表观遗传学
间充质干细胞
鉴定(生物学)
癌症研究
危险分层
医学
甲基化
肿瘤科
DNA甲基化
计算生物学
生物
生物信息学
病理
内科学
A组
子群分析
免疫组织化学
分子病理学
作者
Yong Lin,Yun Ning,Lan Yang,Yu‐Juan Cao,Ruijiao Zhao,Hainan Li,Song Duan,W. Fu,Haibo Wu,Feng Wu,Xiu‐Wu Bian,Tao Luo,Xiaohong Yao
摘要
Intracranial mesenchymal tumors (IMTs) with FET::CREB fusion are newly recognized molecular entities, provisionally classified into subgroups A and B. Although Group B has been partially characterized, the clinicopathological and molecular heterogeneity of Group A remains poorly defined. This study aimed to conduct an integrated analysis of 6 newly diagnosed and 20 previously reported IMTs with FET::CREB fusion. Notably, Group A was further stratified into two distinct entities A1 and A2 based on unsupervised methylation profiling. Compared to Group A1, Group A2 demonstrated significantly shorter progression-free survival (PFS), a higher proportion of male patients, and less frequent occurrence of myxoid-rich stroma. Amplification of 10p15.3 was frequently observed in Group A2. Furthermore, GLUT-1 could serve as a potential diagnostic indicator in IMTs with FET::CREB fusion. Overall, we identified a new subgroup of IMTs with FET::CREB fusion with poor PFS and distinct clinicopathological and molecular features, offering actionable insights to refine therapeutic strategies and improve risk stratification in this emerging diagnostic category.
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