Fetal cell microchimerism: a protective role in autoimmune thyroid diseases
| Autor: | Carla Colombo, Laura Fugazzola, Roberta Rizzo, Federica de Liso, Valentina Cirello, Maria Antonia Maffini, Milena Crippa, Palma Finelli, Silvia Bolzani, Daria Bortolotti, Stefano Ferrero, Guia Vannucchi, Irene Campi |
|---|---|
| Rok vydání: | 2015 |
| Předmět: |
Male
leukocyte antigen G Endocrinology Diabetes and Metabolism Thyroid Gland insertion/deletion polymorphism Disease Polymerase Chain Reaction Thyroiditis Endocrinology Pregnancy Hashimotos thyroiditis Aged 80 and over medicine.diagnostic_test Thyroid Microchimerism General Medicine progenitor cells Middle Aged Graves Disease medicine.anatomical_structure parity Female women Adult medicine.medical_specialty Human leukocyte antigen Hashimoto Disease Chimerism NO Immune system Fetus Internal medicine medicine microchimerism cancer Humans HLA-G Antigens Chromosomes Human Y Polymorphism Genetic business.industry Thyroiditis Autoimmune microchimerism leukocyte antigen G insertion/deletion polymorphism Hashimotos thyroiditis progenitor cells women pregnancy cancer parity DNA medicine.disease Immunology Blood Vessels business Fluorescence in situ hybridization |
| Zdroj: | European journal of endocrinology. 173(1) |
| ISSN: | 1479-683X |
| Popis: | ObjectiveThe physiological persistence of fetal cells in the circulation and tissue of a previously pregnant woman is called fetal cell microchimerism (FCM). It has been hypothesized to play a role in systemic autoimmune disease; however, only limited data are available regarding its role in autoimmune thyroid disease (AITD).DesignCirculating FCM was analyzed in a large series of previously pregnant women with Graves' disease (GD), Hashimoto's thyroiditis (HT), or no disease (healthy controls (HCs)). To exclude the possible bias related to placental factors, the polymorphic pattern of human leukocyte antigen-G (HLA-G) gene, which is known to be involved in the tolerance of fetal cells by the maternal immune system, was investigated.MethodsFCM was evaluated by PCR in the peripheral blood, and the Y chromosome was identified by fluorescencein situhybridization in some GD tissues.HLA-Gpolymorphism typing was assessed by real-time PCR.ResultsFCM was significantly more frequent in HC (63.6%) than in GD (33.3%) or HT (27.8%) women (P=0.0004 andP=0.001 respectively). A quantitative analysis confirmed that circulating male DNA was more abundant in HC than it was in GD or HT. Microchimeric cells were documented in vessels and in thyroid follicles. In neither GD/HT patients nor HC women was theHLA-Gtyping different between FCM-positive and FCM-negative cases.ConclusionThe higher prevalence of FCM in HC as compared to GD and HT patients suggests that it plays a possible protective role in autoimmune thyroid disorders. Placental factors have been excluded as determinants of the differences found. The vascular and tissue localization of microchimeric cells further highlights the ability of those cells to migrate to damaged tissues. |
| Databáze: | OpenAIRE |
| Externí odkaz: |
|