Systemic chemokine and chemokine receptor responses are divergent in allergic versus non‐allergic humans

JD Campbell, MJ Stinson, FER Simons… - International …, 2002 - academic.oup.com
JD Campbell, MJ Stinson, FER Simons, KT HayGlass
International immunology, 2002academic.oup.com
Abstract Th1‐and Th2‐polarized human T cell clones display distinct patterns of chemokine
receptor expression and selective chemokine responsiveness in vitro. We hypothesized that
natural exposure to environmental grass pollen would induce differential systemic
chemokine and chemokine receptor expression patterns in individuals with allergic rhinitis
compared to healthy controls with type 2‐and type 1‐dominated responses to allergen
respectively. To this end, we compared chemokine receptor expression on peripheral blood …
Abstract
Th1‐ and Th2‐polarized human T cell clones display distinct patterns of chemokine receptor expression and selective chemokine responsiveness in vitro. We hypothesized that natural exposure to environmental grass pollen would induce differential systemic chemokine and chemokine receptor expression patterns in individuals with allergic rhinitis compared to healthy controls with type 2‐ and type 1‐dominated responses to allergen respectively. To this end, we compared chemokine receptor expression on peripheral blood T cells directly ex vivo and plasma chemokine levels between these two groups of study participants prior to and during the grass pollen season. Th1‐associated CXC chemokine receptor (CXCR) 3 was strongly expressed on >50% CD4+/CD45RO+ cells of all subjects. When examined longitudinally, CXCR3 expression increased over the grass pollen season (P < 0.0001), solely in non‐allergic subjects. In contrast, for both allergic and non‐allergic subjects, CC chemokine receptor (CCR) 5 (Th1‐associated) and CCR3 (Th2‐associated) were weakly expressed on <10% of CD4+/CD45RO+ cells both prior to and during the grass pollen season. Type 1 chemokines CXC chemokine ligand (CXCL) 9 and CXCL10 (monokine induced by IFN‐γ and IFN‐γ‐inducible protein of 10 kDa: CXCR3 ligands), and type 2 chemokines CC chemokine ligand (CCL) 11 (eotaxin: CCR3 ligand), CCL17 (thymus and activation‐regulated chemokine: CCR4 ligand) and CCL22 (monocyte‐derived chemokine: CCR4 ligand) were readily detectable in the plasma of most participants. Systemic CXCL9 levels decreased from pre‐ to grass pollen season in allergics (P < 0.05), whereas CCL17 decreased in non‐allergics (P < 0.05) over the same period. Taken together, these longitudinal data suggest a systemic shift to more intensely type 1‐dominated responses in non‐allergic individuals and, conversely, to more type 2‐dominated responses in allergic individuals upon natural re‐exposure to grass pollen.
Oxford University Press