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dc.contributor.authorShozu M.en
dc.contributor.authorUmezawa A.en
dc.contributor.authorShihara D.en
dc.contributor.authorNakabayashi K.en
dc.contributor.authorBulun S.E.en
dc.contributor.authorOgata T.en
dc.contributor.authorFukami M.en
dc.contributor.authorTsuchiya T.en
dc.contributor.authorVollbach H.en
dc.contributor.authorBrown K.A.en
dc.contributor.authorAbe S.en
dc.contributor.authorOhtsu S.en
dc.contributor.authorWabitsch M.en
dc.contributor.authorBurger H.en
dc.contributor.authorSimpson E.R.en
dc.date.accessioned2021-05-14T09:18:27Zen
dc.date.available2021-05-14T09:18:27Zen
dc.date.copyright2013en
dc.date.created20140113en
dc.date.issued2014-01-13en
dc.identifier.citationJournal of Clinical Endocrinology and Metabolism. 98 (12) (pp E2013-E2021), 2013. Date of Publication: December 2013.en
dc.identifier.issn0021-972Xen
dc.identifier.urihttps://repository.monashhealth.org/monashhealthjspui/handle/1/27638en
dc.description.abstractContext: Genomic rearrangements at 15q21 have been shown to cause overexpression of CYP19A1 and resultant aromatase excess syndrome (AEXS). However, mutation spectrum, clinical consequences, and underlying mechanisms of these rearrangements remain to be elucidated. Objective(s): The aim of the study was to clarify such unsolved matters. Design, Setting, and Methods: We characterized six new rearrangements and investigated clinical outcome and local genomic environments of these rearrangements and of three previously reported duplications/deletions. Result(s): Novel rearrangements included simple duplication involving exons 1-10 of CYP19A1 and simple and complex rearrangements that presumably generated chimeric genes consisting of the coding region of CYP19A1 and promoter-associated exons of neighboring genes. Clinical severities were primarily determined by the copy number of CYP19A1 and the property of the fused promoters. Sequences at the fusion junctions suggested nonallelic homologous recombination, nonhomologous end-joining, and replication-based errors as the underlying mechanisms. The breakpoint- flanking regions were not enriched with GC content, palindromes, noncanonical DNA structures, or known rearrangement-associated motifs. The rearrangements resided in early-replicating segments. Conclusion(s): These results indicate that AEXS is caused by duplications involving CYP19A1 and simple and complex rearrangements that presumably lead to the usage of cryptic promoters of several neighboring genes. Our data support the notion that phenotypes depend on the dosage of CYP19A1 and the characteristics of the fused promoters. Furthermore,weshowthat the rearrangements inAEXSare generated by both recombination- and replication-mediated mechanisms, independent of theknown rearrangement-inducing DNA features or late-replication timing. Thus, AEXS represents a unique model for human genomic disorders. © 2013 by The Endocrine Society.en
dc.languageEnglishen
dc.languageenen
dc.publisherEndocrine Society (8401 Connecticut Ave. Suite 900, Chevy Chase MD 20815, United States)en
dc.titleGenomic basis of aromatase excess syndrome: Recombination- and replication-Mediated rearrangements leading to CYP19A1 overexpression.en
dc.typeArticleen
dc.identifier.doihttp://monash.idm.oclc.org/login?url=http://dx.doi.org/10.1210/jc.2013-2520en
dc.publisher.placeUnited Statesen
dc.identifier.pubmedid24064691 [http://www.ncbi.nlm.nih.gov/pubmed/?term=24064691]en
dc.identifier.source370458369en
dc.identifier.institution(Fukami, Tsuchiya, Shihara, Ogata) Department of Molecular Endocrinology, National Research Institute for Child Health and Development, 157-8535 Tokyo, Japan (Tsuchiya) Department of Pediatrics, Dokkyo Medical University Koshigaya Hospital, 343-8555 Koshigaya, Japan (Vollbach, Wabitsch) Department of Pediatrics and Adolescent Medicine, University Medical Center Ulm, 89081 Ulm, Germany (Brown, Burger, Simpson) Metabolism and Cancer Laboratory, Prince Henry's Institute, Monash Medical Centre, Clayton, 3168 VIC, Australia (Abe) Department of Pediatrics, Hakodate Goryoukaku Hospital, 040-8611 Hakodate, Japan (Ohtsu) Department of Pediatrics, Kitasato University School of Medicine, 252-0375 Kanagawa, Japan (Umezawa) Department of Reproductive Biology, Center for Regenerative Medicine, National Institute for Child Health and Development, 157-8535 Tokyo, Japan (Nakabayashi) Department of Maternal-Fetal Biology, National Research Institute for Child Health and Development, 157-8535 Tokyo, Japan (Bulun) Division of Reproductive Biology Research, Department of Obstetrics and Gynecology, Feinberg School of Medicine, Chicago, 60611 IL, United States (Shozu) Department of Reproductive Medicine, Graduate School of Medicine, Chiba University, 260-8670 Chiba, Japan (Ogata) Department of Pediatrics, Hamamatsu University School of Medicine, 431-3192 Hamamatsu, Japanen
dc.description.addressM. Fukami, Department of Molecular Endocrinology, National Research Institute for Child Health and Development, 157-8535 Tokyo, Japan. E-mail: fukami-m@ncchd.go.jpen
dc.description.publicationstatusEmbaseen
dc.rights.statementCopyright 2014 Elsevier B.V., All rights reserved.en
dc.identifier.authoremailFukami M.; fukami-m@ncchd.go.jpen
item.cerifentitytypePublications-
item.grantfulltextnone-
item.fulltextNo Fulltext-
item.openairetypeArticle-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
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