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用于理解刺参溶素(一种来自海葵的成孔蛋白)的膜结合和孔形成的生物物理和生化策略。

Biophysical and biochemical strategies to understand membrane binding and pore formation by sticholysins, pore-forming proteins from a sea anemone.

作者信息

Alvarez Carlos, Ros Uris, Valle Aisel, Pedrera Lohans, Soto Carmen, Hervis Yadira P, Cabezas Sheila, Valiente Pedro A, Pazos Fabiola, Lanio Maria E

机构信息

Center for Protein Studies, Faculty of Biology, University of Havana, Calle 25 No 455, Vedado, Havana, Cuba.

Interfaculty Institute of Biochemistry, University of Tübingen, Hoppe-Seyler-Str. 4, 72076, Tübingen, Germany.

出版信息

Biophys Rev. 2017 Oct;9(5):529-544. doi: 10.1007/s12551-017-0316-0. Epub 2017 Aug 29.

DOI:10.1007/s12551-017-0316-0
PMID:28853034
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5662052/
Abstract

Actinoporins constitute a unique class of pore-forming toxins found in sea anemones that are able to bind and oligomerize in membranes, leading to cell swelling, impairment of ionic gradients and, eventually, to cell death. In this review we summarize the knowledge generated from the combination of biochemical and biophysical approaches to the study of sticholysins I and II (Sts, StI/II), two actinoporins largely characterized by the Center of Protein Studies at the University of Havana during the last 20 years. These approaches include strategies for understanding the toxin structure-function relationship, the protein-membrane association process leading to pore formation and the interaction of toxin with cells. The rational combination of experimental and theoretical tools have allowed unraveling, at least partially, of the complex mechanisms involved in toxin-membrane interaction and of the molecular pathways triggered upon this interaction. The study of actinoporins is important not only to gain an understanding of their biological roles in anemone venom but also to investigate basic molecular mechanisms of protein insertion into membranes, protein-lipid interactions and the modulation of protein conformation by lipid binding. A deeper knowledge of the basic molecular mechanisms involved in Sts-cell interaction, as described in this review, will support the current investigations conducted by our group which focus on the design of immunotoxins against tumor cells and antigen-releasing systems to cell cytosol as Sts-based vaccine platforms.

摘要

放线孔蛋白是海葵中发现的一类独特的成孔毒素,能够在膜中结合并寡聚化,导致细胞肿胀、离子梯度受损,最终导致细胞死亡。在本综述中,我们总结了结合生化和生物物理方法对刺参毒素I和II(Sts,StI/II)进行研究所产生的知识,这两种放线孔蛋白在过去20年中主要由哈瓦那大学蛋白质研究中心进行了表征。这些方法包括理解毒素结构-功能关系的策略、导致孔形成的蛋白质-膜结合过程以及毒素与细胞的相互作用。实验和理论工具的合理结合使得至少部分地揭示了毒素-膜相互作用所涉及的复杂机制以及这种相互作用引发的分子途径。对放线孔蛋白的研究不仅对于理解它们在海葵毒液中的生物学作用很重要,而且对于研究蛋白质插入膜的基本分子机制、蛋白质-脂质相互作用以及脂质结合对蛋白质构象的调节也很重要。如本综述所述,对Sts-细胞相互作用所涉及的基本分子机制有更深入的了解,将支持我们小组目前进行的研究,这些研究专注于设计针对肿瘤细胞的免疫毒素以及作为基于Sts的疫苗平台向细胞胞质溶胶释放抗原的系统。

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Differential binding and activity of the pore-forming toxin sticholysin II in model membranes containing diverse ceramide-derived lipids.在含有多种神经酰胺衍生脂质的模型膜中,穿孔毒素Ⅱ型刺参溶细胞素的差异结合与活性
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