Patterns of Cytogenomic Findings from a Case Series of Recurrent Pregnancy Loss Provide Insight into the Extent of Genetic Defects Causing Miscarriages.

IF 1.2 Q4 GENETICS & HEREDITY Global Medical Genetics Pub Date : 2024-03-29 eCollection Date: 2024-01-01 DOI:10.1055/s-0044-1785227
Autumn DiAdamo, Hongyan Chai, Mei Ling Chong, Guilin Wang, Jiadi Wen, Yong-Hui Jiang, Peining Li
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Abstract

Background  A retrospective study was performed to evaluate the patterns of cytogenomic findings detected from a case series of products of conception (POC) in recurrent pregnancy loss (RPL) over a 16-year period from 2007 to 2023. Results  This case series of RPL was divided into a single analysis (SA) group of 266 women and a consecutive analysis (CA) group of 225 women with two to three miscarriages analyzed. Of the 269 POC from the SA group and the 469 POC from the CA group, a spectrum of cytogenomic abnormalities of simple aneuploidies, compound aneuploidies, polyploidies, and structural rearrangements/pathogenic copy number variants (pCNVs) were detected in 109 (41%) and 160 cases (34%), five (2%) and 11 cases (2%), 35 (13%) and 36 cases (8%), and 10 (4%) and 19 cases (4%), respectively. Patterns with recurrent normal karyotypes, alternating normal and abnormal karyotypes, and recurrent abnormal karyotypes were detected in 74 (33%), 71 (32%), and 80 (35%) of consecutive miscarriages, respectively. Repeat aneuploidies of monosomy X and trisomy 16, triploidy, and tetraploidy were detected in nine women. Conclusions  A comparable spectrum of cytogenomic abnormalities was noted in the SA and CA groups of RPL. A skewed likelihood of 2/3 for recurrent normal and abnormal karyotypes and 1/3 for alternating normal and abnormal karyotypes in consecutive miscarriages was observed. Routine cytogenetic analysis should be performed for consecutive miscarriages. Further genomic sequencing to search for detrimental and embryonic lethal variants causing miscarriages and pathogenic variants inducing aneuploidies and polyploidies should be considered for RPL with recurrent normal and abnormal karyotypes.

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从复发性妊娠流产病例系列中发现的细胞基因组学模式,有助于了解导致流产的遗传缺陷的程度。
背景 一项回顾性研究评估了从 2007 年到 2023 年的 16 年间,从复发性妊娠丢失(RPL)的受孕产物(POC)病例系列中检测到的细胞基因组结果的模式。结果 这一系列 RPL 病例分为单一分析组(SA)和连续分析组(CA),前者有 266 名妇女,后者有 225 名妇女,其中有两到三次流产。在SA组的269例POC和CA组的469例POC中,分别有109例(41%)和160例(34%)、5例(2%)和11例(2%)、35例(13%)和36例(8%)、10例(4%)和19例(4%)检测到细胞基因组异常,包括单纯非整倍体、复合非整倍体、多倍体和结构重排/致病拷贝数变异(pCNVs)。在连续流产的病例中,分别有 74 例(33%)、71 例(32%)和 80 例(35%)检测到重复正常核型、正常与异常核型交替出现以及重复异常核型。在 9 名妇女中检测到重复非整倍体,包括单体 X 和三体 16、三倍体和四倍体。结论 在 RPL 的 SA 组和 CA 组中,细胞基因组异常的范围相当。在连续流产中,正常和异常核型重复出现的概率分别为 2/3和 1/3。连续流产应进行常规细胞遗传学分析。对于反复出现正常和异常核型的 RPL,应考虑进一步进行基因组测序,以寻找导致流产的有害变体和胚胎致死变体,以及诱发非整倍体和多倍体的致病变体。
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来源期刊
Global Medical Genetics
Global Medical Genetics GENETICS & HEREDITY-
自引率
11.80%
发文量
30
审稿时长
14 weeks
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