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Changes in primary DNA sequence complexity influence the phenotypic consequences of mutations in human gene regulatory regions.

机译:主要DNA序列复杂性的变化会影响人类基因调控区域突变的表型后果。

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No general rules have been proposed to account for the functional consequences of gene regulatory mutations. In a first attempt to establish the nature of such rules, an analysis was performed of the DNA sequence context of 153 different single base-pair substitutions in the regulatory regions of 65 different human genes underlying inherited disease. Use of a recently proposed measure of DNA sequence complexity (taking into account the level of structural repetitiveness of a DNA sequence, rather than simply the oligonucleotide composition) has served to demonstrate that the concomitant change in local DNA sequence complexity surrounding a substituted nucleotide is related to the likelihood of a regulatory mutation coming to clinical attention. Mutations that led to an increase in complexity exhibited higher odds ratios in favour of pathological consequences than mutations that led to a decrease or left complexity unchanged. This relationship, however, was discernible only for pyrimidine-to-purine transversions. Odds ratios for other types of substitution were not found to be significantly associated with local changes in sequence complexity, even though a trend similar to that observed for Y-->R transversions was also apparent for transitions. These findings suggest that the maintenance of a defined level of DNA sequence complexity, or at least the avoidance of an increase in sequence complexity, is a critical prerequisite for the function of gene regulatory regions.
机译:尚未提出一般规则来解释基因调节突变的功能后果。在首次尝试确定此类规则的性质时,对65种不同遗传基因的人类基因调控区域中的153种不同单碱基对取代的DNA序列进行了分析。使用最近提出的DNA序列复杂性测量方法(考虑到DNA序列的结构重复性水平,而不是简单地寡核苷酸组成)已经证明了围绕取代核苷酸的局部DNA序列复杂性的伴随变化是相关的引起临床关注的调节突变的可能性。与导致复杂性降低或使复杂性保持不变的突变相比,导致复杂性增加的突变显示出更高的优势比,有利于病理结果。然而,仅对于嘧啶至嘌呤的转化而言,这种关系是可辨别的。没有发现其他类型取代的几率与序列复杂性的局部变化显着相关,尽管对于转变而言,与Y-> R转变所观察到的趋势相似的趋势也是如此。这些发现表明,维持确定水平的DNA序列复杂性,或至少避免避免序列复杂性的增加,是基因调节区功能的关键前提。

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