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Reprogramming of fatty acid metabolism in thyroid cancer:Potential targets and mechanisms

摘要Thyroid cancer(TC)is one of the most common endocrine system tumors,and its incidence continues to increase worldwide.Although most TC patients have a good prognosis,especially with continuous advancements in surgery,radioactive iodine therapy,chemotherapy,endocrine therapy and targeted therapy,the effectiveness of disease treatment has significantly improved.However,there are still some cases with a higher risk of death and greater aggressiveness.In these more challenging advanced or highly aggressive cases,tyrosine kinase inhibitors appear to be an effective treatment option.Unfortunately,these drugs are less than ideal in terms of efficacy because of their toxicity and potential for intrinsic or acquired resistance.Therefore,exploring new strategies targeting the metabolic characteristics of TC cells and overcoming drug resistance barriers in existing treatments have become key topics in the current field of TC research.In recent years,lipid metabolic reprogramming has gained attention as an important aspect of cancer development.Lipid metabolic reprogramming not only participates in the formation of the cell membrane structure,but also plays an important role in signal transduction and promoting cell proliferation.In particular,fatty acid(FA)metabolic reprogramming has attracted widespread attention and plays an important role in multiple aspects such as tumor growth,metastasis,enhanced invasive ability,immune escape,and drug resistance.Although TC is considered a disease that is highly dependent on specific types of metabolic activities,a comprehensive understanding of the specific mechanism of action of FA metabolic reprogramming in this process is lacking.This article aims to review how FA metabolic reprogramming participates in the occurrence and development of TC,focusing on the impact of abnormal FA metabolic pathways and changes in the expression and regulation of related genes over the course of this disease.By examining the complex interactions between FA metabolic disorders and carcinogenic signaling pathways in depth,we aim to identify new therapeutic targets and develop more precise and effective treatments for TC.

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作者 Pengbin Ping [1] Yuhong Ma [2] Xiaoying Xu [2] Juan Li [2] 学术成果认领
作者单位 Department of Radiotherapy Oncology,the Second Affiliated Hospital of Dalian Medical University,Dalian 116023,China;Department of Radiation Therapy,Zhengzhou Central Hospital Affiliated to Zhengzhou University,Zhengzhou 450007,China [1] Department of Radiotherapy Oncology,the Second Affiliated Hospital of Dalian Medical University,Dalian 116023,China [2]
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DOI 10.21147/j.issn.1000-9604.2025.02.09
发布时间 2025-06-16(万方平台首次上网日期,不代表论文的发表时间)
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中国癌症研究(英文版)

中国癌症研究(英文版)

2025年37卷2期

227-249页

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