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SNP microarray-based 24 chromosome aneuploidy screening demonstrates that cleavage-stage FISH poorly predicts aneuploidy in embryos that develop to morphologically normal blastocysts

机译:基于SNP基因芯片的24染色体非整倍性筛选表明,卵裂期的FISH不能很好地预测发育为形态正常的胚泡的胚胎中的非整倍性

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摘要

Although selection of chromosomally normal embryos has the potential to improve outcomes for patients undergoing IVF, the clinical impact of aneuploidy screening by fluorescence in situ hybridization (FISH) has been controversial. There are many putative explanations including sampling error due to mosaicism, negative impact of biopsy, a lack of comprehensive chromosome screening, the possibility of embryo self-correction and poor predictive value of the technology itself. Direct analysis of the negative predictive value of FISH-based aneuploidy screening for an embryo's reproductive potential has not been performed. Although previous studies have found that cleavage-stage FISH is poorly predictive of aneuploidy in morphologically normal blastocysts, putative explanations have not been investigated. The present study used a single nucleotide polymorphism (SNP) microarray-based 24 chromosome aneuploidy screening technology to re-evaluate morphologically normal blastocysts that were diagnosed as aneuploid by FISH at the cleavage stage. Mosaicism and preferential segregation of aneuploidy to the trophectoderm (TE) were evaluated by characterization of multiple sections of the blastocyst. SNP microarray technology also provided the first opportunity to evaluate self-correction mechanisms involving extrusion or duplication of aneuploid chromosomes resulting in uniparental disomy (UPD). Of all blastocysts evaluated (n = 50), 58% were euploid in all sections despite an aneuploid FISH result. Aneuploid blastocysts displayed no evidence of preferential segregation of abnormalities to the TE. In addition, extrusion or duplication of aneuploid chromosomes resulting in UPD did not occur. These findings support the conclusion that cleavage-stage FISH technology is poorly predictive of aneuploidy in morphologically normal blastocysts.
机译:尽管选择染色体正常的胚胎有可能改善接受IVF患者的预后,但是通过荧光原位杂交(FISH)筛选非整倍性的临床影响一直存在争议。有许多假定的解释,包括由于镶嵌术引起的采样误差,活检的负面影响,缺乏全面的染色体筛查,胚胎自我校正的可能性以及该技术本身的预测价值不佳。尚未进行基于FISH的非整倍性筛查对胚胎繁殖潜能的阴性预测值的直接分析。尽管以前的研究已经发现卵裂期的FISH不能很好地预测形态正常的胚泡中的非整倍性,但尚未研究推测的解释。本研究使用基于单核苷酸多态性(SNP)微阵列的24染色体非整倍性筛选技术,重新评估在切割阶段被FISH诊断为非整倍性的形态正常的胚泡。镶嵌和非整倍体优先分离到滋养外胚层(TE)通过囊胚的多个部分的表征进行了评估。 SNP微阵列技术还提供了第一个机会来评估自我纠正机制,该机制涉及导致单亲二体性(UPD)的非整倍体染色体的挤出或复制。在评估的所有胚泡中(n = 50),尽管FISH结果为非整倍体,但所有切片中58%为整倍体。非整倍体胚泡没有显示出异常优先分离到TE的证据。另外,没有发生导致UPD的非整倍体染色体的挤出或复制。这些发现支持这样的结论,即卵裂期的FISH技术不能很好地预测形态正常的胚泡中的非整倍性。

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