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通过高分辨率动态染色体显带分析S期的DNA复制。

Analysis of DNA replication during S-phase by means of dynamic chromosome banding at high resolution.

作者信息

Drouin R, Lemieux N, Richer C L

机构信息

Département d'Anatomie, Faculté de Médecine, Université de Montréal, Québec, Canada.

出版信息

Chromosoma. 1990 Aug;99(4):273-80. doi: 10.1007/BF01731703.

Abstract

The characteristic patterns of dynamic banding (replication banding) were analysed. Extremely high resolution (850 to 1,250 bands per genome) G- and R-band patterns were obtained after 5-bromo-2'-deoxyuridine (BrdUrd) incorporation either during the early or the late S-phase. We synchronized human lymphocytes with high concentrations of thymidine or BrdUrd as blocking agents, followed by low concentrations of BrdUrd or thymidine respectively as releasing agents, and obtained R- or G-band patterns respectively. The dynamic R- and G-band patterns were complementary for all chromosomes, even for the late-replicating X chromosome. There was no overlapping and every part of each chromosome was positively stained by one of the two banding procedures. The complementarity of the two patterns shows that both high thymidine and high BrdUrd concentrations blocked S-phase progression near the R-band to G-band replication transition in the middle of S-phase. Some bands of the inactive X chromosome replicate before this transition concurrently with R-band replication. The 48 different telomeric regions could be classified into 5 distinct morphotypes based upon the distribution of early and late-replicating DNA in each telomeric region. The dynamic band patterns are particularly useful for the study of the structural and physiological organization of chromosomes at high resolution and should prove invaluable for assessing the replication behavior of rearranged chromosomes.

摘要

分析了动态显带(复制显带)的特征模式。在S期早期或晚期掺入5-溴-2'-脱氧尿苷(BrdUrd)后,获得了极高分辨率(每个基因组850至1250条带)的G带和R带模式。我们用高浓度的胸苷或BrdUrd作为阻断剂同步人淋巴细胞,随后分别用低浓度的BrdUrd或胸苷作为释放剂,分别获得了R带或G带模式。动态R带和G带模式对所有染色体都是互补的,即使对于晚复制的X染色体也是如此。没有重叠,并且每条染色体的每个部分都被两种显带程序之一阳性染色。两种模式的互补性表明,高胸苷浓度和高BrdUrd浓度都在S期中期阻断了R带至G带复制转变附近的S期进程。失活X染色体的一些带在这种转变之前与R带复制同时进行复制。根据每个端粒区域中早期和晚期复制DNA的分布,48个不同的端粒区域可分为5种不同的形态类型。动态带模式对于高分辨率研究染色体的结构和生理组织特别有用,并且对于评估重排染色体的复制行为应该是非常有价值的。

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