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基于互补决定区3(CDR3)的融合疫苗进行基因免疫可在淋巴瘤小鼠模型中提供保护并实现长期无瘤存活。

Genetic immunization with CDR3-based fusion vaccine confers protection and long-term tumor-free survival in a mouse model of lymphoma.

作者信息

Iurescia Sandra, Fioretti Daniela, Pierimarchi Pasquale, Signori Emanuela, Zonfrillo Manuela, Tonon Giancarlo, Fazio Vito M, Rinaldi Monica

机构信息

Institute of Neurobiology and Molecular Medicine, Department of Medicine, National Research Council (CNR), Via Fosso del Cavaliere 100, 00133 Rome, Italy.

出版信息

J Biomed Biotechnol. 2010;2010:316069. doi: 10.1155/2010/316069. Epub 2010 Apr 27.

Abstract

Therapeutic vaccination against idiotype is a promising strategy for immunotherapy of B-cell malignancies. We have previously shown that CDR3-based DNA immunization can induce immune response against lymphoma and explored this strategy to provide protection in a murine B-cell lymphoma model. Here we performed vaccination employing as immunogen a naked DNA fusion product. The DNA vaccine was generated following fusion of a sequence derived from tetanus toxin fragment C to the V(H)CDR3(109-116) epitope. Induction of tumor-specific immunity as well as ability to inhibit growth of the aggressive 38C13 lymphoma and to prolong survival of vaccinated mice has been tested. We determined that DNA fusion vaccine induced immune response, elicited a strong protective antitumor immunity, and ensured almost complete long-term tumor-free survival of vaccinated mice. Our results show that CDR3-based DNA fusion vaccines hold promise for vaccination against lymphoma.

摘要

抗独特型治疗性疫苗接种是B细胞恶性肿瘤免疫治疗的一种有前景的策略。我们之前已经表明,基于互补决定区3(CDR3)的DNA免疫接种可诱导针对淋巴瘤的免疫反应,并探索了该策略以在小鼠B细胞淋巴瘤模型中提供保护。在此,我们使用一种裸DNA融合产物作为免疫原进行疫苗接种。该DNA疫苗是通过将源自破伤风毒素片段C的序列与V(H)CDR3(109 - 116)表位融合后产生的。我们测试了其诱导肿瘤特异性免疫的能力、抑制侵袭性38C13淋巴瘤生长的能力以及延长接种疫苗小鼠生存期的能力。我们确定,DNA融合疫苗可诱导免疫反应,引发强大的保护性抗肿瘤免疫,并确保接种疫苗的小鼠几乎完全长期无瘤生存。我们的结果表明,基于CDR3的DNA融合疫苗在淋巴瘤疫苗接种方面具有前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8690/2860581/ec9d7f58ec43/JBB2010-316069.001.jpg

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