Zeng Yanni, Luo Chun-Ling, Lin Guo-Wang, Li Fugui, Bai Xiaomeng, Ko Josephine Mun-Yee, Xiong Lei, Liu Yang, He Shuai, Jiang Jia-Xin, Yan Wen-Xin, Ong Enya Hui Wen, Li Zheng, Zhou Ya-Qing, Zhou Yun-He, Xu An-Yi, Liu Shu-Qiang, Guo Yun-Miao, Chen Jie-Rong, Cheng Xi-Xi, Cao Yu-Lu, Yu Xia, Wu Biaohua, Wei Pan-Pan, Ruan Zhao-Hui, Chen Qiu-Yan, Tang Lin-Quan, McKay James D, Jia Wei-Hua, Mai Hai-Qiang, Lim Soon Thye, Liu Jian-Jun, Lin Dong-Xin, Khor Chiea Chuen, Chua Melvin Lee Kiang, Ji Mingfang, Lung Maria Li, Zeng Yi-Xin, Bei Jin-Xin
State Key Laboratory of Oncology in South China, Guangdong Key Laboratory of Nasopharyngeal Carcinoma Diagnosis and Therapy, Guangdong Provincial Clinical Research Center for Cancer, Sun Yat-sen University Cancer Center - Zhongshan School of Medicine.
Faculty of Forensic Medicine, Guangdong Province Translational Forensic Medicine Engineering Technology Research Center, and.
J Clin Invest. 2025 Jan 2;135(1):e182768. doi: 10.1172/JCI182768.
Nasopharyngeal carcinoma (NPC) presents a substantial clinical challenge due to the limited understanding of its genetic underpinnings. Here we conduct the largest scale whole-exome sequencing association study of NPC to date, encompassing 6,969 NPC cases and 7,100 controls. We unveil 3 germline genetic variants linked to NPC susceptibility: a common rs2276868 in RPL14, a rare rs5361 in SELE, and a common rs1050462 in HLA-B. We also underscore the critical impact of rare genetic variants on NPC heritability and introduce a refined composite polygenic risk score (rcPRS), which outperforms existing models in predicting NPC risk. Importantly, we reveal that the polygenic risk for NPC is mediated by EBV infection status. Utilizing a comprehensive multiomics approach that integrates both bulk-transcriptomic (n = 356) and single-cell RNA sequencing (n = 56) data with experimental validations, we demonstrate that the RPL14 variant modulates the EBV life cycle and NPC pathogenesis. Furthermore, our data indicate that the SELE variant contributes to modifying endothelial cell function, thereby facilitating NPC progression. Collectively, our study provides crucial insights into the intricate genetic architecture of NPC, spotlighting the vital interplay between genetic variations and tumor microenvironment components, including EBV and endothelial cells, in predisposing to NPC. This study opens new avenues for advancements in personalized risk assessments, early diagnosis, and targeted therapies for NPC.
由于对鼻咽癌(NPC)的遗传基础了解有限,它带来了重大的临床挑战。在此,我们开展了迄今为止规模最大的NPC全外显子测序关联研究,涵盖6969例NPC病例和7100例对照。我们发现了3个与NPC易感性相关的种系遗传变异:RPL14中常见的rs2276868、SELE中罕见的rs5361以及HLA - B中常见的rs1050462。我们还强调了罕见遗传变异对NPC遗传度的关键影响,并引入了一种改进的复合多基因风险评分(rcPRS),其在预测NPC风险方面优于现有模型。重要的是,我们发现NPC的多基因风险由EB病毒感染状态介导。利用一种综合的多组学方法,将批量转录组学(n = 356)和单细胞RNA测序(n = 56)数据与实验验证相结合,我们证明RPL14变异调节EB病毒生命周期和NPC发病机制。此外,我们的数据表明SELE变异有助于改变内皮细胞功能,从而促进NPC进展。总体而言,我们的研究为NPC复杂的遗传结构提供了关键见解,突出了遗传变异与肿瘤微环境成分(包括EB病毒和内皮细胞)之间在NPC易感性方面的重要相互作用。这项研究为NPC的个性化风险评估、早期诊断和靶向治疗的进展开辟了新途径。
