A novel molecular classification method for osteosarcoma based on tumor cell differentiation trajectories

基于肿瘤细胞分化轨迹的骨肉瘤分子分类新方法

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作者:Hao Zhang #, Ting Wang #, Haiyi Gong, Runyi Jiang, Wang Zhou, Haitao Sun, Runzhi Huang, Yao Wang, Zhipeng Wu, Wei Xu, Zhenxi Li, Quan Huang, Xiaopan Cai, Zaijun Lin, Jinbo Hu, Qi Jia, Chen Ye, Haifeng Wei, Jianru Xiao

Abstract

Subclassification of tumors based on molecular features may facilitate therapeutic choice and increase the response rate of cancer patients. However, the highly complex cell origin involved in osteosarcoma (OS) limits the utility of traditional bulk RNA sequencing for OS subclassification. Single-cell RNA sequencing (scRNA-seq) holds great promise for identifying cell heterogeneity. However, this technique has rarely been used in the study of tumor subclassification. By analyzing scRNA-seq data for six conventional OS and nine cancellous bone (CB) samples, we identified 29 clusters in OS and CB samples and discovered three differentiation trajectories from the cancer stem cell (CSC)-like subset, which allowed us to classify OS samples into three groups. The classification model was further examined using the TARGET dataset. Each subgroup of OS had different prognoses and possible drug sensitivities, and OS cells in the three differentiation branches showed distinct interactions with other clusters in the OS microenvironment. In addition, we verified the classification model through IHC staining in 138 OS samples, revealing a worse prognosis for Group B patients. Furthermore, we describe the novel transcriptional program of CSCs and highlight the activation of EZH2 in CSCs of OS. These findings provide a novel subclassification method based on scRNA-seq and shed new light on the molecular features of CSCs in OS and may serve as valuable references for precision treatment for and therapeutic development in OS.

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