Observation of antitumor mechanism of GE11-modified paclitaxel and curcumin liposomes based on cellular morphology changes

Hailing Tang, Lijuan Li, Baoshan Wang
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Abstract

Curcumin and paclitaxel are widely used as anti-tumor hydrophobic model drugs for the designation of smart tumor-targeting nanocarriers and the study of the correlation between structural characteristics of nanoparticles and in vivo therapeutic efficacy. Various signaling pathways on cell growth and proliferation have been comprehensively studied in vitro and in vivo under the action of curcumin and paclitaxel nanoparticles. In this paper, we prepared EGFR-targeted GE11 peptide-modified curcumin and paclitaxel compound liposomes (CUR-PTX@GE11-L). The tumor suppression mechanism of CUR-PTX@GE11-L is observed from the aspects of drug release behavior, changes of cell morphology, liver retention, and tumor-targeting efficiency. We hope it can provide a new vision for the rational construction of smart nanoscale drug delivery system through the observation of cytotoxic effects of CUR-PTX@GE11-L, especially on the cellular morphology change.
基于细胞形态变化观察 GE11 改性紫杉醇和姜黄素脂质体的抗肿瘤机制
姜黄素和紫杉醇被广泛用作抗肿瘤疏水性模型药物,用于指定智能肿瘤靶向纳米载体以及研究纳米颗粒结构特征与体内疗效之间的相关性。在姜黄素和紫杉醇纳米颗粒的作用下,对细胞生长和增殖的各种信号通路进行了全面的体外和体内研究。本文制备了靶向 EGFR 的 GE11 肽修饰姜黄素和紫杉醇复合脂质体(CUR-PTX@GE11-L)。从药物释放行为、细胞形态变化、肝脏滞留和肿瘤靶向效率等方面观察了CUR-PTX@GE11-L的抑瘤机制。通过观察CUR-PTX@GE11-L的细胞毒性作用,特别是细胞形态的变化,希望能为合理构建智能纳米级给药系统提供新的思路。
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