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多倍体巨癌细胞:高危致癌性 HCMV 株诱导上皮细胞转化的一个显著特征。

Polyploid Giant Cancer Cells: A Distinctive Feature in the Transformation of Epithelial Cells by High-Risk Oncogenic HCMV Strains.

机构信息

Department Pathogens & Inflammation-EPILAB EA4266, University of Franche-Comté UFC, 25000 Besancon, France.

Department of Virology, CHU Besançon, 250000 Besancon, France.

出版信息

Viruses. 2024 Jul 31;16(8):1225. doi: 10.3390/v16081225.

Abstract

Human cytomegalovirus (HCMV) infection is common in tumor tissues across different types of cancer. While HCMV has not been recognized as a cancer-causing virus, numerous studies hint at its potential role in cancer development where its presence in various cancers corresponds with the hallmarks of cancer. Herein, we discuss and demonstrate that high-risk HCMV-DB and BL strains have the potential to trigger transformation in epithelial cells, including human mammary epithelial cells (HMECs), ovarian epithelial cells (OECs), and prostate epithelial cells (PECs), through the generation of polyploid giant cancer cells (PGCCs). A discussion is provided on how HCMV infection creates a cellular environment that promotes oncogenesis, supporting the continuous growth of CMV-transformed cells. The aforementioned transformed cells, named CTH, CTO, and CTP cells, underwent giant cell cycling with PGCC generation parallel to dedifferentiation, displaying stem-like characteristics and an epithelial-mesenchymal transition (EMT) phenotype. Furthermore, we propose that giant cell cycling through PGCCs, increased EZH2 expression, EMT, and the acquisition of malignant traits represent a deleterious response to the cellular stress induced by high-risk oncogenic HCMV strains, the latter being the origin of the transformation process in epithelial cells upon HCMV infection and leading to adenocarcinoma of poor prognosis.

摘要

人巨细胞病毒(HCMV)感染在不同类型癌症的肿瘤组织中很常见。虽然 HCMV 尚未被认为是致癌病毒,但许多研究表明其在癌症发展中具有潜在作用,其在各种癌症中的存在与癌症的标志相一致。在此,我们讨论并证明高风险 HCMV-DB 和 BL 株有可能通过产生多倍体巨大癌细胞(PGCC),引发包括人乳腺上皮细胞(HMEC)、卵巢上皮细胞(OEC)和前列腺上皮细胞(PEC)在内的上皮细胞发生转化。本文还讨论了 HCMV 感染如何创造促进致癌的细胞环境,支持 CMV 转化细胞的持续生长。上述转化细胞分别命名为 CTH、CTO 和 CTP 细胞,经历了伴随去分化的巨细胞周期循环和 PGCC 生成,表现出类似干细胞的特征和上皮-间充质转化(EMT)表型。此外,我们提出,通过 PGCC 进行巨细胞周期循环、EZH2 表达增加、EMT 和获得恶性特征,代表了对高风险致癌 HCMV 株诱导的细胞应激的有害反应,后者是上皮细胞在 HCMV 感染后发生转化过程的起源,并导致预后不良的腺癌。

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