蛋白质组
蛋白质组学
酵母
钙调蛋白
生物
蛋白质阵列分析
DNA微阵列
人类蛋白质组计划
计算生物学
酿酒酵母
蛋白质微阵列
生物化学
酶
基因
基因表达
作者
Heng Zhu,Metin Bilgin,Rhonda Bangham,David A. Hall,Antonio Casamayor,Paul Bertone,Ning Lan,Ronald Jansen,Scott Bidlingmaier,Thomas D. Houfek,Tom M. Mitchell,Perry L. Miller,Ralph A. Dean,Mark Gerstein,M Snyder
出处
期刊:Science
[American Association for the Advancement of Science]
日期:2001-09-14
卷期号:293 (5537): 2101-2105
被引量:1864
标识
DOI:10.1126/science.1062191
摘要
To facilitate studies of the yeast proteome, we cloned 5800 open reading frames and overexpressed and purified their corresponding proteins. The proteins were printed onto slides at high spatial density to form a yeast proteome microarray and screened for their ability to interact with proteins and phospholipids. We identified many new calmodulin- and phospholipid-interacting proteins; a common potential binding motif was identified for many of the calmodulin-binding proteins. Thus, microarrays of an entire eukaryotic proteome can be prepared and screened for diverse biochemical activities. The microarrays can also be used to screen protein-drug interactions and to detect posttranslational modifications.
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