Analysis of Cdc20-Mad2 in spindle checkpoint signalling

Cdc20-Mad2 在纺锤体检查点信号传导中的分析

• 批准号: 6948897
• 负责人: CLINTON L COPELAND
• 金额: $ 2.78万
• 依托单位: UNIVERSITY OF VIRGINIA
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-09-29 至 2007-09-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6948897
• 关键词: biological signal transduction; cell cycle; cell cycle proteins; cell growth regulation; centromere; chromatin immunoprecipitation; fluorescence recovery after photobleaching; genetic screening; mitotic spindle apparatus; predoctoral investigator; protein binding; protein localization; protein protein interaction; protein structure function; temperature sensitive mutant

It has been well-documented that Mad1, Mad2, and Cdc20 have important roles in the spindle checkpoint in mitosis. In mammalian cells, Mad1 is responsible for Mad2 localization at the kinetochore. The Mad1-Mad2 complex has been shown to have a 'seat belt' binding conformation. This complex can also remain stable in 4m urea or 2M NaCI. Regardless of this extremely stable interaction, there is a Mad2 switch between Mad1 and Cdc20 at the kinetochore. In the presence of Mad2, Cdc20 is not able to activate the anaphase-promoting complex (APC). This inhibition causes cells to remain arrested in metaphase. We will use a collection of four cdc20 mutants to analyze the mechanism of Cdc20-Mad2 inhibition of the cell cycle in mitosis. Three of the cdc20 mutants are deficient in Mad2 binding, and the other has an increased affinity for Mad2. These mutants will also be used to identify other genes involved in the Mad2 switch between Mad1 and Cdc20. Another aim of this proposal is to identify genes involved in the tension-sensing aspect of the spindle checkpoint. We will use temperature sensitive mcd1-1 mutants to screen for genes involved in this process. Mcd1 is a member of the cohesion complex that is essential for sister chromatid association.

有充分证据表明，Mad1、Mad2和Cdc20在有丝分裂的纺锤体检查点中起重要作用。在哺乳动物细胞中，Mad1负责Mad2在着丝点的定位。Mad1-Mad2配合物已被证明具有“安全带”结合构象。该络合物在4m尿素或2M NaCI中也能保持稳定。不管这种极其稳定的相互作用如何，在着丝点上Mad1和Cdc20之间存在Mad2开关。在Mad2存在的情况下，Cdc20不能激活后期促进复合体（APC）。这种抑制使细胞在中期保持停滞状态。我们将