18F‐Labeled benzylpiperazine derivatives as highly selective ligands for imaging σ1 receptor with positron emission tomography

We report the design, synthesis, and evaluation of a new series of benzylpiperazine derivatives as selective σ₁ receptor ligands. All seven ligands possessed low nanomolar affinity for σ₁ receptors (K_i(σ₁) = 0.31‐4.19 nM) and high subtype selectivity (K_i(σ₂)/K_i(σ₁) = 50‐2448). The fluoroethoxy analogues also exhibited high selectivity toward the vesicular acetylcholine transporter (K_i(VAChT)/K_i(σ₁) = 99‐18252). The corresponding radiotracers ¹⁸F] 13 , ¹⁸F] 14 , and ¹⁸F] 16 with high selectivity (K_i(σ₂)/K_i(σ₁) > 100, K_i(VAChT)/K_i(σ₁) > 1000) were prepared in 42% to 55% radiochemical yields (corrected for decay), greater than 99% radiochemical purity (RCP), and molar activity of about 120 GBq/μmol at the end of synthesis (EOS). All three radiotracers showed high initial brain uptake in mouse (8.37‐11.48% ID/g at 2 min), which was not affected by pretreatment with cyclosporine A, suggesting that they are not substrates for permeability‐glycoprotein (P‐gp). Pretreatment with SA4503 or haloperidol resulted in significantly reduced brain uptake (35%‐62% decrease at 30 min). In particular, ¹⁸F] 16 displayed high brain‐to‐blood ratios and high in vivo metabolic stability. Although it may not be an optimal neuroimaging agent because of its slow kinetics in the mouse brain, ¹⁸F] 16 can serve as a lead compound for further structural modifications to explore new potential radiotracers for σ₁ receptors.