The role of regulatory T cell (Treg) subsets in gestational diabetes mellitus.

6533b854fe1ef96bd12aebf9

RESEARCH PRODUCT

The role of regulatory T cell (Treg) subsets in gestational diabetes mellitus.

Andrea Steinborn Edgar Schmitt Julia Spratte Christof Sohn Linda Schober D. Radnai Herbert Fluhr Lorenz Uhlmann A. Kisielewicz Karsten Mahnke

subject

Adult medicine.medical_specialty endocrine system diseases Regulatory T cell Immunology chemical and pharmacologic phenomena Cell Separation Lymphocyte Activation T-Lymphocytes Regulatory Immunophenotyping Young Adult Immune system Insulin resistance immune system diseases Pregnancy T-Lymphocyte Subsets hemic and lymphatic diseases Internal medicine medicine Immune Tolerance Immunology and Allergy Homeostasis Humans IL-2 receptor Interleukin-7 receptor business.industry FOXP3 hemic and immune systems Cell Differentiation Forkhead Transcription Factors T helper cell Original Articles medicine.disease Flow Cytometry Gestational diabetes Diabetes Gestational Endocrinology medicine.anatomical_structure Immunology CD4 Antigens Female business Immunologic Memory

description

Physiological changes during normal pregnancy are characterized by an inflammatory immune response and insulin resistance. Therefore, we hypothesize that gestational diabetes mellitus (GDM) may be caused by an inappropriate adaption of the maternal immune system to pregnancy. In this study we examined the role of regulatory T cell (Treg) differentiation for the development of GDM during pregnancy. We used six-colour flow cytometric analysis to demonstrate that the total CD4(+) CD127(low+/-) CD25(+) forkhead box protein 3 (FoxP3(+)) T(reg) pool consists of four different T(reg) subsets: naive CD45RA(+) T(regs), HLA-DR(-) CD45RA(-) memory T(regs) (DR(-) T(regs)) and the highly differentiated and activated HLA-DR(low+) CD45RA(-) and HLA-DR(high+) CD45RA(-) memory T(regs) (DR(low+) and DR(high+) T(regs)). Compared to healthy pregnancies, the percentage of CD4(+) CD127(low+/-) CD25(+) FoxP3(+) T(regs) within the total CD4(+) T helper cell pool was not different in patients affected by GDM. However, the suppressive activity of the total CD4(+) CD127(low+/-) CD25(+) T(reg) pool was significantly reduced in GDM patients. The composition of the total T(reg) pool changed in the way that its percentage of naive CD45RA(+) T(regs) was decreased significantly in both patients with dietary-adjusted GDM and patients with insulin-dependent GDM. In contrast, the percentage of DR(-) -memory T(regs) was increased significantly in patients with dietary-adjusted GDM, while the percentage of DR(low+) and DR(high+) memory T(regs) was increased significantly in patients with insulin-dependent GDM. Hence, our findings propose that alterations in homeostatic parameters related to the development and function of naive and memory T(regs) may cause the reduction of the suppressive capacity of the total T(reg) pool in GDM patients. However, as this is an exploratory analysis, the results are only suggestive and require further validation.

year	journal	country	edition	language
2014-02-13	Clinical and experimental immunology

10.1111/cei.12300 https://pubmed.ncbi.nlm.nih.gov/24547967