Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration

Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration

Abstract Background Diagnostic Exome Sequencing (DES) has been shown to be an effective tool for diagnosis individuals with suspected genetic conditions. Case Presentation We report a male infant born with multiple anomalies including bilateral dysplastic kidneys, cleft palate, bilateral talipes, an...

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Main Authors: Zöe Powis, Alexa Hart, Sara Cherny, Igor Petrik, Erika Palmaer, Sha Tang, Carolyn Jones
Format: Article
Language:English
Published: BMC 2017-06-01
Series:BMC Medical Genetics
Subjects:
RBM10 protein
Human
Exome
Clinical diagnostic sequencing
TARP syndrome
Oligodactyly
Online Access:http://link.springer.com/article/10.1186/s12881-017-0426-3
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spelling doaj-3b4a8130ebde489a9e0710d09cf2e8ab2021-04-02T07:38:43ZengBMCBMC Medical Genetics1471-23502017-06-011811510.1186/s12881-017-0426-3Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alterationZöe Powis0Alexa Hart1Sara Cherny2Igor Petrik3Erika Palmaer4Sha Tang5Carolyn Jones6Ambry GeneticsRush University Medical CenterRush University Medical CenterAmbry GeneticsAmbry GeneticsAmbry GeneticsRush University Medical CenterAbstract Background Diagnostic Exome Sequencing (DES) has been shown to be an effective tool for diagnosis individuals with suspected genetic conditions. Case Presentation We report a male infant born with multiple anomalies including bilateral dysplastic kidneys, cleft palate, bilateral talipes, and bilateral absence of thumbs and first toes. Prenatal testing including chromosome analysis and microarray did not identify a cause for the multiple congenital anomalies. Postnatal diagnostic exome studies (DES) were utilized to find a molecular diagnosis for the patient. Exome sequencing of the proband, mother, and father showed a previously unreported maternally inherited RNA binding motif protein 10 (RBM10) c.1352_1353delAG (p.E451Vfs*66) alteration. Mutations in RBM10 are associated with TARP syndrome, an X-linked recessive disorder originally described with cardinal features of talipes equinovarus, atrial septal defect, Robin sequence, and persistent left superior vena cava. Conclusion DES established a molecular genetic diagnosis of TARP syndrome for a neonatal patient with a poor prognosis in whom traditional testing methods were uninformative and allowed for efficient diagnosis and future reproductive options for the parents. Other reported cases of TARP syndrome demonstrate significant variability in clinical phenotype. The reported features in this infant including multiple hemivertebrae, imperforate anus, aplasia of thumbs and first toes have not been reported in previous patients, thus expanding the clinical phenotype for this rare disorder.http://link.springer.com/article/10.1186/s12881-017-0426-3RBM10 proteinHumanExomeClinical diagnostic sequencingTARP syndromeOligodactyly
collection DOAJ
language English
format Article
sources DOAJ
author Zöe Powis
Alexa Hart
Sara Cherny
Igor Petrik
Erika Palmaer
Sha Tang
Carolyn Jones
spellingShingle Zöe Powis
Alexa Hart
Sara Cherny
Igor Petrik
Erika Palmaer
Sha Tang
Carolyn Jones
Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
BMC Medical Genetics
RBM10 protein
Human
Exome
Clinical diagnostic sequencing
TARP syndrome
Oligodactyly
author_facet Zöe Powis
Alexa Hart
Sara Cherny
Igor Petrik
Erika Palmaer
Sha Tang
Carolyn Jones
author_sort Zöe Powis
title Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
title_short Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
title_full Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
title_fullStr Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
title_full_unstemmed Clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of TARP syndrome and expansion of the phenotype in a patient with a newly reported RBM10 alteration
title_sort clinical diagnostic exome evaluation for an infant with a lethal disorder: genetic diagnosis of tarp syndrome and expansion of the phenotype in a patient with a newly reported rbm10 alteration
publisher BMC
series BMC Medical Genetics
issn 1471-2350
publishDate 2017-06-01
description Abstract Background Diagnostic Exome Sequencing (DES) has been shown to be an effective tool for diagnosis individuals with suspected genetic conditions. Case Presentation We report a male infant born with multiple anomalies including bilateral dysplastic kidneys, cleft palate, bilateral talipes, and bilateral absence of thumbs and first toes. Prenatal testing including chromosome analysis and microarray did not identify a cause for the multiple congenital anomalies. Postnatal diagnostic exome studies (DES) were utilized to find a molecular diagnosis for the patient. Exome sequencing of the proband, mother, and father showed a previously unreported maternally inherited RNA binding motif protein 10 (RBM10) c.1352_1353delAG (p.E451Vfs*66) alteration. Mutations in RBM10 are associated with TARP syndrome, an X-linked recessive disorder originally described with cardinal features of talipes equinovarus, atrial septal defect, Robin sequence, and persistent left superior vena cava. Conclusion DES established a molecular genetic diagnosis of TARP syndrome for a neonatal patient with a poor prognosis in whom traditional testing methods were uninformative and allowed for efficient diagnosis and future reproductive options for the parents. Other reported cases of TARP syndrome demonstrate significant variability in clinical phenotype. The reported features in this infant including multiple hemivertebrae, imperforate anus, aplasia of thumbs and first toes have not been reported in previous patients, thus expanding the clinical phenotype for this rare disorder.
topic RBM10 protein
Human
Exome
Clinical diagnostic sequencing
TARP syndrome
Oligodactyly
url http://link.springer.com/article/10.1186/s12881-017-0426-3
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