Protein Metabolism Changes and Alterations in Behavior of Trace Amine-Associated Receptor 1 Knockout Mice Fed a High-Fructose Diet

Author:

Apryatin Sergey A.12ORCID,Zhukov Ilya S.12ORCID,Zolotoverkhaya Ekaterina A.3ORCID,Kuvarzin Saveliy R.2ORCID,Khunagov Temirkan A.4ORCID,Ushmugina Sanelya V.5ORCID,Klimenko Victor M.1

Affiliation:

1. Institute of Experimental Medicine, 197376 Saint Petersburg, Russia

2. Institute of Translational Biomedicine, Saint Petersburg State University, 199034 Saint Petersburg, Russia

3. Golikov Research Center of Toxicology, 193019 Saint Petersburg, Russia

4. Faculty of Biology, Lomonosov Moscow State University, 119991 Moscow, Russia

5. Department of Medical and Biological Disciplines, Moscow Medical University Reaviz, 107564 Moscow, Russia

Abstract

Trace amines and their receptors are a family of G protein-coupled receptors widely distributed in the central nervous system and periphery. The trace amine-associated receptor 1 (TAAR1) plays a significant role as a therapeutic target for schizophrenia, depression, diabetes, and obesity. In this study, TAAR1 knockout mice and WT groups were tested in conditions of a high-fructose diet. The consumption of a high-fructose diet may be due to the influence on the metabolism processes by dopamine in the brain, neuromotor function, and level of anxiety of TAAR1 knockout mice. During a comparative analysis of behavioral, biochemical, and morphological parameters, significant differences were found between liver and biochemical parameters, the regulation of protein metabolism (AST/ALT ratio, creatine kinase activity, urea), and alterations in behavior. An elevated plus maze analysis showed the influence of fructose and genetic factors on the level of anxiety. A new marker of the grooming microstructure (depression ratio) was tested, which showed high efficiency as a marker of depression-like behavioral changes and a possible association with dopamine-dependent regulation of protein metabolism. These results confirm a possible association of the TAAR1 gene knockout with an increase in catabolic reaction levels by AST/ALT-dependent and possible dopamine-mediated protein metabolism regulation and depression-like behavior.

Funder

St. Petersburg State University

Publisher

MDPI AG

Subject

Neurology (clinical)

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