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Chromosomal Abnormalities in Early Pregnancy Losses: A Study of 900 Samples

机译:早期妊娠丢失中的染色体异常:一项 900 个样本的研究

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摘要

Chromosomal abnormalities are the most common causes of early pregnancy losses (EPLs). In this study, we aimed to evaluate the incidence and spectrum of chromosomal abnormalities in EPLs and correlate them with different clinical characteristics. We performed Quantitative Fluorescent PCR (QF-PCR), followed by subtelomeric Multiplex Ligation Probe Amplification (MLPA) analysis to detect chromosomal abnormalities in 900 products of conceptions (POCs) from EPLs collected over a period of 10 years.Chromosomal abnormalities were present in 56.25% of uncontaminated EPLs, with significantly higher incidence in women ≥36 years (71.37%, p<0.0001) in comparison to women ≤30 years of age (43.40%). Trisomies were also more common in women ≥36 years (79.68%, p<0.0001) than in those ≤30 years of age (48.70%). In contrast, triploidy and monosomies were more prevalent in women ≤30 years of age (26.09%, p<0.0001 and 16.52%, p=0.0066 respectively) than in women ≥36 years of age (6.42% and 6.42% respectively). Trisomy 16 was more common in women ≤30 (39.29%, p=0.0009) than in those ≥36 years of age (16.78%), while trisomy 22 was predominant among women ≥36 (23.49%, p=0.013), and was not present in the group of women ≤30 years of age. The frequency of chromosomal abnormalities in POCs from women with sporadic (61.19%) was higher than in those with recurrent EPLs (55.21%). This difference, however, was not statistically significant (p=0.164). Although some differences in the chromosomal aneuploidy rates among women with different ABO blood groups, as well as among 6–8 and 9–11 gestational week EPLs were observed, further larger studies are required to confirm these findings.In conclusion, our study enriches the knowledge about chromosomal abnormalities as a cause of EPLs and confirms the higher incidence of foetal chromosomal abnormalities in EPLs in women of older reproductive age. Furthermore, it shows that using QF-PCR and MLPA methodologies, a high detection rate of chromosomal abnormalities in EPLs can be reached.
机译:染色体异常是早期妊娠丢失 (EPL) 的最常见原因。在这项研究中,我们旨在评估 EPLs 染色体异常的发生率和谱,并将其与不同的临床特征相关联。我们进行了定量荧光 PCR (QF-PCR),然后进行亚端粒多重连接探针扩增 (MLPA) 分析,以检测 900 个受孕产物 (POC) 的染色体异常,这些受孕产物来自 EPL s,收集了 10 年。56.25% 的未污染 EPL 存在染色体异常,与 ≤30 岁 (43.40%) 相比,≥36 岁女性 (71.37%,p<0.0001) 的发生率显著更高。三体性在 ≥36 岁女性 (79.68%,p<0.0001) 中也比 ≤ 30 岁女性 (48.70%) 更常见。相比之下,三倍体和单体性在 30 岁女性 ≤ (分别为 26.09%,p<0.0001 和 16.52%,p=0.0066) 中比在 ≥36 岁女性 (分别为 6.42% 和 6.42%) 中更普遍。16 三体在 ≤30 岁女性中更常见 (39.29%,p=0.0009) 比在 ≥36 岁女性 (16.78%) 中更常见,而 22 三体在女性 ≥36 中占主导地位 (23.49%,p=0.013),并且在 ≤30 岁的女性群体中不存在。散发性女性 (61.19%) POC 染色体异常的频率高于复发性 EPL 女性 (55.21%)。然而,这种差异没有统计学意义 (p=0.164)。尽管观察到不同 ABO 血型的妇女以及孕 6-8 和 9-11 周 EPL 之间的染色体非整倍体发生率存在一些差异,但需要进一步更大规模的研究来证实这些发现。总之,我们的研究丰富了关于染色体异常是 EPL 原因的知识,并证实了高龄妇女 EPL 中胎儿染色体异常的发生率较高。此外,它表明使用 QF-PCR 和 MLPA 方法,可以达到 EPL 染色体异常的高检出率。

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