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Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome

Autosomal dominant (de novo) mutations in PBX1 are known to cause congenital abnormalities of the kidney and urinary tract (CAKUT), with or without extra‐renal abnormalities. Using trio exome sequencing, we identified a PBX1 p.(Arg107Trp) mutation in a deceased one‐day‐old neonate presenting with CA...

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Autores principales: Arts, Peer, Garland, Jessica, Byrne, Alicia B., Hardy, Tristan S.E., Babic, Milena, Feng, Jinghua, Wang, Paul, Ha, Thuong, King‐Smith, Sarah L., Schreiber, Andreas W., Crawford, April, Manton, Nick, Moore, Lynette, Barnett, Christopher P., Scott, Hamish S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Inc. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7217179/
https://www.ncbi.nlm.nih.gov/pubmed/32141698
http://dx.doi.org/10.1002/ajmg.a.61541
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author Arts, Peer
Garland, Jessica
Byrne, Alicia B.
Hardy, Tristan S.E.
Babic, Milena
Feng, Jinghua
Wang, Paul
Ha, Thuong
King‐Smith, Sarah L.
Schreiber, Andreas W.
Crawford, April
Manton, Nick
Moore, Lynette
Barnett, Christopher P.
Scott, Hamish S.
author_facet Arts, Peer
Garland, Jessica
Byrne, Alicia B.
Hardy, Tristan S.E.
Babic, Milena
Feng, Jinghua
Wang, Paul
Ha, Thuong
King‐Smith, Sarah L.
Schreiber, Andreas W.
Crawford, April
Manton, Nick
Moore, Lynette
Barnett, Christopher P.
Scott, Hamish S.
author_sort Arts, Peer
collection PubMed
description Autosomal dominant (de novo) mutations in PBX1 are known to cause congenital abnormalities of the kidney and urinary tract (CAKUT), with or without extra‐renal abnormalities. Using trio exome sequencing, we identified a PBX1 p.(Arg107Trp) mutation in a deceased one‐day‐old neonate presenting with CAKUT, asplenia, and severe bilateral diaphragmatic thinning and eventration. Further investigation by droplet digital PCR revealed that the mutation had occurred post‐zygotically in the father, with different variant allele frequencies of the mosaic PBX1 mutation in blood (10%) and sperm (20%). Interestingly, the father had subclinical hydronephrosis in childhood. With an expected recurrence risk of one in five, chorionic villus sampling and prenatal diagnosis for the PBX1 mutation identified recurrence in a subsequent pregnancy. The family opted to continue the pregnancy and the second affected sibling was stillborn at 35 weeks, presenting with similar severe bilateral diaphragmatic eventration, microsplenia, and complete sex reversal (46, XY female). This study highlights the importance of follow‐up studies for presumed de novo and low‐level mosaic variants and broadens the phenotypic spectrum of developmental abnormalities caused by PBX1 mutations.
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spelling pubmed-72171792020-05-13 Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome Arts, Peer Garland, Jessica Byrne, Alicia B. Hardy, Tristan S.E. Babic, Milena Feng, Jinghua Wang, Paul Ha, Thuong King‐Smith, Sarah L. Schreiber, Andreas W. Crawford, April Manton, Nick Moore, Lynette Barnett, Christopher P. Scott, Hamish S. Am J Med Genet A Clinical Reports Autosomal dominant (de novo) mutations in PBX1 are known to cause congenital abnormalities of the kidney and urinary tract (CAKUT), with or without extra‐renal abnormalities. Using trio exome sequencing, we identified a PBX1 p.(Arg107Trp) mutation in a deceased one‐day‐old neonate presenting with CAKUT, asplenia, and severe bilateral diaphragmatic thinning and eventration. Further investigation by droplet digital PCR revealed that the mutation had occurred post‐zygotically in the father, with different variant allele frequencies of the mosaic PBX1 mutation in blood (10%) and sperm (20%). Interestingly, the father had subclinical hydronephrosis in childhood. With an expected recurrence risk of one in five, chorionic villus sampling and prenatal diagnosis for the PBX1 mutation identified recurrence in a subsequent pregnancy. The family opted to continue the pregnancy and the second affected sibling was stillborn at 35 weeks, presenting with similar severe bilateral diaphragmatic eventration, microsplenia, and complete sex reversal (46, XY female). This study highlights the importance of follow‐up studies for presumed de novo and low‐level mosaic variants and broadens the phenotypic spectrum of developmental abnormalities caused by PBX1 mutations. John Wiley & Sons, Inc. 2020-03-06 2020-05 /pmc/articles/PMC7217179/ /pubmed/32141698 http://dx.doi.org/10.1002/ajmg.a.61541 Text en © 2020 The Authors. American Journal of Medical Genetics Part A published by Wiley Periodicals, Inc. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Clinical Reports
Arts, Peer
Garland, Jessica
Byrne, Alicia B.
Hardy, Tristan S.E.
Babic, Milena
Feng, Jinghua
Wang, Paul
Ha, Thuong
King‐Smith, Sarah L.
Schreiber, Andreas W.
Crawford, April
Manton, Nick
Moore, Lynette
Barnett, Christopher P.
Scott, Hamish S.
Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title_full Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title_fullStr Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title_full_unstemmed Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title_short Paternal mosaicism for a novel PBX1 mutation associated with recurrent perinatal death: Phenotypic expansion of the PBX1‐related syndrome
title_sort paternal mosaicism for a novel pbx1 mutation associated with recurrent perinatal death: phenotypic expansion of the pbx1‐related syndrome
topic Clinical Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7217179/
https://www.ncbi.nlm.nih.gov/pubmed/32141698
http://dx.doi.org/10.1002/ajmg.a.61541
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