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EB 病毒阳性肿瘤被表达 hGM-CSF 和 LMP2A 的 rBCG 抑制。

EB virus-positive tumors are inhibited by rBCG expressing hGM-CSF and LMP2A.

机构信息

School of Mental Health, Jining Medical University, Shandong, China.

School of Basic Medical, Jining Medical University, Shandong, China.

出版信息

Hum Vaccin Immunother. 2020 Mar 3;16(3):654-663. doi: 10.1080/21645515.2019.1670593. Epub 2019 Oct 29.

Abstract

For the development of safe and effective EBV (Epstein-Barr virus) vaccines, the Ag85A signal peptide from H37Rv was used to construct a recombinant secretory BCG (Bacillus Chalmette-Guérin) plasmid. The Ag85A gene, fused to the EBV LMP2A (latent membrane protein) and hGM-CSF (human granulocyte/macrophage colony-stimulating factor) genes, was inserted into the pMV261 vector (secretory BCG plasmid). The expression levels of the hGM-CSF and LMP2A proteins in rBCG (recombinant BCG) were measured by Western blot analysis. Humoral immunity, cellular immunity, and antitumor effects were determined by a series of experiments. The recombinant pMVGCA plasmid effectively expressed GCA (hGM-CSF and LMP2A fusion protein) in BCG after transformation, and the rBCG proteins were recognized by antibodies against hGM-CSF and LMP2A. Six weeks after immunization, the maximum dose of rBCG resulted in antibody titers of 1:19,800 (hGM-CSF antibody) and 1:21,800 (LMP2A antibody). When the effector:target ratio was 40:1, specific lysis was maximal and approximately two times stronger than that in mice immunized with the control. Tumorigenicity was lower in the rBCG treatment group, with a tumor inhibition rate of 0.81 ± 0.09 compared with the control groups. EB virus-positive tumors are inhibited by rBCG expressing an hGM-CSF and LMP2A fusion protein.

摘要

为了开发安全有效的 EBV(Epstein-Barr 病毒)疫苗,使用 H37Rv 的 Ag85A 信号肽构建了重组分泌型 BCG(卡介苗)质粒。Ag85A 基因与 EBV LMP2A(潜伏膜蛋白)和 hGM-CSF(人粒细胞/巨噬细胞集落刺激因子)基因融合,插入 pMV261 载体(分泌型 BCG 质粒)中。通过 Western blot 分析测量 rBCG(重组 BCG)中 hGM-CSF 和 LMP2A 蛋白的表达水平。通过一系列实验确定体液免疫、细胞免疫和抗肿瘤作用。重组 pMVGCA 质粒在转化为 BCG 后有效表达 GCA(hGM-CSF 和 LMP2A 融合蛋白),rBCG 蛋白被针对 hGM-CSF 和 LMP2A 的抗体识别。免疫后 6 周,rBCG 的最大剂量导致 hGM-CSF 抗体的抗体滴度为 1:19,800,LMP2A 抗体的抗体滴度为 1:21,800。当效应物:靶标比为 40:1 时,特异性裂解最大,比对照免疫的小鼠强约两倍。rBCG 治疗组的致瘤性较低,与对照组相比,肿瘤抑制率为 0.81±0.09。表达 hGM-CSF 和 LMP2A 融合蛋白的 rBCG 抑制 EBV 阳性肿瘤。

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本文引用的文献

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