Studies of immunological risk factors in type 1 diabetes / Jenny Walldén.
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Walldén, Jenny, 1977- (författare)
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Vaarala, Outi (preses)
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Ludvigsson, Johnny (preses)
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Malmström, Vivianne (opponent)
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- Linköpings universitet. Institutionen för klinisk och experimentell medicin (utgivare)
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Alternativt namn: Linköping University. Department of Clinical and Experimental Medicine
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Alternativt namn: Linköping University. Faculty of Health Sciences. Department of Clinical and Experimental Medicine
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Alternativt namn: IKE
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- Hälsouniversitetet i Östergötland (utgivare)
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Alternativt namn: Linköpings högskola. Medicinska fakulteten
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Alternativt namn: Linköpings universitet. Medicinska fakulteten
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Alternativt namn: Linköping University. Faculty of Health Sciences
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Alternativt namn: Linköping University. Health University
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Alternativt namn: Hälsouniversitetet i Linköping
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Se även: Universitetet i Linköping. Medicinska fakulteten
(tidigare namn)
- Publicerad: Linköping : Department of Clinical and Experimental Medicine, Linköping University, 2008
- Engelska 1 onlineresurs (106 sidor)
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Serie: Linköping University medical dissertations, 0345-0082 ; 1075
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Läs hela texten (Sammanfattning och ramberättelse från Linköping University Electronic Press)
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Sammanfattning
Ämnesord
Stäng
- Background: Type 1 diabetes (T1D) is a chronic, autoimmune disease caused by a T cell mediated destruction of ß -cells in pancreas. The development of T1D is determined by a combination of genetic susceptibility genes and environmental factors involved in the pathogenesis of T1D. This thesis aimed to investigate diverse environmental and immunological risk factors associated with the development of T1D. This was accomplished by comparing autoantibody development, T cell responses and the function of CD4 + CD25 + regulatory T cells between healthy children, children at risk of T1D and T1D patients. Results: Induction of autoantibodies in as young children as one year old, was associated with previously identified environmental risk factors of T1D, such as maternal gastroenteritis during pregnancy and early introduction of cow’s milk. We did not see any general increase in the activity of peripheral blood T H subtypes in children with HLA class II risk haplotypes associated with T1D, nor were HLA class II risk haplotypes associated with any aberrant cytokine production in response to antigenic stimulation of peripheral blood mononuclear cells. However children with a HLA class II protective haplotype showed an increased production of IFN- γ in response to enteroviral stimulation. CTLA-4 polymorphisms connected with a risk of autoimmune disease were associated with enhanced production of IFN- γ . Healthy children with ß -cell autoantibodies had a lower expression level of GATA-3 compared to health children with HLA risk genotype or children without risk. Instead, children with manifest T1D showed lower expression levels of T-bet, IL-12R ß 1 and IL-4R α . Both T1D and healthy children showed the same expression of the regulatory markers Foxp3, CTLA-4 and ICOS in peripheral blood mononuclear cells, and the amount of CD4 + CD25 + T cells did neither reveal any differences. The regulatory T cells seemed also to be functional in children with T1D, since increased proliferation after depletion of CD4 + CD25 high cells from PBMC was demonstrated in T1D as well as in healthy children.However, T1D children did have more intracellular CTLA-4 per CD4 + CD25 high T cell, increased levels of serum C-reactive protein and higher spontaneous expression of IFN- α in CD25depleted PBMC, all which are signs of activation of the immune system. This suggests a normal or enhanced functional activity of regulatory T cells in T1D at diagnosis. Conclusions: Our findings emphasize that environmental risk factors do have a role in the development of ß -cell autoimmunity. Our results do not support a systemic activation of the immune system in pre-diabetes or T1D, but instead a possible up-regulation of regulatory mechanisms seems to occur after diagnosis of T1D, which probably tries to dampen the autoimmune reaction taking place.
Ämnesord
- Typ 1-diabetes (sao)
- Autoantibodies -- blood (MeSH)
- Diabetes mellitus, type 1 -- epidemiology (MeSH)
- Diabetes mellitus, type 1 -- immunology (MeSH)
- Insulin-secreting cells -- immunology (MeSH)
- Natural Sciences (ssif)
- Biological Sciences (ssif)
- Immunology (ssif)
- Naturvetenskap (ssif)
- Biologi (ssif)
- Immunologi (ssif)
- NATURAL SCIENCES (svep)
- Biology (svep)
- Cell and molecular biology (svep)
- Immunology (svep)
- NATURVETENSKAP (svep)
- Biologi (svep)
- Cell- och molekylärbiologi (svep)
- Immunologi (svep)
- Diabetes (LCSH)
- Diabetes Mellitus, Type 1 (MeSH)
Genre
- government publication (marcgt)
Klassifikation
- 616.4622 (DDC)
- Veod (kssb/8 (machine generated))
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