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CIS-ACTING DETERMINANTS OF REPLICATION TIMING

复制时间的 CIS 作用决定因素

基本信息

批准号：
6329105
负责人：
JOEL A HUBERMAN
金额：
$ 34.53万
依托单位：
ROSWELL PARK CANCER INSTITUTE CORP
依托单位国家：
美国
项目类别：
财政年份：
1999
资助国家：
美国
起止时间：
1999-12-27 至 2001-11-30
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/6329105
关键词：
DNA binding protein DNA replication DNA replication origin Saccharomyces cerevisiae carcinogenesis cell cycle fungal genetics genetic regulatory element neoplasm /cancer genetics transcription factor

项目摘要

One of the cellular alterations required for development of cancer is genomic instability, a term that describes a collection of pathways all leading to increase frequency of gene mutation and altered patterns of gene expression. Among the mechanisms causing genomic instability are chromosome breakage, gene amplification, and changes in levels of gene expression. The latter are frequently associated with changes in gene methylation status. All of the mechanisms have been correlated with changes in replication timing, and it is possible that in some cases changes in replication timing may be the primary cause of these phenomena. So far it has been difficult to evaluate the role of changes in replication timing in cancer development, because so little is known about the mechanisms controlling replication timing. The experiments proposed in this application are intended to provide an entry point into understanding the mechanism of replication timing. We intend to take advantage of previous work in our laboratory and others which shows that ARS301, and 94-bp stretch of chromosomal DNA in the budding yeast, Saccharomyces cerevisiae, is capable of serving as a replication origin but differs from previously studied origins in being inherently late replicating. It is also of interest that ARS301 is an important part of a transcriptional silencer element, and transcriptionally repressed genes tend to replicate late. We intend to determine whether the late firing of ARS301 is due to the presence of late-replication-determining sequences or to the absence of early-replication determining sequences within it. In either case, we shall employ standard mutagenic techniques followed by replication timing tests to narrow down and characterize the responsible cis-acting sequences, so that they can be used to help identify the DNA-binding proteins that are responsible for controlling replication timing.

癌症发展所需的细胞改变之一是基因组不稳定性，这一术语描述了所有导致基因突变频率增加和基因表达模式改变的途径的集合。引起基因组不稳定的机制包括染色体断裂、基因扩增和基因表达水平的变化。后者通常与基因甲基化状态的变化有关。所有的机制都与复制时间的变化相关，在某些情况下，复制时间的变化可能是这些现象的主要原因。到目前为止，很难评估复制时间的变化在癌症发展中的作用，因为对控制复制时间的机制知之甚少。本申请中提出的实验旨在提供理解复制定时机制的切入点。我们打算利用以前的工作在我们的实验室和其他人表明，ARS 301，和94 bp的染色体DNA延伸的芽殖酵母，酿酒酵母，是能够作为一个复制起点，但不同于以前研究的起源是固有的晚期复制。同样有趣的是，ARS301是转录沉默元件的重要组成部分，并且转录抑制的基因往往复制较晚。我们打算确定ARS 301的迟发性是由于其内存在迟发性复制决定序列还是缺乏早发性复制决定序列。无论哪种情况，我们都将采用标准诱变技术，然后进行复制定时试验，以缩小并表征负责的顺式作用序列，因此它们可以用来帮助识别负责控制复制时间的DNA结合蛋白。