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未突变抗原在T细胞库未受干扰的小鼠肿瘤排斥反应中的作用

On the role of unmutated antigens in tumor rejection in mice with unperturbed T-cell repertoires.

作者信息

Sarma Supria, Bai Xue-Feng, Liu Jin-qing, May Kenneth F, Zheng Pan, Liu Yang

机构信息

Division of Cancer Immunology, Department of Pathology, Ohio State University Medical Center, Columbus, Ohio 43210, USA.

出版信息

Cancer Res. 2003 Sep 15;63(18):6051-5.

Abstract

We investigate here whether P1A, which was the first CTL-recognized and unmutated tumor antigen to be identified, is a tumor rejection antigen for J558 plasmacytoma in mice with an unperturbed T-cell repertoire. We show that although transgenic mice expressing P1A in the thymus have almost complete deletion of P1A-reactive T cells, they reject the B7-1-transfected J558 at a rate comparable with wild-type mice. Thus, P1A is not a necessary tumor rejection antigen for the J558 tumor cells. On the other hand, if anti-P1A CTL response is sufficient for tumor rejection, tumor cells must lose the antigenic epitope to evade CTL destruction. To test this, we analyze whether tumor cells escaping J558-B7 immune spleen cells harbor mutations in the P1A epitope. We find that although the spleen contained a high proportion of P1A-reactive T cells, the recurrent tumor cells have no mutation in the P1A antigenic epitope and remain susceptible to lysis by P1CTL. Thus, the antigen-bearing tumor cells can evade immune destruction in the presence of a high number of P1A-reactive T cells. Taken together, our results demonstrate that in mice with a normal TCR repertoire, substantial numbers of P1A-reactive T cells are neither necessary nor sufficient for tumor rejection and raise interesting questions regarding the significance of T-cell response against unmutated tumor antigens.

摘要

我们在此研究首个被CTL识别且未发生突变的肿瘤抗原P1A,对于T细胞库未受干扰的小鼠中的J558浆细胞瘤而言,是否为肿瘤排斥抗原。我们发现,尽管在胸腺中表达P1A的转基因小鼠几乎完全缺失了对P1A有反应的T细胞,但它们排斥B7-1转染的J558的速率与野生型小鼠相当。因此,P1A并非J558肿瘤细胞必需的肿瘤排斥抗原。另一方面,如果抗P1A的CTL反应足以实现肿瘤排斥,肿瘤细胞必须失去抗原表位以逃避CTL的破坏。为了验证这一点,我们分析了从J558-B7免疫脾细胞中逃逸的肿瘤细胞在P1A表位上是否存在突变。我们发现,尽管脾脏中含有高比例的对P1A有反应的T细胞,但复发的肿瘤细胞在P1A抗原表位上没有突变,并且仍然易被P1CTL裂解。因此,携带抗原的肿瘤细胞在存在大量对P1A有反应的T细胞的情况下能够逃避免疫破坏。综上所述,我们的结果表明,在TCR库正常的小鼠中,大量对P1A有反应的T细胞对于肿瘤排斥既非必需也不充分,并引发了关于针对未突变肿瘤抗原的T细胞反应的意义的有趣问题。

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