ESPE Abstracts (2016) 86 P-P1-907

ESPE2016 Poster Presentations Thyroid P1 (48 abstracts)

Dysregulation of the Immune System in Children with Graves Disease – the Role of NK and NKT-Like Cells

Maria Klatka a , Agnieszka Polak b , Ewelina Grywalska b , Witold Kollataj a & Jacek Rolinski b


aDepartment of Pediatric Endocrinology and Diabetology, Medical University, Lublin, Poland; bDepartment of Immunology, Medical University, Lublin, Poland


Background: Almost all cases of hyperthyroidism in children result from Graves’ disease (GD). Recent studies have confirmed a significant role of T cells in the development of autoimmune diseases. However, the interactions between NKT-like cells and NK cells in GD are still poorly understood.

Objective and hypotheses: The aim of the study was to assess the frequencies of peripheral blood T, NK and NKT-like cells in children with GD.

Method: We studied 50 GD and 20 age- and sex-matched healthy children. Percentages of NK and NKT-like cells were evaluated with flow cytometry using monoclonal antibodies: anti-CD3/FITC, CD16CD56/PE, CD45/PerCP (BD Biosciences), which allowed for simultaneous assessment of CD3+T lymphocytes and NK (CD16+CD56+) cells. During analysis, the CD3+CD16+CD56+ population was also determined. Immunofluorescence studies on T cell subsets were performed using a combination of the following mAbs: CD3/FITC, CD19/PE, CD8/FITC, CD4/PE, purchased from R&D Systems. Statistical analysis of the results was conducted using Statistica 9.0. A value p less than 0.05 was considered statistically significant.

Results: The mean frequency of CD3+CD56+CD16+ NKT-like cells in the peripheral blood of children with GD was 10.93%±11.02% and this value was significantly lower in comparison to the control group (21.15%±9.08%, P=0.0005). The mean percentage of CD56+CD16+ NK cells in the group of patients was 14.67%±6.89%, and was significantly higher compared to the healthy controls (4.71%±2.99%, P=0.000002). The mean percentage of CD3+T lymphocytes in the peripheral blood of children with GD was 67.91%±16.56% and was significantly higher in comparison to the control group (51.7%±24.12%, P=0.02). The mean percentage of CD8+T lymphocytes in the study group was 28.89%±11.68% and was significantly higher in comparison to the healthy controls (18.72%±6.86%, P=0.001).

Conclusion: Our findings of the abnormalities in immune cells distribution in peripheral blood of GD children suggest that GD development and progression is related to the dysregulation of the immune system.

Volume 86

55th Annual ESPE (ESPE 2016)

Paris, France
10 Sep 2016 - 12 Sep 2016

European Society for Paediatric Endocrinology 

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