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B 细胞定型过程中免疫球蛋白重链基因座内的 DNA 复制调控。

Regulation of DNA replication within the immunoglobulin heavy-chain locus during B cell commitment.

机构信息

Department of Oncology, Montefiore Medical Center, Moses Division, Bronx, New York, USA.

出版信息

PLoS Biol. 2012 Jul;10(7):e1001360. doi: 10.1371/journal.pbio.1001360. Epub 2012 Jul 10.

Abstract

The temporal order of replication of mammalian chromosomes appears to be linked to their functional organization, but the process that establishes and modifies this order during cell differentiation remains largely unknown. Here, we studied how the replication of the Igh locus initiates, progresses, and terminates in bone marrow pro-B cells undergoing B cell commitment. We show that many aspects of DNA replication can be quantitatively explained by a mechanism involving the stochastic firing of origins (across the S phase and the Igh locus) and extensive variations in their firing rate (along the locus). The firing rate of origins shows a high degree of coordination across Igh domains that span tens to hundreds of kilobases, a phenomenon not observed in simple eukaryotes. Differences in domain sizes and firing rates determine the temporal order of replication. During B cell commitment, the expression of the B-cell-specific factor Pax5 sharply alters the temporal order of replication by modifying the rate of origin firing within various Igh domains (particularly those containing Pax5 binding sites). We propose that, within the Igh C(H)-3'RR domain, Pax5 is responsible for both establishing and maintaining high rates of origin firing, mostly by controlling events downstream of the assembly of pre-replication complexes.

摘要

哺乳动物染色体的复制时序似乎与其功能组织有关,但在细胞分化过程中建立和修改这种顺序的过程在很大程度上仍不清楚。在这里,我们研究了在经历 B 细胞承诺的骨髓前 B 细胞中,Igh 基因座的复制是如何起始、进展和终止的。我们表明,通过涉及随机起始原点(跨越 S 期和 Igh 基因座)和其起始频率的广泛变化(沿基因座)的机制,可以定量解释许多 DNA 复制方面。起源的点火率在跨越数十到数百千碱基的 Igh 结构域之间表现出高度的协调性,这在简单的真核生物中是观察不到的。域大小和点火率的差异决定了复制的时间顺序。在 B 细胞承诺期间,B 细胞特异性因子 Pax5 的表达通过改变各种 Igh 结构域内的起源点火率(特别是那些包含 Pax5 结合位点的结构域),极大地改变了复制的时间顺序。我们提出,在 Igh C(H)-3'RR 结构域内,Pax5 负责建立和维持高的原点点火率,主要通过控制复制前复合物组装下游的事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0d2/3393677/37d5ea8bed6b/pbio.1001360.g001.jpg

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