Application of natural and amplification-created restriction sites in prenatal and preimplantation diagnosis of beta-thalassemia.

P L Kuo, H J Liu, J S Chen, R C Wu, S J Lin, J G Chang
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引用次数: 0

Abstract

We attempted the strategy of natural and amplification-created restriction sites for early prenatal and preimplantation diagnosis of Chinese beta-thalassemia. Mutagenesis primers were designed for 11 mutations reported for the Chinese population. The diagnosis was established after polymerase chain reaction and digestion of products by specific enzymes. The results were confirmed by direct sequencing of enzymatically amplified double-stranded DNA. The beta-globin gene was amplified from triploid embryos and isolated blastomeres using mismatched primers. The mutant and normal alleles can be distinguished clearly by this new method. Early prenatal diagnosis was successfully achieved in 9 cases. The beta-globin gene was successfully amplified from single blastomeres and tripronuclear embryos with mismatched primers. Natural and amplification-created restriction sites are a reliable method for rapid prenatal diagnosis of beta-thalassemia. Furthermore, the strategy provides a possible approach for the preimplantation diagnosis of beta-thalassemia.

自然和扩增产生的限制性内切位点在产前和着床前诊断-地中海贫血中的应用。
我们尝试利用自然限制性位点和扩增限制性位点对中国-地中海贫血进行早期产前和着床前诊断。为中国人群中报道的11个突变设计了诱变引物。诊断是通过聚合酶链反应和特定酶消化产物确定的。结果通过酶扩增双链DNA的直接测序得到证实。利用错配引物从三倍体胚胎和分离的卵裂球中扩增出-珠蛋白基因。该方法可以很好地区分突变等位基因和正常等位基因。早期产前诊断成功9例。用错配引物成功地从单卵裂球和三核胚胎中扩增出-珠蛋白基因。自然和扩增产生的限制性内切位点是快速产前诊断-地中海贫血的可靠方法。此外,该策略为β -地中海贫血的植入前诊断提供了一种可能的方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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