ENO1 blockade augment ferroptosis susceptibility in TKIs-resistant CML through GPX4 autophagic degradation.

IF 8.2 2区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Free Radical Biology and Medicine Pub Date : 2025-09-19 DOI:10.1016/j.freeradbiomed.2025.08.055

Peng Hongwei, Yang Xintong, Chen Zhiwei, Hu Jinfang, Xiong Dongsheng, Wan Jiaqi, Liu Zhen, Li Yue, Wang Xu, Ren Simei, Li Fei

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引用次数: 0

Abstract

The introduction of tyrosine kinase inhibitors (TKIs) has significantly improved the prognosis of chronic myeloid leukemia (CML), however, approximately 20% CML patients developed resistance to TKIs and lead to treatment failure. Enolase 1 (ENO1) is a critical enzyme involved in glycolysis and was found to be closely related to CML carcinogenesis. Our results indicate ENO1 expression was close correlated with drug responses and disease prognosis in CML. The chemo-resistant CML cell K562/G more relied on glycolysis for energy supply than its sensitive counterparts.,Metabolomic analysis revealed that ENOblock, APIII-α4(AP), synergized with multiple TKIs and induce ferroptosis in K562/G cells. Bioinformatics analysis suggested that GPX4 play more crucial role in sustaining chemo-resistant CML cell survival. Transcriptomic analysis and WB results revealed GPX4 autophagic degradation induced by ENO1 downregulation. AMPK/mTOR signaling pathway activated by ENO1 downregulationplayed partial role in GPX4 degradation. More importantly, the expression of ENO1 was found to be inversely correlated with that of a transmembrane protein TMEM164.TMEM164 interference would restore the GPX4 autophagic degradation and ferroptosis susceptibility induced by ENO1 downregulation.Single-cell sequence data revealed a co-expression relationship between ENO1 and GPX4, especially in CML patients with poor TKIs responses. Besides, In vivo animal experiments demonstrated that AP could cooperate with TKIs to relieve the tumor burden with tolerable safety. Taken together, this study demonstrated that ENO1 is a crucial biomarker for CML TKIs responses, and ENO1 blockade could augment TKIs sensitivity and promote the ferroptosis susceptibility in TKIs-resistant cells by ultimately inducing GPX4 autophagic degradation through AMPK/mTOR pathway and ENO1-TMEM164 interaction, which provide a potential novel target for the clinical treatment of CML.

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ENO1阻断通过GPX4自噬降解增强tkis耐药CML的铁中毒敏感性。

酪氨酸激酶抑制剂（TKIs）的引入显著改善了慢性髓性白血病（CML）的预后，然而，约20%的CML患者对TKIs产生耐药性并导致治疗失败。烯醇化酶1 （ENO1）是参与糖酵解的关键酶，被发现与CML的癌变密切相关。结果表明，在CML中，ENO1的表达与药物反应和疾病预后密切相关。耐药CML细胞K562/G比敏感细胞更依赖糖酵解提供能量。代谢组学分析显示，ENOblock、APIII-α4（AP）可与多种TKIs协同作用，诱导K562/G细胞铁凋亡。生物信息学分析表明GPX4在维持化疗耐药CML细胞存活中发挥更重要的作用。转录组学分析和WB结果显示，ENO1下调可诱导GPX4自噬降解。ENO1下调激活的AMPK/mTOR信号通路在GPX4降解中起部分作用。更重要的是，ENO1的表达与跨膜蛋白TMEM164的表达呈负相关。干扰TMEM164可恢复ENO1下调诱导的GPX4自噬降解和铁沉敏感性。单细胞序列数据揭示了ENO1和GPX4之间的共表达关系，特别是在TKIs反应差的CML患者中。此外，体内动物实验表明，AP可与TKIs协同减轻肿瘤负担，且具有可耐受的安全性。综上所述，本研究表明，ENO1是CML TKIs反应的重要生物标志物，而ENO1阻断可以通过AMPK/mTOR途径和ENO1- tmem164相互作用最终诱导GPX4自噬降解，从而增强TKIs敏感性，促进TKIs耐药细胞铁凋亡的易感性，这为CML临床治疗提供了潜在的新靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Free Radical Biology and Medicine 医学-内分泌学与代谢

CiteScore

14.00

自引率

4.10%

发文量

850

审稿时长

22 days

期刊介绍： Free Radical Biology and Medicine is a leading journal in the field of redox biology, which is the study of the role of reactive oxygen species (ROS) and other oxidizing agents in biological systems. The journal serves as a premier forum for publishing innovative and groundbreaking research that explores the redox biology of health and disease, covering a wide range of topics and disciplines. Free Radical Biology and Medicine also commissions Special Issues that highlight recent advances in both basic and clinical research, with a particular emphasis on the mechanisms underlying altered metabolism and redox signaling. These Special Issues aim to provide a focused platform for the latest research in the field, fostering collaboration and knowledge exchange among researchers and clinicians.