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文献速递丨SCI 高分文献(IF值:8)SLC25A39过表达促进肺腺癌进展且受AFG3L2负调控

文献速递丨SCI 高分文献(IF值:8)SLC25A39过表达促进肺腺癌进展且受AFG3L2负调控 金源康生物
2026-04-02
2

高分文献速递


客户单位:苏州大学附属第一医院


期刊:npj Precision Oncology


影响因子(IF):8

文章题目:

slc25a39 overexpression exacerbates lung adenocarcinoma progression and is negatively regulated by afg3l2

Lung adenocarcinoma (LUAD), the most common lung cancer subtype, has a poor prognosis and limited treatments, underscoring the need for new biomarkers and targets, particularly in mitochondrial metabolism. Our study identifies SLC25A39, a mitochondrial glutathione transporter, as a key oncogenic factor in LUAD. Bioinformatics and tissue analyses revealed significantly elevated SLC25A39 protein levels despite stable mRNA expression, correlating with poorer patient survival. Functionally, SLC25A39 overexpression promoted LUAD cell proliferation and migration, while its knockdown or deletion suppressed these malignant traits in vitro and in vivo. Mechanistically, SLC25A39 loss impaired mitochondrial oxidative phosphorylation, increased reactive oxygen species (ROS), and triggered apoptosis. Notably, we found that reduced expression of the m-AAA protease AFG3L2 in LUAD post-translationally stabilizes SLC25A39, leading to its accumulation. These findings demonstrate that AFG3L2 downregulation drives SLC25A39's oncogenic activity, positioning SLC25A39 as a promising therapeutic target for LUAD.

原文链接:

https://pubmed.ncbi.nlm.nih.gov/40993178/

引用产品及培养细胞:FBS-301 A549

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金源康生物 金源康生物是一家专注动物血清、培养基、疫苗佐剂、细胞库及周边产品等研发与生产应用的国家级高新技术企业,奥普赛生物为金源康所属子品牌。咨询热线:400-880-5811,官方网址:www.nmjyk.com
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