Department of Surgery, Stanford University School of Medicine, Stanford, CA, United States.
Department of Pediatric Oncology, Roswell Park Comprehensive Cancer Center, Buffalo, NY, United States.
Front Immunol. 2022 Oct 7;13:994552. doi: 10.3389/fimmu.2022.994552. eCollection 2022.
Post-transplant lymphoproliferative disorder (PTLD) is a serious complication of solid organ transplantation. Predisposing factors include primary Epstein-Barr virus (EBV) infection, reactivation of EBV in recipient B cells, and decreased T cell immunity due to immunosuppression. In our previous studies EBV infection was demonstrated to markedly alter the expression of host B cell microRNA (miR). Specifically, miR-194 expression was uniquely suppressed in EBV+ B cell lines from PTLD patients and the 3'untranslated region of IL-10 was determined to be targeted by miR-194. Although EBV has been shown to regulate host miR expression in B cell lymphoma cell lines, the expression of miRs in the circulation of patients with EBV-associated PTLD has not been studied. The objective of this study was to determine if changes in miR expression are associated with EBV+ PTLD. In this study, we have shown that miR-194 is significantly decreased in EBV+PTLD tumors and that additional miRs, including miRs-17, 19 and 106a are also reduced in EBV+PTLD as compared to EBV-PTLD. We quantitated the levels of miRs-17, 19, 106a, 155, and 194 in the plasma and extracellular vesicles (EV; 50-70 nm as determined by nanoparticle tracking analysis) from pediatric recipients of solid organ transplants with EBV+ PTLD+ that were matched 1:2 with EBV+ PTLD- pediatric transplant recipients as part of the NIH-sponsored Clinical Trials in Organ Transplantation in Children, (CTOTC-06) study. Levels of miRs-17, 19, 106a, and 194 were reduced in the plasma and extracellular vesicles (EV) of EBV+ PTLD+ group compared to matched controls, with miRs-17 (p = 0.034; plasma), miRs-19 (p = 0.029; EV) and miR-106a (p = 0.007; plasma and EV) being significantly reduced. Similar levels of miR-155 were detected in the plasma and EV of all pediatric SOT recipients. Importantly, ~90% of the cell-free miR were contained within the EV supporting that EBV+ PTLD tumor miR are detected in the circulation and suggesting that EVs, containing miRs, may have the potential to target and regulate cells of the immune system. Further development of diagnostic, mechanistic and potential therapeutic uses of the miRs in PTLD is warranted.
移植后淋巴组织增生性疾病 (PTLD) 是实体器官移植的严重并发症。易患因素包括原发性 EBV (EBV) 感染、受者 B 细胞中 EBV 的再激活以及由于免疫抑制导致 T 细胞免疫功能下降。在我们之前的研究中,已证实 EBV 感染可显著改变宿主 B 细胞 microRNA (miR) 的表达。具体来说,PTLD 患者 EBV+B 细胞系中 miR-194 的表达被特异性抑制,IL-10 的 3'非翻译区被确定为 miR-194 的靶标。尽管 EBV 已被证明可调节 B 细胞淋巴瘤细胞系中的宿主 miR 表达,但 EBV 相关 PTLD 患者循环中的 miR 表达尚未得到研究。本研究旨在确定 miR 表达的变化是否与 EBV+PTLD 相关。在这项研究中,我们已经表明,与 EBV-PTLD 相比,miR-194 在 EBV+PTLD 肿瘤中显著降低,并且其他 miR,包括 miR-17、19 和 106a,也在 EBV+PTLD 中降低。我们定量了在 NIH 赞助的儿童器官移植临床试验 (CTOTC-06) 中,与 EBV+PTLD- 儿科移植受者 1:2 匹配的 EBV+PTLD+ 实体器官移植儿童患者的血浆和细胞外囊泡 (EV; 通过纳米颗粒跟踪分析确定为 50-70nm) 中 miR-17、19、106a、155 和 194 的水平。与匹配对照相比,EBV+PTLD+ 组的血浆和细胞外囊泡 (EV) 中的 miR-17、19、106a 和 194 水平降低,miR-17(p=0.034;血浆)、miR-19(p=0.029;EV)和 miR-106a(p=0.007;血浆和 EV) 显著降低。所有儿科 SOT 受者的血浆和 EV 中均检测到相似水平的 miR-155。重要的是,约 90%的无细胞 miR 存在于 EV 中,这支持 EBV+PTLD 肿瘤 miR 可在循环中检测到,并表明含有 miR 的 EV 可能具有靶向和调节免疫系统细胞的潜力。进一步开发用于 PTLD 的 miR 的诊断、机制和潜在治疗用途是合理的。
Zotero 插件
