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针对表达模型抗原的大鼠神经胶质瘤的 DNA 疫苗接种后不完全肿瘤控制。

Incomplete tumour control following DNA vaccination against rat gliomas expressing a model antigen.

机构信息

Department of Neurosurgery, University of Schleswig-Holstein, Campus Kiel, Kiel, Germany.

出版信息

Acta Neurochir (Wien). 2013 Jan;155(1):51-8; discussion 59. doi: 10.1007/s00701-012-1526-7. Epub 2012 Nov 8.

Abstract

BACKGROUND

Vaccination against tumour-associated antigens is one approach to elicit anti-tumour responses. We investigated the effect of polynucleotide (DNA) vaccination using a model antigen (E. coli lacZ) in a syngeneic gliosarcoma model (9L).

METHODS

Fisher 344 rats were vaccinated thrice by intramuscular injection of a lacZ-encoding or a control plasmid in weekly intervals. One week after the last vaccination, lacZ-expressing 9L cells were implanted into the striatum.

RESULTS

After 3 weeks, in lacZ-vaccinated animals the tumours were significantly smaller than in control-vaccinated animals. In cytotoxic T cell assays lysis rates of >50 % could only be observed in a few of the lacZ-vaccinated animals. This response was directed against lacZ-expressing and parental 9L cells but not against syngeneic MADB 106 adenocarcinoma cells. In Elispot assays interferon-γ production was observed upon stimulation with 9LlacZ and 9L wild-type but not MADB 106 cells. This response was higher for lacZ-immunized animals. All animals revealed dense infiltrates with CD8+ lymphocytes and, to a lesser extent, with NK cells. CD25-staining indicated cells possibly associated with the maintenance of peripheral tolerance to self-antigens. All tumours were densely infiltrated by microglia consisting mostly of ramified cells. Only focal accumulation of macrophage-like cells expressing ED1, a marker for phagocytic activity, was observed.

CONCLUSION

Prophylactic DNA vaccination resulted in effective but incomplete suppression of brain tumour formation. Mechanisms other than cytotoxic T cell responses as measured in the generally used in vitro assays appear to play a role in tumour suppression.

摘要

背景

针对肿瘤相关抗原的疫苗接种是引发抗肿瘤反应的一种方法。我们在同基因神经胶质瘤肉瘤模型(9L)中研究了使用模型抗原(大肠杆菌 lacZ)的多核苷酸(DNA)疫苗接种的效果。

方法

Fisher 344 大鼠通过肌肉内注射每周间隔一次的 lacZ 编码或对照质粒进行了三次疫苗接种。最后一次接种后一周,将表达 lacZ 的 9L 细胞植入纹状体。

结果

3 周后,在 lacZ 疫苗接种的动物中,肿瘤明显小于对照组。在细胞毒性 T 细胞测定中,仅在少数 lacZ 疫苗接种的动物中观察到 >50%的裂解率。这种反应针对表达 lacZ 的和亲本 9L 细胞,但不针对同基因 MADB 106 腺癌细胞。在 Elispot 测定中,在用 9LlacZ 和 9L 野生型但不用 MADB 106 细胞刺激时观察到干扰素-γ的产生。这种反应在 lacZ 免疫的动物中更高。所有动物均显示 CD8+淋巴细胞浸润密集,其次是 NK 细胞。CD25 染色表明存在可能与自身抗原外周耐受维持相关的细胞。所有肿瘤均由主要为分枝状细胞的小胶质细胞密集浸润。仅观察到表达 ED1 的巨噬细胞样细胞的局灶性积聚,ED1 是吞噬活性的标志物。

结论

预防性 DNA 疫苗接种导致脑肿瘤形成的有效但不完全抑制。在通常使用的体外测定中测量的细胞毒性 T 细胞反应以外的机制似乎在肿瘤抑制中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11cc/3535398/01e8b7122477/701_2012_1526_Fig1_HTML.jpg

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