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Translational Database Selection and Multiplexed Sequence Capture for Up Front Filtering of Reliable Breast Cancer Biomarker Candidates

机译:翻译数据库选择和多路复用序列捕获,可对可靠的乳腺癌生物标志物候选对象进行预先过滤

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摘要

Biomarker identification is of utmost importance for the development of novel diagnostics and therapeutics. Here we make use of a translational database selection strategy, utilizing data from the Human Protein Atlas (HPA) on differentially expressed protein patterns in healthy and breast cancer tissues as a means to filter out potential biomarkers for underlying genetic causatives of the disease. DNA was isolated from ten breast cancer biopsies, and the protein coding and flanking non-coding genomic regions corresponding to the selected proteins were extracted in a multiplexed format from the samples using a single DNA sequence capture array. Deep sequencing revealed an even enrichment of the multiplexed samples and a great variation of genetic alterations in the tumors of the sampled individuals. Benefiting from the upstream filtering method, the final set of biomarker candidates could be completely verified through bidirectional Sanger sequencing, revealing a 40 percent false positive rate despite high read coverage. Of the variants encountered in translated regions, nine novel non-synonymous variations were identified and verified, two of which were present in more than one of the ten tumor samples.
机译:生物标志物的鉴定对于新型诊断和治疗方法的发展至关重要。在这里,我们利用翻译数据库选择策略,利用来自人类蛋白质图谱(HPA)的健康和乳腺癌组织中差异表达的蛋白质模式的数据,作为筛选出潜在的疾病遗传原因的生物标志物的手段。从十个乳腺癌活检组织中分离出DNA,并使用单个DNA序列捕获阵列以多重形式从样品中提取了与所选蛋白质相对应的蛋白质编码和侧翼非编码基因组区域。深度测序揭示了多重样本的均匀富集,以及样本个体肿瘤中遗传改变的巨大变化。得益于上游过滤方法,最终的生物标志物候选集可以通过双向Sanger测序进行完全验证,尽管读取覆盖率很高,但仍有40%的假阳性率。在翻译区域中遇到的变体中,鉴定并验证了9个新的非同义变体,其中两个存在于十个肿瘤样本中的一个以上。

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