Cyclic analogs of 2-amino-4-phosphonobutanoic acid (APB) and their inhibition of hippocampal excitatory transmission and displacement of [3H]APB binding

• Published in: Journal of medicinal chemistry Vol. 29; no. 10; pp. 1988 - 1995
• Main Authors: Crooks, Stephen L, Robinson, Michael B, Koerner, James F, Johnson, Rodney L
• Format: Journal Article
• Language: English
• Published: Washington, DC American Chemical Society 01.10.1986
• Subjects: Aminobutyrates - chemical synthesis; Aminobutyrates - metabolism; Aminobutyrates - pharmacology; Animals; Chemistry; Exact sciences and technology; Hippocampus - drug effects; In Vitro Techniques; Magnetic Resonance Spectroscopy; Male; Molecular Conformation; Organic chemistry; Organometalloidal and organometallic compounds; P derivatives; Preparations and properties; Rats; Structure-Activity Relationship; Synaptic Transmission - drug effects; Synaptosomes - metabolism; Tritium; NMR spectrum; Aminoacid; Relative configuration; Biological activity; Monocyclic compound; Phosphorus Organic compounds
• ISSN: 0022-2623; 1520-4804
• DOI: 10.1021/jm00160a031

Conformationally restricted analogues of 2-amino-4-phosphonobutanoic acid (APB,2) were prepared where the structure of APB was incorporated into cyclopentane (3) or cyclohexane (4) rings. Hydrophosphinylation of the appropriate cycloalkenones followed by Strecker amino acid syntheses provided the desired analogues. Assignments of the relative configurations for 3a (trans), 3b (cis), 4a (cis), and 4b (trans) were determined through 13C NMR studies. Compounds 3b, 4a, and 4b possessed low activity as inhibitors of excitatory synaptic field potentials in the rat hippocampal perforant path. Analogues 4a and 4b also showed little activity in displacing [3H]APB from synaptic plasma membranes. The cyclopentyl APB analogue 36, on the other hand, was extremely potent in inhibiting the binding of [3H]APB, possessing an IC50 = 4.7 microM, thus giving further credence to the idea that the APB binding site in the rat brain synaptosomal membrane preparation is not the same as the receptor mediating APB-induced inhibition of the lateral perforant path. Of the four cyclic APB analogues, 3a most resembled APB in its spectrum of biological activity. It showed significant potency (IC50 = 130 microM) in inhibiting lateral entorhinal projections to hippocampal granule cells. Analogous to APB, 3a also showed selectivity for the lateral perforant path over the medial perforant path. Its activity in the radioligand binding assay paralleled its activity in inhibiting the lateral perforant path. It thus appears that 3a comes closest to mimicking the active conformation of APB and suggests that a folded conformation wherein the amino and phosphonate moieties are in a cis relationship to one another may approximate the active conformation of APB.