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婴猴和兔β-珠蛋白基因座控制区的完整序列:脱氧核糖核酸酶超敏位点核心区域之外的延伸序列及功能保守性

The complete sequences of the galago and rabbit beta-globin locus control regions: extended sequence and functional conservation outside the cores of DNase hypersensitive sites.

作者信息

Slightom J L, Bock J H, Tagle D A, Gumucio D L, Goodman M, Stojanovic N, Jackson J, Miller W, Hardison R

机构信息

Molecular Biology Unit 7242, Pharmacia & Upjohn, Inc., Kalamazoo, Michigan 49007, USA.

出版信息

Genomics. 1997 Jan 1;39(1):90-4. doi: 10.1006/geno.1996.4458.

Abstract

The locus control region (LCR) of mammalian beta-globin genes covers at least 17 kb at the 5' end of the gene cluster and has been implicated in chromatin domain opening, enhancement, and insulation from neighboring sequences. Functional dissection of the LCR has defined the minimal cores for four of the five major DNase hypersensitive sites (HSs) that mark this regulatory region. To examine fully the patterns of conserved sequences in the mammalian homologs to the beta-globin LCR, we determined the complete DNA sequence of the galago beta-globin LCR and completed previously unsequenced regions of the rabbit LCR. Simultaneous alignment of these sequences with the human, goat, and mouse LCRs revealed conserved sequences (phylogenetic footprints) detected using three largely independent methods. The most highly conserved segments are found both within the HS cores and in some but not all regions flanking the cores. These results argue for an extended pattern of well-conserved sequences, many of which lie outside the minimal cores, and we show that a key sequence required for domain opening by the region including HS3 maps about 1 kb 5' to the minimal core. Differential phylogenetic footprints, containing sequences conserved in nonhuman mammals but not in humans, are found primarily around HS3, consistent with some species-specific differences in function that may be important for differences in hemoglobin switching during development.

摘要

哺乳动物β-珠蛋白基因的基因座控制区(LCR)在基因簇的5'端覆盖至少17 kb,并且与染色质结构域开放、增强以及与相邻序列绝缘有关。对LCR的功能剖析已经确定了标记该调控区域的五个主要DNase超敏位点(HSs)中四个位点的最小核心。为了全面研究哺乳动物β-珠蛋白LCR同源物中的保守序列模式,我们确定了婴猴β-珠蛋白LCR的完整DNA序列,并完成了兔LCR先前未测序的区域。将这些序列与人类、山羊和小鼠的LCR同时比对,揭示了使用三种基本独立的方法检测到的保守序列(系统发育足迹)。在HS核心区域内以及某些但并非所有核心侧翼区域都发现了高度保守的片段。这些结果表明存在一种广泛的保守序列模式,其中许多位于最小核心之外,并且我们表明由包括HS3在内的区域进行结构域开放所需的关键序列位于最小核心5'端约1 kb处。主要在HS3周围发现了差异系统发育足迹,其中包含在非人类哺乳动物中保守但在人类中不保守的序列,这与某些物种特异性的功能差异一致,这些差异可能对发育过程中血红蛋白转换的差异很重要。

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