Expanded clinical spectrum in hepatocyte nuclear factor 1B-maturity-onset 
diabetes of the young

Raile, Klemens; Klopocki, Eva; Holder, Martin; Wessel, Theda; Galler, Angela; Deiss, Dorothee; Müller, Dominik; Riebel, Thomas; Horn, Denise; Maringa, Monika; Weber, Jürgen; Ullmann, Reinhard; Grüters, Annette

doi:10.1210/jc.2008-2189

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Expanded clinical spectrum in hepatocyte nuclear factor 1B-maturity-onset diabetes of the young

Raile, K., Klopocki, E., Holder, M., Wessel, T., Galler, A., Deiss, D., et al. (2009). Expanded clinical spectrum in hepatocyte nuclear factor 1B-maturity-onset diabetes of the young. Journal of Clinical Endocrinology & Metabolism, 94(7), 2658-2664. doi:10.1210/jc.2008-2189.

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Datensatz-Permalink: https://hdl.handle.net/11858/00-001M-0000-0010-7D62-A Versions-Permalink: https://hdl.handle.net/11858/00-001M-0000-0010-7D63-8

Genre: Zeitschriftenartikel

Alternativer Titel : J Clin Endocrinol Metab

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Urheber:
Raile, Klemens, Autor
Klopocki, Eva¹, Autor
Holder, Martin, Autor
Wessel, Theda, Autor
Galler, Angela, Autor
Deiss, Dorothee, Autor
Müller, Dominik, Autor
Riebel, Thomas, Autor
Horn, Denise, Autor
Maringa, Monika, Autor
Weber, Jürgen, Autor
Ullmann, Reinhard², Autor
Grüters, Annette, Autor

Affiliations:
1Research Group Development & Disease (Head: Stefan Mundlos), Max Planck Institute for Molecular Genetics, Max Planck Society, ou_1433557
2Molecular Cytogenetics (Reinhard Ullmann), Dept. of Human Molecular Genetics (Head: Hans-Hilger Ropers), Max Planck Institute for Molecular Genetics, Max Planck Society, ou_1479645

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Zusammenfassung: Aims: HNF1B-maturity-onset diabetes of the young is caused by abnormalities in the HNF1B gene encoding the transcription factor HNF-1β. We aimed to investigate detailed clinical features and the type of HNF1B gene anomaly in five pediatric cases with HNF1B-MODY. Methods: From a cohort of 995 children and adolescents with diabetes, we analyzed the most frequent maturity-onset diabetes of the young genes (GCK, HNF1A, HNF4A) including HNF1B sequencing and deletion analysis by quantitative Multiplex-PCR of Short Fluorescent Fragments (QMPSF) if patients were islet autoantibody-negative and had one parent with diabetes or associated extrapancreatic features or detectable C-peptide outside honeymoon phase. Presence and size of disease-causing chromosomal rearrangements detected by QMPSF were further analyzed by array comparative genomic hybridization. Results: Overall, five patients had a heterozygous HNF1B deletion, presenting renal disease, elevated liver enzymes, and diabetes. Diabetes was characterized by insulin resistance and adolescent onset of hyperglycemia. Additionally, clinical features in some patients were pancreas dysplasia and exocrine insufficiency (two of five patients), genital defects (three of five), mental retardation (two of five), and eye abnormalities (coloboma, cataract in two of five). One case also had severe growth deficit combined with congenital cholestasis, and another case had common variable immune deficiency. All patients reported here had monoallelic loss of the entire HNF1B gene. Whole genome array comparative genomic hybridization confirmed a precurrent genomic deletion of approximately 1.3–1.7 Mb in size. Conclusion: The clinical data of our cases enlarge the wide spectrum of patients with HNF1B anomaly. The underlying molecular defect in all cases was a 1.3- to 1.7-Mb deletion, and paired, segmental duplications along with breakpoints were most likely involved in this recurrent chromosomal microdeletion.