(S)-2-Amino-3-(5-methyl-3-hydroxyisoxazol-4-yl)propanoic Acid (AMPA) and Kainate Receptor Ligands: Further Exploration of Bioisosteric Replacements and Structural and Biological Investigation

Simone Brogi,Margherita Brindisi,Stefania Butini,Giridhar Kshirsagar,Samuele Maramai,Giulia Chemi,Sandra Gemma,Giuseppe Campiani,Ettore Novellino,Paolo Fiorenzani,Jessica Pinassi,Anna Maria Aloisi,Mikko Gynther,Raminta Venskutonytė,Liwei Han,Karla Frydenvang,Jette S. Kastrup,Darryl S. Pickering

(S)-2-Amino-3-(5-methyl-3-hydroxyisoxazol-4-yl)propanoic Acid (AMPA) and Kainate Receptor Ligands: Further Exploration of Bioisosteric Replacements and Structural and Biological Investigation

2018

Simone Brogi
Margherita Brindisi
Stefania Butini
Giridhar Kshirsagar
Samuele Maramai
Giulia Chemi
Sandra Gemma
Giuseppe Campiani
Ettore Novellino
Paolo Fiorenzani
Jessica Pinassi
Anna Maria Aloisi
Mikko Gynther
Raminta Venskutonytė
Liwei Han
Karla Frydenvang
Jette S. Kastrup
Darryl S. Pickering

Starting from 1–4 and 7 structural templates, analogues based on bioisosteric replacements (5a–c vs 1, 2 and 6 vs 7) were synthesized for completing the SAR analysis. Interesting binding properties at GluA2, GluK1, and GluK3 receptors were discovered. The requirements for GluK3 interaction were elucidated by determining the X-ray structures of the GluK3-LBD with 2 and 5c and by computational studies. Antinociceptive potential was demonstrated for GluK1 partial agonist 3 and antagonist 7 (2 mg/kg ip).

Keywords:

Antagonist
Stereochemistry
Partial agonist
AMPA receptor
Organic chemistry
Chemistry
Membrane protein
Propanoic acid
Kainate receptor
Ligand
Receptor

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