RUNX2 stimulates BMP8A to facilitate fatty acid metabolism and cause osimertinib resistance in lung adenocarcinoma.

IF 2.2 4区医学 Q3 PHYSIOLOGY

Physiology international Pub Date : 2025-08-18 Print Date: 2025-10-07 DOI:10.1556/2060.2025.00482

Yilai Yu, Lifei Huang, Xingxing Zhu, Yahong Sun

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引用次数: 0

Abstract

Background: The most prevalent form of lung cancer, lung adenocarcinoma (LUAD), has significant incidence and fatality rates worldwide. When treating LUAD, osimertinib resistance is a typical problem. Thus, it is imperative to address the concerns of clarifying the mechanism of osimertinib resistance in LUAD and enhancing medication sensitivity.

Methods: Using bioinformatics techniques, expression and possible biological roles of BMP8A in LUAD were examined, and predictions were made about upstream regulatory variables and binding locations. H1975 cell line, resistant to osimertinib, was created. Western blot and RT-qPCR were instrumental to determine mRNA and protein expression of FABP5, ACC1, and FASN associated to lipid metabolism. A fluorescent lipid synthesis test kit was utilized to detect amount of triglycerides present in culture medium. BMP8A and RUNX2 mRNA levels were assayed using RT-qPCR. Utilizing CCK-8 and ANNEXIN V-FITC/PI flow cytometry, cell viability was assessed. Through the use of dual luciferase assays, whether RUNX2 could regulate BMP8A was confirmed. CHIP was further employed to confirm whether the two were bound together.

Results: BMP8A and fatty acid metabolism (FAM) have a strong association, as revealed by bioinformatics investigation, and RUNX2 is its upstream transcription factor. Osimertinib-resistant H1975 cell lines were successfully created, and these cell lines showed a significant upregulation of BMP8A expression. The drug sensitivity of the resistant cell lines was decreased, and their FAM level was considerably enhanced by overexpressing BMP8A. Changes in drug sensitivity and FAM were reversed by using FAM inhibitors. An efficient binding of RUNX2 to the BMP8A promoter region was demonstrated by experimental validation, hence activating the production of the BMP8A gene. Lowering LUAD cell survival rates, lipid metabolism levels, and BMP8A expression were all caused by RUNX2 knockdown.

Conclusion: RUNX2 activated BMP8A-mediated FAM to facilitate osimertinib resistance in LUAD.

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RUNX2刺激BMP8A促进脂肪酸代谢，在肺腺癌中引起奥希替尼耐药。

背景：肺腺癌（LUAD）是最常见的肺癌形式，在世界范围内具有显著的发病率和死亡率。在治疗LUAD时，奥西替尼耐药是一个典型的问题。因此，澄清LUAD中奥西替尼耐药机制，提高用药敏感性是当务之急。方法：利用生物信息学技术，研究BMP8A在LUAD中的表达及其可能的生物学作用，并对上游调控变量和结合位点进行预测。培育出对奥西替尼具有耐药性的H1975细胞系。Western blot和RT-qPCR检测与脂质代谢相关的FABP5、ACC1和FASN mRNA和蛋白表达。采用荧光脂质合成检测试剂盒检测培养基中甘油三酯的含量。RT-qPCR检测BMP8A、RUNX2 mRNA表达水平。采用CCK-8和ANNEXIN V-FITC/PI流式细胞术检测细胞活力。通过双荧光素酶测定，确认RUNX2是否能调控BMP8A。进一步使用CHIP确认两者是否绑定在一起。结果：生物信息学研究显示BMP8A与脂肪酸代谢（FAM）有较强的相关性，RUNX2是其上游转录因子。成功建立了抗奥西替尼的H1975细胞系，这些细胞系显示出BMP8A表达的显著上调。过表达BMP8A使耐药细胞株的药物敏感性降低，FAM水平显著提高。使用FAM抑制剂可逆转药物敏感性和FAM的变化。实验验证了RUNX2与BMP8A启动子区域的有效结合，从而激活了BMP8A基因的产生。RUNX2敲低可导致LUAD细胞存活率降低、脂质代谢水平降低、BMP8A表达降低。结论：RUNX2激活bmp8a介导的FAM促进LUAD患者对奥希替尼的耐药。

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来源期刊

Physiology international Medicine-Physiology (medical)

CiteScore

3.40

自引率

0.00%

发文量

期刊介绍： The journal provides a forum for important new research papers written by eminent scientists on experimental medical sciences. Papers reporting on both original work and review articles in the fields of basic and clinical physiology, pathophysiology (from the subcellular organization level up to the oranizmic one), as well as related disciplines, including history of physiological sciences, are accepted.