Biogenic amines activate blood leukocytes via trace amine-associated receptors TAAR1 and TAAR2

被引:92
作者
Babusyte, Agne [1 ]
Kotthoff, Matthias [1 ]
Fiedler, Julia [1 ]
Krautwurst, Dietmar [1 ]
机构
[1] Leibniz Inst, German Res Ctr Food Chem, D-85354 Freising Weihenstephan, Germany
关键词
Olfactory receptors; GPCR; dimers; siRNA; cytokines; immune response; 3-IODOTHYRONAMINE; EXPRESSION; IDENTIFICATION; RESPONSES; AGONISTS; SUBSET;
D O I
10.1189/jlb.0912433
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Certain biogenic amines, such as 2-PEA, TYR, or T1AM, modulate blood pressure, cardiac function, brain monoaminergic systems, and olfaction-guided behavior by specifically interacting with members of a group of rhodopsin-like receptors, TAAR. A receptor that is absent from olfactory epithelia but had long been identified in the brain and a variety of peripheral tissues, TAAR1 has been found recently in blood B cells, suggesting a functional role of TAAR1 in these cells. With the present study, we have set out to clarify the expression and functional roles of TAAR in different isolated human blood leukocyte types. Here, we report the functional expression of TAAR1 and its closest relative TAAR2 in blood PMN and T and B cells. Both receptors are coexpressed in a subpopulation of PMN, where they are necessary for the chemosensory migration toward the TAAR1 ligands 2-PEA, TYR, and T1AM, with EC50 values of 0.43 +/- 0.05 nM, 0.52 +/- 0.05 nM, and 0.25 +/- 0.04 nM, respectively. The same amines, with similar potencies, triggered cytokine or Ig secretion, in purified blood T or B cells, respectively. Notably, 2-PEA regulated mRNA expression of 28 T cell function-related genes, above all of the CCL5. In siRNA-guided experiments, TAAR1 and TAAR2 proved to be necessary for amine-induced blood leukocyte functions. In summary, our results demonstrate that biogenic amines potently regulate blood cell functions via TAAR1 and TAAR2 and open the perspective of their specific pharmacological modulation. J. Leukoc. Biol. 93: 387-394; 2013.
引用
收藏
页码:387 / 394
页数:8
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