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Pro‐inflammatory chemokine–chemokine receptor interactions within the Ewing sarcoma microenvironment determine CD8 + T‐lymphocyte infiltration and affect tumour progression
Author(s) -
Berghuis Dagmar,
Santos Susy J,
Baelde Hans J,
Taminiau Antonie HM,
Maarten Egeler R,
Schilham Marco W,
Hogendoorn Pancras CW,
Lankester Arjan C
Publication year - 2011
Publication title -
the journal of pathology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.964
H-Index - 184
eISSN - 1096-9896
pISSN - 0022-3417
DOI - 10.1002/path.2819
Subject(s) - ccl5 , cxcl10 , tumor microenvironment , chemokine , stromal cell , cxcl9 , chemokine receptor , biology , cd8 , cancer research , cxcr3 , cytotoxic t cell , immune system , ccl17 , cxcl16 , cc chemokine receptors , immunology , t cell , il 2 receptor , biochemistry , in vitro
Ewing sarcoma is an aggressive round cell sarcoma with poor patient prognosis, particularly in cases of advanced‐stage disease. Dynamic tumor‐host immune interations within the tumor microenvironment may polarize in situ immune responses and shape tumor development and/or progression. To gain insight into the nature of tumour–host immune interactions within the Ewing sarcoma microenvironment, the presence and spatial distribution of infiltrating CD8 + /CD4 + T‐lymphocytes were evaluated in therapy‐naive Ewing sarcoma. Expression profiling of 40 different chemokines and several chemokine receptors was performed in therapy‐naive tumours and cell lines by qPCR, immunohistochemistry, and flow cytometry. Considerable inter‐tumour variation was observed regarding density, type, and distribution of infiltrating T‐lymphocytes. Tumour‐infiltrating T‐cells contained significantly higher percentages of CD8 + T‐lymphocytes as compared to stroma‐infiltrating cells, suggesting preferential migration of this T‐cell type into tumour areas. Gene expression levels of several type 1‐associated, pro‐inflammatory chemokines (CXCR3‐ and CCR5‐ligands CXCL9, CXCL10 , and CCL5 ) correlated positively with infiltrating (CD8 + ) T‐lymphocyte numbers expressing corresponding chemokine receptors. Survival analyses demonstrated an impact of tumour‐infiltrating, and not stroma‐infiltrating, CD8 + T‐lymphocytes on tumour progression. At protein level, both tumour and stromal cells expressed the IFNγ‐inducible chemokines CXCL9 and CXCL10. CCR5‐ligand CCL5 was exclusively expressed by non‐tumoural stromal/infiltrating cells. Together, our results indicate that an inflammatory immune microenvironment with high expression of type 1‐associated chemokines may be critical for the recruitment of (CD8 + ) T‐lymphocytes expressing corresponding chemokine receptors. The observed impact of tumour‐infiltrating (CD8 + ) T‐lymphocytes is consistent with a role for adaptive anti‐tumour immunity in the prevention of Ewing sarcoma progression. Recognition of the merits and exploitation/induction of an inflammatory microenvironment may improve the efficacy of natural immune responses against, and (adoptive) immunotherapeutic approaches for, Ewing sarcoma. Copyright © 2010 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.