结直肠癌患者粪便DNA的下一代测序突变-文献综述和我们使用该方法的经验

O. Youssef, V. Sarhadi, L. Lehtimäki, Milja Tikkanen, A. Kokkola, P. Puolakkainen, G. Armengol, S. Knuutila
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引用次数: 1

摘要

众所周知,结直肠癌是一种涉及多阶段癌变(增生-腺瘤-癌-转移癌)的疾病。它也是一种治疗上重要的驱动突变(特别是在EGFR信号通路中)已被确定的疾病。由于基因突变可以作为良好的诊断和预测标记,因此在疾病的早期阶段可靠地检测它们以及在治疗效果的随访中至关重要。从活检的肿瘤组织中提取常用的福尔马林固定石蜡包埋(FFPE)标本存在一个根本问题,即在疾病的早期阶段或治疗期间不太可能获得突变分析的材料。因此,最近已尝试从血浆/血清或粪便标本中确定可靠的标记物。特别是,非侵入性粪便标本被推测可以代表正在进行的肿瘤发生情况,因此可以在患者的随访中用于评估治疗效果。本文的主要目的是首先回顾从粪便标本中提取的细胞中研究DNA基因组改变的关键方法要点,其次回顾与生物标志物筛选相关的结果及其治疗意义。进一步的目的是通过关注胃肠道肿瘤患者粪便标本的下一代测序所固有的问题来展示我们的新发现。尽管我们论文的重点是粪便标本中的人类基因组变化,但在我们的“未来方面”章节中,我们也讨论了细菌谱及其与基因组突变可能的相互作用。
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Mutations by Next Generation Sequencing in Stool DNA from Colorectal Carcinoma Patients - A Literature Review and our Experience with this Methodology
It is well-known that colorectal carcinoma is a disease involving multistep carcinogenesis (hyperplasia-adenoma-carcinoma-metastasizing carcinoma). It is also a disease where therapeutically important driver mutations (especially in the EGFR signaling pathway) have been identified. Since genetic mutations can serve as good diagnostic and predictive markers, their reliable detection in the early stages of the disease and also in the follow-up of treatment efficacy is crucial. There is a fundamental problem encountered with the commonly used formalin-fixed paraffin-embedded (FFPE) specimens from biopsied tumor tissue i.e. it is unlikely that the material for the mutation analysis will be available in either the early stage of the disease or during the treatment period. Therefore recently attempts have been made to identify reliable markers from plasma/serum or from stool specimens. In particular, non-invasive stool specimens have been speculated to represent the situation of ongoing tumorigenesis and thus they can be used to assess treatment efficacy in the follow-up of the patient. The key aims of this paper are firstly, to review the key methodological points when studying genomic alterations in DNA extracted from cells in stool specimens, and secondly, to review results related to biomarker screening and their therapeutic importance. A further aim is to present our new findings by focusing on the issues inherent in Next Generation Sequencing of stool specimens from patients with gastrointestinal tumors. Even though the focus of our paper is human genomic alterations in stool specimens, in our “future aspects” chapter, we also deal with the bacterial spectrum and its possible interaction with the genomic mutations.
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