Partial trisomy 4q and monosomy 5p inherited from a maternal translocationt(4;5)(q33;p15) in three adverse pregnancies

Zhang, Jingbo; Zhang, Bei; Liu, Tong; Xie, Huihui; Zhai, Jingfang

doi:10.21203/rs.3.rs-17019/v1

Cited by 3 publications

(5 citation statements)

References 25 publications

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“…30 A case study showed a copy gain of the distal region of chromosome 4 at segment 4q32.3q35.2 in a pregnant patient that presented with fetal edema and subsequent fetal loss. 31 Furthermore, the duplication of 16p13.11 is implicated in multiple congenital anomalies in pediatric patients (n=1645). 32 Mutations in MYH11 (myosin heavy chain 11) gene, among several genes in the 16p13.11 region, cause thoracic aortic aneurysms and/or dissections.…”

Section: Discussionmentioning

confidence: 99%

Copy number variants and placental abnormalities in stillborn fetuses: a secondary analysis of the Stillbirth Collaborative Research Network study

Workalemahu

Dalton

Allshouse

et al. 2022

Preprint

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Objective To examine the association of DNA copy number variants (CNVs) with pathologic placental lesions (PPLs) in stillborn fetuses. Design A secondary analysis of stillbirth cases in the Stillbirth Collaborative Research Network case-control study. Setting Multicenter, 59 hospitals in 5 geographic regions in the USA. Population 387 stillbirth cases (2006-2008). Methods Using standard definitions, PPLs were categorized by type including maternal and fetal vascular, inflammatory and immune/idiopathic lesions. Using single-nucleotide polymorphism array, CNVs of at least 500 kb were detected. CNVs were classified into two groups: normal, defined as no CNVs>500 kb or benign CNVs, and abnormal, defined as pathogenic or variants of unknown clinical significance. Main outcome measures The proportions of abnormal CNVs and normal CNVs were compared between stillbirth cases with and without PPLs using the Wald Chi-squared test. Results Of 387 stillborn fetuses, 327 (84.5%) had maternal vascular PPLs and 60 (15.6%) had abnormal CNVs. Maternal vascular PPLs were more common in stillborn fetuses with abnormal CNVs compared with those with normal CNVs (81.7% vs. 64.2%; p=0.008). The proportions of fetal vascular, maternal/fetal inflammatory, and immune/idiopathic PPLs were similar among stillborn fetuses with abnormal CNVs compared to those with normal CNVs. Pathogenic CNVs in stillborn fetuses with maternal vascular PPLs spanned several genes with known relevant mechanisms. Conclusions Abnormal placental/fetal CNVs were associated with maternal vascular PPLs in stillborn fetuses. Findings may provide insight on the mechanisms of specific genetic abnormalities associated with placental dysfunction and stillbirth.

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Section: Discussionmentioning

confidence: 99%

Copy number variants and placental abnormalities in stillborn fetuses: a secondary analysis of the Stillbirth Collaborative Research Network study

Workalemahu

Dalton

Allshouse

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…30 A case study showed a copy gain of the distal region of chromosome 4 at segment 4q32.3q35.2 in a pregnant patient that presented with fetal edema and subsequent fetal loss. 31 Furthermore, the duplication of 16p13.11 is implicated in multiple congenital anomalies in paediatric patients (n = 1645). 32 Mutations in MYH11 (myosin heavy chain 11) gene, among several genes in the 16p13.11 region, cause thoracic aortic aneurysms and/ or dissections.…”

Section: Discussionmentioning

confidence: 99%

“…Pathologic placental lesions are found in DiGeorge sequence, characterised by hypoplasia in the umbilical cord arteries and widespread calcification of microthrombi in the arteries of the second and third order villous branches 30 . A case study showed a copy gain of the distal region of chromosome 4 at segment 4q32.3q35.2 in a pregnant patient that presented with fetal edema and subsequent fetal loss 31 . Furthermore, the duplication of 16p13.11 is implicated in multiple congenital anomalies in paediatric patients ( n = 1645) 32 .…”

Section: Discussionmentioning

confidence: 99%

Copy number variants and placental abnormalities in stillborn fetuses: A secondary analysis of the Stillbirth Collaborative Research Network study

Workalemahu

Dalton

Allshouse

et al. 2022

BJOG

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“…Briefly, ultrasound was used to break genomic DNA into 250–300 bp fragments. DNA libraries were constructed by end filling, adapter ligation, and polymerase chain reaction amplification 9 . Then, the DNA libraries underwent hybridization capture and were enriched by the xGen Exome Research Panel v2.0 (IDT).…”

Section: Methodsmentioning

confidence: 99%

“…DNA libraries were constructed by end filling, adapter ligation, and polymerase chain reaction amplification. 9 Then, the DNA libraries underwent hybridization capture and were enriched by the xGen Exome Research Panel v2.0 (IDT). High throughput sequencing was performed on the DNBSEQ-T7 platform (Beijing Genomics Institute).…”

Section: Wesmentioning

confidence: 99%

A novel chromosome 2q24.3‐q32.1 microdeletion in a fetus with multiple malformations

Zhu

Wang

Guan

et al. 2022

Clinical Laboratory Analysis

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Background Terminal or interstitial deletion of chromosome 2q is rarely reported but clinically significant, which can result in developmental malformations and psychomotor retardation in humans. In the present study, we analyzed this deletion to comprehensively clarify the relationship between phenotype and microdeletion region. Methods We collected clinical records of the fetus and summarized patient symptoms. Subsequently, genomic DNA was extracted from fetal tissue or peripheral blood collected from parents. In addition, whole‐exome sequencing (WES) and copy number variation sequencing (CNV‐seq) were performed. Results The fetus presented a previously unreported interstitial deletion of 2q24.3‐q32.1. WES and CNV‐seq revealed a de novo 18.46 Mb deletion at 2q24.3‐q32.1, a region involving 94 protein‐coding genes, including HOXD13, MAP3K20, DLX1, DLX2, SCN2A, and SCN1A. The fetus had upper and lower limb malformations, including camptodactyly and syndactyly, along with congenital cardiac defects. Conclusion Herein, we report a fetus with a novel microdeletion of chromosome 2q24.3‐q32.1, likely a heterozygous pathogenic variant. Haploinsufficiency of HOXD13 might be related to limb deformity in the fetus.

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Partial trisomy 4q and monosomy 5p inherited from a maternal translocationt(4;5)(q33;p15) in three adverse pregnancies

Cited by 3 publications

References 25 publications

Copy number variants and placental abnormalities in stillborn fetuses: a secondary analysis of the Stillbirth Collaborative Research Network study

Copy number variants and placental abnormalities in stillborn fetuses: a secondary analysis of the Stillbirth Collaborative Research Network study

Copy number variants and placental abnormalities in stillborn fetuses: A secondary analysis of the Stillbirth Collaborative Research Network study

A novel chromosome 2q24.3‐q32.1 microdeletion in a fetus with multiple malformations

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