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在HLA - A*0201阳性且BK病毒血清学阳性的供体中,针对人多瘤病毒BK大肿瘤抗原p53结合域的高频表位特异性CD45RA + /CCR7 +/- T淋巴细胞反应的特征分析

Characterization of highly frequent epitope-specific CD45RA+/CCR7+/- T lymphocyte responses against p53-binding domains of the human polyomavirus BK large tumor antigen in HLA-A*0201+ BKV-seropositive donors.

作者信息

Provenzano Maurizio, Bracci Laura, Wyler Stephen, Hudolin Tvrtko, Sais Giovanni, Gosert Rainer, Zajac Paul, Palu' Giorgio, Heberer Michael, Hirsch Hans H, Spagnoli Giulio C

机构信息

Institute of Surgical Research and Hospital Management, University Hospital Basel, Switzerland.

出版信息

J Transl Med. 2006 Nov 10;4:47. doi: 10.1186/1479-5876-4-47.

DOI:10.1186/1479-5876-4-47
PMID:17096832
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1660549/
Abstract

Human polyomavirus BK (BKV) has been implicated in oncogenic transformation. Its ability to replicate is determined by the binding of its large tumor antigen (LTag) to products of tumor-suppressor genes regulating cell cycle, as specifically p53. We investigated CD8+ T immune responses to BKV LTag portions involved in p53 binding in HLA-A0201+ BKV LTag experienced individuals. Peptides selected from either p53-binding region (LTag351-450 and LTag533-626) by current algorithms and capacity to bind HLA-A0201 molecule were used to stimulate CD8+ T responses, as assessed by IFN-gamma gene expression ex vivo and detected by cytotoxicity assays following in vitro culture. We observed epitope-specific immune responses in all HLA-A*0201+ BKV LTag experienced individuals tested. At least one epitope, LTag579-587; LLLIWFRPV, was naturally processed in non professional antigen presenting cells and induced cytotoxic responses with CTL precursor frequencies in the order of 1/20'000. Antigen specific CD8+ T cells were only detectable in the CD45RA+ subset, in both CCR7+ and CCR7- subpopulations. These data indicate that widespread cellular immune responses against epitopes within BKV LTag-p53 binding regions exist and question their roles in immunosurveillance against tumors possibly associated with BKV infection.

摘要

人多瘤病毒BK(BKV)与致癌转化有关。其复制能力取决于其大T抗原(LTag)与调节细胞周期的肿瘤抑制基因产物(特别是p53)的结合。我们研究了HLA - A0201阳性且有BKV LTag接触史个体对参与p53结合的BKV LTag部分的CD8 + T免疫反应。通过当前算法从p53结合区域(LTag351 - 450和LTag533 - 626)中选择并具有结合HLA - A0201分子能力的肽用于刺激CD8 + T反应,通过体外干扰素 - γ基因表达评估,并在体外培养后通过细胞毒性试验检测。我们在所有测试的HLA - A*0201阳性且有BKV LTag接触史的个体中观察到表位特异性免疫反应。至少一个表位LTag579 - 587;LLLIWFRPV在非专职抗原呈递细胞中自然加工,并诱导细胞毒性反应,CTL前体频率约为1/20000。抗原特异性CD8 + T细胞仅在CD45RA +亚群中可检测到,在CCR7 +和CCR7 -亚群中均有。这些数据表明,针对BKV LTag - p53结合区域内表位存在广泛的细胞免疫反应,并对它们在针对可能与BKV感染相关肿瘤的免疫监视中的作用提出了疑问。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d0ed/1660549/b6358dc1c038/1479-5876-4-47-7.jpg
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Detection of CD8+ T cells sensitized to BK virus large T antigen in healthy volunteers and kidney transplant recipients.
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