O. A. Deeva, A. S. Pantileev, O. Yu. Kravtsova, S. V. Nikolaev, N. A. Zefirov, P. Yu. Povarnina, T. A. Antipova, T. A. Gudasheva, V. L. Dorofeev, “Tripeptide Phe-Trp-Leu-NH<sub>2</sub> as a putative endogenous ligand of TSPO: molecular modeling, synthesis and pharmacological activity”, Mendeleev Commun., 2024, Volume 34, Issue 5,Pages <nobr>682

Communications

Tripeptide Phe-Trp-Leu-NH₂ as a putative endogenous ligand of TSPO: molecular modeling, synthesis and pharmacological activity

O. A. Deeva^a, A. S. Pantileev^a, O. Yu. Kravtsova^a, S. V. Nikolaev^a, N. A. Zefirov^b, P. Yu. Povarnina^a, T. A. Antipova^a, T. A. Gudasheva^a, V. L. Dorofeev^a

^a Federal Research Center for Innovator and Emerging Biomedical and Pharmaceutical Technologies, Moscow, Russian Federation
^b Department of Chemistry, M.V. Lomonosov Moscow State University, Moscow, Russian Federation

Abstract: The putative endogenous tripeptide ligand of the translocator protein (TSPO) l-phenylalanyl-l-tryptophanyl-l-leucine amide was obtained using the drug-based peptide design strategy and molecular modeling. This tripeptide demonstrated anxiolytic activity in the elevated plus-maze test and antidepressant-like activity in the forced swimming test in BALB/c mice at the doses of 10 mg kg⁻¹ (i.p.) and also showed neuroprotective activity in the concentration range of 10⁻⁵–10⁻⁷ m in vitro under conditions of oxidative stress using HT-22 neuronal cell line.

Keywords: tripeptide, TSPO ligand, anxiolytic activity, antidepressant-like activity, neuroprotective activity.

Language: English

DOI: 10.1016/j.mencom.2024.09.018

	*Supplementary materials:*
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