NIT2 dampens BRD1 phase separation and restrains oxidative phosphorylation to enhance chemosensitivity in gastric cancer

IF 15.8 1区 医学 Q1 CELL BIOLOGY Science Translational Medicine Pub Date : 2024-11-20 DOI:10.1126/scitranslmed.ado8333
Ziyang Wang, Yuqin Di, Xiangqiong Wen, Ye Liu, Lvlan Ye, Xiang Zhang, Jiale Qin, Youpeng Wang, Huiying Chu, Guohui Li, Weijing Zhang, Xiongjun Wang, Weiling He
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Abstract

5-Fluorouracil (5-FU) chemoresistance contributes to poor therapeutic response and prognosis of gastric cancer (GC), for which effective strategies to overcome chemoresistance are limited. Here, using a CRISPR-Cas9 system, we identified that nitrilase family member 2 (NIT2) reverses chemoresistance independent of its metabolic function. Depletion or low expression of NIT2 led to 5-FU resistance in GC cell lines, patient-derived organoids, and xenografted tumors. Mechanistically, NIT2 interacted with bromodomain-containing protein 1 (BRD1) to inhibit HBO1-mediated acetylation of histone H3 at lysine-14 (H3K14ac) and RELA-targeted oxidative phosphorylation (OXPHOS) gene expression. Upon 5-FU stimulation, NIT2 phosphorylation by Src at Y49 promoted the dissociation of NIT2 from BRD1, followed by binding to E3 ligase CCNB1IP1, causing autophagic degradation of NIT2. Consequently, reduced NIT2 protein resulted in BRD1 forming phase separation and binding to histone H3, as well as increased RELA stability due to suppression of inhibitor of growth family member 4–mediated RELA ubiquitination. In addition, NIT2 expression negatively correlated with H3K14ac and OXPHOS and positively correlated with the chemotherapeutic responses and prognosis of patients with GC. Our findings reveal the moonlighting function of NIT2 in chemoresistance and underscore that OXPHOS blockade by metformin enhances 5-FU chemosensitivity upon NIT2 loss.
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NIT2 可抑制 BRD1 相分离并抑制氧化磷酸化,从而增强胃癌的化疗敏感性
5-氟尿嘧啶(5-FU)化疗耐药性是导致胃癌(GC)治疗反应和预后不良的原因之一,而克服化疗耐药性的有效策略却很有限。在这里,我们利用 CRISPR-Cas9 系统发现,硝化酶家族成员 2(NIT2)能逆转化疗耐药性,而与其代谢功能无关。NIT2的耗竭或低表达会导致GC细胞系、患者衍生的器官组织和异种移植肿瘤对5-FU产生耐药性。从机理上讲,NIT2与含溴域蛋白1(BRD1)相互作用,抑制HBO1介导的组蛋白H3赖氨酸-14乙酰化(H3K14ac)和RELA靶向氧化磷酸化(OXPHOS)基因表达。5-FU刺激后,NIT2在Y49处被Src磷酸化,促进了NIT2与BRD1的分离,随后与E3连接酶CCNB1IP1结合,导致NIT2自噬降解。因此,NIT2 蛋白减少会导致 BRD1 形成相分离并与组蛋白 H3 结合,同时由于生长抑素家族成员 4 介导的 RELA 泛素化被抑制,RELA 的稳定性也会增加。此外,NIT2的表达与H3K14ac和OXPHOS呈负相关,与GC患者的化疗反应和预后呈正相关。我们的研究结果揭示了NIT2在化疗耐药中的月光功能,并强调二甲双胍阻断OXPHOS可在NIT2缺失时增强5-FU化疗敏感性。
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
Science Translational Medicine
Science Translational Medicine CELL BIOLOGY-MEDICINE, RESEARCH & EXPERIMENTAL
CiteScore
26.70
自引率
1.20%
发文量
309
审稿时长
1.7 months
期刊介绍: Science Translational Medicine is an online journal that focuses on publishing research at the intersection of science, engineering, and medicine. The goal of the journal is to promote human health by providing a platform for researchers from various disciplines to communicate their latest advancements in biomedical, translational, and clinical research. The journal aims to address the slow translation of scientific knowledge into effective treatments and health measures. It publishes articles that fill the knowledge gaps between preclinical research and medical applications, with a focus on accelerating the translation of knowledge into new ways of preventing, diagnosing, and treating human diseases. The scope of Science Translational Medicine includes various areas such as cardiovascular disease, immunology/vaccines, metabolism/diabetes/obesity, neuroscience/neurology/psychiatry, cancer, infectious diseases, policy, behavior, bioengineering, chemical genomics/drug discovery, imaging, applied physical sciences, medical nanotechnology, drug delivery, biomarkers, gene therapy/regenerative medicine, toxicology and pharmacokinetics, data mining, cell culture, animal and human studies, medical informatics, and other interdisciplinary approaches to medicine. The target audience of the journal includes researchers and management in academia, government, and the biotechnology and pharmaceutical industries. It is also relevant to physician scientists, regulators, policy makers, investors, business developers, and funding agencies.
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