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Preimplantation genetic diagnosis and screening (PGD/S) using a semiconductor sequencing platform

机译:使用半导体测序平台的植入前遗传学诊断和筛选(PGD / S)

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Background Recent advances in semiconductor sequencing platform (SSP) have provided new methods for preimplantation genetic diagnosis/screening (PGD/S). The present study aimed to evaluate the applicability and efficiency of SSP in PGD/S. Methods The artificial positive single-cell-like DNAs and normal single-cell samples were chosen to test our semiconductor sequencing platform for preimplantation genetic diagnosis/screening (SSP-PGD/S) method with two widely used whole-genome amplification (WGA) kits. A total of 557 single blastomeres were collected from in vitro fertilization (IVF) couples, and their WGA products were processed and analyzed by our SSP-PGD/S method in comparison with array comparative genomic hybridization (array-CGH). Results Our SSP-PGD/S method indicated high compatibilities with two commercial WGA kits. For 557 single blastomeres, our method with four million reads in average could detect 24-chromosome aneuploidies as well as microdeletion/microduplication of the size over 4?Mb, providing 100% consistent conclusion with array-CGH method in the classification of whether it was transplantable. Conclusions Our studies suggested that SSP-PGD/S represents a valuable alternative to array-CGH and brought PGD/S into a new era of more rapid, accurate, and economic.
机译:背景技术半导体测序平台(SSP)的最新进展为植入前遗传学诊断/筛选(PGD / S)提供了新方法。本研究旨在评估SSP在PGD / S中的适用性和效率。方法选择人工阳性单细胞样DNA和正常单细胞样品,用两个广泛使用的全基因组扩增(WGA)试剂盒测试我们的半导体测序平台,以进行植入前遗传诊断/筛选(SSP-PGD / S)方法。 。从体外受精(IVF)夫妇中总共收集了557个单卵裂球,并通过SSP-PGD / S方法与阵列比较基因组杂交(array-CGH)进行比较,对其WGA产品进行了处理和分析。结果我们的SSP-PGD / S方法表明与两种商业WGA试剂盒具有高度的兼容性。对于557个单卵裂球,我们的方法平均读取400万次,可以检测24染色体非整倍性以及大小超过4?Mb的微缺失/微复制,与array-CGH方法分类是否为100%一致。可移植的。结论我们的研究表明SSP-PGD / S代表了阵列CGH的宝贵替代品,并将PGD / S带入了更加快速,准确和经济的新时代。

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