SPERM FUNCTION IN FERTILIZATION EVENTS

受精事件中的精子功能

• 批准号: 3318475
• 负责人: GARY E OLSON
• 金额: $ 13.16万
• 依托单位: VANDERBILT UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 1985
• 资助国家: 美国
• 起止时间: 1985-07-01 至 1993-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/3318475
• 关键词: acrosome; adenosinetriphosphatase; antibody; cell membrane; cytoskeleton; electron microscopy; fertility immunology; fertilization; gel electrophoresis; guinea pigs; hamsters; immunochemistry; intracellular membranes; laboratory mouse; laboratory rabbit; membrane activity; membrane proteins; sperm

The spermatozoan plasma and acrosomal membranes are partitioned into domains of distinct molecular and structural composition which display specific functions at defined fertilization steps. The long range goals of this proposal are to define the molecular and structural mechanisms which generate the mosaic character of the spermatozoan membranes and to identify the role of cytoskeletal assemblies in sperm development and fertilization. First we will determine if cytoskeletal assemblies function in the segregation of membrane proteins to selected domains by identifying plasma membrane components associated with the cytoskeleton and preparing antibodies against them to immunolocalize their surface distributions. The submembranous assembly with which they associate and changes in their cytoskeletal associations during sperm development and fertilization events will be determined the using electron microscopy and immunolocalization techniques. Second we will define the molecular and structural properties of the sperm membrane skeleton obtained from plasma membranes treated with nonionic detergents; we will employ electron microscopy to define its ultrastructure and electrophoretic techniques to define its polypeptide composition and specific protein-protein interactions with integral membrane proteins. Third we will isolate the acrosomal cytoskeleton utilizing cell fractionation procedures and define its polypeptide composition and interaction with specific components of the plasma membrane. Fourth we will characterize the detergent-stable aerosomal matrix components with respect to their polypeptide composition and define their role in segregating acrosomal hydrolases within the acrosome. Finally we will define the protein composition of a cytoskeletal assembly restricted to the sperm midpiece and determine if it functions in directing the mitochondria to the forming midpiece during spermiogenesis or in maintaining mitochondrial distribution in mature spermatozoa. Completion of these specific aims will provide new data on the mechanisms underlying the mosaic construction of the sperm plasma membrane and provide needed data on the molecular basis of specific fertilization events.

精子的质膜和顶体膜被分割 分成不同的分子和结构组成的区域 在定义的施肥步骤中显示特定功能。这个 这项提议的长期目标是定义分子和 产生马赛克特征的结构机制 精子膜和鉴定细胞骨架的作用 精子发育和受精过程中的组装。首先，我们会 确定细胞骨架组件是否在分离中起作用 通过识别血浆将膜蛋白定位到选定的结构域 与细胞骨架相关的膜成分及其制备 针对它们的抗体免疫定位于它们的表面 分配。它们所用的膜下组件 它们的细胞骨架关联性和变化 精子发育和受精事件将由 使用电子显微镜和免疫定位技术。 第二，我们将定义分子和结构属性 质膜处理后获得的精子膜骨架 使用非离子洗涤剂；我们将使用电子显微镜 确定其超微结构和电泳技术，以确定 其多肽组成和特异性蛋白-蛋白质 与完整膜蛋白的相互作用。第三，我们会 用细胞分离法分离顶体细胞骨架 程序和定义其多肽组成和相互作用 质膜的特定成分。第四，我们会 用来表征洗涤剂稳定的气雾体基质成分 尊重它们的多肽组成，并确定它们在 分离顶体内的顶体水解酶。最后我们 将定义细胞骨架组件的蛋白质组成 限制在精子中段，并确定它是否在 将线粒体引导到形成中段 精子发生或维持线粒体分布 成熟的精子。完成这些具体目标将提供 关于镶嵌结构背后的机制的新数据 精子质膜，并提供所需的分子数据 具体受精事件的基础。