Advances in Research on Immunocyte Iron Metabolism, Ferroptosis, and Their Regulatory Roles in Autoimmune and Autoinflammatory Diseases

Overview

Journal Cell Death Dis

Specialties Cell Biology
General Medicine

Date 2024 Jul 4

PMID 38965216

Authors

Liuting Zeng

Kailin Yang

Ganpeng Yu

Wensa Hao

Xiaofei Zhu

Anqi Ge

Junpeng Chen

Lingyun Sun

Affiliations

Soon will be listed here.

Abstract

Autoimmune diseases commonly affect various systems, but their etiology and pathogenesis remain unclear. Currently, increasing research has highlighted the role of ferroptosis in immune regulation, with immune cells being a crucial component of the body's immune system. This review provides an overview and discusses the relationship between ferroptosis, programmed cell death in immune cells, and autoimmune diseases. Additionally, it summarizes the role of various key targets of ferroptosis, such as GPX4 and TFR, in immune cell immune responses. Furthermore, the release of multiple molecules, including damage-associated molecular patterns (DAMPs), following cell death by ferroptosis, is examined, as these molecules further influence the differentiation and function of immune cells, thereby affecting the occurrence and progression of autoimmune diseases. Moreover, immune cells secrete immune factors or their metabolites, which also impact the occurrence of ferroptosis in target organs and tissues involved in autoimmune diseases. Iron chelators, chloroquine and its derivatives, antioxidants, chloroquine derivatives, and calreticulin have been demonstrated to be effective in animal studies for certain autoimmune diseases, exerting anti-inflammatory and immunomodulatory effects. Finally, a brief summary and future perspectives on the research of autoimmune diseases are provided, aiming to guide disease treatment strategies.

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