School of Cancer Sciences and Medical Research Council Centre for Immune Regulation, The University of Birmingham, Birmingham, United Kingdom.
Blood. 2012 Mar 1;119(9):2083-92. doi: 10.1182/blood-2011-07-366476. Epub 2012 Jan 10.
T-cell immunity is important for controlling Kaposi sarcoma-associated herpesvirus (KSHV) diseases such as the endothelial cell malignancy Kaposi sarcoma, or the B-cell malignancy, primary effusion lymphoma (PEL). However, little is known about KSHV-specific T-cell immunity in healthy donors and immune control of disease. Using PBMCs from healthy KSHV-infected donors, we found weak ex vivo responses to the KSHV latent antigens LANA, vFLIP, vCyclin, and Kaposin, with LANA most frequently recognized. CD4(+) T-cell clones specific to LANA, a protein expressed in all KSHV-infected cells and malignancies, were established to determine whether they could recognize LANA-expressing cells. B-cell targets expressing or fed LANA protein were consistently recognized by the clones; however, most PEL cell lines were not. PELs express the KSHV protein vIRF3 that inhibits promoter function of the HLA class II transactivator, decreasing expression of genes controlled by this transactivator. Re-expressing the class II transactivator in the PELs increased expression of downstream targets such as HLA class II and restored recognition but not killing by the LANA-specific clones. We suggest that PELs are poorly controlled in vivo because of inefficient recognition and killing by T cells.
T 细胞免疫对于控制卡波西肉瘤相关疱疹病毒(KSHV)疾病至关重要,如内皮细胞恶性肿瘤卡波西肉瘤,或 B 细胞恶性肿瘤原发性渗出淋巴瘤(PEL)。然而,对于健康供体中的 KSHV 特异性 T 细胞免疫以及疾病的免疫控制,我们知之甚少。我们使用来自健康 KSHV 感染供体的 PBMCs,发现对 KSHV 潜伏抗原 LANA、vFLIP、vCyclin 和 Kaposin 的体外反应较弱,其中 LANA 最常被识别。为了确定它们是否能够识别表达 LANA 的细胞,我们建立了针对 LANA 的 CD4(+) T 细胞克隆,该蛋白在所有 KSHV 感染的细胞和恶性肿瘤中表达。表达或摄取 LANA 蛋白的 B 细胞靶标被克隆一致识别;然而,大多数 PEL 细胞系则不然。PEL 表达 KSHV 蛋白 vIRF3,该蛋白抑制 HLA 类 II 转录激活物的启动子功能,降低该转录激活物控制的基因的表达。在 PEL 中重新表达 II 类转录激活物增加了下游靶标的表达,如 HLA 类 II,并恢复了对 LANA 特异性克隆的识别,但不能杀伤。我们认为 PEL 在体内受到控制不佳,是因为 T 细胞的识别和杀伤效率低下。
