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Cytotoxic T cell immunity against telomerase reverse transcriptase in humans

机译:抗人端粒酶逆转录酶的细胞毒性T细胞免疫

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摘要

Telomerase is a ribonucleoprotein enzyme which has been linked to malignant transformation in human cells. Telomerase activity is in- creased in the vast majority of human tumors, making its gene product the first molecule common to all human tumors. The gener- ation of endogenously processed telomerase peptides bound to Class ⅠMHC molecules could therefore target cytotoxic T lymphocytes (CTL) to tumors of different origins. This could advance vaccine therapy against cancer provided that precursor CTL recognizing telomerase peptides in normal adults and cancer patients can be expanded through immunization. We demonstrate here that the majority of normal individuals and patients with prostate cancer immunized in vbo against two HLA-A2.1 restricted peptides from telomerase reverse transcriptase (hTRT) develop hTRT-specific CTL. This suggests the existence of precursor CTL for hTRT in the repertoire of normal individuals and in cancer patients. Most importantly, the CTL of cancer patients specifically lysed a variety of HLA-A2~+ cancer cell lines, demonstrating immunological recognition of endogenously pro- cessed hTRT peptides. Moreover, in vivo immunization of HLA-A2.1 transgenic mice generated a specific CTL response against both hTRT peptides. Based on the induction of CTL responses in vitro and in vivo, and the susceptibility to lysis of tumor cells of various origins by hTRT CTL, we suggest that hTRT could serve as a universal cancer vaccine for humans.
机译:端粒酶是一种核糖核酸蛋白酶,已与人类细胞的恶性转化有关。端粒酶活性在绝大多数人类肿瘤中都得到增强,使其基因产物成为所有人类肿瘤共有的第一个分子。因此,与Ⅰ类MHC分子结合的内源性端粒酶肽的产生可将细胞毒性T淋巴细胞(CTL)靶向不同来源的肿瘤。只要可以通过免疫扩大正常成年人和癌症患者中识别端粒酶肽的前体CTL,就可以推进针对癌症的疫苗治疗。我们在这里证明,大多数正常个体和前列腺癌患者在vbo中针对端粒酶逆转录酶(hTRT)的两种HLA-A2.1限制性肽进行了免疫接种,从而开发了hTRT特异性CTL。这表明在正常人和癌症患者中存在hTRT的前体CTL。最重要的是,癌症患者的CTL特异性裂解了多种HLA-A2〜+癌细胞系,证明了对内源性hTRT肽的免疫学识别。此外,HLA-A2.1转基因小鼠的体内免疫产生了针对两种hTRT肽的特异性CTL反应。基于体外和体内诱导CTL反应以及hTRT CTL对各种来源的肿瘤细胞裂解的敏感性,我们建议hTRT可以作为人类通用的癌症疫苗。

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