靶向 ALDH1A1,通过铁凋亡提高 KRAS 靶向疗法的疗效

IF 10.7 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Redox Biology Pub Date : 2024-09-19 DOI:10.1016/j.redox.2024.103361
Yunyi Bian , Guangyao Shan , Guoshu Bi , Jiaqi Liang , Zhengyang Hu , Qihai Sui , Haochun Shi , Zhaolin Zheng , Guangyu Yao , Qun Wang , Hong Fan , Cheng Zhan
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引用次数: 0

摘要

KRAS 是人类恶性肿瘤中最常见的突变癌基因之一。尽管索托拉西布(sotorasib)和阿达格拉西布(adagrasib)的出现解除了KRAS "不可药用 "的烙印,但KRAS抑制剂的耐药性很快成为一个主要问题。在这里,我们报告了醛脱氢酶 1 家族成员 A1(ALDH1A1)--一种参与维甲酸生物合成和氧化还原平衡的酶--对 KRAS 抑制剂的反应增加,并在一系列癌症类型中产生耐药性。通过 ALDH1A1 基因敲除、酶功能缺失或抑制剂,KRAS 抑制剂在敏感或耐药细胞、患者衍生器官组织(PDO)和异种移植模型中的疗效显著提高。此外,我们还发现,ALDH1A1 通过对抗铁变态反应抑制 KRAS 抑制剂的疗效。ALDH1A1 能解毒有害的醛,促进 NADH 和视黄酸(RA)的合成,并改善 RARA 的功能。ALDH1A1 还能激活 CREB1/GPX4 通路,以 pH 依赖性方式刺激脂滴的产生,进而防止 KRAS 抑制剂诱导的铁突变。同时,我们还发现 GTF2I 在 KRAS 抑制剂的作用下通过 ERK 在 S784 处去磷酸化,从而阻碍了其核转位,并介导了 ALDH1A1 在 KRAS 抑制剂作用下的上调。总之,研究结果为在癌症治疗中通过铁变态反应靶向 ALDH1A1 以提高 KRAS 靶向治疗的有效性提供了有价值的见解。
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Targeting ALDH1A1 to enhance the efficacy of KRAS-targeted therapy through ferroptosis
KRAS is among the most commonly mutated oncogenes in human malignancies. Although the advent of sotorasib and adagrasib, has lifted the “undruggable” stigma of KRAS, the resistance to KRAS inhibitors quickly becomes a major issue. Here, we reported that aldehyde dehydrogenase 1 family member A1 (ALDH1A1), an enzyme in retinoic acid biosynthesis and redox balance, increases in response to KRAS inhibitors and confers resistance in a range of cancer types. KRAS inhibitors' efficacy is significantly improved in sensitive or drug-resistant cells, patient-derived organoids (PDO), and xenograft models by ALDH1A1 knockout, loss of enzyme function, or inhibitor. Furthermore, we discovered that ALDH1A1 suppresses the efficacy of KRAS inhibitors by counteracting ferroptosis. ALDH1A1 detoxicates deleterious aldehydes, boosts the synthesis of NADH and retinoic acid (RA), and improves RARA function. ALDH1A1 also activates the CREB1/GPX4 pathway, stimulates the production of lipid droplets in a pH-dependent manner, and subsequently prevents ferroptosis induced by KRAS inhibitors. Meanwhile, we established that GTF2I is dephosphorylated at S784 via ERK by KRAS inhibitors, which hinders its nuclear translocation and mediates ALDH1A1's upregulation in response to KRAS inhibitors. In summary, the results offer valuable insights into targeting ALDH1A1 to enhance the effectiveness of KRAS-targeted therapy through ferroptosis in cancer treatment.
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来源期刊
Redox Biology
Redox Biology BIOCHEMISTRY & MOLECULAR BIOLOGY-
CiteScore
19.90
自引率
3.50%
发文量
318
审稿时长
25 days
期刊介绍: Redox Biology is the official journal of the Society for Redox Biology and Medicine and the Society for Free Radical Research-Europe. It is also affiliated with the International Society for Free Radical Research (SFRRI). This journal serves as a platform for publishing pioneering research, innovative methods, and comprehensive review articles in the field of redox biology, encompassing both health and disease. Redox Biology welcomes various forms of contributions, including research articles (short or full communications), methods, mini-reviews, and commentaries. Through its diverse range of published content, Redox Biology aims to foster advancements and insights in the understanding of redox biology and its implications.
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