Synovial Sarcomas (SS) are characterized by the presence of the SS18::SSX fusion gene, which protein product induce chromatin changes through remodeling of the BAF complex. To elucidate the genomic events that drive phenotypic diversity in SS, we performed RNA and targeted DNA sequencing on 91 tumors from 55 patients. Our results were verified by proteomic analysis, public gene expression cohorts and single-cell RNA sequencing. Transcriptome profiling identified three distinct SS subtypes resembling the known histological subtypes: SS subtype I and was characterized by hyperproliferation, evasion of immune detection and a poor prognosis. SS subtype II and was dominated by a vascular-stromal component and had a significantly better outcome. SS Subtype III was characterized by biphasic differentiation, increased genomic complexity and immune suppression mediated by checkpoint inhibition, and poor prognosis despite good responses to neoadjuvant therapy. Chromosomal abnormalities were an independent significant risk factor for metastasis. KRT8 was identified as a key component for epithelial differentiation in biphasic tumors, potentially controlled by OVOL1 regulation. Our findings explain the histological grounds for SS classification and indicate that a significantly larger proportion of patients have high risk tumors (corresponding to SS subtype I) than previously believed.
Molecular Profiling Defines Three Subtypes of Synovial Sarcoma.
分子谱分析将滑膜肉瘤分为三种亚型
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作者:Chen Yi, Su Yanhong, Cao Xiaofang, Siavelis Ioannis, Leo Isabelle Rose, Zeng Jianming, Tsagkozis Panagiotis, Hesla Asle C, Papakonstantinou Andri, Liu Xiao, Huang Wen-Kuan, Zhao Binbin, Haglund Cecilia, Ehnman Monika, Johansson Henrik, Lin Yingbo, Lehtiö Janne, Zhang Yifan, Larsson Olle, Li Xuexin, de Flon Felix Haglund
| 期刊: | Advanced Science | 影响因子: | 14.100 |
| 时间: | 2024 | 起止号: | 2024 Nov;11(41):e2404510 |
| doi: | 10.1002/advs.202404510 | 研究方向: | 肿瘤 |
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