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迈向优化的基于碳水化合物的抗癌疫苗:表位聚类、载体结构和佐剂均影响小鼠对Lewis(y)缀合物的抗体反应。

Toward optimized carbohydrate-based anticancer vaccines: epitope clustering, carrier structure, and adjuvant all influence antibody responses to Lewis(y) conjugates in mice.

作者信息

Kudryashov V, Glunz P W, Williams L J, Hintermann S, Danishefsky S J, Lloyd K O

机构信息

Tumor Antigen Laboratory, Immunology Program and Bioorganic Chemistry Laboratory, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, NY 10021, USA.

出版信息

Proc Natl Acad Sci U S A. 2001 Mar 13;98(6):3264-9. doi: 10.1073/pnas.051623598.

Abstract

The feasibility of using carbohydrate-based vaccines for the immunotherapy of cancer is being actively explored at the present time. Although a number of clinical trials have already been conducted with glycoconjugate vaccines, the optimal design and composition of the vaccines has yet to be determined. Among the candidate antigens being examined is Lewis(y) (Le(y)), a blood group-related antigen that is overexpressed on the majority of human carcinomas. Using Le(y) as a model for specificity, we have examined the role of epitope clustering, carrier structure, and adjuvant on the immunogenicity of Le(y) conjugates in mice. A glycolipopeptide containing a cluster of three contiguous Le(y)-serine epitopes and the Pam(3)Cys immunostimulating moiety was found to be superior to a similar construct containing only one Le(y)-serine epitope in eliciting antitumor cell antibodies. Because only IgM antibodies were produced by this vaccine, the effect on immunogenicity of coupling the glycopeptide to keyhole limpet hemocyanin was examined; although both IgM and IgG antibodies were formed, the antibodies reacted only with the immunizing structure. Reexamination of the clustered Le(y)-serine Pam(3)Cys conjugate with the adjuvant QS-21 resulted in the identification of both IgG and IgM antibodies reacting with tumor cells, thus demonstrating the feasibility of an entirely synthetic carbohydrate-based anticancer vaccine in an animal model.

摘要

目前正在积极探索使用基于碳水化合物的疫苗进行癌症免疫治疗的可行性。尽管已经对糖缀合物疫苗进行了多项临床试验,但疫苗的最佳设计和组成尚未确定。正在研究的候选抗原中包括Lewis(y)(Le(y)),一种在大多数人类癌症中过度表达的血型相关抗原。以Le(y)作为特异性模型,我们研究了表位聚类、载体结构和佐剂对Le(y)缀合物在小鼠体内免疫原性的作用。发现含有三个连续Le(y)-丝氨酸表位簇和Pam(3)Cys免疫刺激部分的糖脂肽在诱导抗肿瘤细胞抗体方面优于仅含有一个Le(y)-丝氨酸表位的类似构建体。由于该疫苗仅产生IgM抗体,因此研究了将糖肽与钥孔戚血蓝蛋白偶联对免疫原性的影响;虽然形成了IgM和IgG抗体,但这些抗体仅与免疫结构发生反应。用佐剂QS-21对聚集的Le(y)-丝氨酸Pam(3)Cys缀合物进行重新检测,结果鉴定出与肿瘤细胞发生反应的IgG和IgM抗体,从而证明了在动物模型中完全合成的基于碳水化合物的抗癌疫苗的可行性。

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