Genome-Wide Single-Molecule Analysis of Human Replication Kinetics - Diversity Supplement
人类复制动力学的全基因组单分子分析 - 多样性补充
基本信息
- 批准号:10402129
- 负责人:
- 金额:$ 1.72万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2018
- 资助国家:美国
- 起止时间:2018-08-23 至 2023-10-31
- 项目状态:已结题
- 来源:
- 关键词:Biological AssayBiologyCancer EtiologyCell Differentiation processChromatinChromosome StructuresChromosomesDNA Replication TimingDNA biosynthesisDNA replication forkDevelopmentDiagnosticEpigenetic ProcessEvolutionGenetic TranscriptionGenomeGenomic InstabilityHumanHuman GenomeKineticsLaboratoriesLeadLocationMalignant NeoplasmsMapsMetabolismMutationNoiseOpticsPatternPreventionRegulationReplication OriginResearchSignal TransductionSiteTechniquesTechnologyTimeTranscriptional RegulationWorkcell growthchromatin modificationgenome-wideinterestnew therapeutic targetpreventsingle moleculetool
项目摘要
PROJECT SUMMARY
The timing of DNA replication is a critical parameter of cellular growth. It correlates with
patterns of transcriptional regulation, chromatin modification, chromosome structure and
genome evolution. Furthermore, replication timing changes as cells differentiate, and
disruption of replication timing correlates with genome instability, suggesting an intimate
relation between replication timing and other important aspects of chromosome metabolism. A
major impediment to understand the regulation of replication timing in the human genome has
been the lack of robust assays for identifying the location and firing times of human replication
origins. Current approaches suffer from low signal-to-noise ratios and poor concordance
between independent laboratories. Moreover, ensemble techniques are unable to probe the
coordination of origin firing, a subject significant interest in the field, because it has been
proposed as a key factor in replication timing and efficiency. We propose to apply two new
high-throughput single-molecule approaches that we have developed—Optical Replication
Mapping and SMRT Repli-seq—to map replication origins and replication fork progression
across the human genome. We will use replication profiles that we obtain to develop
hypotheses about fundamental aspects of genome biology, such as such as how replication and
transcription are coordinated, if the location of replication termination sites are regulated and
how forks navigate difficult-to-replicate sequences. Successful completion of this work will
elucidate the regulation of replication timing across the human genome, allow for the
characterization of the sequence and epigenetic determinants for origin function, and provide
robust origin maps and replication profiles for others to use. Moreover, dissemination of this
technology will change the questions that biologists are able to ask about the regulation of DNA
replication timing and its repercussions in diverse fields, such as development, chromatin
biology, and epigenetics.
项目摘要
DNA复制的时间是细胞生长的关键参数。它与
转录调控模式、染色质修饰、染色体结构和
基因组进化此外,复制时间随着细胞分化而改变,
复制时间的中断与基因组的不稳定性相关,这表明一个亲密的
复制时间和染色体代谢的其他重要方面之间的关系。一
了解人类基因组复制时间调节的主要障碍是
一直缺乏可靠的检测方法来确定人类复制的位置和启动时间
起源.目前的方法存在信噪比低、一致性差的问题
在独立的实验室之间。此外,集成技术无法探测
起源射击的协调,在该领域中的一个重要兴趣的主题,因为它已经被
建议作为复制时间和效率的关键因素。我们建议采用两种新的
我们开发的高通量单分子方法-光学复制
映射和SMRT d-seq-映射复制起点和复制叉进展
在人类基因组中。我们将使用获得的复制配置文件来开发
关于基因组生物学基本方面的假设,例如复制和
如果复制终止位点的位置受到调节,
forks是如何导航难以复制的序列的。这项工作的顺利完成将
阐明整个人类基因组复制时间的调节,允许
表征的序列和表观遗传决定因素的起源功能,并提供
强大的起源图和复制谱供他人使用。此外,传播这种
技术将改变生物学家对DNA调控的疑问
复制时间及其在不同领域的影响,如发育,染色质
生物学和表观遗传学。
项目成果
期刊论文数量(6)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
f = m*a: A Framework for Investigating the Regulation of Replication Timing.
- DOI:10.3390/genes13020249
- 发表时间:2022-01-28
- 期刊:
- 影响因子:3.5
- 作者:Rhind N
- 通讯作者:Rhind N
Mapping replication forks, one replicon at a time.
- DOI:10.1016/j.molcel.2022.03.014
- 发表时间:2022-04-07
- 期刊:
- 影响因子:16
- 作者:Rhind, Nicholas
- 通讯作者:Rhind, Nicholas
Genome-wide mapping of human DNA replication by optical replication mapping supports a stochastic model of eukaryotic replication.
- DOI:10.1016/j.molcel.2021.05.024
- 发表时间:2021-07-15
- 期刊:
- 影响因子:16
- 作者:Wang W;Klein KN;Proesmans K;Yang H;Marchal C;Zhu X;Borrman T;Hastie A;Weng Z;Bechhoefer J;Chen CL;Gilbert DM;Rhind N
- 通讯作者:Rhind N
Short-term molecular consequences of chromosome mis-segregation for genome stability.
- DOI:10.1038/s41467-023-37095-7
- 发表时间:2023-03-11
- 期刊:
- 影响因子:16.6
- 作者:Garribba, Lorenza;De Feudis, Giuseppina;Martis, Valentino;Galli, Martina;Dumont, Marie;Eliezer, Yonatan;Wardenaar, Rene;Ippolito, Marica Rosaria;Iyer, Divya Ramalingam;Tijhuis, Andrea E.;Spierings, Diana C. J.;Schubert, Michael;Taglietti, Silvia;Soriani, Chiara;Gemble, Simon;Basto, Renata;Rhind, Nick;Foijer, Floris;Ben-David, Uri;Fachinetti, Daniele;Doksani, Ylli;Santaguida, Stefano
- 通讯作者:Santaguida, Stefano
The capacity of origins to load MCM establishes replication timing patterns.
- DOI:10.1371/journal.pgen.1009467
- 发表时间:2021-03
- 期刊:
- 影响因子:4.5
- 作者:Dukaj L;Rhind N
- 通讯作者:Rhind N
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NICHOLAS R RHIND其他文献
NICHOLAS R RHIND的其他文献
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{{ truncateString('NICHOLAS R RHIND', 18)}}的其他基金
The Mechanism of Cell Size Regulation - Administrative Supplement
细胞大小调节机制-行政补充
- 批准号:
10810077 - 财政年份:2020
- 资助金额:
$ 1.72万 - 项目类别:
The Mechanism of Cell Size Regulation - Administrative Supplement
细胞大小调节机制-行政补充
- 批准号:
10592224 - 财政年份:2020
- 资助金额:
$ 1.72万 - 项目类别:
Genome-Wide Single-Molecule Analysis of Human Replication Kinetics
人类复制动力学的全基因组单分子分析
- 批准号:
10221728 - 财政年份:2018
- 资助金额:
$ 1.72万 - 项目类别:
Genome-Wide Single-Molecule Analysis of Human Replication Kinetics
人类复制动力学的全基因组单分子分析
- 批准号:
9769068 - 财政年份:2018
- 资助金额:
$ 1.72万 - 项目类别:
Genome-Wide Single-Molecule Analysis of Replication Kinetics
复制动力学的全基因组单分子分析
- 批准号:
8969943 - 财政年份:2015
- 资助金额:
$ 1.72万 - 项目类别:
Genome-Wide Single-Molecule Analysis of Replication Kinetics
复制动力学的全基因组单分子分析
- 批准号:
9145244 - 财政年份:2015
- 资助金额:
$ 1.72万 - 项目类别:
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