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Research ArticleDrug Discovery and Translational Medicine

In silico screening identified novel small-molecule antagonists of PAC1 receptor

Ichiro Takasaki, Ai Watanabe, Masafumi Yokai, Yurie Watanabe, Daichi Hayakawa, Ryota Nagashima, Mamoru Fukuchi, Takuya Okada, Naoki Toyooka, Atsuro Miyata, Hiroaki Gouda and Takashi Kurihara
Journal of Pharmacology and Experimental Therapeutics January 23, 2018, jpet.117.245415; DOI: https://doi.org/10.1124/jpet.117.245415
Ichiro Takasaki
1 University of Toyama;
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Ai Watanabe
1 University of Toyama;
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Masafumi Yokai
2 Kagoshima University;
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Yurie Watanabe
3 Showa University
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Daichi Hayakawa
3 Showa University
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Ryota Nagashima
1 University of Toyama;
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Mamoru Fukuchi
1 University of Toyama;
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Takuya Okada
1 University of Toyama;
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Naoki Toyooka
1 University of Toyama;
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Atsuro Miyata
2 Kagoshima University;
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Hiroaki Gouda
3 Showa University
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Takashi Kurihara
2 Kagoshima University;
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Abstract

Pituitary adenylate cyclase-activating polypeptide (PACAP) and its receptors are present in the spinal dorsal horn and dorsal root ganglia, suggesting an important role of PACAP signaling systems in the modulation of spinal nociceptive transmission. Previously, we found that intrathecal (i.t.) injection of PACAP or maxadilan, a selective PACAP type I (PAC1) receptor agonist, induced transient aversive responses followed by a long-lasting mechanical allodynia in mice, suggesting that PACAP-PAC1 receptor systems are involved in chronic pain and that selective PAC1 antagonists may become a new class of analgesics. Although several PAC1 antagonists, such as PACAP 6-38, have been reported, all of them are peptide compounds. In the present study, we identified new small-molecule antagonists of the PAC1 receptor using in silico screening and in vitro/vivo pharmacological assays. The identified small-molecule compounds, named PA-8 and PA-9, dose-dependently inhibited the phosphorylation of CREB induced by PACAP in PAC1-, but not VPAC1- or VPAC2-receptor-expressing CHO cells. PA-8 and PA-9 also dose-dependently inhibited PACAP-induced cAMP elevation with an IC50 of 2.0 and 5.6 nM, respectively. In vivo pharmacological assays showed that i.t. injection of these compounds blocked the induction of PACAP-induced aversive responses and mechanical allodynia in mice. In contrast, the compounds when administered alone exerted neither agonistic nor algesic actions in the in vitro/vivo assays. The compounds identified in the present study are new and the first small-molecule antagonists of the PAC1 receptor; they may become seed compounds for developing novel analgesics.

  • analgesics
  • cAMP
  • drug design
  • drug discovery
  • pain
  • The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics: 377 (2)
Journal of Pharmacology and Experimental Therapeutics
Vol. 377, Issue 2
1 May 2021
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Research ArticleDrug Discovery and Translational Medicine

In silico screening identified novel small-molecule antagonists of PAC1 receptor

Ichiro Takasaki, Ai Watanabe, Masafumi Yokai, Yurie Watanabe, Daichi Hayakawa, Ryota Nagashima, Mamoru Fukuchi, Takuya Okada, Naoki Toyooka, Atsuro Miyata, Hiroaki Gouda and Takashi Kurihara
Journal of Pharmacology and Experimental Therapeutics January 23, 2018, jpet.117.245415; DOI: https://doi.org/10.1124/jpet.117.245415

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Research ArticleDrug Discovery and Translational Medicine

In silico screening identified novel small-molecule antagonists of PAC1 receptor

Ichiro Takasaki, Ai Watanabe, Masafumi Yokai, Yurie Watanabe, Daichi Hayakawa, Ryota Nagashima, Mamoru Fukuchi, Takuya Okada, Naoki Toyooka, Atsuro Miyata, Hiroaki Gouda and Takashi Kurihara
Journal of Pharmacology and Experimental Therapeutics January 23, 2018, jpet.117.245415; DOI: https://doi.org/10.1124/jpet.117.245415
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