GPR84 blockade in macrophages mitigates sepsis-induced liver injury via PPARα-driven metabolic reprogramming and M2 polarization - PubMed

5 hours ago

GPR84 blockade in macrophages reduces sepsis-induced liver injury.
The protective mechanism involves PPARα-driven metabolic reprogramming.
GPR84 inhibition shifts macrophage phenotype from inflammatory M1 to anti-inflammatory M2.
PPARα activation is restored via the cAMP-PKA-CREB signaling pathway, enhancing mitochondrial fatty acid oxidation.
In Pparα-deficient mice, the benefits of GPR84 blockade are lost, confirming its essential role.

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