AI Article Synopsis
- The 620Trp variant of the LYP protein, linked to autoimmunity, was studied for its impact on lymphocyte activation in children with T1D, autoantibody-positive children, and healthy controls.
- Analysis revealed that T1D patients with the 620Trp variant showed decreased CD4(+)T cell proliferation and IL-2 production after specific stimulation.
- No significant effects were observed in PBMC proliferation or cytokine secretion in other groups, suggesting that the LYP 620Trp variant contributes to reduced T-cell activation specifically in T1D patients and may play a role in the development of autoimmunity against beta cells.
Article Abstract
The 620Trp variant of the LYP protein, encoded by the lymphoid tyrosine phosphatase 22 gene (PTPN22), is associated with autoimmunity. In this study we aimed at characterising the role of this variant on lymphocyte activation. We analysed cytokine secretion and proliferation of peripheral blood mononuclear cells (PBMCs) and CD4(+)T cells in a cohort of clinically non-diabetic, multiple autoantibody-positive children, healthy controls and in children with type 1 diabetes (T1D). We found a decreased proliferation and IL-2 production of CD4(+)T cells after anti-CD3/anti-CD28 stimulation (p=0.04 for IL-2) among T1D patients. In addition, a profoundly decreased intracellular calcium flux in CD4(+)T cells after PHA stimulus was detected among 620Trp carriers. In contrast, no effect of this polymorphism on tuberculin and tetanus toxoid induced PBMC proliferation and cytokine secretion was observed in autoantibody positive children, healthy controls and children with newly-diagnosed T1D. In conclusion, the LYP 620Trp variant is associated with reduced activation, proliferation and IL-2 production in CD4(+)T cells among T1D patients. In accordance with our previous findings on the key role of this variant on disease progression, this mechanism is likely to contribute to the development of beta-cell specific autoimmunity.
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| http://dx.doi.org/10.1016/j.jaut.2008.01.001 | DOI Listing |
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