In the present study, we investigated anti-hyperuricemic effect of isorhamnetin adopting both cultured hepatocytes and mice with hyperuricemia induced by purine bodies. In cultured hepatocytes, isorhamnetin as well as quercetin significantly and dose-dependently inhibited uric acid (UA) production. We also examined the inhibitory effects on UA production of other mono-methylquercetins, i.e., tamarixetin, 3-O-methylquercetin, azaleatin, and rhamnetin in addition to isorhamnetin for studying their structure-activity relationships. From the results obtained, hydroxyl groups at C-3, C-5, and especially C-7, but not C-3' and C-4' of quercetin are demonstrated to play a critical role in suppressing UA production in the AML12 hepatocytes. Oral administration of isorhamnetin significantly reduced plasma and hepatic UA levels in the hyperuricemic model mice. Isorhamnetin also decreased hepatic xanthine oxidase (XO) activity without changes in XO protein expression, indicating that anti-hyperuricemic effect of isorhamnetin could be, at least partly, attributable to suppression of UA production by directly inhibiting XO activity in the liver. These findings demonstrate that isorhamnetin has a potent anti-hyperuricemic effect and may be a potential candidate for prevention and remediation of hyperuricemia.

摘要

高尿酸血症是痛风的重要危险因素。异鼠李素(3'-O-甲基槲皮素)是一种O-甲基化黄酮醇,存在于洋葱、杏仁和沙棘中。它也是槲皮素在哺乳动物体内的代谢产物之一。在本研究中,我们采用培养的肝细胞和由嘌呤体诱导的高尿酸血症小鼠,研究了异鼠李素的抗高尿酸血症作用。在培养的肝细胞中,异鼠李素和槲皮素均能显著且呈剂量依赖性地抑制尿酸(UA)生成。我们还研究了除异鼠李素外的其他单甲基槲皮素,即山柰酚、3-O-甲基槲皮素、杜鹃花素和鼠李素对UA生成的抑制作用,以研究它们的构效关系。从所得结果来看,槲皮素C-3、C-5尤其是C-7位的羟基,而非C-3'和C-4'位的羟基,在抑制AML12肝细胞中UA生成方面起着关键作用。对高尿酸血症模型小鼠口服异鼠李素可显著降低血浆和肝脏中的UA水平。异鼠李素还降低了肝脏黄嘌呤氧化酶(XO)的活性,而XO蛋白表达没有变化,这表明异鼠李素的抗高尿酸血症作用至少部分归因于通过直接抑制肝脏中的XO活性来抑制UA生成。这些发现表明异鼠李素具有强大的抗高尿酸血症作用,可能是预防和治疗高尿酸血症的潜在候选药物。

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