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首页> 外文期刊>Bone marrow transplantation >CD8+ T-cell responses to tumor-associated antigens correlate with superior relapse-free survival after allo-SCT.
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CD8+ T-cell responses to tumor-associated antigens correlate with superior relapse-free survival after allo-SCT.

机译:CD8 + T细胞对肿瘤相关抗原的反应与同种异体移植后优良的无复发生存相关。

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摘要

The GVL effect following allo-SCT is one of the most prominent examples showing the ability of the immune system to eliminate malignant hematological diseases. Tumor-associated Ags (TAA), for instance WT1 and proteinase-3, have been proposed as targets for T cells to establish a GVL effect. Here, we examined an additional TAA (MUC1) as a possible T-cell target of GVL-related immune responses. We have defined new peptide epitopes from the MUC1 Ag to broaden patients' screening and to expand the repertoire of immunologic monitoring as well as for therapeutic approaches in the future. Twenty-eight patients after allo-SCT have been screened for T-cell responses toward TAA (proteinase-3, WT1, MUC1). We could detect a significant relationship between relapse and the absence of a TAA-specific T-cell response, whereby only 2/13 (15%) patients with TAA-specific CTL relapsed, in contrast to 9/15 (60%) patients without TAA-specific CTL responses (P<0.05). In conclusion, CD8(+) T-cell responses directed to TAA might contribute to the GVL effect. These observations highlight both the importance and the potential of immunotherapeutic approaches after allo-SCT.
机译:异源SCT后的GVL效应是最突出的例子之一,显示了免疫系统消除恶性血液病的能力。肿瘤相关的抗原(TAA),例如WT1和蛋白酶3,已被提议作为T细胞的靶标,以建立GVL效应。在这里,我们检查了额外的TAA(MUC1)作为GVL相关免疫反应的可能T细胞靶标。我们已经定义了MUC1 Ag的新肽表位,以扩大患者的筛查范围,并扩大免疫学监测范围以及将来的治疗方法。筛选了28名同种SCT后的患者针对TAA的T细胞应答(蛋白酶3,WT1,MUC1)。我们可以检测到复发与不存在TAA特异性T细胞反应之间存在显着相关性,从而只有2/13(15%)的TAA特异性CTL患者复发,而9/15(60%)的患者没有复发TAA特异性CTL反应(P <0.05)。总之,针对TAA的CD8(+)T细胞应答可能有助于GVL效应。这些观察结果突出了异源SCT后免疫治疗方法的重要性和潜力。

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