Inflammation-associated lysophospholipids as ligands for CD1d-restricted T cells in human cancer

DH Chang, H Deng, P Matthews… - Blood, The Journal …, 2008 - ashpublications.org
DH Chang, H Deng, P Matthews, J Krasovsky, G Ragupathi, R Spisek, A Mazumder…
Blood, The Journal of the American Society of Hematology, 2008ashpublications.org
CD1d-restricted T cells have been implicated in the pathogenesis of several chronic
inflammatory states. However, the nature of the specific ligands recognized by these cells in
vivo in patients with inflammatory or malignant diseases remains unknown. We took a
biochemical approach to directly isolate and characterize the nature of CD1d-binding
ligands from the plasma of myeloma patients. Characterization of these ligands revealed
several lysophosphatidylcholine (LPC) species. Human LPC-CD1d dimer binding cells are …
Abstract
CD1d-restricted T cells have been implicated in the pathogenesis of several chronic inflammatory states. However, the nature of the specific ligands recognized by these cells in vivo in patients with inflammatory or malignant diseases remains unknown. We took a biochemical approach to directly isolate and characterize the nature of CD1d-binding ligands from the plasma of myeloma patients. Characterization of these ligands revealed several lysophosphatidylcholine (LPC) species. Human LPC-CD1d dimer binding cells are T-cell receptorαβ+ T cells but predominantly Vα24Vβ11. Cytokine secretion by LPC-specific T cells is skewed toward IL-13 secretion, and the frequencies of these cells are increased in myeloma patients relative to healthy donors. These data identify a distinct population of human CD1d-restricted T cells specific for inflammation-associated lysolipids and suggest a novel mechanism for inflammation mediated immune regulation in human cancer.
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