Exome Sequencing Identifies A Branch Point Variant in AarskogScott Syndrome

Emmelien Aten; Yu Sun; Rowida Almomani; Gijs W. E. Santen; Tobias Messemaker; Saskia M. Maas; Martijn H. Breuning; Johan T. den Dunnen

doi:https://doi.org/10.1002/humu.22252

Exome Sequencing Identifies A Branch Point Variant in AarskogScott Syndrome

Emmelien Aten, Yu Sun, Rowida Almomani, Gijs W. E. Santen, Tobias Messemaker, Saskia M. Maas, Martijn H. Breuning, Johan T. den Dunnen

Research output: Contribution to journal › Article › Academic › peer-review

15 Citations (Scopus)

Abstract

AarskogScott syndrome (ASS) is a rare disorder with characteristic facial, skeletal, and genital abnormalities. Mutations in the FGD1 gene (Xp11.21) are responsible for ASS. However, mutation detection rates are low. Here, we report a family with ASS where conventional Sanger sequencing failed to detect a pathogenic change in FGD1. To identify the causative gene, we performed whole-exome sequencing in two patients. An initial analysis did not reveal a likely candidate gene. After relaxing our filtering criteria, accepting larger intronic segments, we unexpectedly identified a branch point (BP) variant in FGD1. Analysis of patient-derived RNA showed complete skipping of exon 13, leading to premature translation termination. The BP variant detected is one of very few reported so far proven to affect splicing. Our results show that besides digging deeper to reveal nonobvious variants, isolation and analysis of RNA provides a valuable but under-appreciated tool to resolve cas!

Original language	English
Pages (from-to)	430-434
Journal	Human mutation
Volume	34
Issue number	3
DOIs	https://doi.org/10.1002/humu.22252
Publication status	Published - 2013

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https://doi.org/10.1002/humu.22252

Cite this

@article{3cfbb07e4bb44687b5a3e306cd6699a7,

title = "Exome Sequencing Identifies A Branch Point Variant in AarskogScott Syndrome",

abstract = "AarskogScott syndrome (ASS) is a rare disorder with characteristic facial, skeletal, and genital abnormalities. Mutations in the FGD1 gene (Xp11.21) are responsible for ASS. However, mutation detection rates are low. Here, we report a family with ASS where conventional Sanger sequencing failed to detect a pathogenic change in FGD1. To identify the causative gene, we performed whole-exome sequencing in two patients. An initial analysis did not reveal a likely candidate gene. After relaxing our filtering criteria, accepting larger intronic segments, we unexpectedly identified a branch point (BP) variant in FGD1. Analysis of patient-derived RNA showed complete skipping of exon 13, leading to premature translation termination. The BP variant detected is one of very few reported so far proven to affect splicing. Our results show that besides digging deeper to reveal nonobvious variants, isolation and analysis of RNA provides a valuable but under-appreciated tool to resolve cas!",

author = "Emmelien Aten and Yu Sun and Rowida Almomani and Santen, {Gijs W. E.} and Tobias Messemaker and Maas, {Saskia M.} and Breuning, {Martijn H.} and {den Dunnen}, {Johan T.}",

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T1 - Exome Sequencing Identifies A Branch Point Variant in AarskogScott Syndrome

AU - Aten, Emmelien

AU - Sun, Yu

AU - Almomani, Rowida

AU - Santen, Gijs W. E.

AU - Messemaker, Tobias

AU - Maas, Saskia M.

AU - Breuning, Martijn H.

AU - den Dunnen, Johan T.

PY - 2013

Y1 - 2013

N2 - AarskogScott syndrome (ASS) is a rare disorder with characteristic facial, skeletal, and genital abnormalities. Mutations in the FGD1 gene (Xp11.21) are responsible for ASS. However, mutation detection rates are low. Here, we report a family with ASS where conventional Sanger sequencing failed to detect a pathogenic change in FGD1. To identify the causative gene, we performed whole-exome sequencing in two patients. An initial analysis did not reveal a likely candidate gene. After relaxing our filtering criteria, accepting larger intronic segments, we unexpectedly identified a branch point (BP) variant in FGD1. Analysis of patient-derived RNA showed complete skipping of exon 13, leading to premature translation termination. The BP variant detected is one of very few reported so far proven to affect splicing. Our results show that besides digging deeper to reveal nonobvious variants, isolation and analysis of RNA provides a valuable but under-appreciated tool to resolve cas!

AB - AarskogScott syndrome (ASS) is a rare disorder with characteristic facial, skeletal, and genital abnormalities. Mutations in the FGD1 gene (Xp11.21) are responsible for ASS. However, mutation detection rates are low. Here, we report a family with ASS where conventional Sanger sequencing failed to detect a pathogenic change in FGD1. To identify the causative gene, we performed whole-exome sequencing in two patients. An initial analysis did not reveal a likely candidate gene. After relaxing our filtering criteria, accepting larger intronic segments, we unexpectedly identified a branch point (BP) variant in FGD1. Analysis of patient-derived RNA showed complete skipping of exon 13, leading to premature translation termination. The BP variant detected is one of very few reported so far proven to affect splicing. Our results show that besides digging deeper to reveal nonobvious variants, isolation and analysis of RNA provides a valuable but under-appreciated tool to resolve cas!

U2 - https://doi.org/10.1002/humu.22252

DO - https://doi.org/10.1002/humu.22252

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