Aarskog-Scott syndrome: phenotypic and genetic heterogeneity

Aarskog-Scott syndrome: phenotypic and genetic heterogeneity

Aarskog-Scott syndrome (AAS) is a rare developmental disorder which primarily affects males and has a relative prevalence of 1 in 25,000 in the general population. AAS patients usually present with developmental complications including short stature and facial, skeletal and urogenital anomalies. The...

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Main Authors: Ignacio Briceno, Julio Martinez, M. Reza Jabalameli, Reuben J. Pengelly, Sarah Ennis, Andrew Collins
Format: Article
Language:English
Published: AIMS Press 2016-03-01
Series:AIMS Genetics
Subjects:
Aarskog-Scott Syndrome
<em>FGD1</em> gene
genetic heterogeneity
phenotypic heterogeneity
next generation sequencing
Online Access:http://www.aimspress.com/Genetics/article/713/fulltext.html
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spelling doaj-1611fd39bbf54fa7beb0a1386f6151dd2021-01-02T16:30:03ZengAIMS PressAIMS Genetics2377-11432016-03-0131495910.3934/genet.2016.1.49genet-03-00049Aarskog-Scott syndrome: phenotypic and genetic heterogeneityIgnacio Briceno0Julio Martinez1M. Reza Jabalameli2Reuben J. Pengelly3Sarah Ennis4Andrew Collins5Department of Biomedical Sciences, Medical School, Universidad de La Sabana, Bogota, ColombiDepartment of Biomedical Sciences, Medical School, Universidad de La Sabana, Bogota, ColombiGenetic Epidemiology & Genomic Informatics, Faculty of Medicine, University of Southampton, Southampton, UGenetic Epidemiology & Genomic Informatics, Faculty of Medicine, University of Southampton, Southampton, UGenetic Epidemiology & Genomic Informatics, Faculty of Medicine, University of Southampton, Southampton, UGenetic Epidemiology & Genomic Informatics, Faculty of Medicine, University of Southampton, Southampton, UAarskog-Scott syndrome (AAS) is a rare developmental disorder which primarily affects males and has a relative prevalence of 1 in 25,000 in the general population. AAS patients usually present with developmental complications including short stature and facial, skeletal and urogenital anomalies. The spectrum of genotype-phenotype correlations in AAS is unclear and mutations of the <em>FGD1</em> gene on the proximal short arm of chromosome X account for only 20% of the incidence of the disorder. Failure to identify pathogenic variants in patients referred for <em>FGD1</em> screening suggests heterogeneity underlying pathophysiology of the condition. Furthermore, overlapping features of AAS with several other developmental disorders increase the complexity of diagnosis. Cytoskeletal signaling may be involved in the pathophysiology of AAS. The FGD1 protein family has a role in activation of CDC42 (Cell Division Control protein 42 homolog) which has a core function in remodeling of extracellular matrix and the transcriptional activation of many modulators of development. Therefore, mutations in components in the EGFR1 (Epidermal Growth Factor Receptor 1) signaling pathway, to which CDC42 belongs, may contribute to pathophysiology. Parallel sequencing strategies (so-called next generation sequencing or high throughput sequencing) enables simultaneous production of millions of sequencing reads that enormously facilitate cost-effective identification of cryptic mutations in heterogeneous monogenic disorders. Here we review the source of phenotypic and genetic heterogeneity in the context of AAS and discuss the applicability of next generation sequencing for identification of novel mutations underlying AAS.http://www.aimspress.com/Genetics/article/713/fulltext.htmlAarskog-Scott Syndrome<em>FGD1</em> genegenetic heterogeneityphenotypic heterogeneitynext generation sequencing
collection DOAJ
language English
format Article
sources DOAJ
author Ignacio Briceno
Julio Martinez
M. Reza Jabalameli
Reuben J. Pengelly
Sarah Ennis
Andrew Collins
spellingShingle Ignacio Briceno
Julio Martinez
M. Reza Jabalameli
Reuben J. Pengelly
Sarah Ennis
Andrew Collins
Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
AIMS Genetics
Aarskog-Scott Syndrome
<em>FGD1</em> gene
genetic heterogeneity
phenotypic heterogeneity
next generation sequencing
author_facet Ignacio Briceno
Julio Martinez
M. Reza Jabalameli
Reuben J. Pengelly
Sarah Ennis
Andrew Collins
author_sort Ignacio Briceno
title Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
title_short Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
title_full Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
title_fullStr Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
title_full_unstemmed Aarskog-Scott syndrome: phenotypic and genetic heterogeneity
title_sort aarskog-scott syndrome: phenotypic and genetic heterogeneity
publisher AIMS Press
series AIMS Genetics
issn 2377-1143
publishDate 2016-03-01
description Aarskog-Scott syndrome (AAS) is a rare developmental disorder which primarily affects males and has a relative prevalence of 1 in 25,000 in the general population. AAS patients usually present with developmental complications including short stature and facial, skeletal and urogenital anomalies. The spectrum of genotype-phenotype correlations in AAS is unclear and mutations of the <em>FGD1</em> gene on the proximal short arm of chromosome X account for only 20% of the incidence of the disorder. Failure to identify pathogenic variants in patients referred for <em>FGD1</em> screening suggests heterogeneity underlying pathophysiology of the condition. Furthermore, overlapping features of AAS with several other developmental disorders increase the complexity of diagnosis. Cytoskeletal signaling may be involved in the pathophysiology of AAS. The FGD1 protein family has a role in activation of CDC42 (Cell Division Control protein 42 homolog) which has a core function in remodeling of extracellular matrix and the transcriptional activation of many modulators of development. Therefore, mutations in components in the EGFR1 (Epidermal Growth Factor Receptor 1) signaling pathway, to which CDC42 belongs, may contribute to pathophysiology. Parallel sequencing strategies (so-called next generation sequencing or high throughput sequencing) enables simultaneous production of millions of sequencing reads that enormously facilitate cost-effective identification of cryptic mutations in heterogeneous monogenic disorders. Here we review the source of phenotypic and genetic heterogeneity in the context of AAS and discuss the applicability of next generation sequencing for identification of novel mutations underlying AAS.
topic Aarskog-Scott Syndrome
<em>FGD1</em> gene
genetic heterogeneity
phenotypic heterogeneity
next generation sequencing
url http://www.aimspress.com/Genetics/article/713/fulltext.html
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