Effect of Dopamine D2 Receptor Antagonists
on [18F]-FEOBV Binding

Schildt, Anna; de Vries, Erik F.J.; Willemsen, Antoon T.M.; Giacobbo, Bruno Lima; Moraga-Amaro, Rodrigo; Sijbesma, Jürgen W.A.; van Waarde, Aren; Sossi, Vesna; Dierckx, Rudi A.J.O.; Doorduin, Janine

doi:10.1021/acs.molpharmaceut.9b01129.s001

mp9b01129_si_001.pdf (58.14 kB)

Effect of Dopamine D₂ Receptor Antagonists on [¹⁸F]-FEOBV Binding

journal contribution

posted on 2020-02-17, 17:05 authored by Anna Schildt, Erik F.J. de Vries, Antoon T.M. Willemsen, Bruno Lima Giacobbo, Rodrigo Moraga-Amaro, Jürgen W.A. Sijbesma, Aren van Waarde, Vesna Sossi, Rudi A.J.O. Dierckx, Janine Doorduin

The interaction of dopaminergic and cholinergic neurotransmission in, e.g., Parkinson’s disease has been well established. Here, D₂ receptor antagonists were used to assess changes in [¹⁸F]-FEOBV binding to the vesicular acetylcholine transporter (VAChT) in rodents using positron emission tomography (PET). After pretreatment with either 10 mg/kg haloperidol, 1 mg/kg raclopride, or vehicle, 90 min dynamic PET scans were performed with arterial blood sampling. The net influx rate (K_i) was obtained from Patlak graphical analysis, using a metabolite-corrected plasma input function and dynamic PET data. [¹⁸F]-FEOBV concentration in whole-blood or plasma and the metabolite-corrected plasma input function were not significantly changed by the pretreatments (adjusted p > 0.07, Cohen’s d 0.28–1.89) while the area-under-the-curve (AUC) of the parent fraction of [¹⁸F]-FEOBV was significantly higher after haloperidol treatment (adjusted p = 0.022, Cohen’s d = 2.51) than in controls. Compared to controls, the AUC of [¹⁸F]-FEOBV, normalized for injected dose and body weight, was nonsignificantly increased in the striatum after haloperidol (adjusted p = 0.4, Cohen’s d = 1.77) and raclopride (adjusted p = 0.052, Cohen’s d = 1.49) treatment, respectively. No changes in the AUC of [¹⁸F]-FEOBV were found in the cerebellum (Cohen’s d 0.63–0.74). Raclopride treatment nonsignificantly increased K_i in the striatum 1.3-fold compared to control rats (adjusted p = 0.1, Cohen’s d = 1.1) while it reduced K_i in the cerebellum by 28% (adjusted p = 0.0004, Cohen’s d = 2.2) compared to control rats. Pretreatment with haloperidol led to a nonsignificant reduction in K_i in the striatum (10%, adjusted p = 1, Cohen’s d = 0.44) and a 40–50% lower K_i than controls in all other brain regions (adjusted p < 0.0005, Cohen’s d = 3.3–4.7). The changes in K_i induced by the selective D₂ receptor antagonist raclopride can in part be quantified using [¹⁸F]-FEOBV PET imaging. Haloperidol, a nonselective D₂/σ receptor antagonist, either paradoxically decreased cholinergic activity or blocked off-target [¹⁸F]-FEOBV binding to σ receptors. Hence, further studies evaluating the binding of [¹⁸F]-FEOBV to σ receptors using selective σ receptor ligands are necessary.