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Simultaneous delivery of cytotoxic and biologic therapeutics using nanophotoactivatable liposomes enhances treatment efficacy in a mouse model of pancreatic cancer

机译:使用纳米可光活化脂质体同时递送细胞毒性和生物疗法可增强胰腺癌小鼠模型的治疗功效

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摘要

A lack of intracellular delivery systems has limited the use of biologics such as monoclonal antibodies (mAb) that abrogate molecular signaling pathways activated to promote escape from cancer treatment. We hypothesized that intracellular co-delivery of the photocytotoxic chromophore benzoporphyrin derivative monoacid A (BPD) and the anti-VEGF mAb bevacizumab in a nanophotoactivatable liposome (nanoPAL) might enhance the efficacy of photodynamic therapy (PDT) combined with suppression of VEGF-mediated signaling pathways. As a proof-of-concept we found that nanoPAL-PDT induced enhanced extra- and intracellular bevacizumab delivery and enhanced acute cytotoxicity in vitro. In an in vivo subcutaneous mouse model of pancreatic ductal adenocarcinoma, nanoPAL-PDT achieved significantly enhanced tumor reduction. We attribute this to the optimal incorporation of insoluble BPD into the lipid bilayer, enhancing photocytotoxicity, and the simultaneous spatiotemporal delivery of bevacizumab, ensuring efficient neutralization of the rapid but transient burst of VEGF following PDT.
机译:细胞内传递系统的缺乏限制了诸如单克隆抗体(mAb)之类的生物制剂的使用,这些抗体可消除激活的分子信号通路以促进从癌症治疗中逃脱。我们假设光细胞毒性生色团苯并卟啉衍生物单酸A(BPD)和抗VEGF mAb贝伐单抗在纳米可光激活脂质体(nanoPAL)中的细胞内共递送可能增强光动力疗法(PDT)的功效并抑制VEGF介导的信号传导途径。作为概念验证,我们发现nanoPAL-PDT在体外诱导增强的贝伐单抗细胞外和细胞内传递,并增强急性细胞毒性。在胰腺导管腺癌的体内皮下小鼠模型中,nanoPAL-PDT显着增强了肿瘤的减少。我们将其归因于将不溶性BPD最佳结合到脂质双层中,增强了光细胞毒性,同时贝伐单抗同时时空传递,确保有效中和了PDT后VEGF的快速但短暂的爆发。

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