Oleic Acid Inhibits SDC4 and Promotes Ferroptosis in Lung Cancer Through GPX4/ACSL4

IF 1.9 4区医学 Q3 RESPIRATORY SYSTEM Clinical Respiratory Journal Pub Date : 2024-10-13 DOI:10.1111/crj.70014

Jingfei Dong, Fei Qi, Huiqing Qie, Shibu Du, Li Li, Yan Zhang, Kaiyue Xu, Dehui Li, Yapei Xu

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Abstract

Introduction

As a common malignancy, lung cancer has a relatively poor prognosis and a low survival rate. In recent years, ferroptosis, as an emerging filed, has great promise in the potential treatment of cancer. Brucea javanica oil (BJO) is often used to treat various cancers. Oleic acid (OA) is the main ingredient of BJO. In this study, we investigated the role and molecular mechanism of OA in lung cancer treatment by promoting ferroptosis.

Methods

In this study, A549 cells and H1299 cells were used for in vitro experiments, and a CCK-8 test, scratch test, and MTT experiment were carried out. We examined reactive oxygen species (ROS), the JC-1 probe, glutathione (GSH) expression, lipid peroxidation, SDC4 mRNA levels, and ACSL4, SLC7A11, GPX4, and SDC4 protein levels.

Results

The results showed that OA could inhibit the proliferation and migration of A549 cells and H1299 cells, SDC4 was a potential therapeutic target of OA against lung cancer, and OA treatment significantly inhibited the expression of SDC4 in A549 cells and H1299 cells. OA induces ferroptosis in A549 cells and H1299 cells, decreases GSH levels, increases lipid peroxidation levels, and decreases SDC4 mRNA expression; in addition, OA upregulates ACSL4 expression and decreases SLC7A11, GPX4, and SDC4 expression.

Conclusion

This study confirmed that OA could inhibit SDC4 expression and promote the occurrence of ferroptosis in A549 cells and H1299 cells through the GPX4/ACSL4 pathway, providing an effective basis for the use of drugs targeting ferroptosis in lung cancer treatment.

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油酸通过 GPX4/ACSL4 抑制 SDC4 并促进肺癌中的铁凋亡

导言肺癌是一种常见的恶性肿瘤，预后较差，生存率低。近年来，作为一种新兴的治疗方法，阿魏化疗在潜在的癌症治疗中大有可为。Brucea javanica 油（BJO）常用于治疗各种癌症。油酸（OA）是 BJO 的主要成分。在本研究中，我们探讨了 OA 通过促进铁突变在肺癌治疗中的作用和分子机制。方法本研究使用 A549 细胞和 H1299 细胞进行体外实验，并进行了 CCK-8 试验、划痕试验和 MTT 实验。我们检测了活性氧（ROS）、JC-1探针、谷胱甘肽（GSH）表达、脂质过氧化、SDC4 mRNA水平以及ACSL4、SLC7A11、GPX4和SDC4蛋白水平。结果表明，OA能抑制A549细胞和H1299细胞的增殖和迁移，SDC4是OA治疗肺癌的潜在靶点，OA治疗能显著抑制SDC4在A549细胞和H1299细胞中的表达。OA诱导A549细胞和H1299细胞的铁变态反应，降低GSH水平，增加脂质过氧化水平，降低SDC4 mRNA的表达；此外，OA上调ACSL4的表达，降低SLC7A11、GPX4和SDC4的表达。结论本研究证实 OA 可通过 GPX4/ACSL4 通路抑制 A549 细胞和 H1299 细胞中 SDC4 的表达并促进铁变态反应的发生，为肺癌治疗中使用靶向铁变态反应的药物提供了有效依据。

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

Clinical Respiratory Journal 医学-呼吸系统

CiteScore

3.70

自引率

0.00%

发文量

104

审稿时长

>12 weeks

期刊介绍： Overview Effective with the 2016 volume, this journal will be published in an online-only format. Aims and Scope The Clinical Respiratory Journal (CRJ) provides a forum for clinical research in all areas of respiratory medicine from clinical lung disease to basic research relevant to the clinic. We publish original research, review articles, case studies, editorials and book reviews in all areas of clinical lung disease including: Asthma Allergy COPD Non-invasive ventilation Sleep related breathing disorders Interstitial lung diseases Lung cancer Clinical genetics Rhinitis Airway and lung infection Epidemiology Pediatrics CRJ provides a fast-track service for selected Phase II and Phase III trial studies. Keywords Clinical Respiratory Journal, respiratory, pulmonary, medicine, clinical, lung disease, Abstracting and Indexing Information Academic Search (EBSCO Publishing) Academic Search Alumni Edition (EBSCO Publishing) Embase (Elsevier) Health & Medical Collection (ProQuest) Health Research Premium Collection (ProQuest) HEED: Health Economic Evaluations Database (Wiley-Blackwell) Hospital Premium Collection (ProQuest) Journal Citation Reports/Science Edition (Clarivate Analytics) MEDLINE/PubMed (NLM) ProQuest Central (ProQuest) Science Citation Index Expanded (Clarivate Analytics) SCOPUS (Elsevier)