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利用 DNA 诱导的免疫反应来改进癌症疫苗。

Harnessing DNA-induced immune responses for improving cancer vaccines.

机构信息

Laboratory of Gene Immunotherapy, Fundación Ciencia & Vida, Santiago, Chile.

出版信息

Hum Vaccin Immunother. 2012 Nov 1;8(11):1682-93. doi: 10.4161/hv.22345. Epub 2012 Oct 30.

Abstract

DNA vaccines have emerged as an attractive strategy to promote protective cellular and humoral immunity against the encoded antigen. DNA vaccines are easy to generate, inexpensive to produce and purify at large-scale, highly stable and safe. In addition, plasmids used for DNA vaccines act as powerful "danger signals" by stimulating several DNA-sensing innate immune receptors that promote the induction of protective adaptive immunity. The induction of tumor-specific immune responses represents a major challenge for DNA vaccines because most of tumor-associated antigens are normal non-mutated self-antigens. As a consequence, induction of potentially self-reactive T cell responses against such poorly immunogenic antigens is controlled by mechanisms of central and peripheral tolerance as well as tumor-induced immunosuppression. Although several DNA vaccines against cancer have reached clinical testing, disappointing results have been observed. Therefore, the development of new adjuvants that strongly stimulate the induction of antitumor T cell immunity and counteract immune-suppressive regulation is an attractive approach to enhance the potency of DNA vaccines and overcome tumor-associated tolerance. Understanding the DNA-sensing signaling pathways of innate immunity that mediate the induction of T cell responses elicited by DNA vaccines represents a unique opportunity to develop novel adjuvants that enhance vaccine potency. The advance of DNA adjuvants needs to be complemented with the development of potent delivery systems, in order to step toward successful clinical application. Here, we briefly discuss recent evidence showing how to harness DNA-induced immune response to improve the potency of cancer vaccines and counteract tumor-associated tolerance.

摘要

DNA 疫苗作为一种有吸引力的策略,已被广泛用于促进针对编码抗原的保护性细胞和体液免疫。DNA 疫苗易于制备,生产成本低,可大规模、高效、稳定、安全地生产和纯化。此外,用于 DNA 疫苗的质粒通过刺激几种 DNA 感应先天免疫受体,充当强大的“危险信号”,从而促进保护性适应性免疫的诱导。肿瘤特异性免疫反应的诱导是 DNA 疫苗的一个主要挑战,因为大多数肿瘤相关抗原是正常的非突变自身抗原。因此,对这些免疫原性差的抗原诱导潜在的自身反应性 T 细胞反应受到中枢和外周耐受以及肿瘤诱导的免疫抑制机制的控制。尽管有几种针对癌症的 DNA 疫苗已进入临床测试,但观察到的结果令人失望。因此,开发能够强烈刺激抗肿瘤 T 细胞免疫诱导并抵消免疫抑制调节的新型佐剂,是增强 DNA 疫苗效力和克服肿瘤相关耐受的一种有吸引力的方法。了解先天免疫的 DNA 感应信号通路,这些通路介导 DNA 疫苗诱导的 T 细胞反应,为开发增强疫苗效力的新型佐剂提供了独特的机会。DNA 佐剂的进步需要与有效的递药系统的开发相结合,以迈向成功的临床应用。在这里,我们简要讨论了最近的证据,这些证据表明如何利用 DNA 诱导的免疫反应来提高癌症疫苗的效力并抵抗肿瘤相关的耐受。

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