Jahn Thomas R, Radford Sheena E
Astbury Centre for Structural Molecular Biology and Institute of Molecular and Cellular Biology, Gerstang Building, University of Leeds, UK.
FEBS J. 2005 Dec;272(23):5962-70. doi: 10.1111/j.1742-4658.2005.05021.x.
The study of protein aggregation saw a renaissance in the last decade, when it was discovered that aggregation is the cause of several human diseases, making this field of research one of the most exciting frontiers in science today. Building on knowledge about protein folding energy landscapes, determined using an array of biophysical methods, theory and simulation, new light is now being shed on some of the key questions in protein-misfolding diseases. This review will focus on the mechanisms of protein folding and amyloid fibril formation, concentrating on the role of partially folded states in these processes, the complexity of the free energy landscape, and the potentials for the development of future therapeutic strategies based on a full biophysical description of the combined folding and aggregation free-energy surface.
在过去十年中,蛋白质聚集的研究迎来了复兴,当时人们发现聚集是多种人类疾病的病因,这使得该研究领域成为当今科学界最令人兴奋的前沿领域之一。基于通过一系列生物物理方法、理论和模拟确定的蛋白质折叠能量景观的知识,现在人们对蛋白质错误折叠疾病中的一些关键问题有了新的认识。本综述将重点关注蛋白质折叠和淀粉样原纤维形成的机制,着重探讨部分折叠状态在这些过程中的作用、自由能景观的复杂性,以及基于对折叠和聚集自由能表面的完整生物物理描述开发未来治疗策略的潜力。
Zotero 插件