The Effect of Meclofenoxate on the Transcriptome of Aging Brain of Annual Killifish

Overview

Journal Int J Mol Sci

Publisher MDPI

Specialties Biochemistry
Chemistry
Molecular Biology

Date 2022 Mar 10

PMID 35269638

Authors

Ildar R Bakhtogarimov

Anna V Kudryavtseva

George S Krasnov

Natalya S Gladysh

Vsevolod V Volodin

Alexander A Kudryavtsev

Elizaveta V Bulavkina

Margarita A Goncharova

Veronika S Ledyaeva

Ivan S Pastukhov

Yulia S Vershinina

Anna M Starkova

Anastasiya V Snezhkina

Anastasija I Shuvalova

Vladislav S Pavlov

Dmitry L Nikiforov-Nikishin

Alexey A Moskalev

Zulfiya G Guvatova

Affiliations

Soon will be listed here.

Abstract

Annual fish of the genus are promising models for aging research. reproduces typical aspects of vertebrate aging, including hallmarks of brain aging. Meclofenoxate (MF) is a well-known compound that can enhance cognitive performance. The drug is prescribed for asthenic conditions, trauma, and vascular diseases of the brain. It is believed that MF is able to delay age-dependent changes in the human brain. However, until now, there has been no study of the MF effect on the brain transcriptome. In the present work, we performed an RNA-Seq study of brain tissues from aged , which were almost lifetime administered with MF, as well as young and aged control fish. As expected, in response to MF, we revealed significant overexpression of neuron-specific genes including genes involved in synaptic activity and plasticity, neurotransmitter secretion, and neuron projection. The effect was more pronounced in female fish. In this aspect, MF alleviated age-dependent decreased expression of genes involved in neuronal activity. In both treated and untreated animals, we observed strong aging-associated overexpression of immune and inflammatory response genes. MF treatment did not prevent this effect, and moreover, some of these genes tended to be slightly upregulated under MF treatment. Additionally, we noticed upregulation of some genes associated with aging and cellular senescence, including isoforms of putative vascular cell adhesion molecule 1 (VCAM1), protein O-GlcNAcase (OGA), protein kinase C alpha type (KPCA), prolow-density lipoprotein receptor-related protein 1 (LRP1). Noteworthy, MF treatment was also associated with the elevated transcription of transposons, which are highly abundant in the genome. In conclusion, MF compensates for the age-dependent downregulation of neuronal activity genes, but its effect on aging brain transcriptome still cannot be considered unambiguously positive.

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