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Molecular cytogenetic evidence for multistep tumorigenesis: Implications for risk assessment and early detection

机译:多步骤肿瘤发生的分子细胞遗传学证据:风险评估和早期发现的意义

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摘要

There is strong evidence that multistep tumorigenesis begins with the acquisition of somatic mutations which promote genomic instability. Genomic instability is an important malignant trait because genomic instability can generate the genetic diversity that is necessary for the transforming cell to acquire increasingly variable and aggressive tumor phenotypes. Genomic instability often manifests in the form of chromosomal instability (CIN) leading to the induction of aneuploidy, a phenomenon identified by high resolution molecular cytogenetic techniques. Fluorescent in situ hybridization (FISH) and Array Comparative Genomic Hybridization (aCGH) are two high resolution molecular cytogenetic techniques that allow detection of chromosomal aneuploidy and structural rearrangements occurring in pre-malignant and malignant lesions during tumor progression and invasion. These high resolution molecular cytogenetic techniques are used for genetic screening of single cells in pre-malignant and precursor malignant lesions as well as in exfoliated cells from body fluids and excreta. Consequently, molecular cytogenetic testing offers the promise of an extremely powerful method of risk assessment and early detection of cancer.
机译:有充分的证据表明,多步肿瘤发生始于获得体细胞突变,这种突变会促进基因组的不稳定性。基因组不稳定性是一种重要的恶性特征,因为基因组不稳定性会产生遗传多样性,这对于转化细胞获得越来越多的可变性和侵袭性肿瘤表型是必不可少的。基因组不稳定性通常以染色体不稳定性(CIN)的形式出现,导致诱导非整倍性,这种现象是通过高分辨率分子细胞遗传学技术鉴定的。荧光原位杂交(FISH)和阵列比较基因组杂交(aCGH)是两种高分辨率的分子细胞遗传学技术,可用于检测在肿瘤进展和侵袭期间在恶性前和恶性病变中发生的染色体非整倍性和结构重排。这些高分辨率的分子细胞遗传学技术用于对恶性前病变和前恶性病变以及从体液和排泄物中脱落的细胞中的单细胞进行遗传筛选。因此,分子细胞遗传学检测有望提供一种非常强大的风险评估和癌症早期检测方法。

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