Methionine intervention induces PD-L1 expression to enhance the immune checkpoint therapy response in MTAP-deleted osteosarcoma

蛋氨酸干预诱导PD-L1表达,从而增强MTAP缺失型骨肉瘤的免疫检查点治疗反应

阅读:16
作者:Haoran Mu,Qi Zhang,Dongqing Zuo,Jinzeng Wang,Yining Tao,Zhen Li,Xin He,Huanliang Meng,Hongsheng Wang,Jiakang Shen,Mengxiong Sun,Yafei Jiang,Weisong Zhao,Jing Han,Mengkai Yang,Zhuoying Wang,Yu Lv,Yuqin Yang,Jing Xu,Tao Zhang,Liu Yang,Jun Lin,Feng Tang,Renhong Tang,Haiyan Hu,Zhengdong Cai,Wei Sun,Yingqi Hua
期刊:Cell Reports Medicine影响因子:11.700
时间:2025起止号:2025 Mar 18;6(3):101977.
doi:10.1016/j.xcrm.2025.101977靶点: MTAPPD-L1
研究方向: 免疫/内分泌疾病类型: 骨肉瘤

Abstract

Osteosarcoma (OS), a malignant bone tumor with limited treatment options, exhibits low sensitivity to immune checkpoint therapy (ICT). Through genomics and transcriptomics analyses, we identify a subgroup of OS with methylthioadenosine phosphorylase (MTAP) deletion, which contributes to ICT resistance, leading to a "cold" tumor microenvironment. MTAP-deleted OS relies on methionine metabolism and is sensitive to methionine intervention, achieved through either dietary restriction or inhibition of methionine adenosyltransferase 2a (MAT2A), a key enzyme in methionine metabolism. We further demonstrate that methionine intervention triggers programmed death-ligand 1 (PD-L1) transcription factor IKAROS family zinc finger 1 (IKZF1) and enhances PD-L1 expression in MTAP-deleted OS cells. Methionine intervention also activates the immune-related signaling pathways in MTAP-deleted OS cells and attracts CD8+ T cells, thereby enhancing the efficacy of ICT. Combining methionine intervention with ICT provides a significant survival benefit in MTAP-deleted OS murine models, suggesting a rationale for combination regimens in OS ICT.

特别声明

1、本页面内容包含部分的内容是基于公开信息的合理引用;引用内容仅为补充信息,不代表本站立场。

2、若认为本页面引用内容涉及侵权,请及时与本站联系,我们将第一时间处理。

3、其他媒体/个人如需使用本页面原创内容,需注明“来源:[生知库]”并获得授权;使用引用内容的,需自行联系原作者获得许可。

4、投稿及合作请联系:info@biocloudy.com。