Molecular mechanisms of uric acid transport by the native human URAT1 and its inhibition by anti-gout drugs

bioRxiv - Biochemistry Pub Date : 2024-09-11 DOI:10.1101/2024.09.11.612394

Canrong Wu, Chao Zhang, Sanshan Jin, James Jiqi Wang, Antao Dai, Jiuyin Xu, Heng Zhang, Xuemei Yang, Xinheng He, Qingning Yuan, Wen Hu, Youwei Xu, Ming-Wei Wang, Yi Jiang, Dehua Yang, H. Eric Xu

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Abstract

Gout, a common and painful disease, stems from hyperuricemia, where elevated blood uric acid levels lead to urate crystal formation in joints and kidneys. The human urate transporter 1 (hURAT1) plays a critical role in urate homeostasis by facilitating urate reabsorption in the renal proximal tubule, making it a key target for gout therapy. Pharmacological inhibition of hURAT1 with drugs such as dotinurad, benzbromarone, lesinurad, and verinurad promotes uric acid excretion and alleviates gout symptoms. Here we present cryo-electron microscopy structures of native hURAT1 bound with these anti-gout drugs in the inward-open state, and with uric acid in inward-open, outward-open, and occluded states. Complemented by mutagenesis and cell-based assays, these structures reveal the mechanisms of uric acid reabsorption and hURAT1 inhibition. Our findings elucidate the molecular basis of uric acid transport and anti-gout medication action, and provide a structural framework for the rational design of next-generation therapies for hyperuricemia and gout.

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本地人URAT1转运尿酸的分子机制及其对抗痛风药物的抑制作用

痛风是一种常见的疼痛性疾病，源于高尿酸血症，即血尿酸水平升高导致关节和肾脏中形成尿酸盐晶体。人尿酸盐转运体 1（hURAT1）通过促进肾近曲小管对尿酸盐的重吸收，在尿酸盐平衡中发挥着关键作用，因此成为痛风治疗的关键靶点。通过药物抑制 hURAT1（如 dotinurad、benzbromarone、lesinurad 和 verinurad）可促进尿酸排泄并缓解痛风症状。在这里，我们展示了原生 hURAT1 在内向开放状态下与这些抗痛风药物结合的冷冻电镜结构，以及在内向开放、外向开放和闭塞状态下与尿酸结合的冷冻电镜结构。通过诱变和基于细胞的测定，这些结构揭示了尿酸重吸收和 hURAT1 抑制的机制。我们的发现阐明了尿酸转运和抗痛风药物作用的分子基础，为合理设计治疗高尿酸血症和痛风的下一代疗法提供了结构框架。

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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bioRxiv - Biochemistry

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