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Sequential application of a cytotoxic nanoparticle and a PI3K inhibitor enhances antitumor efficacy

机译:顺序应用细胞毒性纳米颗粒和PI3K抑制剂可增强抗肿瘤功效

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Nanomedicines that preferentially deploy cytotoxic agents to tumors and molecular targeted therapeutics that inhibit specific aberrant oncogenic drivers are emerging as the new paradigm for the management of cancer. While combination therapies are a mainstay of cancer chemotherapy, few studies have addressed the combination of nanomedicines and molecular targeted therapeutics. Furthermore, limited knowledge exists on the impact of sequencing of such therapeutics and nanomedicines on the antitumor outcome. Here, we engineered a supramolecular cis-platinum nanoparticle, which induced apoptosis in breast cancer cells but also elicited prosurvival signaling via an EGF receptor/phosphoinositide 3-kinase (PI3K) pathway. A combination of mathematical modeling and in vitro and in vivo validation using a pharmacologic inhibitor of PI3K, PI828, demonstrate that administration of PI828 following treatment with the supramolecular cis-platinum nanoparticle results in enhanced antitumor efficacy in breast cancer as compared with when the sequence is reversed or when the two treatments are administered simultaneously. This study addresses, for the first time, the impact of drug sequencing in the case of a combination of a nanomedicine and a targeted therapeutic. Furthermore, our results indicate that a rational combination of cis-platinum nanoparticles and a PI3K-targeted therapeutic can emerge as a potential therapy for breast cancer.
机译:优先将细胞毒剂用于肿瘤的纳米药物和抑制特异性异常致癌驱动因子的分子靶向疗法正在成为治疗癌症的新范例。尽管联合疗法是癌症化疗的主要手段,但很少有研究涉及纳米药物和分子靶向疗法的联合。此外,关于这种疗法和纳米药物的测序对抗肿瘤结果的影响的知识有限。在这里,我们设计了一种超分子顺铂纳米颗粒,该颗粒诱导了乳腺癌细胞的凋亡,但也通过EGF受体/磷酸肌醇3-激酶(PI3K)途径引发了生存信号。数学建模以及使用PI3K的药物抑制剂PI828进行的体内和体外验证相结合,证明与超分子顺铂纳米粒子相比,用超分子顺铂纳米粒子治疗后给予PI828可以增强乳腺癌的抗肿瘤功效。逆转或同时进行两种治疗时。这项研究首次解决了纳米药物和靶向治疗药物联合使用时药物测序的影响。此外,我们的结果表明,顺铂纳米颗粒和PI3K靶向治疗剂的合理组合可以作为乳腺癌的潜在治疗方法出现。

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