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分泌型核糖核酸酶作为抗肿瘤药物的优势与挑战

Strengths and Challenges of Secretory Ribonucleases as AntiTumor Agents.

作者信息

Castro Jessica, Ribó Marc, Vilanova Maria, Benito Antoni

机构信息

Laboratori d'Enginyeria de Proteïnes, Departament de Biologia, Facultat de Ciències, Universitat de Girona, Campus de Montilivi, Carrer Maria Aurèlia Capmany, 40, 17003 Girona, Spain.

Institut d'Investigació Biomèdica de Girona Josep Trueta, (IdIBGi), Hospital de Santa Caterina, Carrer del Dr. Castany, s/n, 17190 Salt, Spain.

出版信息

Pharmaceutics. 2021 Jan 9;13(1):82. doi: 10.3390/pharmaceutics13010082.

Abstract

Approaches to develop effective drugs to kill cancer cells are mainly focused either on the improvement of the currently used chemotherapeutics or on the development of targeted therapies aimed at the selective destruction of cancer cells by steering specific molecules and/or enhancing the immune response. The former strategy is limited by its genotoxicity and severe side effects, while the second one is not always effective due to tumor cell heterogeneity and variability of targets in cancer cells. Between these two strategies, several approaches target different types of RNA in tumor cells. RNA degradation alters gene expression at different levels inducing cell death. However, unlike DNA targeting, it is a pleotropic but a non-genotoxic process. Among the ways to destroy RNA, we find the use of ribonucleases with antitumor properties. In the last few years, there has been a significant progress in the understanding of the mechanism by which these enzymes kill cancer cells and in the development of more effective variants. All the approaches seek to maintain the requirements of the ribonucleases to be specifically cytotoxic for tumor cells. These requirements start with the competence of the enzymes to interact with the cell membrane, a process that is critical for their internalization and selectivity for tumor cells and continue with the downstream effects mainly relying on changes in the RNA molecular profile, which are not only due to the ribonucleolytic activity of these enzymes. Although the great improvements achieved in the antitumor activity by designing new ribonuclease variants, some drawbacks still need to be addressed. In the present review, we will focus on the known mechanisms used by ribonucleases to kill cancer cells and on recent strategies to solve the shortcomings that they show as antitumor agents, mainly their pharmacokinetics.

摘要

开发有效抗癌药物的方法主要集中在两个方面

一是改进目前使用的化疗药物,二是开发靶向疗法,即通过调控特定分子和/或增强免疫反应来选择性地破坏癌细胞。前一种策略受限于其基因毒性和严重的副作用,而后一种策略由于肿瘤细胞的异质性和癌细胞中靶点的变异性,并非总是有效。在这两种策略之间,有几种方法针对肿瘤细胞中的不同类型RNA。RNA降解在不同水平上改变基因表达,从而诱导细胞死亡。然而,与靶向DNA不同,这是一个多效性但非基因毒性的过程。在破坏RNA的方法中,我们发现了使用具有抗肿瘤特性的核糖核酸酶。在过去几年里,在理解这些酶杀死癌细胞的机制以及开发更有效的变体方面取得了重大进展。所有这些方法都试图满足核糖核酸酶对肿瘤细胞具有特异性细胞毒性的要求。这些要求首先是酶与细胞膜相互作用的能力,这一过程对于它们内化进入细胞以及对肿瘤细胞的选择性至关重要,接着是下游效应,主要依赖于RNA分子谱的变化,而这些变化不仅仅是由于这些酶的核糖核酸酶活性。尽管通过设计新的核糖核酸酶变体在抗肿瘤活性方面取得了巨大进步,但仍有一些缺点需要解决。在本综述中,我们将重点关注核糖核酸酶杀死癌细胞所使用的已知机制,以及解决它们作为抗肿瘤药物所表现出的缺点(主要是其药代动力学)的最新策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a192/7828032/bb97ee328902/pharmaceutics-13-00082-g001.jpg

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