International Journal of Molecular Sciences (Nov 2014)

Analysis of Human TAAR8 and Murine Taar8b Mediated Signaling Pathways and Expression Profile

  • Jessica Mühlhaus,
  • Juliane Dinter,
  • Daniela Nürnberg,
  • Maren Rehders,
  • Maren Depke,
  • Janine Golchert,
  • Georg Homuth,
  • Chun-Xia Yi,
  • Silke Morin,
  • Josef Köhrle,
  • Klaudia Brix,
  • Matthias Tschöp,
  • Gunnar Kleinau,
  • Heike Biebermann

DOI
https://doi.org/10.3390/ijms151120638
Journal volume & issue
Vol. 15, no. 11
pp. 20638 – 20655

Abstract

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The thyroid hormone derivative 3-iodothyronamine (3-T1AM) exerts metabolic effects in vivo that contradict known effects of thyroid hormones. 3-T1AM acts as a trace amine-associated receptor 1 (TAAR1) agonist and activates Gs signaling in vitro. Interestingly, 3-T1AM-meditated in vivo effects persist in Taar1 knockout-mice indicating that further targets of 3-T1AM might exist. Here, we investigated another member of the TAAR family, the only scarcely studied mouse and human trace-amine-associated receptor 8 (Taar8b, TAAR8). By RT-qPCR and locked-nucleic-acid (LNA) in situ hybridization, Taar8b expression in different mouse tissues was analyzed. Functionally, we characterized TAAR8 and Taar8b with regard to cell surface expression and signaling via different G-protein-mediated pathways. Cell surface expression was verified by ELISA, and cAMP accumulation was quantified by AlphaScreen for detection of Gs and/or Gi/o signaling. Activation of G-proteins Gq/11 and G12/13 was analyzed by reporter gene assays. Expression analyses revealed at most marginal Taar8b expression and no gender differences for almost all analyzed tissues. In heart, LNA-in situ hybridization demonstrated the absence of Taar8b expression. We could not identify 3-T1AM as a ligand for TAAR8 and Taar8b, but both receptors were characterized by a basal Gi/o signaling activity, a so far unknown signaling pathway for TAARs.

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