A novel role for IL-22R1 as a driver of inflammation

作者:Savan Ram; McFarland Adelle P; Reynolds Della A; Feigenbaum Lionel; Ramakrishnan Karthika; Karwan Megan; Shirota Hidekazu; Klinman Dennis M; Dunleavy Kieron; Pittaluga Stefania; Anderson Stephen K; Donnelly Raymond P; Wilson Wyndham H; Young Howard A*
来源:Blood, 2011, 117(2): 575-584.
DOI:10.1182/blood-2010-05-285908

摘要

The interleukin (IL)-22R1 chain of the heterodimeric IL-22 receptor is not expressed on normal leukocytes, but this receptor is expressed on T cells from anaplastic lymphoma kinase-positive (ALK(+)) anaplastic large cell lymphoma (ALCL) patients. To investigate the consequences of aberrant expression of this receptor on lymphocytes, we generated transgenic mice that express IL-22R1 on lymphocytes. The health of these animals progressively deteriorated at 8 to 12 weeks of age, as they displayed respiratory distress, rough coat and sluggish movement, and subsequent lethality due to multiorgan inflammation. The IL-22R1 transgenic animals developed neutrophilia that correlated with increased levels of circulating IL-17 and granulocyte colony-stimulating factor. In addition, these mice had increased serum IL-22 levels, suggesting that T cells expressing IL-22R1 generate IL-22 in a positive autoregulatory loop. As a result of the mouse model findings, we analyzed circulating cytokine levels in ALK(+)ALCL patients and detected elevated levels of IL-22, IL-17, and IL-8 in untreated patient samples. Importantly, IL-22 and IL-17 were undetectable in all patients who were in complete remission after chemotherapy. This study documents a previously unknown role of IL-22R1 in inflammation and identifies the involvement of IL-22R1/IL-22 in ALK(+)ALCL. (Blood. 2011;117(2):575-584)

  • 出版日期2011-1-13