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二维 MoS 纳米片抗胞吐增强协同癌症治疗的细胞内机制理解。

Intracellular Mechanistic Understanding of 2D MoS Nanosheets for Anti-Exocytosis-Enhanced Synergistic Cancer Therapy.

机构信息

School of Life Sciences , Tsinghua University , Beijing 100084 , China.

Department of Biochemistry, Rosalind and Morris Goodman Cancer Research Center , McGill University , Montreal , Quebec H3A 1A3 , Canada.

出版信息

ACS Nano. 2018 Mar 27;12(3):2922-2938. doi: 10.1021/acsnano.8b00516. Epub 2018 Mar 12.

DOI:10.1021/acsnano.8b00516
PMID:29406760
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6097229/
Abstract

Emerging two-dimensional (2D) nanomaterials, such as transition-metal dichalcogenide (TMD) nanosheets (NSs), have shown tremendous potential for use in a wide variety of fields including cancer nanomedicine. The interaction of nanomaterials with biosystems is of critical importance for their safe and efficient application. However, a cellular-level understanding of the nano-bio interactions of these emerging 2D nanomaterials ( i. e., intracellular mechanisms) remains elusive. Here we chose molybdenum disulfide (MoS) NSs as representative 2D nanomaterials to gain a better understanding of their intracellular mechanisms of action in cancer cells, which play a significant role in both their fate and efficacy. MoS NSs were found to be internalized through three pathways: clathrin → early endosomes → lysosomes, caveolae → early endosomes → lysosomes, and macropinocytosis → late endosomes → lysosomes. We also observed autophagy-mediated accumulation in the lysosomes and exocytosis-induced efflux of MoS NSs. Based on these findings, we developed a strategy to achieve effective and synergistic in vivo cancer therapy with MoS NSs loaded with low doses of drug through inhibiting exocytosis pathway-induced loss. To the best of our knowledge, this is the first systematic experimental report on the nano-bio interaction of 2D nanomaterials in cells and their application for anti-exocytosis-enhanced synergistic cancer therapy.

摘要

新兴的二维(2D)纳米材料,如过渡金属二硫属化物(TMD)纳米片(NSs),在癌症纳米医学等众多领域显示出巨大的应用潜力。纳米材料与生物系统的相互作用对于它们的安全和有效应用至关重要。然而,对于这些新兴 2D 纳米材料(即细胞内机制)的纳米-生物相互作用的细胞水平的理解仍然难以捉摸。在这里,我们选择二硫化钼(MoS)NSs 作为代表性的 2D 纳米材料,以更好地了解它们在癌细胞中的作用机制,这对于它们的命运和疗效都有重要影响。MoS NSs 被发现通过三种途径被内化:网格蛋白→早期内体→溶酶体、小窝蛋白→早期内体→溶酶体和巨胞饮→晚期内体→溶酶体。我们还观察到自噬介导的溶酶体积累和外排诱导的 MoS NSs 外排。基于这些发现,我们开发了一种策略,通过抑制外排途径诱导的损失,用载有低剂量药物的 MoS NSs 实现有效的协同体内癌症治疗。据我们所知,这是第一篇关于细胞内 2D 纳米材料的纳米-生物相互作用及其应用于抗外排增强协同癌症治疗的系统性实验报告。

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