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靶向细胞内的生物制品:治疗环境中的毒素途径。

Targeting the Inside of Cells with Biologicals: Toxin Routes in a Therapeutic Context.

机构信息

Institute of Biochemistry, Biotechnology and Bioinformatics, Technische Universität Braunschweig, Biocentre - Spielmannstraße 7, 38106, Braunschweig, Germany.

出版信息

BioDrugs. 2023 Mar;37(2):181-203. doi: 10.1007/s40259-023-00580-y. Epub 2023 Feb 2.

Abstract

Numerous toxins translocate to the cytosol in order to fulfil their function. This demonstrates the existence of routes for proteins from the extracellular space to the cytosol. Understanding these routes is relevant to multiple aspects related to therapeutic applications. These include the development of anti-toxin treatments, the potential use of toxins as shuttles for delivering macromolecular cargo to the cytosol or the use of drugs based on toxins. Compared with other strategies for delivery, such as chemicals as carriers for macromolecular delivery or physical methods like electroporation, toxin routes present paths into the cell that potentially cause less damage and can be specifically targeted. The efficiency of delivery via toxin routes is limited. However, low-delivery efficiencies can be entirely sufficient, if delivered cargoes possess an amplification effect or if very few molecules are sufficient for inducing the desired effects. This is known for example from RNA-based vaccines that have been developed during the coronavirus disease 2019 pandemic as well as for other approved RNA-based drugs, which elicited the desired effect despite their typically low delivery efficiencies. The different mechanisms by which toxins enter cells may have implications for their technological utility. We review the mechanistic principles of the translocation pathway of toxins from the extracellular space to the cytosol, the delivery efficiencies, and therapeutic strategies or applications that exploit toxin routes for intracellular delivery.

摘要

为了发挥作用,许多毒素转移到细胞质溶胶中。这表明存在从细胞外空间到细胞质溶胶的蛋白质途径。了解这些途径与与治疗应用相关的多个方面有关。这些方面包括开发抗毒素治疗、潜在使用毒素作为将大分子货物递送到细胞质溶胶的载体或使用基于毒素的药物。与其他大分子递送载体(如化学物质)或物理方法(如电穿孔)等其他递送策略相比,毒素途径提供了进入细胞的潜在损伤较小且可以特异性靶向的途径。毒素途径的递送效率是有限的。然而,如果递送到细胞内的货物具有放大效应,或者只需少量分子就能诱导所需的效果,那么低的递送效率就完全足够了。这在例如在 2019 年冠状病毒病期间开发的基于 RNA 的疫苗以及其他已批准的基于 RNA 的药物中得到了证明,尽管它们的典型递送效率通常较低,但这些药物还是产生了所需的效果。毒素进入细胞的不同机制可能对其技术用途有影响。我们综述了毒素从细胞外空间到细胞质溶胶的易位途径的机制原理、递送效率以及利用毒素途径进行细胞内递送的治疗策略或应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d9b/9971154/cf5174b9a7ef/40259_2023_580_Fig1_HTML.jpg

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