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CD38hi macrophages promote fibrotic transition following acute kidney injury by modulating NAD+ metabolism

Weijian Yao, Menghan Liu, Zehua Li, Lei Qu, Shuang Sui, Chengang Xiang, Lei Jiang, Suxia Wang, Gang Liu, Ying Chen, Li Yang

2025Molecular Therapy9 citationsDOIOpen Access PDF

Abstract

Acute kidney injury (AKI) encompasses a spectrum of conditions, varying from mild and self-limiting to severe cases that can lead to chronic kidney disease (CKD). Macrophages are crucial in the progression from AKI to CKD, yet the diversity of macrophage subsets complicates the identification of key functional types. We established a detailed single-cell atlas of mononuclear macrophages from the onset of AKI through its progression to CKD. Our results indicate that a macrophage subset with high CD38 expression is closely linked to renal fibrosis following AKI in both mouse model and AKI patients. These CD38 hi macrophages, derived from resident macrophages via Csf1 signaling, secrete the NAD-depleting enzyme CD38, inducing senescence in renal tubular cells and promoting chronic inflammation and renal fibrosis. Knocking out Cd38 in macrophages elevated renal NAD levels, reducing senescence and fibrotic responses. Furthermore, we initiated a dosing regimen for a Cd38 inhibitor, demonstrating its potential to reduce fibrosis post-AKI, suggesting that targeting CD38 hi macrophages mediated NAD+ metabolism could be a promising therapy to halt AKI to CKD progression.

Topics & Concepts

NAD+ kinaseKidneyTransition (genetics)MetabolismAcute kidney injuryFibrosisMacrophageCell biologyChemistryCancer researchBiologyMedicineBiochemistryPathologyInternal medicineEnzymeGeneIn vitroAdenosine and Purinergic SignalingCarbon and Quantum Dots ApplicationsCalcium signaling and nucleotide metabolism