| Literature DB >> 28473463 |
Matthew B Johnson1, Elisa De Franco1, Hana Lango Allen1, Aisha Al Senani2, Nancy Elbarbary3, Zeynep Siklar4, Merih Berberoglu4, Zineb Imane5, Alireza Haghighi6,7,8, Zahra Razavi9, Irfan Ullah10, Saif Alyaarubi10, Daphne Gardner11, Sian Ellard1, Andrew T Hattersley12, Sarah E Flanagan1.
Abstract
Young-onset autoimmune diabetes associated with additional autoimmunity usually reflects a polygenic predisposition, but rare cases result from monogenic autoimmunity. Diagnosing monogenic autoimmunity is crucial for patients' prognosis and clinical management. We sought to identify novel genetic causes of autoimmunity presenting with neonatal diabetes (NDM) (diagnosis <6 months). We performed exome sequencing in a patient with NDM and autoimmune lymphoproliferative syndrome and his unrelated, unaffected parents and identified compound heterozygous null mutations in LRBA Biallelic LRBA mutations cause common variable immunodeficiency-8; however, NDM has not been confirmed in this disorder. We sequenced LRBA in 169 additional patients with diabetes diagnosed <1 year without mutations in the 24 known NDM genes. We identified recessive null mutations in 8 additional probands, of which, 3 had NDM (<6 months). Diabetes was the presenting feature in 6 of 9 probands. Six of 17 (35%) patients born to consanguineous parents and with additional early-onset autoimmunity had recessive LRBA mutations. LRBA testing should be considered in patients with diabetes diagnosed <12 months, particularly if they have additional autoimmunity or are born to consanguineous parents. A genetic diagnosis is important as it can enable personalized therapy with abatacept, a CTLA-4 mimetic, and inform genetic counseling.Entities:
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Year: 2017 PMID: 28473463 PMCID: PMC5524180 DOI: 10.2337/db17-0040
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461