What question did this study set out to answer?

The study aims to explore the role of ApoM in cisplatin-induced nephropathy and its potential mechanisms.

March 27, 2026Open Access

WCN26-6278 ApoM knockout exacerbated proximal tubular injury in cisplatin-induced nephropathy

Key Points

The study aims to explore the role of ApoM in cisplatin-induced nephropathy and its potential mechanisms.
Used a mouse model of cisplatin-induced nephropathy
Manipulated ApoM levels through knockout techniques
Examined changes in proximal tubular injury
ApoM knockout led to increased proximal tubular injury
Deterioration was linked to impaired S1P1 receptor signaling
Results suggest ApoM has protective effects in kidney injury

Abstract

Apolipoprotein M (ApoM) is a carrier of sphingosine-1-phosphate (S1P) and ApoM-S1P exerts potent physiological effects mainly through S1P1 receptor. We previously reported protective effects of ApoM in a multiple organ failure in sepsis mouse model, IgA nephropathy mouse model, and diabetic nephropathy mouse model and its potential as a therapeutic target. Here, we investigated the roles of ApoM in cisplatin-induced nephropathy using a mouse model and potential novel downstream mechanisms modulated by ApoM.

WCN26-6278 ApoM knockout exacerbated proximal tubular injury in cisplatin-induced nephropathy

Key Points

Abstract

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