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Multilocus genetic analysis of single interphase cells by spectral imaging.

机译:单间期细胞的多基因遗传分析的光谱成像。

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Numerical chromosome aberrations are detrimental to early embryonic, fetal and perinatal development of mammals. When fetuses carrying a chromosomal imbalance survive to term, an aberrant gene dosage typically leads to stillbirth or causes a severely altered phenotype. Aneuploidy of any of the 24 chromosomes will negatively impact on human development, and a preimplantation and prenatal genetic diagnosis test should thus score as many chromosomes as possible. Since cells available for analysis are likely to be in interphase, we set out to develop a rapid enumeration procedure based on hybridization of chromosome-specific probes and spectral imaging detection. The probe set was chosen to allow the simultaneous enumeration of ten chromosome types and was expected to detect more than 70% of all numerical chromosome aberrations responsible for spontaneous abortions, i.e., human chromosomes 9, 13, 14, 15, 16, 18, 21, 22, X, and Y. Cell fixation protocols were optimized to achieve the desired detection sensitivity and reproducibility. We were able to resolve and identify ten separate chromosomal signals in interphase nuclei from different types of cells, including lymphocytes, uncultured amniocytes, and blastomeres. In summary, this study demonstrates the strength of spectral imaging, allowing us to construct partial spectral imaging karyotypes for individual interphase cells by assessing the number of each of the target chromosome types.
机译:染色体数字畸变对哺乳动物的早期胚胎,胎儿和围产期发育有害。当携带染色体失衡的胎儿存活至足月时,异常的基因剂量通常会导致死产或导致严重的表型改变。 24条染色体中任何一条的非整倍性都会对人类发育产生负面影响,因此,植入前和产前遗传学诊断测试应计入尽可能多的染色体。由于可用于分析的细胞可能处于中间相,因此我们着手开发基于染色体特异性探针杂交和光谱成像检测的快速枚举程序。选择该探针组以允许同时枚举十种染色体类型,并有望检测到所有可导致自然流产的数字染色体畸变中的70%以上,即人类9、13、14、15、15、16、18、21号染色体,22,X和Y。对细胞固定方案进行了优化,以实现所需的检测灵敏度和可重复性。我们能够分辨和识别来自不同类型细胞(包括淋巴细胞,未培养的羊水细胞和卵裂球)的相间核中的十个独立的染色体信号。总而言之,这项研究证明了光谱成像的优势,使我们能够通过评估每种目标染色体类型的数量来构建单个相间细胞的部分光谱成像核型。

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