The application of late amniocentesis: a retrospective study in a tertiary fetal medicine center in China

Li, Yingting; Yan, Huanchen; Chen, Jingsi; Chen, Fei; Jian, Wenhua; Wang, Jiayan; Ye, Xiaoqing; Li, Yufan; Li, Nan; Chiu, Philip C.N.; Chen, Min

doi:10.1186/s12884-021-03723-7

Cited by 8 publications

(12 citation statements)

References 17 publications

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“…Our cohort of 483 fetal VUS is the second largest reported to date. Our live birth rate for fetuses with a VUS (64%) was higher than for those with a pCNV (20%) and was within the range reported in other fetal VUS cohorts (35%–90%) 10–13,15,16,19 . Similarly to Chen et al., who followed up 721 fetal VUS, we found that an inherited VUS was more likely to result in a live birth than a non‐inherited VUS 17 .…”

Section: Discussionsupporting

confidence: 87%

“…The prevalence of pCNVs in our cohort was 3.3%, which was similar to that reported in a published review of 23,865 pCNVs 29 . Our study of 230 pCNVs is the largest to include birth outcomes, with previous publications containing smaller cohorts (range 5–93) and/or only reporting perinatal outcomes for a small subset 10–14,18 . Our summary statistics on preterm birth and low birth weight provide general prognostic information that can be used for counseling couples about obstetric outcomes for pCNVs, particularly for rare pCNVs where data on obstetric outcomes are lacking and planning ongoing management in a high risk model of prenatal care.…”

Section: Discussionsupporting

confidence: 82%

“…Our VUS prevalence of 7.0% was higher than some studies, 1,3,10–16,19,33,34 but comparable to 7.2% recorded in the Belgium national prenatal cohort 33 . The most common VUS in our study was the 15q11.2 deletion, which has a highly variable phenotype including neurodevelopmental delay, autism spectrum disorders, and obsessive‐compulsive disorders 35 .…”

Section: Discussionsupporting

confidence: 73%

“…Had CMA only been performed in pregnancies with an ultrasound abnormality, 27.9% (90/322, Table 3) of pCNVs in our cohort would have gone undetected before birth. 3 Our VUS prevalence of 7.0% was higher than some studies, 1,3,[10][11][12][13][14][15][16]19,33,34 but comparable to 7.2% recorded in the Belgium national prenatal cohort. 33 The most common VUS in our study was the 15q11.2 deletion, which has a highly variable phenotype including neurodevelopmental delay, autism spectrum disorders, and obsessive-compulsive disorders.…”

Section: Variants Of Uncertain Significancesupporting

confidence: 60%

“…There is a dearth of current literature on perinatal outcomes of fetal pCNVs and VUS, in terms of the number of live births and perinatal deaths. Published studies are limited by small sample sizes, selection bias due to limited indications for prenatal diagnosis, and incomplete reporting of perinatal outcomes 10–19 . Perinatal outcomes are likely influenced by indication for prenatal diagnosis, such as an ultrasound abnormality, as well as genomic location and CNV size.…”

Section: Introductionmentioning

confidence: 99%

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Perinatal outcomes and genomic characteristics of fetal copy number variants: An individual record linkage study of 713 pregnancies

et al. 2023

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Objective: To determine the perinatal outcomes of fetuses diagnosed with a pathogenic copy number variant (CNV) or variant of uncertain significance (VUS); and to characterize these variants in terms of testing indication, genomic location, size, and inheritance. Methods:Retrospective study of singleton pregnancies with a pathogenic CNV or VUS from a single laboratory during 2012-2018. Probabilistic record linkage between the prenatal diagnosis dataset and perinatal outcome data for births from 20 weeks gestation was performed. If no birth record was found, this implied a pregnancy loss <20 weeks. Results:We included 6945 prenatal microarray results; a pathogenic CNV was detected in 230 (3.3%, 95% CI: 2.9%-3.8%) and a VUS in 483 (7.0%, 95% CI: 6.4%-7.6%). Of pregnancies with a pathogenic CNV, 20.0% (95% CI: 15.3%-25.6%) had a live birth, 3.0% (95% CI: 1.5%-6.2%) had a perinatal death (stillbirth or neonatal death), and 77% (95% CI: 71.1%-81.9%) had no birth record. Of those with a VUS, 64.4% (95% CI: 60.0%-68.5%) had a live birth, 1.8% (95% CI: 1.0%-3.5%) had a perinatal death, and no birth record was found for 33.7% (95% CI: 29.7%-38.1%).Most pathogenic CNVs (61.1%) were <7 Mb in size. The most common microdeletion syndromes were DiGeorge, Wolf-Hirschhorn, and Cri-du-chat syndromes. Conclusion:This study provides an overview of perinatal outcomes and frequency of recurrent CNVs observed in the prenatal microarray era. Key points What is already known about this topic?� Fetal copy number variants (CNVs) detected on chromosomal microarray have a wide range of clinical significance.� Large studies reporting perinatal outcome rates after a prenatal diagnosis of a CNV are rare.

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Section: Discussionsupporting

confidence: 87%

Section: Discussionsupporting

confidence: 82%

Section: Discussionsupporting

confidence: 73%

Section: Variants Of Uncertain Significancesupporting

confidence: 60%

Section: Introductionmentioning

confidence: 99%

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Perinatal outcomes and genomic characteristics of fetal copy number variants: An individual record linkage study of 713 pregnancies

et al. 2023

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Obstetrical outcomes following amniocentesis performed after 24 weeks of gestation: A systematic review and meta‐analysis

Nassr,

Hessami,

D’Alberti

et al. 2023

Prenatal Diagnosis

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To evaluate obstetrical outcomes for women having late amniocentesis (on or after 24 weeks). Electronic databases were searched from inception to January 1st, 2023. The obstetrical outcomes evaluated were gestational age at delivery, preterm birth (PTB) < 37 weeks, PTB within 1 week from amniocentesis, premature prelabor rupture of membranes (pPROM), chorionamnionitis, placental abruption, intrauterine fetal demise (IUFD) and termination of pregnancy (TOP). The incidence of PTB <37 weeks was 4.85% (95% CI 3.48–6.56), while the incidence of PTB within 1 week was 1.42% (95% CI 0.66–2.45). The rate of pPROM was 2.85% (95% CI 1.21–3.32). The incidence of placental abruption was 0.91% (95% CI 0.16–2.25), while the rate of IUFD was 3.66% (95% CI 0.00–14.04). The rate of women who underwent TOP was 6.37% (95%CI 1.05–15.72). When comparing amniocentesis performed before or after 32 weeks, the incidence of PTB within 1 week was 1.48% (95% CI 0.42–3.19) and 2.38% (95% CI 0.40–5.95). Amniocentesis performed late after 24 weeks of gestation is an acceptable option for patients needing prenatal diagnosis in later gestation.

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Amniocentesis in pregnancies at or beyond 24 weeks: an international multicenter study

Zemet,

Maktabi,

Tinfow

et al. 2024

American Journal of Obstetrics and Gynecology

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The application of late amniocentesis: a retrospective study in a tertiary fetal medicine center in China

Cited by 8 publications

References 17 publications

Perinatal outcomes and genomic characteristics of fetal copy number variants: An individual record linkage study of 713 pregnancies

Perinatal outcomes and genomic characteristics of fetal copy number variants: An individual record linkage study of 713 pregnancies

Obstetrical outcomes following amniocentesis performed after 24 weeks of gestation: A systematic review and meta‐analysis

Amniocentesis in pregnancies at or beyond 24 weeks: an international multicenter study

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