DNA Replication Initiation Sites in Mammalian Cells

哺乳动物细胞中的 DNA 复制起始位点

• 批准号: 7989249
• 负责人: CARL L SCHILDKRAUT
• 金额: $ 7.37万
• 依托单位: ALBERT EINSTEIN COLLEGE OF MEDICINE
• 依托单位国家: 美国
• 财政年份: 2009
• 资助国家: 美国
• 起止时间: 2009-12-17 至 2011-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7989249
• 关键词: Affect; Architecture; B cell differentiation; B-Cell Development; Cell Lineage; Cell Nucleus; Cells; Chimeric Proteins; Chromatin; Chromatin Structure; Chromosome Structures; DNA; DNA biosynthesis; Development; Engineering; Epigenetic Process; Exhibits; Gene Expression Regulation; Gene Silencing; Genes; Genetic; Genetic Recombination; Genomics; Heavy-Chain Immunoglobulins; Heterochromatin; Higher Order Chromatin Structure; Histones; IGH@ gene cluster; Knock-in Mouse; Location; Mammalian Cell; Mediating; Modification; Mus; Nuclear; Phase; Play; Positioning Attribute; Proteins; Regulation; Replication Initiation; Replication Origin; Resolution; Role; Saccharomyces; Site; Staging; System; Time; Transcription Coactivator; chromatin modification; embryonic stem cell; flexibility; heterochromatin-specific nonhistone chromosomal protein HP-1; histone modification; initiation site of DNA replication; mouse model; novel strategies; single molecule

DESCRIPTION (provided by applicant): We will determine the effects of epigenetic modifications on replication origin activation and silencing within the immunoglobulin heavy chain (Igh) locus. We have established the location of many replication initiation sites throughout the Igh locus and have determined how they change during B cell development. We will now focus on modifying the Igh locus in murine ES and proB cells to understand how chromatin modifications associated with active and inactive chromatin domains affect the activation of initiation domains of DNA replication within the locus. For these studies, we have engineered ES cells to contain an exchangeable cassette at two sites within the Igh locus. Using these ES cells, we propose to target to these sites, specific proteins that modify chromatin structure and have histone modifying activities. We already have demonstrated that we can tether a transcriptional activator to Gal4 target sites that we have inserted in the Igh region, resulting in histone modifications and the activation of a previously silent gene. We will also modify the locus by inserting much larger targeting sequences containing frequent recognition sites. We will determine the effects of epigenetic modifications on replication initiation, the direction and rate of replication fork progression and on the time in S phase during which the Igh and flanking regions replicate. We will use two novel approaches that we have recently developed: single molecule analysis of replicated DNA (SMARD) and high-resolution timing array (HRTA) analysis. The role of higher order chromosome structure in regulating replication will also be investigated. We will use the ES cells with the Igh locus, modified by cassette exchange, to produce chimeric mice and homozygous knock-in mice to determine the effect on B cell development of epigenetic changes in the Igh locus. We will characterize these changes using the detailed information we have already obtained about replication initiation and fork direction, and nuclear organization of the Igh locus at different stages of normal development in the B lineage.

描述（由申请方提供）：我们将确定表观遗传修饰对免疫球蛋白重链（Igh）基因座内复制起点激活和沉默的影响。我们已经确定了许多复制起始位点在整个免疫球蛋白基因座的位置，并确定了它们在B细胞发育过程中的变化。现在，我们将集中在修改小鼠ES和proB细胞中的Igh基因座，以了解与活性和非活性染色质结构域相关的染色质修饰如何影响基因座内DNA复制起始结构域的激活。对于这些研究，我们已经改造了ES细胞，使其在Igh基因座内的两个位点含有可交换盒。使用这些ES细胞，我们建议靶向这些位点，特定的蛋白质，修改染色质结构，并具有组蛋白修饰活性。我们已经证明，我们可以将转录激活因子拴在我们插入Igh区域的Gal4靶位点上，导致组蛋白修饰和先前沉默基因的激活。我们还将通过插入含有频繁识别位点的更大的靶向序列来修饰基因座。 我们将确定表观遗传修饰对复制起始、复制叉进展的方向和速率以及Igh和侧翼区域复制的S期时间的影响。我们将使用我们最近开发的两种新方法：复制DNA的单分子分析（SMARD）和高分辨率定时阵列（HRTA）分析。高阶染色体结构在调节复制中的作用也将被研究。 我们将使用通过盒交换修饰的具有Igh基因座的ES细胞来产生嵌合小鼠和纯合敲入小鼠，以确定Igh基因座中的表观遗传变化对B细胞发育的影响。我们将使用我们已经获得的关于复制起始和分叉方向以及B谱系正常发育不同阶段Igh基因座的核组织的详细信息来表征这些变化。