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Monogenic Diabetes Not Caused By Mutations in Mody Genes: A Very Heterogenous Group of Diabetes
Author(s) -
Zeynep Şıklar,
Elisa De Franco,
Matthew B. Johnson,
Sarah E. Flanagan,
Sian Ellard,
Serdar Ceylaner,
Kaan Boztuğ,
Figen Doğu,
Aydan İkincioğulları,
Zarife Kuloğlu,
Aydan Kansu,
Merih Berberoğlu
Publication year - 2017
Publication title -
experimental and clinical endocrinology and diabetes
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.632
H-Index - 76
eISSN - 1439-3646
pISSN - 0947-7349
DOI - 10.1055/s-0043-120571
Subject(s) - diabetes mellitus , medicine , cohort , autoimmunity , maturity onset diabetes of the young , autoantibody , insulin , type 1 diabetes , type 2 diabetes , endocrinology , pediatrics , gastroenterology , immunology , disease , antibody
Monogenic diabetes represents a heterogeneous group of disorders resulting from a single gene defect leading to disruption of insulin secretion or a reduction in the number of beta cells. Despite the classification of monogenic diabetes into neonatal diabetes or maturity onset diabetes of the young (MODY) according to age of onset, not every case can be classified into those 2 groups. We evaluated patients with monogenic diabetes diagnosed during the last 10 year period. Type 1 DM, MODY, and patients with negative autoantibodies and no mutation in a known gene were excluded from the study. Thirteen patients were diagnosed with monogenic diabetes in Department of Pediatric Endocrinology, Ankara University School of Medicine, Ankara, Turkey. Five of them were diagnosed after 6 months of age. Five had a KATP channel defect. Mutations in genes resulting in destruction of beta cells were detected in 7 patients, with 4 cases having a WFS, 2 an LRBA, and one a IL2RA mutation. Additional systemic findings were seen in 6/13 patients, with 5/6 having severe immune system dysfunction. Treatment with sulphonylurea was successful in two patients.. The other patients were given insulin in differing doses. Four patients died during follow-up, three of which had immune system dysfunction. Monogenic diabetes can be diagnosed after 6 months of age, even with positive autoantibodies. Immune dysfunction was a common feature in our cohort and should be investigated in all patients with early-onset monogenic diabetes. Mortality of patients with monogenic diabetes and additional autoimmunity was high in our cohort and is likely to reflect the multisystem nature of these diseases.

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