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巨噬细胞作为主动型纳米载体用于靶向早期和辅助癌症化疗。

Macrophages as Active Nanocarriers for Targeted Early and Adjuvant Cancer Chemotherapy.

机构信息

Department of Respiratory Medicine, The Second Affiliated Hospital of School of Medicine, Zhejiang University, Hangzhou, 310009, China.

Key Laboratory of Tumor Molecular Diagnosis and Individualized Medicine of Zhejiang Province, Clinical Research Institute, Zhejiang Provincial People's Hospital, Hangzhou, 310014, China.

出版信息

Small. 2016 Oct;12(37):5108-5119. doi: 10.1002/smll.201601282. Epub 2016 Aug 25.

Abstract

Taking advantage of the highly permeable vasculature and lack of lymphatic drainage in solid tumors (EPR effect), nanosized drug delivery systems or nanomedicines have been extensively explored for tumor-targeted drug delivery. However, in most clinical cases tumors such as the early stage tumors and post-surgery microscopic residual tumors have not yet developed such pathological EPR features, i.e., EPR-deficient. Therefore, nanomedicines may not be applicable for such these tumors. Macrophages by nature can actively home and extravasate through the tight vascular wall into tumors and migrate to their hypoxic regions, and possess perfect stealth ability for long blood circulation and impressive phagocytosis for drug loadings. Thus, nanomedicines loaded in macrophages would harness both merits and gain the active tumor homing capability independent of the EPR effect for treatments of the EPR-deficient tumors. Herein, the critical considerations, current progress, challenges and future prospects of macrophages as carriers for nanomedicines are summarized, aiming at rational design of EPR-independent tumor-targeting active nanomedicines for targeted early and adjuvant cancer chemotherapy.

摘要

利用实体瘤中高度可渗透的血管系统和缺乏淋巴引流的特点(EPR 效应),纳米药物递送系统或纳米药物已被广泛探索用于肿瘤靶向药物递送。然而,在大多数临床情况下,肿瘤如早期肿瘤和手术后的微小残留肿瘤尚未发展出这种病理性 EPR 特征,即 EPR 缺乏。因此,纳米药物可能不适用于这些肿瘤。巨噬细胞本质上可以主动归巢并通过紧密的血管壁外渗进入肿瘤,并迁移到其缺氧区域,并且具有出色的隐身能力,可以实现长时间的血液循环和对药物负载的显著吞噬作用。因此,负载在巨噬细胞中的纳米药物将同时利用这两个优点,并获得独立于 EPR 效应的主动肿瘤归巢能力,用于治疗 EPR 缺乏的肿瘤。本文总结了巨噬细胞作为纳米药物载体的关键考虑因素、当前进展、挑战和未来展望,旨在合理设计用于靶向早期和辅助癌症化疗的 EPR 非依赖性肿瘤靶向主动纳米药物。

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