A novel dimeric dipeptide mimetic of the BDNF selectively activates the MAPK-Erk signaling pathway

T. A. Gudasheva; A. V. Tarasiuk; N. M. Sazonova; P. Yu. Povarnina; T. A. Antipova; S. B. Seredenin

doi:10.1134/S1607672917050027

A novel dimeric dipeptide mimetic of the BDNF selectively activates the MAPK-Erk signaling pathway

Authors: Gudasheva T.A.¹, Tarasiuk A.V.¹, Sazonova N.M.¹, Povarnina P.Y.¹, Antipova T.A.¹, Seredenin S.B.¹
Affiliations:
1. Zakusov Research Institute of Pharmacology
Issue: Vol 476, No 1 (2017)
Pages: 291-295
Section: Biochemistry, Biophysics, and Molecular Biology
URL: https://journal-vniispk.ru/1607-6729/article/view/211964
DOI: https://doi.org/10.1134/S1607672917050027
ID: 211964

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Abstract

On the basis of the structure of beta-turn of loop 2 of brain-derived neurotrophic factor (BDNF), its new dimeric dipeptide mimetic bis-(N-hexanoyl-L-seryl-L-lysine) hexamethylenediamide (GTS-201) was created. It activated TrkB and Erk, did not activate Akt, and exhibited neuroprotective activity in vitro at concentrations of 10^–5–10^–8 M. Unlike the mimetics that activate Erk and Akt, GTS-201 did not exhibit antidepressant properties. For the manifestation of the antidepressant activity of BDNF mimetics, the activation of its both major signaling pathways is required.

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A novel dimeric dipeptide mimetic of the BDNF selectively activates the MAPK-Erk signaling pathway

Full Text

Abstract

About the authors

T. A. Gudasheva

A. V. Tarasiuk

N. M. Sazonova

P. Yu. Povarnina

T. A. Antipova

S. B. Seredenin

Supplementary files