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In vitro and ex vivo evaluation of a multi-epitope heparinase vaccine for various malignancies

机译:多表位肝素酶疫苗在各种恶性肿瘤中的体外和离体评估

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摘要

Previous studies have indicated that heparanase (Hpa) might represent a candidate universal tumor-associated antigen. However, vaccine therapy targeting only one cytotoxic T lymphocyte (CTL) epitope is suboptimal in preventing cancer. In the present study, we designed heparanase multi-epitope vaccines to increase the immune response to standard single heparanase epitopes. The results showed that multi-epitope vaccines Hpa525 + 277 + 405 + 16 and Hpa8 + 310 + 315 + 363 induced higher Hpa-specific lysis of various cancer cells from different tissues in a HLA-A2-restricted and heparanase-specific manner compared with the single epitope vaccines Hpa525, Hpa277, Hpa405, Hpa16, Hpa8, Hpa310, Hpa315 and Hpa363, both in vitro and ex vivo. Heparanase multi-epitope vaccines not only induced the heparanase-specific CTL to lyse tumor cells but also increased CTL secretion of interferon-γ. However, these heparanase-specific CTL did not lyse heparanase-expressing autologous lymphocytes and dendritic cells, which confirms the safety of these multi-epitope vaccines. Therefore, the present study provides theoretical evidence for the use of heparanase multi-epitope vaccines for clinical application.
机译:先前的研究表明,乙酰肝素酶(Hpa)可能代表一种候选的普遍性肿瘤相关抗原。但是,仅针对一种细胞毒性T淋巴细胞(CTL)表位的疫苗治疗在预防癌症方面不理想。在本研究中,我们设计了乙酰肝素酶多表位疫苗,以增加对标准单一乙酰肝素酶表位的免疫反应。结果显示,多表位疫苗Hpa525 + 277 + 405 + 16和Hpa8 + 310 + 315 + 363与HLA-A2限制性和乙酰肝素酶特异性方式相比,诱导了来自不同组织的各种癌细胞更高的Hpa特异性裂解。体外和离体的单一表位疫苗Hpa525,Hpa277,Hpa405,Hpa16,Hpa8,Hpa310,Hpa315和Hpa363。乙酰肝素酶多表位疫苗不仅诱导了乙酰肝素酶特异性CTL裂解肿瘤细胞,而且还增加了干扰素-γ的CTL分泌。但是,这些乙酰肝素酶特异性CTL不能裂解表达乙酰肝素酶的自体淋巴细胞和树突状细胞,这证实了这些多表位疫苗的安全性。因此,本研究为肝素酶多表位疫苗在临床上的应用提供了理论依据。

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