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Review
. 2025 Jan;21(1):39-56.
doi: 10.1038/s41581-024-00889-z. Epub 2024 Sep 17.

Metabolism at the crossroads of inflammation and fibrosis in chronic kidney disease

Verónica Miguel  1 Isaac W Shaw  1 Rafael Kramann  2   3
Affiliations
Review

Metabolism at the crossroads of inflammation and fibrosis in chronic kidney disease

Verónica Miguel et al. Nat Rev Nephrol. 2025 Jan.

Abstract

Chronic kidney disease (CKD), defined as persistent (>3 months) kidney functional loss, has a growing prevalence (>10% worldwide population) and limited treatment options. Fibrosis driven by the aberrant accumulation of extracellular matrix is the final common pathway of nearly all types of chronic repetitive injury in the kidney and is considered a hallmark of CKD. Myofibroblasts are key extracellular matrix-producing cells that are activated by crosstalk between damaged tubules and immune cells. Emerging evidence indicates that metabolic alterations are crucial contributors to the pathogenesis of kidney fibrosis by affecting cellular bioenergetics and metabolite signalling. Immune cell functions are intricately connected to their metabolic characteristics, and kidney cells seem to undergo cell-type-specific metabolic shifts in response to damage, all of which can determine injury and repair responses in CKD. A detailed understanding of the heterogeneity in metabolic reprogramming of different kidney cellular subsets is essential to elucidating communication processes between cell types and to enabling the development of metabolism-based innovative therapeutic strategies against CKD.

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Conflict of interest statement

Competing interests: R.K. is founder and shareholder of Sequantrix GmbH, has grants from Travere Therapeutics, Galapagos, Chugai, AskBio and Novo Nordisk, and is a consultant for Bayer, Pfizer, Novo Nordisk, Hybridize Therapeutics and Gruenenthal. The other authors declare no competing interests.

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