肿瘤微环境
生物
免疫系统
癌症研究
免疫疗法
肿瘤浸润淋巴细胞
病理
免疫学
医学
作者
Zhihua Ou,Shitong Lin,Jiaying Qiu,Wencheng Ding,Peidi Ren,Dongsheng Chen,Jiaxuan Wang,Yihan Tong,Di Wu,Ao Chen,Yuan Deng,Mengnan Cheng,Ting Peng,Haorong Lu,Huanming Yang,Jian Wang,Xin Jin,Ding Ma,Xun Xu,Yanzhou Wang,Junhua Li,Peng Wu
标识
DOI:10.1002/advs.202203040
摘要
Abstract The effective treatment of advanced cervical cancer remains challenging. Herein, single‐nucleus RNA sequencing (snRNA‐seq) and SpaTial enhanced resolution omics‐sequencing (Stereo‐seq) are used to investigate the immunological microenvironment of cervical squamous cell carcinoma (CSCC). The expression levels of most immune suppressive genes in the tumor and inflammation areas of CSCC are not significantly higher than those in the non‐cancer samples, except for LGALS9 and IDO1 . Stronger signals of CD56 + NK cells and immature dendritic cells are found in the hypermetabolic tumor areas, whereas more eosinophils, immature B cells, and Treg cells are found in the hypometabolic tumor areas. Moreover, a cluster of pro‐tumorigenic cancer‐associated myofibroblasts (myCAFs) are identified. The myCAFs may support the growth and metastasis of tumors by inhibiting lymphocyte infiltration and remodeling of the tumor extracellular matrix. Furthermore, these myCAFs are associated with poorer survival probability in patients with CSCC, predict resistance to immunotherapy, and might be present in a small fraction (< 30%) of patients with advanced cancer. Immunohistochemistry and multiplex immunofluorescence staining are conducted to validate the spatial distribution and potential function of myCAFs. Collectively, these findings enhance the understanding of the immunological microenvironment of CSCC and shed light on the treatment of advanced CSCC.
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