Clinical outcomes in carriers of insertional translocation: a retrospective analysis of comprehensive chromosome screening results

Zhiqi Zhang M.A.Sc. , Keli Luo Ph.D. , Senlin Zhang B.S. , Dehua Cheng Ph.D. , Liang Hu Ph.D. , Yue-Qiu Tan Ph.D. , Shuoping Zhang Ph.D. , Fei Gong Ph.D. , Pingyuan Xie Ph.D. , Ge Lin Ph.D.
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引用次数: 0

Abstract

Objective

To evaluate the clinical outcomes in the carriers of insertional translocation (IT).

Design

Retrospective case series.

Setting

University-affiliated reproductive medical center.

Patients

Twenty-three couples with ITs.

Intervention

No direct interventions were involved; however, this study included patients who underwent preimplantation genetic testing for structural chromosomal rearrangements (PGT-SR).

Main Outcome Measure

Outcome of preimplantation genetic testing for structural chromosomal rearrangements and percentage of blastocysts available for transfer.

Results

Among 23 IT carriers, 15 were simple interchromosome ITs (type A), 3 were intrachromosome IT carriers (type B), and 5 were interchromosome IT carriers combined with other translocations (type C). A total of 190 blastocysts from 30 cycles were biopsied, 187 embryos were tested successfully, and only 57 blastocysts (30.5%) from 21 patients were available for transfer (normal or balanced). The unbalanced rearrangement rate of type C was 79.2% (42/53), and the proportion of type A was 50.0% (57/114), which was significantly higher than that of type B (5%, 1/20). In type A, the probability of embryos harboring unbalanced rearrangement in female carriers was 56.0% (51/91), which was higher than that in male carriers (26.1%, 6/23). Furthermore, the haploid autosomal length value of the inserted fragment was correlated linearly with the incidence of abnormal embryos. In type A gametes, most gametes produced by 2:2 separation without crossover, and no 3:1 separation gamete was observed.

Conclusions

The chance of identifying normal or balanced and mosaic blastocysts per mature oocytes in patients with ITs are 16.6% (67/404). Greater IT complexity results in fewer transferable embryos. For simple interchromosome ITs, female carriers and those with higher haploid autosomal length values have a higher risk of producing embryos with unbalanced rearrangement.

插入易位携带者的临床结果:染色体全面筛查结果的回顾性分析
干预未进行直接干预,但本研究纳入了接受植入前染色体结构重排基因检测(PGT-SR)的患者。主要结果测量胚胎植入前染色体结构重排基因检测的结果和可移植囊胚的百分比。共对 30 个周期的 190 个囊胚进行了活检,成功检测了 187 个胚胎,只有 21 名患者的 57 个囊胚(30.5%)可用于移植(正常或平衡)。C 型的不平衡重排率为 79.2%(42/53),A 型的比例为 50.0%(57/114),明显高于 B 型(5%,1/20)。在 A 型中,女性携带者的胚胎出现不平衡重排的概率为 56.0%(51/91),高于男性携带者(26.1%,6/23)。此外,插入片段的单倍体常染色体长度值与异常胚胎的发生率呈线性相关。在 A 型配子中,大多数配子是通过 2:2 分离产生的,没有交叉,也没有观察到 3:1 分离配子。IT 复杂性越高,可移植胚胎越少。对于简单染色体间ITs,女性携带者和单倍体常染色体长度值较高者产生不平衡重排胚胎的风险较高。
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
FS Reports
FS Reports Medicine-Embryology
CiteScore
3.50
自引率
0.00%
发文量
78
审稿时长
60 days
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