Agonist signalling properties of radiotracers used for imaging of dopamine D2/3 receptors

نویسندگان

  • Jan-Peter van Wieringen
  • Martin C Michel
  • Henk M Janssen
  • Anton G Janssen
  • Philip H Elsinga
  • Jan Booij
چکیده

BACKGROUND Dopamine D2/3 receptor (D2/3R) agonist radiopharmaceuticals are considered superior to antagonists to detect dopamine release, e.g. induced by amphetamines. Agonists bind preferentially to the high-affinity state of the dopamine D2R, which has been proposed as the reason why agonists are more sensitive to detect dopamine release than antagonist radiopharmaceuticals, but this theory has been challenged. Interestingly, not all agonists similarly activate the classic cyclic adenosine mono phosphate (cAMP) and the ?-arrestin-2 pathway, some stimulate preferentially one of these pathways; a phenomenon called biased agonism. Because these pathways can be affected separately by pathologies or drugs (including dopamine releasers), it is important to know how agonist radiotracers act on these pathways. Therefore, we characterized the intracellular signalling of the well-known D2/3R agonist radiopharmaceuticals NPA and PHNO and of several novel D2/3R agonists. METHODS cAMP accumulation and ?-arrestin-2 recruitment were measured on cells expressing human D2R. RESULTS All tested agonists showed (almost) full agonism in both pathways. CONCLUSIONS The tested D2/3R agonist radiopharmaceuticals did not exhibit biased agonism in vitro. Consequently, it is likely that drugs (including psychostimulants like amphetamines) and/or pathologies that influence the cAMP and/or the ?-arrestin-2 pathway may influence the binding of these radiopharmaceuticals.

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عنوان ژورنال:

دوره 4  شماره 

صفحات  -

تاریخ انتشار 2014