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多能性与分化的人类细胞中基因组复制进程的发育变化。

Developmental Changes in Genome Replication Progression in Pluripotent versus Differentiated Human Cells.

机构信息

Cell Biology and Epigenetics, Department of Biology, Technical University of Darmstadt, 64287 Darmstadt, Germany.

Center for Tissue Engineering and Stem Cell Research, Guizhou Medical University, Guiyang 550004, China.

出版信息

Genes (Basel). 2024 Feb 27;15(3):305. doi: 10.3390/genes15030305.

Abstract

DNA replication is a fundamental process ensuring the maintenance of the genome each time cells divide. This is particularly relevant early in development when cells divide profusely, later giving rise to entire organs. Here, we analyze and compare the genome replication progression in human embryonic stem cells, induced pluripotent stem cells, and differentiated cells. Using single-cell microscopic approaches, we map the spatio-temporal genome replication as a function of chromatin marks/compaction level. Furthermore, we mapped the replication timing of subchromosomal tandem repeat regions and interspersed repeat sequence elements. Albeit the majority of these genomic repeats did not change their replication timing from pluripotent to differentiated cells, we found developmental changes in the replication timing of rDNA repeats. Comparing single-cell super-resolution microscopic data with data from genome-wide sequencing approaches showed comparable numbers of replicons and large overlap in origins numbers and genomic location among developmental states with a generally higher origin variability in pluripotent cells. Using ratiometric analysis of incorporated nucleotides normalized per replisome in single cells, we uncovered differences in fork speed throughout the S phase in pluripotent cells but not in somatic cells. Altogether, our data define similarities and differences on the replication program and characteristics in human cells at different developmental states.

摘要

DNA 复制是一个基本的过程,确保了细胞每次分裂时基因组的维持。这在早期发育中尤为重要,此时细胞大量分裂,后来形成整个器官。在这里,我们分析和比较了人类胚胎干细胞、诱导多能干细胞和分化细胞中的基因组复制进展。我们使用单细胞显微镜方法,根据染色质标记/压缩水平绘制时空基因组复制图谱。此外,我们还绘制了亚染色体串联重复区域和散在重复序列元件的复制时间。尽管这些基因组重复中的大多数在多能到分化细胞的过程中没有改变它们的复制时间,但我们发现 rDNA 重复的复制时间存在发育变化。将单细胞超分辨率显微镜数据与全基因组测序方法的数据进行比较,显示在不同发育状态下复制子的数量相当,起始点的数量和基因组位置有很大的重叠,并且多能细胞中的起始点变异性通常更高。使用单细胞中每个复制体整合核苷酸的比例分析,我们发现多能细胞中 S 期叉速度存在差异,但体细胞中不存在这种差异。总的来说,我们的数据定义了人类细胞在不同发育状态下复制程序和特征的相似性和差异。

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