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Costimulation enhances the active immunotherapy effect of recombinant anticancer vaccines.共刺激增强重组抗癌疫苗的主动免疫治疗效果。
Cancer Res. 1996 Jun 15;56(12):2832-6.
2
IL-12 is an effective adjuvant to recombinant vaccinia virus-based tumor vaccines: enhancement by simultaneous B7-1 expression.白细胞介素-12是基于重组痘苗病毒的肿瘤疫苗的有效佐剂:通过同时表达B7-1增强效果。
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J Immunol. 1995 May 15;154(10):5282-92.
4
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Proc Natl Acad Sci U S A. 1997 Apr 1;94(7):3183-8. doi: 10.1073/pnas.94.7.3183.

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本文引用的文献

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IL-12 is an effective adjuvant to recombinant vaccinia virus-based tumor vaccines: enhancement by simultaneous B7-1 expression.白细胞介素-12是基于重组痘苗病毒的肿瘤疫苗的有效佐剂:通过同时表达B7-1增强效果。
J Immunol. 1996 May 1;156(9):3357-65.
2
B7-1 but not B7-2 efficiently costimulates CD8+ T lymphocytes in the P815 tumor system in vitro.在体外P815肿瘤系统中,B7-1而非B7-2能有效地共刺激CD8 + T淋巴细胞。
J Immunol. 1996 Jan 15;156(2):465-72.
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Tumor antigens recognized by T lymphocytes.被T淋巴细胞识别的肿瘤抗原。
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IL-2 enhances the function of recombinant poxvirus-based vaccines in the treatment of established pulmonary metastases.白细胞介素-2可增强基于重组痘病毒的疫苗在治疗已形成的肺转移瘤中的功能。
J Immunol. 1995 May 15;154(10):5282-92.
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Active immunotherapy of cancer with a nonreplicating recombinant fowlpox virus encoding a model tumor-associated antigen.用编码一种典型肿瘤相关抗原的非复制重组鸡痘病毒对癌症进行主动免疫治疗。
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Tumor rejection after direct costimulation of CD8+ T cells by B7-transfected melanoma cells.通过B7转染的黑色素瘤细胞直接共刺激CD8 + T细胞后的肿瘤排斥反应。
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CD28 costimulation can promote T cell survival by enhancing the expression of Bcl-XL.CD28共刺激可通过增强Bcl-XL的表达来促进T细胞存活。
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Selection of recombinant vaccinia viruses on the basis of plaque formation.基于噬斑形成对重组痘苗病毒进行筛选。
Gene. 1995 Jun 9;158(2):157-62. doi: 10.1016/0378-1119(95)00149-z.
10
Admixture of a recombinant vaccinia virus containing the gene for the costimulatory molecule B7 and a recombinant vaccinia virus containing a tumor-associated antigen gene results in enhanced specific T-cell responses and antitumor immunity.包含共刺激分子B7基因的重组痘苗病毒与包含肿瘤相关抗原基因的重组痘苗病毒混合,可增强特异性T细胞反应和抗肿瘤免疫力。
Cancer Res. 1995 Aug 15;55(16):3598-603.

共刺激增强重组抗癌疫苗的主动免疫治疗效果。

Costimulation enhances the active immunotherapy effect of recombinant anticancer vaccines.

作者信息

Chamberlain R S, Carroll M W, Bronte V, Hwu P, Warren S, Yang J C, Nishimura M, Moss B, Rosenberg S A, Restifo N P

机构信息

Surgery Branch, National Cancer Institute, NIH, Bethesda, Maryland 20892, USA.

出版信息

Cancer Res. 1996 Jun 15;56(12):2832-6.

PMID:8665522
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2248455/
Abstract

Activation of T lymphocytes in the absence of a costimulatory signal can result in anergy or apoptotic cell death. Two molecules capable of providing a costimulatory signal, B7-1 (CD80) and B7-2 (CD86), have been shown to augment the immunogenicity of whole-tumor cell vaccines. To explore a potential role for costimulation in the design of recombinant anticancer vaccines, we used lacZ-transduced CT26 as an experimental tumor and beta-galactosidase (beta-gal) as the model tumor antigen. Attempts to augment the function of a recombinant vaccinia virus (rVV) expressing beta-gal by admixture with rVV expressing murine B7-1 were unsuccessful. However, a double recombinant vaccinia virus engineered to express both B7-1 and the model antigen beta-gal was capable of significantly reducing the number of pulmonary metastases when administered to mice bearing tumors established for 3 or 6 days. Most important, the double recombinant vaccinia virus prolonged the survival of tumor-bearing mice. These effects were antigen specific. The related costimulatory molecule B7-2 was found to have a similar, although less impressive enhancing effect on the function of a rVV expressing beta-gal. Thus, the addition of B7-1 and, to a lesser extent, B7-2 to a rVV encoding a model antigen significantly enhanced the therapeutic antitumor effects of these poxvirus-based, therapeutic anticancer vaccines.

摘要

在缺乏共刺激信号的情况下,T淋巴细胞的激活可导致无反应性或凋亡性细胞死亡。两种能够提供共刺激信号的分子,B7-1(CD80)和B7-2(CD86),已被证明可增强全肿瘤细胞疫苗的免疫原性。为了探索共刺激在重组抗癌疫苗设计中的潜在作用,我们使用了用lacZ转导的CT26作为实验性肿瘤,并将β-半乳糖苷酶(β-gal)作为模型肿瘤抗原。试图通过与表达小鼠B7-1的重组痘苗病毒(rVV)混合来增强表达β-gal的重组痘苗病毒的功能未成功。然而,一种经过基因工程改造以同时表达B7-1和模型抗原β-gal的双重组痘苗病毒,在给已建立肿瘤3天或6天的小鼠接种时,能够显著减少肺转移灶的数量。最重要的是,双重组痘苗病毒延长了荷瘤小鼠的存活时间。这些效应具有抗原特异性。发现相关的共刺激分子B7-2对表达β-gal的重组痘苗病毒的功能也有类似的增强作用,尽管效果不太显著。因此,将B7-1以及程度稍轻的B7-2添加到编码模型抗原的重组痘苗病毒中,可显著增强这些基于痘病毒的治疗性抗癌疫苗的治疗性抗肿瘤效果。