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Structural and conformational changes induced by missense variants in the zinc finger domains of GATA3 involved in breast cancer

机译:乳腺癌锌指域的锌指域中的畸形变种诱导的结构和构象变化

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摘要

Breast cancer (BC) is the main cancer in women having multiple receptor based tumour subtypes. Large scale genome sequencing studies of BC have identified several genes among which GATA3 is reported as a highly mutated gene followed by TP53 and PIK3CA. GATA3 is a crucial transcription factor, and was initially identified as a DNA-binding protein involved in the regulation of immune cell functions. Different missense mutations in the region of the DNA-binding domain of GATA3 are associated with BC and other neoplastic disorders. In this study, computational based approaches have been exploited to reveal associations of various mutations on structure, stability, conformation and function of GATA3. Our findings have suggested that, all analysed missense mutations were deleterious and highly pathogenic in nature. A molecular dynamics simulation study showed that all mutations led to structural destabilisation by reducing protein globularity and flexibility, by altering secondary structural configuration and decreasing protein ligand stability. Essential dynamics analysis indicated that mutations in GATA3 decreased protein mobility and increased its conformational instability. Furthermore, residue network analysis showed that the mutations affected the signal transduction of important residues that potentially influenced GATA3-DNA binding. The present study highlights the importance of different variants of GATA3 which have potential impact on neoplastic progression in breast cancer and may facilitate development of precise and personalized therapeutics.
机译:乳腺癌(BC)是患有多种受体基肿瘤亚型的女性的主要癌症。 BC的大规模基因组测序研究已经鉴定了几种基因,其中GATA3被报告为高度突变的基因,然后是TP53和PIK3CA。 GATA3是关键转录因子,最初被鉴定为参与免疫细胞功能调节的DNA结合蛋白。 GATA3的DNA结合结构域的区域中的不同的畸形突变与BC和其他肿瘤疾病有关。在本研究中,已经利用计算基于的方法来揭示各种突变对GATA3的结构,稳定性,构象和功能的关联。我们的研究结果表明,所有分析的畸形突变都是有害和高度致病性的。分子动力学模拟研究表明,通过改变二次结构配置和降低蛋白质配体稳定性,所有突变通过降低蛋白质球状和柔韧性而导致结构稳定性。基本动态分析表明,GATA3中的突变降低了蛋白质迁移率并增加了其构象不稳定性。此外,残留网络分析表明,该突变影响了可能影响GATA3-DNA结合的重要残留的信号转导。本研究强调了GATA3不同变体对乳腺癌肿瘤进展产生潜在影响的重要性,并有助于开发精确和个性化的治疗方法。

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