Synthesis, molecular docking, electrochemical and fluorimetric analysis of new caffeic and cinnamic acid-conjugated hemorphin derivatives designed as potential anticonvulsant and antinociceptive agents

Petar Todorov; Stela Georgieva; Petia Peneva; Spas Nikolov; Miroslav Rangelov; Nadezhda Todorova; Daniela Pechlivanova; Jana Tchekalarova

doi:10.1016/j.bioorg.2023.107063

Synthesis, molecular docking, electrochemical and fluorimetric analysis of new caffeic and cinnamic acid-conjugated hemorphin derivatives designed as potential anticonvulsant and antinociceptive agents

Bioorg Chem. 2024 Feb:143:107063. doi: 10.1016/j.bioorg.2023.107063. Epub 2023 Dec 25.

Authors

Petar Todorov¹, Stela Georgieva², Petia Peneva³, Spas Nikolov⁴, Miroslav Rangelov⁵, Nadezhda Todorova⁶, Daniela Pechlivanova⁷, Jana Tchekalarova⁸

Affiliations

¹ Department of Organic Chemistry, University of Chemical Technology and Metallurgy, 1756 Sofia, Bulgaria. Electronic address: pepi_37@abv.bg.
² Department of Analytical Chemistry, University of Chemical Technology and Metallurgy, 1756 Sofia, Bulgaria.
³ Department of Organic Chemistry, University of Chemical Technology and Metallurgy, 1756 Sofia, Bulgaria.
⁴ Department of Organic Chemistry, University of Chemical Technology and Metallurgy, 1756 Sofia, Bulgaria; Department of Analytical Chemistry, University of Chemical Technology and Metallurgy, 1756 Sofia, Bulgaria.
⁵ Institute of Organic Chemistry with Centre of Phytochemistry, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria.
⁶ Institute of Biodiversity and Ecosystem Research, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria.
⁷ Faculty of Medicine, Sofia University "St. Kliment Ohridski", 1407 Sofia, Bulgaria; Institute of Neurobiology, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria.
⁸ Institute of Neurobiology, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria.

PMID: 38150935
DOI: 10.1016/j.bioorg.2023.107063

Abstract

Based on the pharmacophore model of opioid receptors, our team recently synthesized a series of short-chain hemorphin peptide analogs containing non-natural amino acids. They demonstrated anticonvulsant and antinociceptive activity with low neurotoxicity. In the present study, a series of novel bioconjugates of N-modified hemorphin analogs containing second pharmacophore cinnamic acids (CA) or caffeic (KA) were synthesized by a traditional solid-phase Fmoc chemistry method for peptide synthesis. Electrochemical and fluorimetric analysis, in vivo anticonvulsant and antinociceptive activity in mice were conducted on the compounds. The three CA acid- (H4-CA, H5-CA, and H7-CA) and three KA acid- (H4-KA, H5-KA, and H7-KA) conjugated hemorphin derivatives exhibited potency at the highest doses of 2 µg/5 µl, administered by intracerebroventricular (icv) mode, against seizure spread in the maximal electroshock test (MES) in mice. The KA-conjugated H5-KA derivate, at the lowest dose, was the only compound that suppressed clonic seizures in the subcutaneous pentylenetetrazol (scPTZ) test. Except for the H5-CA, all tested CA acid- and KA acid-conjugated peptide derivates had the potency to increase the latency for clonic seizures in a dose-dependent mode. The activity against the psychomotor seizures in the 6-Hz test was detected only for the H4-CA (0.5 µg) and H4-KA (0.5 µg and 1 µg), respectively. All investigated peptides showed a more pronounced antinociceptive effect in the "intraplantar formalin" test compared to the "hot plate" test. Shorter chain analogs showed a better antinociceptive profile against tonic pain. The data suggest a DOR and KOR-mediated mechanism of action. According to the docking analysis, H7-CA showed a different antinociceptive profile than other investigated peptides. The novel peptide derivates did not exhibit neurotoxicity in the rotarod test. Our findings suggest that conjugated CA and KA morphine peptides can be used to develop novel morphine-related analogs with anticonvulsant and antinociceptive activity.

Keywords: Anticonvulsant activity; Antinociception; Caffeic/cinnamic acid; Electrochemistry; FRET efficiency; Hemorphins.

MeSH terms

Analgesics / chemistry
Analgesics / pharmacology
Analgesics / therapeutic use
Animals
Anticonvulsants* / chemistry
Anticonvulsants* / pharmacology
Anticonvulsants* / therapeutic use
Cinnamates*
Electroshock
Mice
Molecular Docking Simulation
Morphine Derivatives / therapeutic use
Pentylenetetrazole
Peptides / therapeutic use
Seizures* / chemically induced
Seizures* / drug therapy
Seizures* / metabolism

Substances

Anticonvulsants
cinnamic acid
Pentylenetetrazole
Analgesics
Peptides
Morphine Derivatives
Cinnamates