Crystallin aggregation and stabilization

晶体蛋白聚集和稳定

• 批准号: 9130222
• 负责人: Martin T Zanni
• 金额: $ 27.98万
• 依托单位: UNIVERSITY OF WISCONSIN-MADISON
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-09-01 至 2018-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9130222
• 关键词: Acids; Adopted; Affect; Age; American; Amyloid; Amyloid fibers; Binding; Blindness; C-terminal; Cataract; Chemicals; Communities; Crystallins; Data; Deposition; Disease; Exposure to; Goals; Health; Heating; Human; In Vitro; Individual; Isotope Labeling; Journals; Kinetics; Label; Lead; Learning; Ligation; Light; Mass Spectrum Analysis; Methodology; Molecular; Molecular Chaperones; Monitor; N-terminal; Pathway interactions; Peptides; Play; Precipitation; Prevalence; Process; Proteins; Publications; Publishing; Research; Role; Scientist; Site; Societies; Solar Energy; Source; Spectrum Analysis; Structural Genes; Structural Models; Structure; Surgeon; Testing; Time; Tissue Extracts; Tissues; Translating; UV induced; UVB induced; Ultraviolet B Radiation; United States; United States National Academy of Sciences; Vision; Work; aged; aggregation pathway; base; beta pleated sheet; crosslink; gel electrophoresis; in vivo; insight; interest; lens; lens protein; novel; novel strategies; prevent; protein aggregate; research study; tandem mass spectrometry

DESCRIPTION (provided by applicant): Cataracts affect the vision of 1 in 6 people over the age of 40 in the United States and most people by the age of 80. It is the leading cause of blindness worldwide. As a result, there is much interest in understanding the cause of cataracts and the mechanism by which they form. Cataracts are classified as a misfolding disease whereby degradation of the crystallin lens proteins leads to their aggregation and precipitation. However, critical structural and mechanistic information is lacking largely because it is experimentally difficult to obtain structural information about aggregated proteins and even more difficult to characterize intermediates that are responsible for precipitation. In this proposal, w will use a novel combination of 2D IR spectroscopy, isotope labeling, and mass spectrometry to uncover details about the structure and kinetic mechanism by which γD- crystallin aggregates and the way in which the chaperone protein αB-crystallin inhibits precipitation. Using expressed protein ligation to semi-synthesize γD-crystallin, we will isotope label its individual domains so that their structures and kinetics can be monitored by 2D IR spectroscopy. Using UVB light to mimic covalent damage from solar radiation and initiate aggregation, we will monitor the kinetics and structures of the precipitates as they form. We know from our initial publications that acid-induced denaturation of γD-crystallin leads solely to amyloid fiber formation with the C-terminal domain forming the fibril core, not the N-terminal domain as was previously thought. In contrast, preliminary results on UVB-denaturation reveal that covalent damage leads to both fibrillar and amorphous aggregates. Clearly, there is a competition between pathways that depends on the type of protein damage. Once these pathways are characterized, we will study how they are modified by the chaperone protein αB-crystallin. For many proteins αB-crystallin is a better chaperone against amorphous than fibrillar aggregates, but cataract deposits appear to be mostly amorphous aggregates, implying that the chaperone mechanism is quite different for the crystallin proteins. Finally, the in vitro mechanisms will be tested against in vivo protein extracs collected from human lenses. We want to know if naturally occurring damage or composition of the crystallins alters the in vitro mechanisms and/or structure of the precipitates. Preliminary results are shown for nearly every step in this proposal. Our novel approach of using semi-synthesis and 2D IR spectroscopy is providing molecular-level insights that are important to the large community of scientists devoted to understanding the chaperone mechanisms of αB-crystallin and cataract formation.

描述（由申请人提供）：白内障影响美国40岁以上人群中1/6的视力，大多数人到80岁。它是全球失明的主要原因。因此，人们对了解白内障的原因及其形成机制非常感兴趣。白内障被归类为错误折叠疾病，其中晶状体蛋白透镜蛋白的降解导致其聚集和沉淀。然而，关键的结构和机制信息是缺乏很大程度上，因为它是实验上难以获得有关聚集蛋白质的结构信息，甚至更难以表征中间体，负责沉淀。在这项提议中，我们将使用2D IR光谱、同位素标记和质谱的新组合来揭示γD-晶体蛋白聚集的结构和动力学机制以及伴侣蛋白α B-晶体蛋白抑制沉淀的方式的细节。利用表达的蛋白质连接物半合成γ D-晶状体蛋白，我们将同位素标记其各个结构域，以便通过二维红外光谱监测其结构和动力学。使用UVB光模拟太阳辐射的共价损伤并引发聚集，我们将监测沉淀物形成时的动力学和结构。从我们最初的出版物中我们知道，酸诱导的γ D-晶状体蛋白变性仅导致淀粉样纤维形成，C-末端结构域形成纤维核心，而不是之前认为的N-末端结构域。与此相反，UVB-变性的初步结果表明，共价损伤导致纤维状和无定形聚集体。很明显，不同途径之间存在竞争，这取决于蛋白质损伤的类型。一旦这些途径的特点，我们将研究它们是如何修改的伴侣蛋白α B-晶状体蛋白。对于许多蛋白质，α B-晶状体蛋白是比纤维状聚集体更好的无定形分子伴侣，但白内障沉积物似乎主要是无定形聚集体，这意味着晶状体蛋白的分子伴侣机制完全不同。最后，将针对从人晶状体收集的体内蛋白质提取物测试体外机制。我们想知道晶体蛋白的自然发生的损伤或组成是否改变了沉淀物的体外机制和/或结构。该提案中几乎每一步都显示了初步结果。我们使用半合成和2D IR光谱的新方法提供了分子水平的见解，这对致力于了解α B-晶状体蛋白和白内障形成的分子伴侣机制的广大科学家社区非常重要。