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载卡紫杉醇靶向氧化还原敏感壳聚糖纳米粒:光声和光学成像的双重靶向癌症治疗、肺部分布和靶向研究

EGFR Targeted Redox Sensitive Chitosan Nanoparticles of Cabazitaxel: Dual-Targeted Cancer Therapy, Lung Distribution, and Targeting Studies by Photoacoustic and Optical Imaging.

机构信息

Department of Pharmaceutical Engineering and Technology, IIT BHU, Varanasi 221005, Uttar Pradesh, India.

Department of Pharmaceutics, College of Pharmacy, K.L. Deemed-to-be-University, Greenfields, Vaddeswaram 522302, Andhra Pradesh, India.

出版信息

Biomacromolecules. 2023 Nov 13;24(11):4989-5003. doi: 10.1021/acs.biomac.3c00658. Epub 2023 Oct 23.

DOI:10.1021/acs.biomac.3c00658
PMID:37871263
Abstract

In this research, we have modified tocopheryl polyethylene glycol succinate (TPGS) to a redox-sensitive material, denoted as TPGS-SH, and employed the same to develop dual-receptor-targeted nanoparticles of chitosan loaded with cabazitaxel (CZT). The physicochemical properties and morphological characteristics of all nanoparticle formulations were assessed. Dual-receptor targeting redox-sensitive nanoparticles of CZT (F-CTX-CZT-CS-SH-NPs) were developed by a combination of pre- and postconjugation techniques by incorporating synthesized chitosan-folate (F) and TPGS-SH during nanoparticle synthesis and further postconjugated with cetuximab (CTX) for epidermal growth factor receptor (EGFR) targeting. The release of the drug was seemingly higher in the redox-sensitive buffer media (GSH, 20 mM) compared to that in physiological buffer. However, the extent of cellular uptake of dual-targeted nanoparticles was significantly higher in A549 cells than other control nanoparticles. The IC values of F-CTX-CZT-CS-SH-NPs against A549 cells was 0.26 ± 0.12 μg/mL, indicating a 6.3-fold and 60-fold enhancement in cytotoxicity relative to that of dual-receptor targeted, nonredox sensitive nanoparticles and CZT clinical injection, respectively. Furthermore, F-CTX-CZT-CS-SH-NPs demonstrated improved anticancer activity in the benzo(a)pyrene lung cancer model with a higher survival rate. Due to the synergistic combination of enhanced permeability and retention (EPR) effect of small-sized nanoparticles, the innovative and redox sensitive TPGS-SH moiety and the dual folate and EGFR mediated augmented endocytosis have all together significantly enhanced their biodistribution and targeting exclusively to the lung which is evident from their ultrasound/photoacoustic and imaging system (IVIS) studies.

摘要

在这项研究中,我们将生育酚聚乙二醇琥珀酸酯(TPGS)修饰为一种氧化还原敏感材料,标记为 TPGS-SH,并利用其开发载有卡巴他赛(CZT)的壳聚糖的双受体靶向纳米颗粒。评估了所有纳米颗粒制剂的理化性质和形态特征。通过在纳米颗粒合成过程中结合合成的壳聚糖叶酸(F)和 TPGS-SH,并进一步与西妥昔单抗(CTX)进行后缀合以靶向表皮生长因子受体(EGFR),开发了载有 CZT 的双受体靶向氧化还原敏感纳米颗粒(F-CTX-CZT-CS-SH-NPs)。与生理缓冲液相比,药物在氧化还原敏感缓冲液(GSH,20 mM)中的释放似乎更高。然而,双靶向纳米颗粒在 A549 细胞中的细胞摄取程度明显高于其他对照纳米颗粒。F-CTX-CZT-CS-SH-NPs 对 A549 细胞的 IC 值为 0.26±0.12 μg/mL,与双受体靶向、非氧化还原敏感纳米颗粒和 CZT 临床注射相比,细胞毒性分别提高了 6.3 倍和 60 倍。此外,F-CTX-CZT-CS-SH-NPs 在苯并(a)芘肺癌模型中表现出更好的抗癌活性,存活率更高。由于小尺寸纳米颗粒的增强渗透和保留(EPR)效应、创新的氧化还原敏感 TPGS-SH 部分以及双叶酸和 EGFR 介导的增强内吞作用的协同组合,它们的生物分布和专门靶向肺部的靶向性都得到了显著增强,这从它们的超声/光声和成像系统(IVIS)研究中可以明显看出。

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