Delta-opioid receptors expressed by Jurkat T cells enhance IL-2 secretion by increasing AP-1 complexes and activity of the NF-AT/AP-1-binding promoter element.

KE Hedin, MP Bell, KR Kalli, CJ Huntoon… - … (Baltimore, Md.: 1950 …, 1997 - journals.aai.org
KE Hedin, MP Bell, KR Kalli, CJ Huntoon, BM Sharp, DJ McKean
Journal of immunology (Baltimore, Md.: 1950), 1997journals.aai.org
Recent molecular evidence points to transient and/or stage-specific expression of delta-and
kappa-opioid receptors by thymic and peripheral T lymphocytes. Since medical treatments
or stress commonly increase opioid levels, it is important to understand the mechanisms by
which opioids affect T lymphocyte functions. We therefore created and studied a T cell line
expressing the cloned delta-opioid receptor (DOR1). DOR1 ligation by a specific DOR1
agonist, deltorphin, augmented IL-2 secretion by synergizing with signals from TCR-CD3 …
Abstract
Recent molecular evidence points to transient and/or stage-specific expression of delta- and kappa-opioid receptors by thymic and peripheral T lymphocytes. Since medical treatments or stress commonly increase opioid levels, it is important to understand the mechanisms by which opioids affect T lymphocyte functions. We therefore created and studied a T cell line expressing the cloned delta-opioid receptor (DOR1). DOR1 ligation by a specific DOR1 agonist, deltorphin, augmented IL-2 secretion by synergizing with signals from TCR-CD3 and CD28. Reporter gene constructs were used to map this effect of deltorphin to the AP-1- and NF-AT/AP-1-binding sites of the IL-2 promoter. Although DOR1 signaling increased [Ca2+]i, deltorphin enhanced transcriptional activity of the NF-AT/AP-1-binding site via a mechanism independent of calcineurin and distinct from the effects of elevated [Ca2+]i. Deltorphin also increased accumulation of AP-1 transcription factor complexes, suggesting that DOR1 augments IL-2 secretion by increasing the AP-1 component of the NF-AT/AP-1 transcription factor. These results advance the molecular understanding of opioid effects on lymphocytes, and in addition, demonstrate regulation of IL-2 synthesis and secretion by the novel mechanism of receptor-mediated AP-1 induction.
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