National Center for International Research in Cell and Gene Therapy, Sino-British Research Centre for Molecular Oncology, State Key Laboratory of Esophageal Cancer Prevention Treatment, School of Basic Medical Sciences, Academy of Medical Sciences, Zhengzhou University, Zhengzhou, China.
Department of Molecular Pathology, The Affiliated Cancer Hospital of Zhengzhou University, Henan Cancer Hospital, Zhengzhou, China.
Front Immunol. 2022 Jun 22;13:896627. doi: 10.3389/fimmu.2022.896627. eCollection 2022.
Esophageal Squamous Cell carcinomas (ESCC) is a highly heterogeneous malignancy that is among the leading cause of cancer-related death worldwide. B cells play pivotal roles in the immune defense system and cancer progression and regression, yet the repertoire of tumor infiltrating B cells (TIBs) and its association with clinical outcome remains unexplored in ESCC. Here we collected bulk RNA-seq sequencing data from 119 ESCC tumors and matched adjacent normal samples to delineate the B cell repertoire. We found that ESCC is more heavily infiltrated by B cells and plasma cells compared to activated T cells. The immunoglobulin heavy chain variable region (IGHV) gene usage was remarkably biased and was under-represented in ESCC tumors. The TIBs showed a more oligoclonal profile along with widespread clonal expansion and IgG subclass switch events (CSRs). Survival analysis revealed several unexpected associations between tumor infiltrating B cells and prognosis. Higher levels of immunoglobulin expression (IGH), CD138 expression, IGH to ratio, CSR events and clone diversity are all associated with better survival. Notably, we found that the abundance of -negative IgG2-producing plasma cells has a strong positive effect on overall survival with a hazard ratio (HR) of 0.40 (log-rank p: 0.002). Combing molecular subtyping, the IgG2-producing plasma cells could stratify high-risk patients more accurately with a HR of 0.253 (log-rank p: 0.0006). The direct link between protective B cell populations and ESCC prognosis provides biomarkers for high-risk patient selection and holds great promise for developing strategies for immunotherapy targeting B cells in ESCC patients.
食管鳞状细胞癌 (ESCC) 是一种高度异质性的恶性肿瘤,是全球癌症相关死亡的主要原因之一。B 细胞在免疫防御系统和癌症的发生和消退中起着关键作用,但肿瘤浸润 B 细胞 (TIB) 的组成及其与临床结局的关系在 ESCC 中仍未得到探索。在这里,我们收集了 119 例 ESCC 肿瘤和匹配的相邻正常样本的批量 RNA-seq 测序数据,以描绘 B 细胞库。我们发现,与活化的 T 细胞相比,ESCC 中 B 细胞和浆细胞的浸润更为严重。免疫球蛋白重链可变区 (IGHV) 基因的使用明显偏向,在 ESCC 肿瘤中表达不足。TIB 显示出更具寡克隆特征,同时存在广泛的克隆扩增和 IgG 亚类转换事件 (CSRs)。生存分析揭示了肿瘤浸润 B 细胞与预后之间的一些意外关联。较高的免疫球蛋白表达 (IGH)、CD138 表达、IGH 与 比值、CSR 事件和克隆多样性均与更好的生存相关。值得注意的是,我们发现 -阴性 IgG2 产生浆细胞的丰度对总生存率有很强的正效应,风险比 (HR) 为 0.40(对数秩检验 p:0.002)。结合分子亚型,IgG2 产生浆细胞可以更准确地对高危患者进行分层,HR 为 0.253(对数秩检验 p:0.0006)。保护性 B 细胞群体与 ESCC 预后之间的直接联系为高危患者选择提供了生物标志物,并为开发针对 ESCC 患者 B 细胞的免疫治疗策略提供了很大的希望。
