Differential expression of CXCR3 targeting chemokines CXCL10, CXCL9, and CXCL11 in different types of skin inflammation

Flier, Jacoba; Boorsma, D. M.; Beek, Peter J. van; Nieboer, C.; Stoof, T.J.; Willemze, Rein; Tensen, Cornelis P.

doi:10.1002/1096-9896(200108)194:4<397::aid-path899>3.0.co;2-s

Cited by 318 publications

(248 citation statements)

References 27 publications

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“…We have analyzed a subset of CKRs that are important in memory T cell biology, and addressed which of these CKRs are coexpressed on CCR10 ϩ memory CD4 T cells. The ligands for CCR4 (16 -18), CCR6 (19,20), and CXCR3 (18,21) are found in inflamed skin, and ligands for CCR7 are found in both lymphoid and peripheral tissues (1). Coexpression of different CKRs investigates the potential for cooperative or redundant mechanisms to facilitate T cell entry into peripheral tissues during immune surveillance or during T cell-mediated disease episodes.…”

Section: Resultsmentioning

confidence: 99%

Immune Surveillance and Effector Functions of CCR10+ Skin Homing T Cells

Hudak¹,

Hagen²,

Liu³

et al. 2002

The Journal of Immunology

106

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Skin homing T cells carry memory for cutaneous Ags and play an important sentinel and effector role in host defense against pathogens that enter via the skin. CCR10 is a chemokine receptor that is preferentially expressed among blood leukocytes by a subset of memory CD4 and CD8 T cells that coexpress the skin-homing receptor cutaneous lymphocyte Ag (CLA), but not the gut-homing receptor α4β7. Homing and chemokine receptor coexpression studies detailed in this study suggest that the CLA+/CCR10+ memory CD4 T cell population contains members that have access to both secondary lymphoid organ and skin compartments; and therefore, can act as both “central” and “effector” memory T cells. Consistent with this effector phenotype, CLA+/CCR10+ memory CD4 T cells from normal donors secrete TNF and IFN-γ but minimal IL-4 and IL-10 following in vitro stimulation. Interactions of CCR10 and its skin-associated ligand CC ligand 27 may play an important role in facilitating memory T cell entry into cutaneous sites during times of inflammation.

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Section: Resultsmentioning

confidence: 99%

Immune Surveillance and Effector Functions of CCR10+ Skin Homing T Cells

Hudak¹,

Hagen²,

Liu³

et al. 2002

The Journal of Immunology

106

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“…Expression of IP-10 and its receptor CXCR3 has been shown to be associated with the development of several Th1-type human inflammatory diseases, including psoriasis, multiple sclerosis, atherosclerosis, rheumatoid arthritis, and myasthenia gravis (41)(42)(43)(44)(45)(46). In addition, elevated IP-10 gene expression has been found in association with rejection of human cardiac allografts and mouse cardiac, small bowel, and pancreatic islet allografts (47,48).…”

Section: Discussionmentioning

confidence: 99%

Antagonist of interferon‐inducible protein 10/CXCL10 ameliorates the progression of autoimmune sialadenitis in MRL/lpr mice

Hasegawa¹,

Inoue²,

Kohno³

et al. 2006

Arthritis & Rheumatism

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Objective. Mononuclear cell infiltration of the salivary glands is a major feature of Sjögren's syndrome (SS) and its animal model. Local generation of chemokines and the presence of chemokine receptors on the infiltrating cells may be involved in this process. We undertook the present study to investigate the expression of chemokines during the development of autoimmune sialadenitis in MRL/lpr mice and the therapeutic effect of chemokine antagonists on sialadenitis.Methods. NH 2 -terminal-truncated interferoninducible protein 10 (IP-10)/CXCL10 analogs were transfected into a nonmetastatic fibroblastoid cell line, MRL/N-1, and injected subcutaneously into MRL/lpr mice, and the effects on sialadenitis were monitored.Results. IP-10 analogs truncated by 5 or more amino acid residues from the N-terminal failed to induce chemotaxis and calcium influx by CXCR3-expressing cells. Of these, the most potent antagonist (AT) (IP-10-AT) was a molecule with methionine added after removal of the 5 N-terminal amino acid residues. Significantly increased expression of the Th1-associated chemokines IP-10, monokine induced by interferon-␥/ CXCL9, and interferon-inducible T cell chemoattractant/CXCL11 was induced in the ductal epithelium by interferon-␥ produced in the salivary glands, whereas expression of the Th2-associated chemokines thymus and activation-regulated chemokine (TARC)/ CCL17 and monocyte-derived chemokine/CCL22 was almost undetectable during sialadenitis. Inoculation of IP-10-AT into MRL/lpr mice during the early stage of sialadenitis significantly reduced periductal mononuclear cell infiltration and parenchymal destruction compared with these features in control and TARC-ATbearing mice. This was due to a significant reduction in infiltration of CXCR3؉ T cells, predominantly Th1 cells, resulting in decreased interferon-␥ production.Conclusion. We prepared a novel potent IP-10 antagonist and demonstrated its ability to ameliorate the progression of autoimmune sialadenitis. This agent may provide a new therapeutic approach to SS.

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“…During the past few years, several studies have demonstrated a pathogenetic role of CXCR3 and its ligands in human inflammatory diseases [12][13][14][15][16][17][18]. Blockade of CXCR3 interactions with its ligands in vivo therefore represents a possible therapeutic goal for the treatment of these disorders.…”

Section: Discussionmentioning

confidence: 99%

“…CXCR3 and its ligands play an important role in the induction and perpetuation of several human inflammatory disorders including autoimmune diseases, arteriosclerosis, transplant rejection and viral infections [12][13][14][15]. Recent studies have shown that the CXCR3 ligands exhibit unique temporal and spatial expression patterns, suggesting that they have nonredundant functions in vivo [16][17][18]. Moreover, the CXCR3 ligands share low sequence homology (around 40% amino acid identity) and exhibit differences in their potencies and efficacies at CXCR3, with CXCL11 being the dominant ligand [11,19].…”

Section: Introductionmentioning

confidence: 99%

Molecular characterization of the chemokine receptor CXCR3: evidence for the involvement of distinct extracellular domains in a multi‐step model of ligand binding and receptor activation

2003

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CXCR3 is a chemokine receptor predominantly expressed on T lymphocytes, and binds the chemokines CXCL9 (Mig), CXCL10 (IP-10) and CXCL11 (I-TAC). Here, we have investigated the role of the extracellular domains of CXCR3 in ligand selectivity and receptor activation by assessing the ligand binding and chemotactic responses of chimeric CXCR3/CXCR1 constructs. Our data reveal that the second extracellular loop of CXCR3 is essential for receptor activation in response to all CXCR3 ligands. In contrast, the N terminus and first extracellular loop of CXCR3 play some role in CXCL10-and CXCL11-mediated activation but are dispensable for CXCL9-induced signaling. The third extracellular loop of CXCR3 is important only for CXCL9-and CXCL10-induced chemotaxis. Binding studies suggest that the CXCR3 ligands bind to distinct sites composed of multiple domains of CXCR3 and that high-affinity binding and receptor activation are disparate functions. Collectively, our data support a multi-site model for CXCR3 interactions with its agonists, in which several extracellular domains of CXCR3 contribute to ligand binding and the induction of receptor activation. The development of antagonists targeting the second extracellular loop of CXCR3 should impede receptor activation and aid the treatment of several human inflammatory disorders.

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Differential expression of CXCR3 targeting chemokines CXCL10, CXCL9, and CXCL11 in different types of skin inflammation

Cited by 318 publications

References 27 publications

Immune Surveillance and Effector Functions of CCR10+ Skin Homing T Cells

Immune Surveillance and Effector Functions of CCR10+ Skin Homing T Cells

Antagonist of interferon‐inducible protein 10/CXCL10 ameliorates the progression of autoimmune sialadenitis in MRL/lpr mice

Molecular characterization of the chemokine receptor CXCR3: evidence for the involvement of distinct extracellular domains in a multi‐step model of ligand binding and receptor activation

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