IGF2BP1: A Critical Driver of Cancer Progression and Therapeutic Target

The RNA-binding protein IGF2BP1 has emerged as a key regulator of cancer hallmarks, influencing tumor proliferation, metastasis, immune evasion, and resistance to cell death. As an m6A reader, IGF2BP1 binds to methylated mRNA, stabilizing oncogenic transcripts and promoting cancer progression. Its role in regulating gene expression at the post-transcriptional level has positioned IGF2BP1 as a potential biomarker for cancer prognosis and a target for novel anti-tumor therapies.

Elevated expression of IGF2BP1 has been observed in multiple cancers, including lung, liver, breast, and colorectal cancers, correlating with poor prognosis and therapy resistance. Through its interaction with m6A-modified mRNAs, IGF2BP1 enhances the stability and translation of cancer-related genes, driving tumor growth, invasion, and metabolic reprogramming. Its ability to promote immune evasion by stabilizing PD-L1 mRNA further highlights its role in suppressing anti-tumor immunity.

By influencing ferroptosis resistance, IGF2BP1 contributes to the survival of cancer cells under oxidative stress. Additionally, its impact on tumor metabolism, particularly in regulating glycolysis and lipid metabolism, enables cancer cells to adapt to hostile microenvironments. The tumor microenvironment, characterized by hypoxia and immune suppression, is further influenced by IGF2BP1, making it a key player in the dynamic interactions that sustain tumor progression.

Given its central role in cancer biology, targeting IGF2BP1 represents a promising therapeutic strategy. Recent research has identified small-molecule inhibitors capable of disrupting IGF2BP1-RNA interactions, leading to reduced tumor cell viability and increased sensitivity to chemotherapy. These findings pave the way for the development of IGF2BP1-targeted therapies aimed at enhancing cancer treatment outcomes.

As research continues to uncover the molecular mechanisms underlying IGF2BP1’s functions, its potential as a biomarker for early cancer detection and a target for precision medicine becomes increasingly clear. Further studies and clinical trials will be crucial in translating these discoveries into effective cancer therapies, offering hope for improved patient survival and treatment efficacy.

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Reference
Li Qiu, Shourong Wu, Lei Zhang, Wenfang Li, Debing Xiang, Vivi Kasim, The biological roles and molecular mechanisms of m6A reader IGF2BP1 in the hallmarks of cancer, Genes & Diseases, Volume 12, Issue 5, 2025, 101567, https://doi.org/10.1016/j.gendis.2025.101567

Funding Information:

National Natural Science Foundation of China 82173029
National Natural Science Foundation of China 32270778
National Natural Science Foundation of China 82372655
Natural Science Foundation of Chongqing, China CSTB2022NSCQ-MSX0611
Natural Science Foundation of Chongqing, China CSTB2022NSCQ-MSX0612
Talent Project of Chongqing University Jiangjin Hospital (Chongqing, China) 2024LJXM005

Li Qiu, Shourong Wu, Lei Zhang, Wenfang Li, Debing Xiang, Vivi Kasim, The biological roles and molecular mechanisms of m6A reader IGF2BP1 in the hallmarks of cancer, Genes & Diseases, Volume 12, Issue 5, 2025, 101567, https://doi.org/10.1016/j.gendis.2025.101567

Archivos adjuntos

IGF2BP1's regulation on cancer's hallmarks. IGF2BP1 mainly regulates six cancer hallmarks, including sustained cell proliferation, cell death resistance, activation of invasion and metastasis, deregulated cellular energetics, immune evasion, and unlocking phenotypic plasticity.
Working model of m6A regulator (writers, erasers, and readers) on m6A modification.
Regulation of IGF2BP1 on mRNA stability and mRNA translation. (A) Domain structure of IGF2BP1. IGF2BP1 contains two RRM domains (orange) and four KH domains (red). (B) IGF2BP1 binds to target mRNAs and RNA-binding proteins (RBPs) in the cytoplasm to regulate mRNA transport, stability, and translation by recruiting transcripts into protective messenger ribonucleoprotein particles (mRNPs).

19/06/2025 Compuscript Ltd

Regions: Europe, Ireland, Asia, China

Keywords: Health, Medical, People in health research, Public Dialogue - health, Science, Life Sciences, People in science

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