Unique alterations of an ultraconserved non-coding element in the 3'UTR of ZIC2 in holoprosencephaly

Coding region alterations of ZIC2 are the second most common type of mutation in holoprosencephaly (HPE). Here we use several complementary bioinformatic approaches to identify ultraconserved cis-regulatory sequences potentially driving the expression of human ZIC2. We demonstrate that an 804 bp ele...

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Published in	PloS one Vol. 7; no. 7; p. e39026
Main Authors	Roessler, Erich, Hu, Ping, Hong, Sung-Kook, Srivastava, Kshitij, Carrington, Blake, Sood, Raman, Petrykowska, Hanna, Elnitski, Laura, Ribeiro, Lucilene A, Richieri-Costa, Antonio, Feldman, Benjamin, Odenwald, Ward F, Muenke, Maximilian
Format	Journal Article
Language	English
Published	United States Public Library of Science 31.07.2012 Public Library of Science (PLoS)
Subjects	3' Untranslated Regions Animals Base Sequence Body Patterning Conserved Sequence DNA Mutational Analysis Gene Regulatory Networks Genetic Association Studies Holoprosencephaly - genetics Humans Molecular Sequence Data Nuclear Proteins - genetics Prosencephalon - growth & development Sequence Alignment Transcription Factors - genetics Zebrafish
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Abstract	Coding region alterations of ZIC2 are the second most common type of mutation in holoprosencephaly (HPE). Here we use several complementary bioinformatic approaches to identify ultraconserved cis-regulatory sequences potentially driving the expression of human ZIC2. We demonstrate that an 804 bp element in the 3' untranslated region (3'UTR) is highly conserved across the evolutionary history of vertebrates from fish to humans. Furthermore, we show that while genetic variation of this element is unexpectedly common among holoprosencephaly subjects (6/528 or >1%), it is not present in control individuals. Two of six proband-unique variants are de novo, supporting their pathogenic involvement in HPE outcomes. These findings support a general recommendation that the identification and analysis of key ultraconserved elements should be incorporated into the genetic risk assessment of holoprosencephaly cases.
AbstractList	Coding region alterations of ZIC2 are the second most common type of mutation in holoprosencephaly (HPE). Here we use several complementary bioinformatic approaches to identify ultraconserved cis-regulatory sequences potentially driving the expression of human ZIC2. We demonstrate that an 804 bp element in the 3' untranslated region (3'UTR) is highly conserved across the evolutionary history of vertebrates from fish to humans. Furthermore, we show that while genetic variation of this element is unexpectedly common among holoprosencephaly subjects (6/528 or >1%), it is not present in control individuals. Two of six proband-unique variants are de novo, supporting their pathogenic involvement in HPE outcomes. These findings support a general recommendation that the identification and analysis of key ultraconserved elements should be incorporated into the genetic risk assessment of holoprosencephaly cases. Coding region alterations of ZIC2 are the second most common type of mutation in holoprosencephaly (HPE). Here we use several complementary bioinformatic approaches to identify ultraconserved cis-regulatory sequences potentially driving the expression of human ZIC2. We demonstrate that an 804 bp element in the 3' untranslated region (3'UTR) is highly conserved across the evolutionary history of vertebrates from fish to humans. Furthermore, we show that while genetic variation of this element is unexpectedly common among holoprosencephaly subjects (6/528 or >1%), it is not present in control individuals. Two of six proband-unique variants are de novo, supporting their pathogenic involvement in HPE outcomes. These findings support a general recommendation that the identification and analysis of key ultraconserved elements should be incorporated into the genetic risk assessment of holoprosencephaly cases.Coding region alterations of ZIC2 are the second most common type of mutation in holoprosencephaly (HPE). Here we use several complementary bioinformatic approaches to identify ultraconserved cis-regulatory sequences potentially driving the expression of human ZIC2. We demonstrate that an 804 bp element in the 3' untranslated region (3'UTR) is highly conserved across the evolutionary history of vertebrates from fish to humans. Furthermore, we show that while genetic variation of this element is unexpectedly common among holoprosencephaly subjects (6/528 or >1%), it is not present in control individuals. Two of six proband-unique variants are de novo, supporting their pathogenic involvement in HPE outcomes. These findings support a general recommendation that the identification and analysis of key ultraconserved elements should be incorporated into the genetic risk assessment of holoprosencephaly cases.
Audience	Academic
Author	Elnitski, Laura Roessler, Erich Odenwald, Ward F Richieri-Costa, Antonio Petrykowska, Hanna Carrington, Blake Srivastava, Kshitij Ribeiro, Lucilene A Hong, Sung-Kook Hu, Ping Sood, Raman Muenke, Maximilian Feldman, Benjamin
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SubjectTerms	3' Untranslated Regions Animals Base Sequence Body Patterning Conserved Sequence DNA Mutational Analysis Gene Regulatory Networks Genetic Association Studies Holoprosencephaly - genetics Humans Molecular Sequence Data Nuclear Proteins - genetics Prosencephalon - growth & development Sequence Alignment Transcription Factors - genetics Zebrafish
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Title	Unique alterations of an ultraconserved non-coding element in the 3'UTR of ZIC2 in holoprosencephaly
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