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利用肽靶向肿瘤。

Targeting Tumors Using Peptides.

机构信息

Institute of Biomedicine and Translational Medicine, University of Tartu, Ravila 14B, Tartu 50411, Estonia.

School of Science and Technology, National University of San Martin (UNSAM) and CONICET, Campus Migueletes, 25 de Mayo y Francia, San Martín, Buenos Aires CP 1650, Argentina.

出版信息

Molecules. 2020 Feb 13;25(4):808. doi: 10.3390/molecules25040808.

Abstract

To penetrate solid tumors, low molecular weight (Mw < 10 KDa) compounds have an edge over antibodies: their higher penetration because of their small size. Because of the dense stroma and high interstitial fluid pressure of solid tumors, the penetration of higher Mw compounds is unfavored and being small thus becomes an advantage. This review covers a wide range of peptidic ligands-linear, cyclic, macrocyclic and cyclotidic peptides-to target tumors: We describe the main tools to identify peptides experimentally, such as phage display, and the possible chemical modifications to enhance the properties of the identified peptides. We also review in silico identification of peptides and the most salient non-peptidic ligands in clinical stages. We later focus the attention on the current validated ligands available to target different tumor compartments: blood vessels, extracelullar matrix, and tumor associated macrophages. The clinical advances and failures of these ligands and their therapeutic conjugates will be discussed. We aim to present the reader with the state-of-the-art in targeting tumors, by using low Mw molecules, and the tools to identify new ligands.

摘要

为了穿透实体瘤,低分子量(Mw<10 kDa)化合物比抗体具有优势:由于其分子量较小,它们的穿透能力更高。由于实体瘤的基质致密和间质液压力高,高分子量化合物的穿透性较差,因此分子量小成为优势。本综述涵盖了广泛的靶向肿瘤的肽类配体-线性、环状、大环和环肽-:我们描述了实验中识别肽的主要工具,如噬菌体展示,以及增强已识别肽性质的可能化学修饰。我们还回顾了肽和临床阶段中最突出的非肽类配体的计算机识别。然后,我们将注意力集中在当前可用于靶向不同肿瘤区室的已验证配体上:血管、细胞外基质和肿瘤相关巨噬细胞。我们将讨论这些配体及其治疗性缀合物的临床进展和失败。我们的目标是通过使用低分子量分子和识别新配体的工具,为读者呈现靶向肿瘤的最新技术。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0a46/7070747/e620356b7480/molecules-25-00808-g001.jpg

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