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Etiology and pathogenesis of robin sequence in a large Dutch cohort

Robin sequence (RS) can be defined as the combination of micrognathia and upper airway obstruction/glossoptosis causing neonatal respiratory problems, with or without a cleft palate and either isolated or non‐isolated. Pathogenesis varies widely. We hypothesize that optimal treatment depends on path...

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Published in:	American journal of medical genetics. Part A 2015-09, Vol.167A (9), p.1983-1992
Main Authors:	Basart, Hanneke, Paes, Emma C., Maas, Saskia M., van den Boogaard, Marie-Jose H., van Hagen, Johanna M., Breugem, Corstiaan C., Cobben, Jan Maarten, Don Griot, J. Peter W., Lachmeijer, Augusta M. A., Lichtenbelt, Klaske D., van Nunen, Daan P. F., van der Horst, Chantal M., Hennekam, Raoul C.
Format:	Article
Language:	English
Subjects:	Airway Obstruction - etiology Airway Obstruction - pathology Arthritis - etiology Arthritis - pathology cause Cleft Palate - pathology Connective Tissue Diseases - etiology Connective Tissue Diseases - pathology Female genetic diagnosis Hearing Loss, Sensorineural - etiology Hearing Loss, Sensorineural - pathology Humans intellectual disability Male Micrognathism - etiology Micrognathism - pathology pathogenesis Pierre Robin Syndrome - etiology Pierre Robin Syndrome - pathology Retinal Detachment - etiology Retinal Detachment - pathology robin sequence stratification syndrome treatment
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cited_by	cdi_FETCH-LOGICAL-c4724-6f897d05a812c28a599612890317a95e80b898924993a0f4ec58e168451d9bbe3
cites	cdi_FETCH-LOGICAL-c4724-6f897d05a812c28a599612890317a95e80b898924993a0f4ec58e168451d9bbe3
container_end_page	1992
container_issue	9
container_start_page	1983
container_title	American journal of medical genetics. Part A
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creator	Basart, Hanneke Paes, Emma C. Maas, Saskia M. van den Boogaard, Marie-Jose H. van Hagen, Johanna M. Breugem, Corstiaan C. Cobben, Jan Maarten Don Griot, J. Peter W. Lachmeijer, Augusta M. A. Lichtenbelt, Klaske D. van Nunen, Daan P. F. van der Horst, Chantal M. Hennekam, Raoul C.
description	Robin sequence (RS) can be defined as the combination of micrognathia and upper airway obstruction/glossoptosis causing neonatal respiratory problems, with or without a cleft palate and either isolated or non‐isolated. Pathogenesis varies widely. We hypothesize that optimal treatment depends on pathogenesis and therefore patients should be stratified according to diagnosis. Here, we evaluate diagnoses and (presumed) pathogeneses in an RS cohort. Medical records of all RS patients presenting between 1995–2013 in three academic hospitals were evaluated. Four clinical geneticists re‐evaluated all information, including initial diagnosis. Diagnoses were either confirmed, considered uncertain, or rejected. If uncertain or rejected, patients were re‐evaluated. Subsequent results were re‐discussed and a final conclusion was drawn. We included 191 RS patients. After re‐evaluation and changing initial diagnoses in 48 of the 191 patients (25.1%), 37.7% of the cohort had isolated RS, 8.9% a chromosome anomaly, 29.3% a Mendelian disorder, and 24.1% no detectable cause. Twenty‐two different Mendelian disorders were diagnosed, of which Stickler syndrome was most frequent. Stratification of diagnoses according to (presumed) pathogenic mechanism in 73 non‐isolated patients with reliable diagnoses showed 43.9% to have a connective tissue dysplasia, 5.5% a neuromuscular disorder, 47.9% a multisystem disorder, and 2.7% an unknown mechanism. We diagnosed more non‐isolated RS patients compared to other studies. Re‐evaluation changed initial diagnosis in a quarter of patients. We suggest standardized re‐evaluation of all RS patients. Despite the relatively high diagnostic yield pathogenesis could be determined in only 59.7% (71/119), due to limited insight in pathogenesis in diagnosed entities. Further studies into pathogenesis of entities causing RS are indicated. © 2015 Wiley Periodicals, Inc.
doi_str_mv	10.1002/ajmg.a.37154
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Peter W. ; Lachmeijer, Augusta M. A. ; Lichtenbelt, Klaske D. ; van Nunen, Daan P. F. ; van der Horst, Chantal M. ; Hennekam, Raoul C.</creator><creatorcontrib>Basart, Hanneke ; Paes, Emma C. ; Maas, Saskia M. ; van den Boogaard, Marie-Jose H. ; van Hagen, Johanna M. ; Breugem, Corstiaan C. ; Cobben, Jan Maarten ; Don Griot, J. Peter W. ; Lachmeijer, Augusta M. A. ; Lichtenbelt, Klaske D. ; van Nunen, Daan P. F. ; van der Horst, Chantal M. ; Hennekam, Raoul C.</creatorcontrib><description>Robin sequence (RS) can be defined as the combination of micrognathia and upper airway obstruction/glossoptosis causing neonatal respiratory problems, with or without a cleft palate and either isolated or non‐isolated. Pathogenesis varies widely. We hypothesize that optimal treatment depends on pathogenesis and therefore patients should be stratified according to diagnosis. Here, we evaluate diagnoses and (presumed) pathogeneses in an RS cohort. Medical records of all RS patients presenting between 1995–2013 in three academic hospitals were evaluated. Four clinical geneticists re‐evaluated all information, including initial diagnosis. Diagnoses were either confirmed, considered uncertain, or rejected. If uncertain or rejected, patients were re‐evaluated. Subsequent results were re‐discussed and a final conclusion was drawn. We included 191 RS patients. After re‐evaluation and changing initial diagnoses in 48 of the 191 patients (25.1%), 37.7% of the cohort had isolated RS, 8.9% a chromosome anomaly, 29.3% a Mendelian disorder, and 24.1% no detectable cause. Twenty‐two different Mendelian disorders were diagnosed, of which Stickler syndrome was most frequent. Stratification of diagnoses according to (presumed) pathogenic mechanism in 73 non‐isolated patients with reliable diagnoses showed 43.9% to have a connective tissue dysplasia, 5.5% a neuromuscular disorder, 47.9% a multisystem disorder, and 2.7% an unknown mechanism. We diagnosed more non‐isolated RS patients compared to other studies. Re‐evaluation changed initial diagnosis in a quarter of patients. We suggest standardized re‐evaluation of all RS patients. Despite the relatively high diagnostic yield pathogenesis could be determined in only 59.7% (71/119), due to limited insight in pathogenesis in diagnosed entities. 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Medical records of all RS patients presenting between 1995–2013 in three academic hospitals were evaluated. Four clinical geneticists re‐evaluated all information, including initial diagnosis. Diagnoses were either confirmed, considered uncertain, or rejected. If uncertain or rejected, patients were re‐evaluated. Subsequent results were re‐discussed and a final conclusion was drawn. We included 191 RS patients. After re‐evaluation and changing initial diagnoses in 48 of the 191 patients (25.1%), 37.7% of the cohort had isolated RS, 8.9% a chromosome anomaly, 29.3% a Mendelian disorder, and 24.1% no detectable cause. Twenty‐two different Mendelian disorders were diagnosed, of which Stickler syndrome was most frequent. Stratification of diagnoses according to (presumed) pathogenic mechanism in 73 non‐isolated patients with reliable diagnoses showed 43.9% to have a connective tissue dysplasia, 5.5% a neuromuscular disorder, 47.9% a multisystem disorder, and 2.7% an unknown mechanism. 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Part A</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Basart, Hanneke</au><au>Paes, Emma C.</au><au>Maas, Saskia M.</au><au>van den Boogaard, Marie-Jose H.</au><au>van Hagen, Johanna M.</au><au>Breugem, Corstiaan C.</au><au>Cobben, Jan Maarten</au><au>Don Griot, J. Peter W.</au><au>Lachmeijer, Augusta M. A.</au><au>Lichtenbelt, Klaske D.</au><au>van Nunen, Daan P. F.</au><au>van der Horst, Chantal M.</au><au>Hennekam, Raoul C.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Etiology and pathogenesis of robin sequence in a large Dutch cohort</atitle><jtitle>American journal of medical genetics. Part A</jtitle><addtitle>Am. J. Med. Genet</addtitle><date>2015-09</date><risdate>2015</risdate><volume>167A</volume><issue>9</issue><spage>1983</spage><epage>1992</epage><pages>1983-1992</pages><issn>1552-4825</issn><eissn>1552-4833</eissn><abstract>Robin sequence (RS) can be defined as the combination of micrognathia and upper airway obstruction/glossoptosis causing neonatal respiratory problems, with or without a cleft palate and either isolated or non‐isolated. Pathogenesis varies widely. We hypothesize that optimal treatment depends on pathogenesis and therefore patients should be stratified according to diagnosis. Here, we evaluate diagnoses and (presumed) pathogeneses in an RS cohort. Medical records of all RS patients presenting between 1995–2013 in three academic hospitals were evaluated. Four clinical geneticists re‐evaluated all information, including initial diagnosis. Diagnoses were either confirmed, considered uncertain, or rejected. If uncertain or rejected, patients were re‐evaluated. Subsequent results were re‐discussed and a final conclusion was drawn. We included 191 RS patients. After re‐evaluation and changing initial diagnoses in 48 of the 191 patients (25.1%), 37.7% of the cohort had isolated RS, 8.9% a chromosome anomaly, 29.3% a Mendelian disorder, and 24.1% no detectable cause. Twenty‐two different Mendelian disorders were diagnosed, of which Stickler syndrome was most frequent. Stratification of diagnoses according to (presumed) pathogenic mechanism in 73 non‐isolated patients with reliable diagnoses showed 43.9% to have a connective tissue dysplasia, 5.5% a neuromuscular disorder, 47.9% a multisystem disorder, and 2.7% an unknown mechanism. We diagnosed more non‐isolated RS patients compared to other studies. Re‐evaluation changed initial diagnosis in a quarter of patients. We suggest standardized re‐evaluation of all RS patients. Despite the relatively high diagnostic yield pathogenesis could be determined in only 59.7% (71/119), due to limited insight in pathogenesis in diagnosed entities. Further studies into pathogenesis of entities causing RS are indicated. © 2015 Wiley Periodicals, Inc.</abstract><cop>United States</cop><pub>Blackwell Publishing Ltd</pub><pmid>26033782</pmid><doi>10.1002/ajmg.a.37154</doi><tpages>10</tpages></addata></record>
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subjects	Airway Obstruction - etiology Airway Obstruction - pathology Arthritis - etiology Arthritis - pathology cause Cleft Palate - pathology Connective Tissue Diseases - etiology Connective Tissue Diseases - pathology Female genetic diagnosis Hearing Loss, Sensorineural - etiology Hearing Loss, Sensorineural - pathology Humans intellectual disability Male Micrognathism - etiology Micrognathism - pathology pathogenesis Pierre Robin Syndrome - etiology Pierre Robin Syndrome - pathology Retinal Detachment - etiology Retinal Detachment - pathology robin sequence stratification syndrome treatment
title	Etiology and pathogenesis of robin sequence in a large Dutch cohort
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