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染色体微阵列检测在鉴定人类囊胚胚胎嵌合现象中的准确性。

The accuracy of chromosomal microarray testing for identification of embryonic mosaicism in human blastocysts.

作者信息

Novik Veronica, Moulton Emily B, Sisson Michael E, Shrestha Shagun L, Tran Khoa D, Stern Harvey J, Mariani Brian D, Stanley Wayne S

机构信息

Genetics and IVF Institute, Fairfax, VA, USA.

出版信息

Mol Cytogenet. 2014 Feb 28;7(1):18. doi: 10.1186/1755-8166-7-18.

Abstract

BACKGROUND

Most previous studies of chromosomal mosaicism in IVF embryos were performed by fluorescence in situ hybridization (FISH) methods. While there are reports implicating chromosome aneuploidy in implantation failure following transfer and pregnancy loss by spontaneous miscarriage, the significance of mosaicism for the developmental potential of growing embryos is unknown. However, the low prevalence of chromosomal mosaicism in chorionic villus sampling and amniotic fluid specimens suggests the presence of selection against mosaic embryos for implantation and early pregnancy. The absence of evidence for selective allocation of abnormal cells to the trophectoderm (TE) of mosaic blastocysts permits these cells to be a good proxy for embryonic mosaicism detection by chromosomal microarrays (CMA). The purpose of this study was to establish the limits of detection and the prevalence of chromosome mosaicism in day 5/6 human embryos using CMA with TE biopsies.

RESULTS

From reconstitution experiments we established log2 ratio thresholds for mosaicism detection. These studies indicated that chromosomal mosaicism at levels as low as between 25-37% can be consistently identified. Follow-up studies by FISH on non-transferred abnormal embryos confirmed the diagnostic accuracy of CMA testing. The number of cells in a TE biopsy can influence mosaicism detection.

CONCLUSIONS

Chromosomal microarrays can detect mosaicism in TE biopsies when present at levels as low as between 25-37% and the prevalence of day 5/6 blastocysts which were mosaic and had no other abnormalities reached 15% among a cohort of 551 embryos examined. Validated protocols for establishing detection thresholds for mosaicism are important to reduce the likelihood of transferring abnormal embryos.

摘要

背景

以往大多数关于体外受精(IVF)胚胎染色体嵌合体的研究都是通过荧光原位杂交(FISH)方法进行的。虽然有报道指出染色体非整倍性与移植后着床失败以及自然流产导致的妊娠丢失有关,但嵌合体对发育中胚胎发育潜力的意义尚不清楚。然而,绒毛取样和羊水样本中染色体嵌合体的低发生率表明,存在针对嵌合胚胎着床和早期妊娠的选择。由于缺乏证据表明异常细胞会选择性地分配到嵌合囊胚的滋养外胚层(TE),这些细胞可以很好地代表通过染色体微阵列(CMA)检测胚胎嵌合体。本研究的目的是使用TE活检的CMA确定第5/6天人类胚胎中染色体嵌合体的检测限和发生率。

结果

通过重组实验,我们确定了嵌合体检测的log2比值阈值。这些研究表明,低至25%-37%水平的染色体嵌合体可以被一致识别。对未移植的异常胚胎进行的FISH后续研究证实了CMA检测的诊断准确性。TE活检中的细胞数量会影响嵌合体检测。

结论

染色体微阵列可以检测到低至25%-37%水平的TE活检中的嵌合体,在一组551个检查的胚胎中,嵌合且无其他异常的第5/6天囊胚的发生率达到了15%。建立嵌合体检测阈值的验证方案对于降低移植异常胚胎的可能性很重要。

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