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一种合理设计的表皮生长因子受体疫苗的免疫原性及抗肿瘤疗效

The Immunogenicity and Anti-Tumor Efficacy of a Rationally Designed EGFR Vaccine.

作者信息

Cheng Chao, Deng Li, Li Rongxiu

机构信息

State Key Laboratory of Microbial Metabolism and School of Life Sciences & Biotechnology, Shanghai Jiao Tong University, Shanghai, China.

Shanghai HyCharm Inc, Shanghai, China.

出版信息

Cell Physiol Biochem. 2018;46(1):46-56. doi: 10.1159/000488408. Epub 2018 Mar 20.

Abstract

BACKGROUND/AIMS: The abnormally activated EGFR promotes tumor growth, invasion and metastasis. Current therapeutics targeting EGFR have markedly improved the clinical outcome, but they are limited in use due to transient efficacy, frequent administration, high cost and significant toxicity.

METHODS

We rationally designed a multiepitope immunogen against EGFR, named as DEGFRm. The immunogen is composed of an epitope peptide (EGFR265-283) and the extracellular domain III (EGFR334-505) of mouse EGFR. EGFR265-283 is grafted onto the translocation domain of diphtheria toxin (DTT), and EGFR334-505 is fused to C-terminal of DTT. Next, the immunogenicity and anti-tumor efficacies of DEGFRm vaccine were examined in mouse tumor models.

RESULTS

When formulated with Alum and CpG, DEGFRm vaccine elicits Th 1 immune responses and inhibits tumor growth in both prophylactic and therapeutic mouse tumor models. Moreover, the tumor microvasculature is markedly reduced and the tumor infiltration of CD8+ T lymphocytes is greatly enhanced.

CONCLUSIONS

These data suggest that active immunization with DEGFRm vaccine is a promising strategy for therapy of various EGFR+ cancers.

摘要

背景/目的:异常激活的表皮生长因子受体(EGFR)促进肿瘤生长、侵袭和转移。目前针对EGFR的治疗方法显著改善了临床疗效,但由于疗效短暂、给药频繁、成本高昂及毒性显著,其应用受到限制。

方法

我们合理设计了一种针对EGFR的多表位免疫原,命名为DEGFRm。该免疫原由一个表位肽(EGFR265-283)和小鼠EGFR的细胞外结构域III(EGFR334-505)组成。EGFR265-283被嫁接到白喉毒素(DTT)的易位结构域上,EGFR334-505与DTT的C末端融合。接下来,在小鼠肿瘤模型中检测DEGFRm疫苗的免疫原性和抗肿瘤疗效。

结果

与明矾和CpG一起配制时,DEGFRm疫苗在预防性和治疗性小鼠肿瘤模型中均能引发Th1免疫反应并抑制肿瘤生长。此外,肿瘤微血管明显减少,CD8+T淋巴细胞的肿瘤浸润显著增强。

结论

这些数据表明,用DEGFRm疫苗进行主动免疫是治疗各种EGFR+癌症的一种有前景的策略。

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