Genetic Analysis of a Mosaic Fra(16)(q22)/Del(16)(q22) Karyotype in a Primary Infertile Woman

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Guiyuan He, Xi Wang, Beiqing Li, Lei Wang, Jing Zhang, Yang Shi, Wenxiu Zhu, Ming Shi
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Abstract

Purpose Fragile sites are specific chromosomal regions showing gaps, poor staining, contractions, or even breaks in the chromosomes. These spontaneous and heritable fragile sites are prone to structural variations which can lead to adverse reproductive outcomes. This paper aims to present a specific case study of a female patient, with a mosaic karyotype involving chromosome 16q22 fragile site which is very rare in clinic and her experience of infertility. Case Presentation A 37-year-old woman is diagnosed with ten-year primary infertility. She worked in a factory, and she was occasionally exposed to paint. She underwent two cycles of follicular monitoring with intrauterine insemination (IUI) using her husband’s sperm six years ago but failed. Most of her prepregnancy tests were normal, except a not smooth right fallopian tube. Her G-band karyotype of peripheral blood lymphocytes was mos 46, XX, del(16)(q22)[40]/46, XX, fra(16)(q22)[29]/46, XX, fra(16)tr(16)(q22)[3]/46, XX[28] which inherited from her mother. The SCE assay detected a significantly higher frequency of SCEs in the 16q region of the patient’s chromosomes compared to her mother and a healthy control. However, the average SCEs per chromosome were quite close. Moreover, copy number variation (CNV) sequencing showed no deletion nor duplication at 16q22. Conclusion Infertility cannot be completely attributed to the fragile site on chromosome 16q22. Assisted reproductive technology combined with preimplantation genetic testing may help in achieving a healthy live birth.
一名原发性不孕妇女Fra(16)(q22)/Del(16)(q22)镶嵌核型的遗传学分析
目的 脆弱位点是染色体上出现间隙、染色不良、收缩甚至断裂的特定染色体区域。这些自发和遗传的脆性位点容易发生结构变异,从而导致不良的生殖结果。本文旨在介绍一例女性患者的具体病例研究,该患者的核型为镶嵌型,涉及临床上非常罕见的染色体 16q22 脆性位点,以及她的不孕经历。病例介绍 一位 37 岁的女性被诊断患有十年原发性不孕症。她在一家工厂工作,偶尔会接触到油漆。六年前,她使用丈夫的精子进行了两个周期的卵泡监测和宫腔内人工授精(IUI),但都失败了。除了右侧输卵管不通畅外,她的大部分孕前检查结果都正常。她的外周血淋巴细胞 G 带核型为 mos 46, XX, del(16)(q22)[40]/46, XX, fra(16)(q22)[29]/46, XX, fra(16)tr(16)(q22)[3]/46, XX[28],遗传自母亲。与母亲和健康对照组相比,SCE 检测在患者染色体的 16q 区域检测到的 SCE 频率明显更高。不过,每条染色体的平均 SCE 非常接近。此外,拷贝数变异(CNV)测序显示 16q22 既没有缺失,也没有重复。结论 不育症不能完全归咎于 16q22 号染色体上的脆性位点。辅助生殖技术与胚胎植入前基因检测相结合,可能有助于实现健康的活产。
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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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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