Uric acid mediates kidney tubular inflammation through the LDHA/ROS/NLRP3 pathway.

IF 1.5 4区 医学 Q3 PERIPHERAL VASCULAR DISEASE
Jun Ouyang, Hui Wang, Yumei Gan, Jiangnan Huang
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Abstract

Purpose: Hyperuricemia (HUA) is an important factor leading to chronic kidney disease (CKD). The kidney tubular inflammatory response is activated in HUA. This study aimed to investigate whether lactate dehydrogenase A (LDHA) is involved in mediating uric acid-induced kidney tubular inflammatory response.

Methods: In vivo, an HUA mouse model was established by continuous intraperitoneal injection of potassium oxonate (PO) for one week. A total of 18 C57BL/6J male adult mice were divided into three groups: control group, HUA group, and HUA+oxamate group, with six mice in each group. Oxamate was intraperitoneally injected into the mice one hour after PO injection. In vitro, an HUA model was simulated by stimulating HK-2 cells with uric acid. Oxamate and tempol inhibited LDHA and reactive oxygen species (ROS) in HK-2 cells.

Results: In HUA mice, blood uric acid levels were significantly elevated. LDHA in kidney tubular cells was significantly increased in both in vivo and in vitro HUA models, accompanied by an increase in kidney tubular inflammation and ROS. Mechanistically, LDHA mediates uric acid-induced inflammation to kidney tubular cells through the ROS/NLRP3 pathway. Pharmacologic inhibition of LDHA or ROS in kidney tubular cells can significantly ameliorate inflammation response caused by uric acid.

Conclusions: LDHA in kidney tubular cells significantly was increased in HUA models. LDHA mediates kidney inflammation response induced by uric acid through the ROS/NLRP3 pathway. This study may provide a new intervention target for preventing kidney tubular inflammation caused by uric acid.

尿酸通过 LDHA/ROS/NLRP3 途径介导肾小管炎症。
目的:高尿酸血症(HUA)是导致慢性肾病(CKD)的一个重要因素。高尿酸血症会激活肾小管炎症反应。本研究旨在探讨乳酸脱氢酶 A(LDHA)是否参与介导尿酸诱导的肾小管炎症反应:方法:通过连续腹腔注射草酸钾(PO)一周,建立体内 HUA 小鼠模型。18只C57BL/6J雄性成年小鼠分为三组:对照组、HUA组和HUA+草酸盐组,每组6只。小鼠腹腔注射草氨酸后一小时再进行PO注射。在体外,通过用尿酸刺激 HK-2 细胞模拟 HUA 模型。结果显示,草酸盐和替普莫能抑制 HK-2 细胞中的 LDHA 和活性氧(ROS):结果:HUA 小鼠的血尿酸水平明显升高。结果:HUA 小鼠血尿酸水平明显升高,体内和体外 HUA 模型肾小管细胞中的 LDHA 均明显增加,同时伴有肾小管炎症和 ROS 的增加。从机制上讲,LDHA 通过 ROS/NLRP3 途径介导尿酸诱导的肾小管细胞炎症。药物抑制肾小管细胞中的LDHA或ROS可显著改善尿酸引起的炎症反应:结论:在 HUA 模型中,肾小管细胞中的 LDHA 明显增加。LDHA通过ROS/NLRP3途径介导尿酸诱导的肾脏炎症反应。这项研究为预防尿酸引起的肾小管炎症提供了新的干预靶点。
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来源期刊
CiteScore
3.90
自引率
0.80%
发文量
66
审稿时长
6-12 weeks
期刊介绍: Clinical and Experimental Hypertension is a reputable journal that has converted to a full Open Access format starting from Volume 45 in 2023. While previous volumes are still accessible through a Pay to Read model, the journal now provides free and open access to its content. It serves as an international platform for the exchange of up-to-date scientific and clinical information concerning both human and animal hypertension. The journal publishes a wide range of articles, including full research papers, solicited and unsolicited reviews, and commentaries. Through these publications, the journal aims to enhance current understanding and support the timely detection, management, control, and prevention of hypertension-related conditions. One notable aspect of Clinical and Experimental Hypertension is its coverage of special issues that focus on the proceedings of symposia dedicated to hypertension research. This feature allows researchers and clinicians to delve deeper into the latest advancements in this field. The journal is abstracted and indexed in several renowned databases, including Pharmacoeconomics and Outcomes News (Online), Reactions Weekly (Online), CABI, EBSCOhost, Elsevier BV, International Atomic Energy Agency, and the National Library of Medicine, among others. These affiliations ensure that the journal's content receives broad visibility and facilitates its discoverability by professionals and researchers in related disciplines.
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