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volume 25 issue 21 pages 5132

The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship

Publication typeJournal Article
Publication date2020-11-04
scimago Q1
wos Q2
SJR0.865
CiteScore8.6
Impact factor4.6
ISSN14203049
Organic Chemistry
Drug Discovery
Physical and Theoretical Chemistry
Pharmaceutical Science
Molecular Medicine
Analytical Chemistry
Chemistry (miscellaneous)
Abstract

The translocator protein (TSPO, 18 kDa) plays an important role in the synthesis of neurosteroids by promoting the transport of cholesterol from the outer to the inner mitochondrial membrane, which is the rate-limiting step in neurosteroidogenesis. Stimulation of TSPO by appropriate ligands increases the level of neurosteroids. The present study describes the design, synthesis and investigation of anxiolytic-like effects of a series of N-acyl-tryptophanyl-containing dipeptides. These novel dipeptide TSPO ligands were designed with the original drug-based peptide design strategy using alpidem as non-peptide prototype. The anxiolytic activities were investigated in Balb/C mice using the illuminated open-field and elevated plus-maze tests in outbred laboratory mice ICR (CD-1). Dipeptide GD-102 (N-phenylpropionyl-l-tryptophanyl-l-leucine amide) in the dose range of 0.01–0.5 mg/kg intraperitoneally (i.p.) has a pronounced anxiolytic activity. The anxiolytic effect of GD-102 was abolished by PK11195, a specific TSPO antagonist. The structure–activity relationship study made it possible to identify a pharmacophore fragment for the dipeptide TSPO ligand. It was shown that l,d-diastereomer of GD-102 has no activity, and the d,l-isomer has less pronounced activity. The anxiolytic activity also disappears by replacing the C-amide group with the methyl ester, a free carboxyl group or methylamide. Consecutive replacement of each amino acid residue with glycine showed the importance of each of the amino acid residues in the structure of the ligand. The most active and technologically available compound GD-102, was selected for evaluation as a potential anxiolytic drug.

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GOST Copy
Gudasheva T. A. et al. The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship // Molecules. 2020. Vol. 25. No. 21. p. 5132.
GOST all authors (up to 50) Copy
Gudasheva T. A., Deeva O. A., Pantileev A., Mokrov G. V., Rybina I. V., Yarkova M. A., Seredenin S. B. The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship // Molecules. 2020. Vol. 25. No. 21. p. 5132.
RIS |
Cite this
RIS Copy
TY - JOUR
DO - 10.3390/molecules25215132
UR - https://doi.org/10.3390/molecules25215132
TI - The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship
T2 - Molecules
AU - Gudasheva, Tatiana A.
AU - Deeva, Olga A.
AU - Pantileev, Andry
AU - Mokrov, Grigory V.
AU - Rybina, Inna V
AU - Yarkova, Milada A.
AU - Seredenin, S. B.
PY - 2020
DA - 2020/11/04
PB - MDPI
SP - 5132
IS - 21
VL - 25
PMID - 33158242
SN - 1420-3049
ER -
BibTex |
Cite this
BibTex (up to 50 authors) Copy
@article{2020_Gudasheva,
author = {Tatiana A. Gudasheva and Olga A. Deeva and Andry Pantileev and Grigory V. Mokrov and Inna V Rybina and Milada A. Yarkova and S. B. Seredenin},
title = {The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship},
journal = {Molecules},
year = {2020},
volume = {25},
publisher = {MDPI},
month = {nov},
url = {https://doi.org/10.3390/molecules25215132},
number = {21},
pages = {5132},
doi = {10.3390/molecules25215132}
}
MLA
Cite this
MLA Copy
Gudasheva, Tatiana A., et al. “The New Dipeptide TSPO Ligands: Design, Synthesis and Structure–Anxiolytic Activity Relationship.” Molecules, vol. 25, no. 21, Nov. 2020, p. 5132. https://doi.org/10.3390/molecules25215132.