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The expanding phenotype of POMT1 mutations: from Walker-Warburg syndrome to congenital muscular dystrophy, microcephaly, and mental retardation

The importance of O‐glycosylation of alpha‐dystroglycan (α‐DG) is evident from the identification of POMT1 mutations in Walker‐Warburg syndrome (WWS). Approximately one‐fifth of the WWS patients show mutations in POMT1, which result in complete loss of protein mannosyltransferase activity. WWS patie...

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Published in:	Human mutation 2006-05, Vol.27 (5), p.453-459
Main Authors:	van Reeuwijk, Jeroen, Maugenre, Svetlana, van den Elzen, Christa, Verrips, Aad, Bertini, Enrico, Muntoni, Francesco, Merlini, Luciano, Scheffer, Hans, Brunner, Han G., Guicheney, Pascale, van Bokhoven, Hans
Format:	Article
Language:	English
Subjects:	Adolescent Brain - abnormalities Brain - pathology Child, Preschool Chromosome Mapping DNA Mutational Analysis dystroglycan Dystroglycans - genetics Dystroglycans - metabolism Eye Abnormalities - genetics Female genotype-phenotype Humans Intellectual Disability - diagnosis Intellectual Disability - genetics Intellectual Disability - pathology Male Mannosyltransferases - genetics Mannosyltransferases - metabolism Microcephaly - diagnosis Microcephaly - genetics Microcephaly - pathology Microsatellite Repeats muscle-eye-brain Muscular Dystrophies - diagnosis Muscular Dystrophies - genetics Muscular Dystrophies - pathology Mutation Phenotype Polymorphism, Genetic POMT1 Syndrome Walker-Warburg syndrome
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creator	van Reeuwijk, Jeroen Maugenre, Svetlana van den Elzen, Christa Verrips, Aad Bertini, Enrico Muntoni, Francesco Merlini, Luciano Scheffer, Hans Brunner, Han G. Guicheney, Pascale van Bokhoven, Hans
description	The importance of O‐glycosylation of alpha‐dystroglycan (α‐DG) is evident from the identification of POMT1 mutations in Walker‐Warburg syndrome (WWS). Approximately one‐fifth of the WWS patients show mutations in POMT1, which result in complete loss of protein mannosyltransferase activity. WWS patients are characterized by congenital muscular dystrophy (CMD) with severe brain and eye abnormalities. This suggests a crucial role for α‐DG during development of these organs and tissues. Here we report new POMT1 mutations and polymorphisms in WWS patients. In addition, we report different compound heterozygous POMT1 mutations in four unrelated families that result in a less severe phenotype than WWS, characterized by CMD with calf hypertrophy, microcephaly, and mental retardation. Compared to WWS patients, these patients have milder structural brain abnormalities, and eye abnormalities were absent, except for myopia in some cases. In these patients we postulate that one or both transcripts for POMT1 confer residual protein O‐mannosyltransferase activity. Our data suggest the existence of a disease spectrum of CMD including brain and eye abnormalities resulting from POMT1 mutations. Hum Mutat 27(5), 453–459, 2006. © 2006 Wiley‐Liss, Inc.
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Approximately one‐fifth of the WWS patients show mutations in POMT1, which result in complete loss of protein mannosyltransferase activity. WWS patients are characterized by congenital muscular dystrophy (CMD) with severe brain and eye abnormalities. This suggests a crucial role for α‐DG during development of these organs and tissues. Here we report new POMT1 mutations and polymorphisms in WWS patients. In addition, we report different compound heterozygous POMT1 mutations in four unrelated families that result in a less severe phenotype than WWS, characterized by CMD with calf hypertrophy, microcephaly, and mental retardation. Compared to WWS patients, these patients have milder structural brain abnormalities, and eye abnormalities were absent, except for myopia in some cases. In these patients we postulate that one or both transcripts for POMT1 confer residual protein O‐mannosyltransferase activity. Our data suggest the existence of a disease spectrum of CMD including brain and eye abnormalities resulting from POMT1 mutations. 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Mutat</addtitle><description>The importance of O‐glycosylation of alpha‐dystroglycan (α‐DG) is evident from the identification of POMT1 mutations in Walker‐Warburg syndrome (WWS). Approximately one‐fifth of the WWS patients show mutations in POMT1, which result in complete loss of protein mannosyltransferase activity. WWS patients are characterized by congenital muscular dystrophy (CMD) with severe brain and eye abnormalities. This suggests a crucial role for α‐DG during development of these organs and tissues. Here we report new POMT1 mutations and polymorphisms in WWS patients. In addition, we report different compound heterozygous POMT1 mutations in four unrelated families that result in a less severe phenotype than WWS, characterized by CMD with calf hypertrophy, microcephaly, and mental retardation. Compared to WWS patients, these patients have milder structural brain abnormalities, and eye abnormalities were absent, except for myopia in some cases. 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Mutat</addtitle><date>2006-05</date><risdate>2006</risdate><volume>27</volume><issue>5</issue><spage>453</spage><epage>459</epage><pages>453-459</pages><issn>1059-7794</issn><eissn>1098-1004</eissn><abstract>The importance of O‐glycosylation of alpha‐dystroglycan (α‐DG) is evident from the identification of POMT1 mutations in Walker‐Warburg syndrome (WWS). Approximately one‐fifth of the WWS patients show mutations in POMT1, which result in complete loss of protein mannosyltransferase activity. WWS patients are characterized by congenital muscular dystrophy (CMD) with severe brain and eye abnormalities. This suggests a crucial role for α‐DG during development of these organs and tissues. Here we report new POMT1 mutations and polymorphisms in WWS patients. In addition, we report different compound heterozygous POMT1 mutations in four unrelated families that result in a less severe phenotype than WWS, characterized by CMD with calf hypertrophy, microcephaly, and mental retardation. Compared to WWS patients, these patients have milder structural brain abnormalities, and eye abnormalities were absent, except for myopia in some cases. In these patients we postulate that one or both transcripts for POMT1 confer residual protein O‐mannosyltransferase activity. Our data suggest the existence of a disease spectrum of CMD including brain and eye abnormalities resulting from POMT1 mutations. Hum Mutat 27(5), 453–459, 2006. © 2006 Wiley‐Liss, Inc.</abstract><cop>Hoboken</cop><pub>Wiley Subscription Services, Inc., A Wiley Company</pub><pmid>16575835</pmid><doi>10.1002/humu.20313</doi><tpages>7</tpages><oa>free_for_read</oa></addata></record>
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subjects	Adolescent Brain - abnormalities Brain - pathology Child, Preschool Chromosome Mapping DNA Mutational Analysis dystroglycan Dystroglycans - genetics Dystroglycans - metabolism Eye Abnormalities - genetics Female genotype-phenotype Humans Intellectual Disability - diagnosis Intellectual Disability - genetics Intellectual Disability - pathology Male Mannosyltransferases - genetics Mannosyltransferases - metabolism Microcephaly - diagnosis Microcephaly - genetics Microcephaly - pathology Microsatellite Repeats muscle-eye-brain Muscular Dystrophies - diagnosis Muscular Dystrophies - genetics Muscular Dystrophies - pathology Mutation Phenotype Polymorphism, Genetic POMT1 Syndrome Walker-Warburg syndrome
title	The expanding phenotype of POMT1 mutations: from Walker-Warburg syndrome to congenital muscular dystrophy, microcephaly, and mental retardation
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