Platelet granule exocytosis and thrombus formation

血小板颗粒胞吐作用和血栓形成

• 批准号: 8793806
• 负责人: Robert C Flaumenhaft
• 金额: $ 42.85万
• 依托单位: BETH ISRAEL DEACONESS MEDICAL CENTER
• 依托单位国家: 美国
• 财政年份: 2013
• 资助国家: 美国
• 起止时间: 2013-02-01 至 2016-01-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8793806
• 关键词: Actins; Address; Adhesions; Alpha Granule; Blood Platelets; Cells; Coagulation Process; Cytoplasmic Granules; Cytoskeleton; Disease; Dynamin; Dynamin 2; Dynamin III; Evaluation; Event; Exocytosis; Foundations; Genetic Screening; Health; Hemostatic function; Heterogeneity; In Vitro; Individual; Inflammation; Kinetics; Laboratories; Learning; Malignant Neoplasms; Mediating; Membrane; Membrane Fusion; Molecular; Molecular Chaperones; Monitor; Morbidity - disease rate; Movement; Mus; Myocardial Infarction; Platelet Activation; Population; Protein Isoforms; Proteins; Regulation; Role; SNAP receptor; Sorting - Cell Movement; Speed; Stroke; Structure; Suspension substance; Suspensions; Thrombosis; Thrombus; Vascular Diseases; Video Microscopy; Wound Healing; angiogenesis; cellubrevin; chaperone machinery; chemical genetics; controlled release; in vivo; intravital microscopy; mortality; neglect; novel; protein function; research study; segregation; trafficking; vesicle-associated membrane protein

DESCRIPTION (provided by applicant): Granule exocytosis is an essential platelet function, contributing not only to hemostasis and thrombosis, but also to inflammation, wound healing, malignancy, and angiogenesis. Previous efforts to understand the molecular mechanisms of granule exocytosis have identified the SNARE machinery and chaperone proteins required for membrane fusion. Studies described in this proposal will evaluate the premise that this machinery serves a role in sorting specific cargos to distinct subpopulations of ¿-granules and enabling differential release of granule contents upon platelet activation. We will study granule segregation and secretion in mice lacking VAMP-3, VAMP-5, VAMP-7, and VAMP-8. Cytoskeleton dynamics that occur during platelet spreading can influence SNARE interactions and modify granule exocytosis. We will evaluate granule exocytosis during platelet spreading. These studies will also assess the role of exocytosis in providing membrane for growing actin structures at the periphery of adherent platelets and for directed spreading and movement on micropatterned matrices of adhesion proteins. Use of high-speed intravital microscopy will be used to monitor release of granules from individual platelets during thrombus formation in vivo. These approaches will allow us to evaluate the hypothesis that the mechanism of granule secretion is altered in adherent platelets compared to suspension platelets. We will also evaluate the role of dynamins in controlling fusion pore dynamics, demonstrating a level of control of platelet exocytosis that occurs following SNARE-mediated membrane fusion. These studies will use single-cell amperometry to monitor the release of individual granules from single platelets. The role of dynamins in controlling platelet exocytosis during thrombus formation in vivo will evaluate the hypothesis that the platelet fusion pore can be regulated to control thrombus formation. These experiments will address poorly understood aspects of platelet granule exocytosis and provide a foundation for targeting select platelet membrane fusion events during thrombosis.

描述（由申请方提供）：颗粒胞吐作用是血小板的一种基本功能，不仅有助于止血和血栓形成，还有助于炎症、伤口愈合、恶性肿瘤和血管生成。以前的努力，以了解颗粒胞吐的分子机制已经确定了陷阱机制和伴侣蛋白所需的膜融合。本提案中描述的研究将评估这样的前提，即这种机制在将特定货物分类为不同的颗粒亚群中发挥作用，并在血小板活化时实现颗粒内容物的差异释放。我们将研究缺乏VAMP-3、VAMP-5、VAMP-7和VAMP-8的小鼠的颗粒分离和分泌。血小板伸展过程中发生的细胞骨架动力学可以影响SNARE相互作用并改变颗粒胞吐作用。我们将评估血小板扩散过程中的颗粒胞吐作用。这些研究还将评估胞吐作用在为粘附血小板外周的肌动蛋白结构的生长和粘附蛋白在微图案基质上的定向扩散和移动提供膜方面的作用。将使用高速活体显微镜监测体内血栓形成期间单个血小板颗粒的释放。这些方法将使我们能够评估的假设，颗粒分泌的机制是改变粘附血小板相比，悬浮血小板。我们还将评估发动蛋白在控制融合孔动力学中的作用，证明在SNARE介导的膜融合后发生的血小板胞吐的控制水平。这些研究将使用单细胞安培法来监测单个血小板中单个颗粒的释放。动力蛋白在体内血栓形成过程中控制血小板胞吐的作用将评估血小板融合孔可以被调节以控制血栓形成的假设。这些实验将解决血小板颗粒胞吐作用知之甚少的方面，并为靶向选择血栓形成过程中的血小板膜融合事件提供基础。