HLA Class II Alleles Susceptibility Markers of Type 1 Diabetes Fail to Specify Phenotypes of Ketosis-Prone Diabetes in Adult Tunisian Patients

Author:

Laadhar Lilia1,Harzallah Fatma2,Zitouni Mondher1,Kallel-Sellami Maryam1,Fekih Moncef3,Kaabachi Naziha3,Slimane Hádia2,Makni Sondès1

Affiliation:

1. Immunology Department, La Rabta Hospital and Al Manar University Tunis, 1007 Tunis, Tunisia

2. Endocrinology Department, La Rabta Hospital and Al Manar University Tunis, 1007 Tunis, Tunisia

3. Biochemistry Department, La Rabta Hospital and Al Manar University Tunis, 1007 Tunis, Tunisia

Abstract

We aimed to characterize the different subgroups of ketosis-prone diabetes (KPD) in a sample of Tunisian patients using the Aβ scheme based on the presence or absence of β-cell autoantibodies (A+ or A−) and β-cell functional reserve (β+ or β−) and we investigated whether HLA class II alleles could contribute to distinct KPD phenotypes. We enrolled 43 adult patients with a first episode of ketosis. For all patients we evaluated clinical parameters, β-cell autoimmunity, β-cell function and HLA class II alleles. Frequency distribution of the 4 subgroups was 23.3% A+β−, 23.3% A−β−, 11.6% A+β+ and 41.9% A−β+. Patients from the group A+β− were significantly younger than those from the group A−β− (P=.002). HLA susceptibility markers were significantly more frequent in patients with autoantibodies (P=.003). These patients also had resistance alleles but they were more frequent in A+β+ than A+β− patients (P=.04). Insulin requirement was not associated to the presence or the absence of HLA susceptibility markers. HLA class II alleles associated with susceptibility to autoimmune diabetes have not allowed us to further define Tunisian KPD groups. However, high prevalence of HLA resistance alleles in our patients may reflect a particular genetic background of Tunisian KPD population.

Funder

Tunisian Ministry of Health

Publisher

Hindawi Limited

Subject

General Medicine,Endocrinology, Diabetes and Metabolism

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