Tumor Biology Program, Sylvester Comprehensive Cancer Center and Miami Center for AIDS Research, Department of Microbiology and Immunology, University of Miami Miller School of Medicine, Miami, Florida, United States of America.
UM-CFAR/ Sylvester CCC Argentina Consortium for Research and Training in Virally induced AIDS-Malignancies University of Miami Miller School of Medicine, Miami, Florida, United States of America.
PLoS Pathog. 2020 Jun 30;16(6):e1008589. doi: 10.1371/journal.ppat.1008589. eCollection 2020 Jun.
Kaposi's sarcoma (KS), is an AIDS-associated neoplasm caused by the KS herpesvirus (KSHV/ HHV-8). KSHV-induced sarcomagenesis is the consequence of oncogenic viral gene expression as well as host genetic and epigenetic alterations. Although KSHV is found in all KS-lesions, the percentage of KSHV-infected (LANA+) spindle-cells of the lesion is variable, suggesting the existence of KS-spindle cells that have lost KSHV and proliferate autonomously or via paracrine mechanisms. A mouse model of KSHVBac36-driven tumorigenesis allowed us to induce KSHV-episome loss before and after tumor development. Although infected cells that lose the KSHV-episome prior to tumor formation lose their tumorigenicity, explanted tumor cells that lost the KSHV-episome remained tumorigenic. This pointed to the existence of virally-induced irreversible oncogenic alterations occurring during KSHV tumorigenesis supporting the possibility of hit and run viral-sarcomagenesis. RNA-sequencing and CpG-methylation analysis were performed on KSHV-positive and KSHV-negative tumors that developed following KSHV-episome loss from explanted tumor cells. When KSHV-positive cells form KSHV-driven tumors, along with viral-gene upregulation there is a tendency for hypo-methylation in genes from oncogenic and differentiation pathways. In contrast, KSHV-negative tumors formed after KSHV-episome loss, show a tendency towards gene hyper-methylation when compared to KSHV-positive tumors. Regarding occurrence of host-mutations, we found the same set of innate-immunity related mutations undetected in KSHV-infected cells but present in all KSHV-positive tumors occurring en exactly the same position, indicating that pre-existing host mutations that provide an in vivo growth advantage are clonally-selected and contribute to KSHV-tumorigenesis. In addition, KSHV-negative tumors display de novo mutations related to cell proliferation that, together with the PDGFRAD842V and other proposed mechanism, could be responsible for driving tumorigenesis in the absence of KSHV-episomes. KSHV-induced irreversible genetic and epigenetic oncogenic alterations support the possibility of "hit and run" KSHV-sarcomagenesis and point to the existence of selectable KSHV-induced host mutations that may impact AIDS-KS treatment.
卡波济肉瘤(KS)是一种与艾滋病相关的肿瘤,由卡波济肉瘤疱疹病毒(KSHV/ HHV-8)引起。KSHV 诱导的肉瘤发生是致癌病毒基因表达以及宿主遗传和表观遗传改变的结果。尽管 KSHV 存在于所有 KS 病变中,但病变中 KSHV 感染的(LANA+)梭形细胞的百分比是可变的,这表明存在已经失去 KSHV 并通过自主或旁分泌机制增殖的 KS 梭形细胞。KSHVBac36 驱动的肿瘤发生的小鼠模型使我们能够在肿瘤发生前后诱导 KSHV episome 丢失。尽管在肿瘤形成之前失去 KSHV-episome 的感染细胞失去了致瘤性,但失去 KSHV-episome 的移植肿瘤细胞仍然具有致瘤性。这表明在 KSHV 肿瘤发生过程中存在病毒诱导的不可逆致癌改变,支持病毒 - 肉瘤发生的“击中并跑”的可能性。对从移植肿瘤细胞中丢失 KSHV-episome 后发展的 KSHV 阳性和 KSHV 阴性肿瘤进行了 RNA 测序和 CpG 甲基化分析。当 KSHV 阳性细胞形成 KSHV 驱动的肿瘤时,随着病毒基因的上调,致癌和分化途径的基因存在低甲基化的趋势。相比之下,在 KSHV-episome 丢失后形成的 KSHV 阴性肿瘤与 KSHV 阳性肿瘤相比,表现出基因高甲基化的趋势。关于宿主突变的发生,我们发现了一组在 KSHV 感染细胞中未检测到但在所有 KSHV 阳性肿瘤中完全相同位置存在的固有免疫相关突变,这表明提供体内生长优势的预先存在的宿主突变被克隆选择并有助于 KSHV 肿瘤发生。此外,KSHV 阴性肿瘤显示与细胞增殖相关的新生突变,与 PDGFRAD842V 和其他提议的机制一起,可能负责在没有 KSHV-episomes 的情况下驱动肿瘤发生。KSHV 诱导的不可逆遗传和表观遗传致癌改变支持“击中并跑”KSHV 肉瘤发生的可能性,并指出存在可选择的 KSHV 诱导的宿主突变,这可能影响艾滋病 - KS 的治疗。
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