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靶向肿瘤促进炎症的仿生方法。

Biomimetic approaches for targeting tumor-promoting inflammation.

作者信息

Parodi Alessandro, Kostyushev Dmitry, Brezgin Sergey, Kostyusheva Anastasiya, Borodina Tatiana, Akasov Roman, Frolova Anastasia, Chulanov Vladimir, Zamyatnin Andrey A

机构信息

Scientific Center for Genetics and Life Sciences, Division of Biotechnology, Sirius University of Science and Technology, 354340 Sochi, Russia; Institute of Molecular Medicine, Sechenov First Moscow State Medical University, 119991 Moscow, Russia.

Scientific Center for Genetics and Life Sciences, Division of Biotechnology, Sirius University of Science and Technology, 354340 Sochi, Russia; National Medical Research Center of Tuberculosis and Infectious Diseases, Ministry of Health, 127994 Moscow, Russia; Infectious Diseases Depaertment, Sechenov First Moscow State Medical University, 119991 Moscow, Russia.

出版信息

Semin Cancer Biol. 2022 Nov;86(Pt 2):555-567. doi: 10.1016/j.semcancer.2022.04.007. Epub 2022 Apr 25.

Abstract

With the ultimate goal of increasing tumor accumulation of therapeutics, various nanocarriers have been designed to overcome biological barriers encountered at each stage, from drug administration to the cancerous lesion. Stabilizing circulation and functionalization of the targeting surface impart high tumor accumulation properties to nanocarriers. However, various cells can recognize and infiltrate the tumor microenvironment more efficiently than synthetic carriers via overexpression of adhesive ligands, particularly in inflamed stroma of tumors. Thus, a new field of nanomedicine, called biomimicry, has evolved to generate nanoparticles with the same biological characteristics as cells that naturally infiltrate tumors. Revolutionary synthetic processes have been developed to transfer the cell membrane of leukocytes and mesenchymal cells to synthetic carriers. In addition, cells can generate their own "nanocarriers," known as exosomes, to transport molecular messages to distant sites, while biomimicry of viral and bacterial agents allows high targeting efficiency towards inflammatory immune cells. Alterations in the protein expression in cancer cells caused by inflammation can also be exploited for drug delivery. Finally, new developments in biomimetic drug delivery focus on turning the infiltrating cells into microcarriers that can actively perfuse the tumor and eventually release their therapeutic payload. In this review, we summarize recent developments in biomimetic drug delivery with a particular focus on targeting the tumor inflammatory microenvironment.

摘要

为了实现提高治疗药物在肿瘤中蓄积的最终目标,人们设计了各种纳米载体,以克服从药物给药到癌灶这一过程中各个阶段所遇到的生物屏障。稳定循环以及靶向表面的功能化赋予了纳米载体较高的肿瘤蓄积特性。然而,各种细胞可以通过过表达黏附配体,比合成载体更有效地识别并浸润肿瘤微环境,尤其是在肿瘤的炎症基质中。因此,一个名为仿生学的纳米医学新领域应运而生,旨在制造出具有与天然浸润肿瘤的细胞相同生物学特性的纳米颗粒。人们已经开发出革命性的合成方法,将白细胞和间充质细胞的细胞膜转移到合成载体上。此外,细胞可以产生自身的“纳米载体”,即外泌体,将分子信息传递到远处,而对病毒和细菌制剂的仿生则可实现对炎性免疫细胞的高效靶向。炎症引起的癌细胞中蛋白质表达的改变也可用于药物递送。最后,仿生药物递送的新进展集中在将浸润细胞转变为能够主动灌注肿瘤并最终释放其治疗载荷的微载体上。在这篇综述中,我们总结了仿生药物递送的最新进展,特别关注对肿瘤炎症微环境的靶向作用。

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