Litcius/Paper detail

Ultrasmall Nanoparticles Regulate Immune Microenvironment by Activating IL‐33/ST2 to Alleviate Renal Ischemia‐Reperfusion Injury

Liyao Xu, Zhaoyu Xing, Jiaxin Yuan, Yaobao Han, Zhilin Jiang, Mengxiao Han, Xianao Hou, Wei Xing, Zhen Li

2024Advanced Healthcare Materials17 citationsDOI

Abstract

Abstract Renal ischemia‐reperfusion injury (IRI) is a common disease with high morbidity and mortality. Renal IRI can cause the disorder of immune microenvironment and reprograming the immune microenvironment to alleviate excessive inflammatory response is crucial for its treatment. Cytokine IL‐33 can improve the immune inflammatory microenvironment by modulating both innate and adaptive immune cells, and serve as an important target for modulating immune microenvironment of renal IRI. Herein, we report that bilobetin‐functionalized ultrasmall Cu 2− x Se nanoparticles (i.e., CSPB NPs) can activate the PKA/p‐CREB/IL‐33/ST2 signaling pathway to regulate innate and adaptive immune cells for reprograming the immune microenvironment of IRI‐induced acute kidney injury. The biocompatible CSPB NPs can promote the polarization of M1‐like macrophages into M2‐like macrophages, and the expansion of ILC2 and Treg cells by activating IL‐33/ST2 to modulate the excessive immune inflammatory response of renal IRI. More importantly, they can rapidly accumulate at the injured kidney to significantly alleviate IRI. This work demonstrates that modulating the expression of cytokines to reprogram immune microenvironment has great potential in the treatment of renal IRI and other ischemic diseases.

Topics & Concepts

Immune systemInnate immune systemInflammationCytokineRenal ischemiaKidneyCancer researchImmunologyMedicineIschemiaReperfusion injuryInternal medicineIL-33, ST2, and ILC PathwaysDialysis and Renal Disease ManagementAcute Kidney Injury Research