Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/31859
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dc.contributor.authorYe, Zimeng-
dc.contributor.authorLin, Sufang-
dc.contributor.authorZhao, Xia-
dc.contributor.authorBennett, Mark F-
dc.contributor.authorBrown, Natasha J-
dc.contributor.authorWallis, Mathew J-
dc.contributor.authorGao, Xinyi-
dc.contributor.authorSun, Li-
dc.contributor.authorWu, Jiarui-
dc.contributor.authorVedururu, Ravikiran-
dc.contributor.authorWitkowski, Tom-
dc.contributor.authorGardiner, Fiona-
dc.contributor.authorStutterd, Chloe A-
dc.contributor.authorDuan, Jing-
dc.contributor.authorMullen, Saul A-
dc.contributor.authorMcGillivray, George-
dc.contributor.authorBodek, Simon-
dc.contributor.authorValente, Giulia M-
dc.contributor.authorReagan, Matthew-
dc.contributor.authorYao, Yi-
dc.contributor.authorLi, Lin-
dc.contributor.authorChen, Li-
dc.contributor.authorBoys, Amber-
dc.contributor.authorAdikari, Thiuni N-
dc.contributor.authorCao, Dezhi-
dc.contributor.authorHu, Zhanqi-
dc.contributor.authorBeshay, Victoria-
dc.contributor.authorZhang, Victor W-
dc.contributor.authorBerkovic, Samuel F-
dc.contributor.authorScheffer, Ingrid E-
dc.contributor.authorLiao, Jianxiang-
dc.contributor.authorHildebrand, Michael S-
dc.date2022-
dc.date.accessioned2023-01-12T04:50:34Z-
dc.date.available2023-01-12T04:50:34Z-
dc.date.issued2022-12-
dc.identifier.citationHuman Mutation 2022; 43(12)en_US
dc.identifier.issn1098-1004-
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/31859-
dc.description.abstractTuberous sclerosis complex (TSC) is a multi-system genetic disorder. Most patients have germline mutations in TSC1 or TSC2 but, 10%-15% patients do not have TSC1/TSC2 mutations detected on routine clinical genetic testing. We investigated the contribution of low-level mosaic TSC1/TSC2 mutations in unsolved sporadic patients and families with TSC. Thirty-one sporadic TSC patients negative on routine testing and eight families with suspected parental mosaicism were sequenced using deep panel sequencing followed by droplet digital polymerase chain reaction. Pathogenic variants were found in 22/31 (71%) unsolved sporadic patients, 16 were mosaic (median variant allele fraction [VAF] 6.8% in blood) and 6 had missed germline mutations. Parental mosaicism was detected in 5/8 families (median VAF 1% in blood). Clinical testing laboratories typically only report pathogenic variants with allele fractions above 10%. Our findings highlight the critical need to change laboratory practice by implementing higher sensitivity assays to improve diagnostic yield, inform patient management and guide reproductive counseling.en_US
dc.language.isoeng-
dc.subjecthigh-depth sequencingen_US
dc.subjectmosaic mutationsen_US
dc.subjectparental mosaicismen_US
dc.subjecttuberous sclerosis complexen_US
dc.titleMosaicism in tuberous sclerosis complex: Lowering the threshold for clinical reporting.en_US
dc.typeJournal Articleen_US
dc.identifier.journaltitleHuman Mutationen_US
dc.identifier.affiliationEpilepsy Research Centreen_US
dc.identifier.affiliationDepartment of Neurology, Epilepsy Centre, Shenzhen Children's Hospital, Shenzhen, Guangdong Province, China.en_US
dc.identifier.affiliationMurdoch Children's Research Institute, Royal Children's Hospital, Parkville, Victoria, Australia.en_US
dc.identifier.affiliationAustin Healthen_US
dc.identifier.affiliationAmCare Genomics Laboratory, Guangzhou, Guangdong Province, China.en_US
dc.identifier.affiliationMolecular Diagnostic Pathology, Peter MacCallum Cancer Centre, Melbourne, Victoria, Australia.en_US
dc.identifier.affiliationVictorian Clinical Genetics Services, Royal Children's Hospital, Parkville, Victoria, Australia.en_US
dc.identifier.affiliationDepartment of Neurology, Epilepsy Centre, Shenzhen Children's Hospital, Shenzhen, Guangdong Province, China.en_US
dc.identifier.affiliationVictorian Clinical Genetics Services, Royal Children's Hospital, Parkville, Victoria, Australia.en_US
dc.identifier.affiliationDepartment of Medicine, Peninsula Health, Monash University, Frankston, Victoria, Australia.en_US
dc.identifier.affiliationMolecular Diagnostic Pathology, Peter MacCallum Cancer Centre, Melbourne, Victoria, Australia.en_US
dc.identifier.affiliationAmCare Genomics Laboratory, Guangzhou, Guangdong Province, China.en_US
dc.identifier.affiliationDepartment of Neurology, Epilepsy Centre, Shenzhen Children's Hospital, Shenzhen, Guangdong Province, China.en_US
dc.identifier.affiliationThe Florey Institute of Neuroscience and Mental Healthen_US
dc.identifier.doi10.1002/humu.24454en_US
dc.type.contentTexten_US
dc.identifier.orcid0000-0002-5578-9374en_US
dc.identifier.pubmedid36030538-
dc.description.volume43-
dc.description.issue12-
dc.description.startpage1956-
dc.description.endpage1969-
dc.subject.meshtermssecondaryTuberous Sclerosis/diagnosis-
dc.subject.meshtermssecondaryTuberous Sclerosis/genetics-
dc.subject.meshtermssecondaryTuberous Sclerosis/pathology-
dc.subject.meshtermssecondaryTuberous Sclerosis Complex 2 Protein/genetics-
dc.subject.meshtermssecondaryTuberous Sclerosis Complex 1 Protein/genetics-
dc.subject.meshtermssecondaryTumor Suppressor Proteins/genetics-
local.name.researcherBennett, Mark F
item.languageiso639-1en-
item.fulltextNo Fulltext-
item.grantfulltextnone-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.cerifentitytypePublications-
item.openairetypeJournal Article-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptClinical Genetics-
crisitem.author.deptOlivia Newton-John Cancer Research Institute-
crisitem.author.deptClinical Genetics-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptClinical Genetics-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptNeurology-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptMedicine (University of Melbourne)-
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