Your search keyword '"Eugene V. Sheval"' showing total 3 results

1. Ectopic expression of HIV-1 Tat modifies gene expression in cultured B cells: implications for the development of B-cell lymphomas in HIV-1-infected patients

Author

Anna A. Valyaeva, Maria A. Tikhomirova, Daria M. Potashnikova, Alexandra N. Bogomazova, Galina P. Snigiryova, Aleksey A. Penin, Maria D. Logacheva, Eugene A. Arifulin, Anna A. Shmakova, Diego Germini, Anastasia I. Kachalova, Aleena A. Saidova, Anastasia A. Zharikova, Yana R. Musinova, Andrey A. Mironov, Yegor S. Vassetzky, and Eugene V. Sheval

Subjects

HIV-1 Tat, B cells, Virus-cell interactions, Gene expression, RNA-seq, Medicine, Biology (General), QH301-705.5

Abstract

An increased frequency of B-cell lymphomas is observed in human immunodeficiency virus-1 (HIV-1)-infected patients, although HIV-1 does not infect B cells. Development of B-cell lymphomas may be potentially due to the action of the HIV-1 Tat protein, which is actively released from HIV-1-infected cells, on uninfected B cells. The exact mechanism of Tat-induced B-cell lymphomagenesis has not yet been precisely identified. Here, we ectopically expressed either Tat or its TatC22G mutant devoid of transactivation activity in the RPMI 8866 lymphoblastoid B cell line and performed a genome-wide analysis of host gene expression. Stable expression of both Tat and TatC22G led to substantial modifications of the host transcriptome, including pronounced changes in antiviral response and cell cycle pathways. We did not find any strong action of Tat on cell proliferation, but during prolonged culturing, Tat-expressing cells were displaced by non-expressing cells, indicating that Tat expression slightly inhibited cell growth. We also found an increased frequency of chromosome aberrations in cells expressing Tat. Thus, Tat can modify gene expression in cultured B cells, leading to subtle modifications in cellular growth and chromosome instability, which could promote lymphomagenesis over time.

Published

2022

2. The GAR domain integrates functions that are necessary for the proper localization of fibrillarin (FBL) inside eukaryotic cells

Author

Maria Y. Shubina, Eugene A. Arifulin, Dmitry V. Sorokin, Mariya A. Sosina, Maria A. Tikhomirova, Marina V. Serebryakova, Tatiana Smirnova, Svyatoslav S. Sokolov, Yana R. Musinova, and Eugene V. Sheval

Subjects

Nucleus, Nucleolus, Fibrillarin (FBL), GAR domain, NLS, NoLS, Medicine, Biology (General), QH301-705.5

Abstract

Fibrillarin (FBL) is an essential nucleolar protein that participates in pre-rRNA methylation and processing. The methyltransferase domain of FBL is an example of an extremely well-conserved protein domain in which the amino acid sequence was not substantially modified during the evolution from Archaea to Eukaryota. An additional N-terminal glycine–arginine-rich (GAR) domain is present in the FBL of eukaryotes. Here, we demonstrate that the GAR domain is involved in FBL functioning and integrates the functions of the nuclear localization signal and the nucleolar localization signal (NoLS). The methylation of the arginine residues in the GAR domain is necessary for nuclear import but decreases the efficiency of nucleolar retention via the NoLS. The presented data indicate that the GAR domain can be considered an evolutionary innovation that integrates several functional activities and thereby adapts FBL to the highly compartmentalized content of the eukaryotic cell.

Published

2020

3. The GAR domain integrates functions that are necessary for the proper localization of fibrillarin (FBL) inside eukaryotic cells

Author

Yana R. Musinova, Mariya A Sosina, Dmitry V. Sorokin, Svyatoslav S. Sokolov, Tatiana A. Smirnova, Eugene A. Arifulin, Maria Y. Shubina, Maria A Tikhomirova, Marina V. Serebryakova, and Eugene V. Sheval

Subjects

Nucleolus, Protein domain, NoLS, NLS, lcsh:Medicine, Biology, Methylation, Fibrillarin (FBL), General Biochemistry, Genetics and Molecular Biology, Nucleus, Domain (software engineering), 03 medical and health sciences, Peptide sequence, Molecular Biology, 030304 developmental biology, Fibrillarin, GAR domain, 0303 health sciences, General Neuroscience, 030302 biochemistry & molecular biology, lcsh:R, General Medicine, Cell Biology, Evolutionary Studies, Cell biology, Nuclear transport, General Agricultural and Biological Sciences, Nuclear localization sequence

Abstract

Fibrillarin (FBL) is an essential nucleolar protein that participates in pre-rRNA methylation and processing. The methyltransferase domain of FBL is an example of an extremely well-conserved protein domain in which the amino acid sequence was not substantially modified during the evolution fromArchaeatoEukaryota. An additional N-terminal glycine–arginine-rich (GAR) domain is present in the FBL of eukaryotes. Here, we demonstrate that the GAR domain is involved in FBL functioning and integrates the functions of the nuclear localization signal and the nucleolar localization signal (NoLS). The methylation of the arginine residues in the GAR domain is necessary for nuclear import but decreases the efficiency of nucleolar retention via the NoLS. The presented data indicate that the GAR domain can be considered an evolutionary innovation that integrates several functional activities and thereby adapts FBL to the highly compartmentalized content of the eukaryotic cell.

Published

2020