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抗癌症的DNA融合基因疫苗:从实验室到临床

DNA fusion gene vaccines against cancer: from the laboratory to the clinic.

作者信息

Stevenson Freda K, Rice Jason, Ottensmeier Christian H, Thirdborough Stephen M, Zhu Delin

机构信息

Molecular Immunology Group, Tenovus Laboratory, Cancer Sciences Division, Southampton University Hospitals, Southampton, UK.

出版信息

Immunol Rev. 2004 Jun;199:156-80. doi: 10.1111/j.0105-2896.2004.00145.x.

Abstract

Vaccination against target antigens expressed by cancer cells has now become a realistic goal. DNA vaccines provide a direct link between identification of genetic markers in tumors and vaccine formulation. Simplicity of manufacture facilitates construction of vaccines against disease subsets or even for individual patients. To engage an immune system that exists to fight pathogens, we have developed fusion gene vaccines encoding tumor antigens fused to pathogen-derived sequences. This strategy activates high levels of T-cell help, the key to induction and maintenance of effective immunity. We have dissected the immunogenic tetanus toxin to obtain specific sequences able to activate antibody, CD4+, or CD8+ T cells to attack selected fused tumor antigens. Principles established in preclinical models are now being tested in patients. So far, objective immune responses against idiotypic antigen of neoplastic B cells have been observed in patients with B-cell malignancies and in normal transplant donors. These responses provide a platform for testing physical methods to improve DNA delivery and strategies to boost responses. For cancer, demands are high, because vaccines have to activate powerful immunity against weak antigens, often in a setting of immune damage or tolerance. Vaccination strategies against cancer and against microbes are sharing knowledge and technology for mutual benefit.

摘要

针对癌细胞表达的靶抗原进行疫苗接种现已成为一个现实的目标。DNA疫苗在肿瘤中遗传标志物的识别与疫苗配方之间提供了直接联系。生产的简易性便于构建针对疾病亚群甚至个体患者的疫苗。为了激活用于对抗病原体的免疫系统,我们开发了融合基因疫苗,其编码与病原体衍生序列融合的肿瘤抗原。这一策略可激活高水平的T细胞辅助,而T细胞辅助是诱导和维持有效免疫的关键。我们剖析了具有免疫原性的破伤风毒素,以获得能够激活抗体、CD4 +或CD8 + T细胞来攻击选定融合肿瘤抗原的特定序列。临床前模型中确立的原则目前正在患者身上进行测试。到目前为止,在B细胞恶性肿瘤患者和正常移植供体中已观察到针对肿瘤性B细胞独特型抗原的客观免疫反应。这些反应为测试改善DNA递送的物理方法和增强反应的策略提供了一个平台。对于癌症来说,要求很高,因为疫苗通常必须在免疫损伤或耐受的情况下激活针对弱抗原的强大免疫力。针对癌症和针对微生物的疫苗接种策略正在共享知识和技术以实现互利。

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