用于人乳头瘤病毒相关癌症的树突状细胞靶向疫苗。
Dendritic cell targeting vaccine for HPV-associated cancer.
作者信息
Yin Wenjie, Duluc Dorothée, Joo HyeMee, Oh SangKon
机构信息
Baylor Institute for Immunology Research, 3434 Live Oak Street, Dallas, TX 75204, USA; Institute of Biomedical Studies, Baylor University, South 5th Street, Waco, TX 76706, USA.
Baylor Institute for Immunology Research, 3434 Live Oak Street, Dallas, TX 75204, USA.
出版信息
Cancer Cell Microenviron. 2016;3(4). Epub 2017 Jan 15.
Dendritic cells (DCs) are major antigen presenting cells that can efficiently prime and activate cellular immune responses. Delivering antigens to DCs has thus been considered as a promising strategy that could allow us to mount T cell-mediated therapeutic immunity against cancers in patients. Successful development of such types of cancer vaccines that can target DCs, however, requires a series of outstanding questions that need to be addressed. These include the proper selection of which DC surface receptors, specific DC subsets and DC activators that can further enhance the efficacy of vaccines by promoting effector T cell infiltration and retention in tumors and their actions against tumors. Supplementing these areas of research with additional strategies that can counteract tumor immune evasion mechanisms is also expected to enhance the efficacy of such therapeutic vaccines against cancers. After more than a decade of study, we have concluded that antigen targeting to DCs via CD40 to evoke cellular responses is more efficient than targeting antigens to the same types of DCs via eleven other DC surface receptors tested. In recent work, we have further demonstrated that a prototype vaccine (anti-CD40-HPV16.E6/7, a recombinant fusion protein of anti-human CD40 and HPV16.E6/7 protein) for HPV16-associated cancers can efficiently activate HPV16.E6/7-specific T cells, particularly CD8 T cells, from the blood of HPV16 head-and-neck cancer patients. Moreover, anti-CD40-HPV16.E6/7 plus poly(I:C) can mount potent therapeutic immunity against TC-1 tumor expressing HPV16.E6/7 protein in human CD40 transgenic mice. In this manuscript, we thus highlight our recent findings for the development of novel CD40 targeting immunotherapeutic vaccines for HPV16-associated malignancies. In addition, we further discuss several of key questions that still remain to be addressed for enhancing therapeutic immunity elicited by our prototype vaccine against HPV16-associated malignancies.
树突状细胞(DCs)是主要的抗原呈递细胞,能够有效地启动和激活细胞免疫反应。因此,将抗原递送至DCs被认为是一种有前景的策略,有望使我们在患者中激发针对癌症的T细胞介导的治疗性免疫。然而,成功开发此类能够靶向DCs的癌症疫苗需要解决一系列突出问题。这些问题包括正确选择哪些DC表面受体、特定的DC亚群以及DC激活剂,它们可以通过促进效应T细胞浸润和在肿瘤中的滞留及其对肿瘤的作用来进一步提高疫苗的疗效。用能够对抗肿瘤免疫逃逸机制的其他策略补充这些研究领域,也有望提高此类治疗性癌症疫苗的疗效。经过十多年的研究,我们得出结论,通过CD40将抗原靶向DCs以引发细胞反应比通过测试的其他十一种DC表面受体将抗原靶向相同类型的DCs更有效。在最近的工作中,我们进一步证明,一种用于HPV16相关癌症的原型疫苗(抗CD40-HPV16.E6/7,抗人CD40和HPV16.E6/7蛋白的重组融合蛋白)可以有效地激活来自HPV16头颈癌患者血液中的HPV16.E6/7特异性T细胞,特别是CD8 T细胞。此外,抗CD40-HPV16.E6/7加聚肌胞(poly(I:C))可以在人CD40转基因小鼠中对表达HPV16.E6/7蛋白的TC-1肿瘤产生强大的治疗性免疫。因此,在本手稿中,我们重点介绍了我们最近在开发用于HPV16相关恶性肿瘤的新型CD40靶向免疫治疗疫苗方面的发现。此外,我们进一步讨论了几个关键问题,这些问题仍有待解决,以增强我们的原型疫苗针对HPV16相关恶性肿瘤引发的治疗性免疫。
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