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Crosstalk between immune cell and oncolytic vaccinia therapy enhances tumor trafficking and antitumor effects

机译:免疫细胞与溶瘤牛痘疗法之间的串扰增强了肿瘤的运输和抗肿瘤作用

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The combination of an oncolytic virus, that directly destroys tumor cells and mediates an acute immune response, with an immune cell therapy, capable of further enlisting and enhancing the host immune response, has the potential to create a potent therapeutic effect. We have previously developed several strategies for optimizing the delivery of oncolytic vaccinia virus vectors to their tumor targets, including the use of immune cell-based carrier vehicles and the incorporation of mutations that increase production of the enveloped form of vaccinia (extracellular enveloped viral (EEV)) that is better adapted to spread within a host. Here, we initially combine these approaches to create a novel therapeutic, consisting of an immune cell (cytokine-induced killer, CIK) preloaded with an oncolytic virus that is EEV enhanced. This resulted in direct interaction between the viral and immune cell components with each assisting the other in directing the therapy to the tumor and so enhancing the antitumor effects. This effect could be further improved through CCL5 expression from the virus. The resulting multicomponent therapy displays the ability for synergistic crosstalk between components, so significantly enhancing tumor trafficking and antitumor effects.
机译:直接破坏肿瘤细胞并介导急性免疫反应的溶瘤病毒与能够进一步征服和增强宿主免疫反应的免疫细胞疗法相结合,有可能产生有效的治疗效果。我们之前已经开发了几种策略来优化溶瘤牛痘病毒载体向其肿瘤靶标的传递,包括使用基于免疫细胞的载体和整合突变以增加包膜形式的牛痘(细胞外包膜病毒(EEV) ))更适合在主机内传播。在这里,我们首先结合这些方法来创建一种新型疗法,该疗法由预载有EEV增强的溶瘤病毒的免疫细胞(细胞因子诱导的杀手,CIK)组成。这导致病毒和免疫细胞成分之间的直接相互作用,彼此之间互相协助,将治疗导向肿瘤,从而增强了抗肿瘤作用。通过从病毒中表达CCL5可以进一步改善这种效果。最终的多组分疗法显示出组分之间协同串扰的能力,因此显着增强了肿瘤的转运和抗肿瘤作用。

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