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Human prostate-infiltrating CD8+ T lymphocytes are oligoclonal and PD-1+

机译:人前列腺浸润CD8 + T淋巴细胞是寡克隆的,PD-1 +

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BACKGROUND. Prostate-infiltrating CD8+ T lymphocytes (CD8 + PIL) are prevalent in men with prostate cancer (PCa), however, it is unclear whether the presence of such cells reflects a non-specific immune infiltrate or an oligoclonal, antigen-driven adaptive immune response. METHODS. We investigated the complexity of the T-cell receptor (TCR) repertoire in the prostate gland by examining the diversity of CD8+ TCR β chain variable region (Vβ) gene sequences in both the peripheral blood and prostates of cancer patients. Vβ repertoire analysis was performed by family-specific Vβ spectratyping and flow cytometry, as well as direct sequence analysis (5′ RACE and cloning). Programmed cell death 1 (PD-1 or PDCD1) expression on peripheral blood CD8+ T cells and CD8 + PIL was analyzed by flow cytometry. RESULTS. CD8+ PIL isolated from cancer patients exhibited restricted TCR Vβ gene usage, and identical clones were identified in multiple sites within the prostate. Furthermore, CD8+ PIL express high levels of the inhibitory receptor PD-1, a cell surface protein associated with an "exhausted" CD8 + T-cell phenotype. CONCLUSIONS. CD8+ PIL appear to have undergone clonal expansion in response to an as yet unidentified antigen; however, due to the high expression of PD-1, these cells are likely incapable of mounting an effective immune response. The results provide an important basis for further efforts aimed at the identification of specific antigens involved in prostatic inflammation, and suggest that PD-1 blockade may be useful in immunotherapy for PCa.
机译:背景。前列腺浸润的CD8 + T淋巴细胞(CD8 + PIL)在前列腺癌(PCa)的男性中普遍存在,但是尚不清楚此类细胞的存在是否反映了非特异性免疫浸润还是寡克隆的,抗原驱动的适应性免疫应答。方法。我们通过检查癌症患者外周血和前列腺中CD8 + TCRβ链可变区(Vβ)基因序列的多样性,研究了前列腺中T细胞受体(TCR)库的复杂性。通过家族特异性Vβ谱型和流式细胞术以及直接序列分析(5'RACE和克隆)进行Vβ库分析。通过流式细胞术分析外周血CD8 + T细胞和CD8 + PIL上的程序性细胞死亡1(PD-1或PDCD1)表达。结果。从癌症患者中分离出的CD8 + PIL显示出受限制的TCRVβ基因使用情况,并且在前列腺内的多个部位鉴定出相同的克隆。此外,CD8 + PIL表达高水平的抑制受体PD-1,PD-1是与“精疲力竭”的CD8 + T细胞表型相关的细胞表面蛋白。结论。 CD8 + PIL似乎已经针对尚未鉴定的抗原发生了克隆扩增;然而,由于PD-1的高表达,这些细胞可能无法进行有效的免疫反应。该结果为进一步努力鉴定与前列腺炎有关的特定抗原提供了重要依据,并提示PD-1阻断可用于PCa的免疫治疗。

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