T cell subsets in asthma and allergy - role of glucocorticoids, plasticity and microRNA-155
Abstract
The focus of this thesis is the different subsets of CD4+ T cells involvement in asthma and
allergy. It encloses studies of asthma and allergy in both humans and mice. The work of the
three papers has been performed during a time where the field has moved from a paradigm of
separate entities of the studied T cell subsets to more flexibility and plasticity in these cells
due to the microenvironment. Furthermore, the field of ribonucleic acid (RNA) has grown to
include new RNAs such as microRNA (miRNA), demonstrating high impact on the
microenvironment.
The aims of this thesis were to determine in: Paper I. Glucocorticoid treatment during natural
pollen exposure and the effects it poses on T regulatory (Treg), T helper 1 (Th) and Th2 cells
in the nasal mucosa of allergic rhinitis patients. Paper II. Plasticity in circulating Treg, Th1,
Th2 and Th17 cells and the relationship to eosinophilia in asthmatic individuals. Paper III.
miRNA-155 affecting T cell dependent allergen induced eosinophilic airway inflammation.
The results demonstrates that glucocorticoid treatment during pollen exposure affected the
number of Treg and Th2 cells as well as the balance between the subsets investigated at site
of inflammation. Furthermore, T cells co-expressing several regulatory transcription factors
were found in asthmatics as well as in healthy controls. Finally, miRNA-155 deficiency
reduced the number of airway eosinophils, Th2, Th17 and Treg cells after allergen challenge
in a mouse model of allergic airway inflammation, while the transcription factor PU.1 was
upregulated. Adoptive transfer of allergen specific CD4+ T cells resulted in a similar degree
of airway eosinophilia in miR-155 KO and WT mice.
We conclude that nasal glucocorticoids attenuate the allergic inflammation by maintaining the
local relationship between Th1 and Th2 cells as well as between Treg and Th2 cells.
Furthermore, T cells ability to co-express several regulatory transcription factors in both
asthmatics and healthy controls indicates plasticity in vivo. Finally, miRNA-155 contributes
to the regulation of allergic airway inflammation by modulating Th2 responses, via the
transcription factor PU.1.
Taken together these studies support that T cell shows flexibility and plasticity which can be
affected by treatment, allergen exposure and miRNA expression and thus are in important
regulators of asthma and allergy. Increasing the understanding of these processes may
hopefully result in more specific future treatments.
Parts of work
I. Malmhäll C, Bossios A, Pullerits T, Lötvall J. Effects of pollen and nasal glucocorticoid on FOXP3+, GATA-3+ and T-bet+ cells in allergic rhinitis. Allergy. 2007 Sep;62(9):1007-13. ::PMID::17686103 II.Malmhäll C, Bossios A, Rådinger M, Sjöstrand M, Lu Y, Lundbäck B, Lötvall J. Immunophenotyping of circulating T helper cells argues for multiple functions and plasticity of T cells in vivo in humans--possible role in asthma. PLoS One. 2012;7(6):e40012. Epub 2012 Jun 29. ::PMID::22768198 III. Malmhäll C, Alawieh S, Lu Y, Sjöstrand M, Bossios A, Eldh M, Rådinger M. MicroRNA-155 is essential for TH2-mediated allergen-induced eosinophilic inflammation in the lung. J Allergy Clin Immunol. 2013 Dec 24. pii: S0091-6749(13)01766-1. [Epub ahead of print]. ::PMID::24373357
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Inst of Medicine. Department of Internal Medicine and Clinical Nutrition
Disputation
Fredagen den 4 april 2014, kl 13:00, Hörsal Lyktan, Konferenscentrum Wallenberg, Medicinaregatan 20A, Göteborg
Date of defence
2014-04-04
carina.malmhall@gu.se
Date
2014-03-28Author
Malmhäll, Carina
Keywords
asthma
Allergy
T regulatory cells
Th1
Th2
Th17
FOXP3
T-bet
GATA-3
RORgt
glucocorticoids
plasticity
microRNA-155
PU.1
Publication type
Doctoral thesis
ISBN
978-91-628-8937-1 (tryckt)
978-91-628-8939-5 (pdf)
Language
eng