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Ice-COLD-PCR enables rapid amplification and robust enrichment for low-abundance unknown DNA mutations

机译:Ice-COLD-PCR可实现快速扩增和强大的富集,以实现低丰度未知DNA突变

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摘要

Identifying low-abundance mutations within wild-type DNA is important in several fields of medicine, including cancer, prenatal diagnosis and infectious diseases. However, utilizing the clinical and diagnostic potential of rare mutations is limited by sensitivity of the molecular techniques employed, especially when the type and position of mutations are unknown. We have developed a novel platform that incorporates a synthetic reference sequence within a polymerase chain reaction (PCR) reaction, designed to enhance amplification of unknown mutant sequences during COLD-PCR (CO-amplification at Lower Denaturation temperature). This new platform enables an Improved and Complete Enrichment (ice-COLD-PCR) for all mutation types and eliminates shortcomings of previous formats of COLD-PCR. We evaluated ice-COLD-PCR enrichment in regions of TP53 in serially diluted mutant and wild-type DNA mixtures. Conventional-PCR, COLD-PCR and ice-COLD-PCR amplicons were run in parallel and sequenced to determine final mutation abundance for a range of mutations representing all possible single base changes. Amplification by ice-COLD-PCR enriched all mutation types and allowed identification of mutation abundances down to 1%, and 0.1% by Sanger sequencing or pyrosequencing, respectively, surpassing the capabilities of other forms of PCR. Ice-COLD-PCR will help elucidate the clinical significance of low-abundance mutations and our understanding of cancer origin, evolution, recurrence-risk and treatment diagnostics.
机译:鉴定野生型DNA中的低丰度突变在许多医学领域都很重要,包括癌症,产前诊断和传染病。但是,利用罕见​​突变的临床和诊断潜力受到所用分子技术的敏感性的限制,特别是当突变的类型和位置未知时。我们已经开发了一种新型平台,该平台在聚合酶链式反应(PCR)反应中纳入了合成参考序列,旨在增强COLD-PCR(较低变性温度下的CO扩增)过程中未知突变序列的扩增。这个新平台可为所有突变类型提供改良和完全富集(ice-COLD-PCR),并消除了以前COLD-PCR格式的缺点。我们评估了连续稀释的突变体和野生型DNA混合物中TP53区域的ice-COLD-PCR富集。并行运行常规PCR,COLD-PCR和ice-COLD-PCR扩增子并进行测序,以确定代表所有可能的单碱基变化的一系列突变的最终突变丰度。通过ice-COLD-PCR进行的扩增丰富了所有突变类型,并通过Sanger测序或焦磷酸测序分别鉴定了低至1%和0.1%的突变丰度,从而超过了其他形式的PCR功能。 Ice-COLD-PCR将有助于阐明低丰度突变的临床意义,以及我们对癌症起源,演变,复发风险和治疗诊断的理解。

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