触发释放增强稳定胶体药物聚集体的细胞毒性。
Triggered Release Enhances the Cytotoxicity of Stable Colloidal Drug Aggregates.
机构信息
Department of Chemical Engineering & Applied Chemistry , University of Toronto , 200 College Street , Toronto , Ontario M5S 3E5 , Canada.
Institute of Biomaterials and Biomedical Engineering , University of Toronto , 164 College Street , Toronto , Ontario M5S 3G9 , Canada.
出版信息
ACS Chem Biol. 2019 Jul 19;14(7):1507-1514. doi: 10.1021/acschembio.9b00247. Epub 2019 Jun 25.
Abstract
Chemotherapeutics that self-assemble into colloids have limited efficacy above their critical aggregation concentration due to their inability to penetrate intact plasma membranes. Even when colloid uptake is promoted, issues with colloid escape from the endolysosomal pathway persist. By stabilizing acid-responsive lapatinib colloids through coaggregation with fulvestrant, and inclusion of transferrin, we demonstrate colloid internalization by cancer cells, where subsequent lapatinib ionization leads to endosomal leakage and increased cytotoxicity. These results demonstrate a strategy for triggered drug release from stable colloidal aggregates.
摘要
自组装成胶体的化疗药物由于无法穿透完整的质膜,在超过其临界聚集浓度时疗效有限。即使促进胶体摄取,胶体从内溶酶体途径逃逸的问题仍然存在。通过与氟维司群共聚集并包含转铁蛋白来稳定酸响应的拉帕替尼胶体,我们证明了癌细胞对胶体的内化,随后拉帕替尼的离子化导致内体泄漏和增加细胞毒性。这些结果证明了从稳定胶体聚集体中触发药物释放的策略。
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