Drug Repurposing Opportunities for Chronic Kidney Disease

Overview

Journal iScience

Publisher Cell Press

Date 2024 Jul 1

PMID 38947510

Authors

Xiong Chen

Runnan Shen

Dongxi Zhu

Shulu Luo

Guochang You

Ruijie Li

Xiaosi Hong

RuiJun Li

Jihao Wu

Yinong Huang

Tianxin Lin

Affiliations

Soon will be listed here.

Abstract

The development of targeted drugs for the early prevention and management of chronic kidney disease (CKD) is of great importance. However, the success rates and cost-effectiveness of traditional drug development approaches are extremely low. Utilizing large sample genome-wide association study data for drug repurposing has shown promise in many diseases but has not yet been explored in CKD. Herein, we investigated actionable druggable targets to improve renal function using large-scale Mendelian randomization and colocalization analyses. We combined two population-scale independent genetic datasets and validated findings with cell-type-dependent eQTL data of kidney tubular and glomerular samples. We ultimately prioritized two drug targets, opioid receptor-like 1 and F12, with potential genetic support for restoring renal function and subsequent treatment of CKD. Our findings explore the potential pathological mechanisms of CKD, bridge the gap between the molecular mechanisms of pathogenesis and clinical intervention, and provide new strategies in future clinical trials of CKD.

Citing Articles

Discovery and prioritization of genetic determinants of kidney function in 297,355 individuals from Taiwan and Japan.

Chen H, Chiang H, Chang D, Cheng C, Wang C, Lu T Nat Commun. 2024; 15(1):9317.

PMID: 39472450 PMC: 11522641. DOI: 10.1038/s41467-024-53516-7.

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