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Combining synthetic carbohydrate vaccines with cancer cell glycoengineering for effective cancer immunotherapy

机译:将合成的碳水化合物疫苗与癌细胞甘油合并有效癌症免疫疗法

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摘要

Tumor-associated carbohydrate antigens (TACAs) are useful targets for the development of cancer vaccines or immunotherapies. However, a major obstacle in this application of TACAs is their poor immunogenicity. To overcome the problem, a new immunotherapeutic strategy combining synthetic vaccines made of artificial TACA derivatives and metabolic glycoengineering of cancer cells to express the artificial TACA derivatives was explored. Using a murine leukemia model FBL3 with GM3 antigen as the target, it was shown that artificial GM3 N-phenylacetyl derivative (GM3NPhAc) elicited robust antigen-specific T cell-dependent immunity and that N-phenylacetyl-D-mannosamine (ManNPhAc) as the biosynthetic precursor of GM3NPhAc selectively glycoengineered cancer cells to express GM3NPhAc both in vitro and in vivo. It was also demonstrated that GM3NPhAc-specific antisera and antibodies mediated strong cytotoxicity to ManNPhAc-treated FBL3 cell. Furthermore, vaccination with a conjugate vaccine made of GM3NPhAc followed by ManNPhAc treatment could significantly suppress tumor growth and prolong the survival of tumor-bearing mouse. These results have proved the feasibility of the new cancer immunotherapeutic strategy, as well as its efficacy to cure cancer, which is of general significance.
机译:肿瘤相关的碳水化合物抗原(TACA)是用于癌症疫苗或免疫疗法的显影的有用靶标。然而,在这种塔可癌应用中的主要障碍是它们差的免疫原性。为了克服问题,探讨了一种新的免疫治疗策略,将由人工炸玉米饼衍生物和癌细胞代谢甘油化的合成疫苗结合以表达人工淋巴衍生物。使用鼠白血病模型FBL3与GM3抗原作为靶标,显示人工GM3正苯基乙酰基衍生物(GM3Nphac)引发了稳健的抗原特异性T细胞依赖性免疫,并将N-苯基乙酰-D-甘露那胺(Mannphac)为GM3Nphac的生物合成前体在体外和体内选择性地甘油癌细胞进行糖精癌细胞表达GM3Nphac。还表明GM3Nphac特异性抗血清和抗体介导对甘露治疗的FBL3细胞的强细胞毒性。此外,用由GM3Nphac的缀合物疫苗接种疫苗接种,随后是Mannphac治疗可以显着抑制肿瘤生长并延长肿瘤小鼠的存活。这些结果证明了新的癌症免疫治疗策略的可行性,以及其治疗癌症的疗效,这是一般意义。

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