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Structure-based predictions broadly link transcription factor mutations to gene expression changes in cancers

机译:基于结构的预测将转录因子突变与癌症中的基因表达变化广泛关联

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Thousands of unique mutations in transcription factors (TFs) arise in cancers, and the functional and biological roles of relatively few of these have been characterized. Here, we used structure-based methods developed specifically for DNA-binding proteins to systematically predict the consequences of mutations in several TFs that are frequently mutated in cancers. The explicit consideration of protein-DNA interactions was crucial to explain the roles and prevalence of mutations in TP53 and RUNX1 in cancers, and resulted in a higher specificity of detection for known p53-regulated genes among genetic associations between TP53 genotypes and genome-wide expression in The Cancer Genome Atlas, compared to existing methods of mutation assessment. Biophysical predictions also indicated that the relative prevalence of TP53 missense mutations in cancer is proportional to their thermodynamic impacts on protein stability and DNA binding, which is consistent with the selection for the loss of p53 transcriptional function in cancers. Structure and thermodynamics-based predictions of the impacts of missense mutations that focus on specific molecular functions may be increasingly useful for the precise and large-scale inference of aberrant molecular phenotypes in cancer and other complex diseases.
机译:成千上万的转录因子(TFs)独特突变发生于癌症中,并且其中相对少数的功能和生物学作用已得到表征。在这里,我们使用了专门为DNA结合蛋白开发的基于结构的方法,以系统地预测在癌症中经常突变的几种TF中突变的后果。蛋白质-DNA相互作用的明确考虑对于解释TP53和RUNX1突变在癌症中的作用和普遍性至关重要,并导致在TP53基因型和全基因组表达之间的遗传关联中检测已知p53调控基因的特异性更高。与现有的突变评估方法进行了比较。生物物理预测还表明,癌症中TP53错义突变的相对患病率与其对蛋白质稳定性和DNA结合的热力学影响成正比,这与癌症中p53转录功能丧失的选择是一致的。基于结构和热力学的,针对特定分子功能的错义突变影响的预测,可能对于癌症和其他复杂疾病中异常分子表型的精确和大规模推论越来越有用。

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