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人类和鼠类布鲁顿酪氨酸激酶基因座的大规模比较序列分析揭示了保守的调控结构域。

Large-scale comparative sequence analysis of the human and murine Bruton's tyrosine kinase loci reveals conserved regulatory domains.

作者信息

Oeltjen J C, Malley T M, Muzny D M, Miller W, Gibbs R A, Belmont J W

机构信息

Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Genome Res. 1997 Apr;7(4):315-29. doi: 10.1101/gr.7.4.315.

Abstract

Large-scale genomic DNA sequencing of orthologous and paralogous loci in different species should contribute to a basic understanding of the evolution of both the protein-coding regions and noncoding regulatory elements. We compared 93 kb of human sequence to 89 kb of mouse sequence in the Bruton's tyrosine kinase (BTK) region. In addition to showing the conservation of both position and orientation of the five functionally unrelated genes in the region (BTK, alpha-D-galactosidase A, L44L, FTP-3, and FCI-12), the comparison revealed conservation of clusters of noncoding sequence flanking the first exon of each gene. Furthermore, in the sequence comparison at the BTK locus, the conservation of clusters of noncoding sequence extends throughout the locus; the noncoding sequence is more highly conserved in the BTK locus in comparison to the flanking loci. This suggests a correlation with the complex developmental regulation of expression of btk. To determine whether a highly conserved 3.5-kb segment flanking the first exon of BTK contains transcriptional regulatory signals, we tested various portions of the segment for promoter and expression activity in several appropriate cell lines. The results demonstrate the contribution of the conserved region flanking the first exon to the cell lineage-specific expression pattern of btk. These data show the usefulness of large scale sequence comparisons to focus investigation on regions of noncoding sequence that play essential roles in complex gene regulation.

摘要

对不同物种直系同源和旁系同源基因座进行大规模基因组DNA测序,应有助于从基础层面理解蛋白质编码区和非编码调控元件的进化。我们将布鲁顿酪氨酸激酶(BTK)区域的93 kb人类序列与89 kb小鼠序列进行了比较。除了显示该区域五个功能不相关基因(BTK、α-D-半乳糖苷酶A、L44L、FTP-3和FCI-12)在位置和方向上的保守性外,比较还揭示了每个基因第一个外显子侧翼非编码序列簇的保守性。此外,在BTK基因座的序列比较中,非编码序列簇的保守性延伸至整个基因座;与侧翼基因座相比,BTK基因座中的非编码序列保守性更高。这表明其与btk表达的复杂发育调控相关。为了确定BTK第一个外显子侧翼高度保守的3.5 kb片段是否包含转录调控信号,我们在几种合适的细胞系中测试了该片段的各个部分的启动子和表达活性。结果证明了第一个外显子侧翼保守区域对btk细胞谱系特异性表达模式的作用。这些数据表明大规模序列比较有助于将研究重点聚焦于在复杂基因调控中起关键作用的非编码序列区域。

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