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首页> 外文期刊>Cellular and molecular biology >High pressure, an alternative approach to understand protein misfolding diseases.
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High pressure, an alternative approach to understand protein misfolding diseases.

机译:高压是了解蛋白质错误折叠疾病的另一种方法。

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Protein folding is essential for the flow of genetic information to biological activity. A failure in this process can result in disease, by causing cell damage and sometimes death. The misfolding of proteins often induces their aggregation, initiating the fibril formation seen in a range of human and animal diseases. Because misfolding and aggregation are of fundamental importance in vivo, there is currently great interest in understanding their mechanisms. To gain insight into the folding and unfolding processes of proteins, for nearly a century, an original biophysical approach has been successfully used: the application of high hydrostatic pressure combined with various spectroscopic and kinetic techniques. Because high pressure provides new insight into protein structure and folding which cannot be obtained by other techniques, the conformations of pressure-induced unfolding intermediates and species involved in the initial states of aggregation of proteins associated with specific diseases are currently being investigated. Our contention is that by exploring folding kinetics, misfolding pathways and stability under pressure, it will be possible to understand the mechanisms of amyloidogenesis, with the ultimate goal to design therapeutic strategies to prevent progression of the disease.
机译:蛋白质折叠对于遗传信息向生物活性的流动至关重要。该过程的失败会导致细胞损伤甚至死亡,从而导致疾病。蛋白质的错误折叠通常会诱导其聚集,从而引发一系列人类和动物疾病中的原纤维形成。由于错误折叠和聚集在体内至关重要,因此目前对了解其机制非常感兴趣。为了深入了解蛋白质的折叠和展开过程,近一个世纪以来,已经成功地使用了一种原始的生物物理方法:将高静水压力与各种光谱和动力学技术结合起来使用。由于高压为蛋白质结构和折叠提供了新的见识,而其他技术无法获得这些信息,因此目前正在研究与特定疾病相关的蛋白质聚集初始状态所涉及的压力诱导的展开中间体和物种的构象。我们的观点是,通过探索折叠动力学,错误折叠途径和在压力下的稳定性,将有可能了解淀粉样蛋白生成的机制,最终目的是设计预防疾病进展的治疗策略。

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