Targeting ferroptosis in gastric cancer: Strategies and opportunities

Author:

Le Jiahan12,Pan Guangzhao2,Zhang Che23,Chen Yitao1,Tiwari Amit K.4ORCID,Qin Jiang‐Jiang23

Affiliation:

1. School of Life Sciences Zhejiang Chinese Medical University Hangzhou China

2. Zhejiang Cancer Hospital, Hangzhou Institute of Medicine (HIM) Chinese Academy of Sciences Hangzhou China

3. School of Molecular Medicine, Hangzhou Institute for Advanced Study UCAS Hangzhou China

4. Department of Pharmaceutical Sciences University of Arkansas for Medical Sciences Little Rock Arkansas USA

Abstract

SummaryFerroptosis is a novel form of programmed cell death morphologically, genetically, and biochemically distinct from other cell death pathways and characterized by the accumulation of iron‐dependent lipid peroxides and oxidative damage. It is now understood that ferroptosis plays an essential role in various biological processes, especially in the metabolism of iron, lipids, and amino acids. Gastric cancer (GC) is a prevalent malignant tumor worldwide with low early diagnosis rates and high metastasis rates, accounting for its relatively poor prognosis. Although chemotherapy is commonly used to treat GC, drug resistance often leads to poor therapeutic outcomes. In the last several years, extensive research on ferroptosis has highlighted its significant potential in GC therapy, providing a promising strategy to address drug resistance associated with standard cancer therapies. In this review, we offer an extensive summary of the key regulatory factors related to the mechanisms underlying ferroptosis. Various inducers and inhibitors specifically targeting ferroptosis are uncovered. Additionally, we explore the prospective applications and outcomes of these agents in the field of GC therapy, emphasizing their capacity to improve the outcomes of this patient population.

Funder

Congressionally Directed Medical Research Programs

Natural Science Foundation of Zhejiang Province

Publisher

Wiley

Subject

Immunology,Immunology and Allergy

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