Your search keyword '"Ryabchikova EI"' showing total 2 results

1. Artificial ribonucleases inactivate a wide range of viruses using their ribonuclease, membranolytic, and chaotropic-like activities.

Author

Fedorova AA, Goncharova EP, Koroleva LS, Burakova EA, Ryabchikova EI, Bichenkova EV, Silnikov VN, Vlassov VV, and Zenkova MA

Subjects

Animals, Antiviral Agents chemistry, Cell Line, Hemolysis drug effects, Humans, Kinetics, Molecular Structure, Ribonucleases chemistry, Vaccinia virus drug effects, Viruses ultrastructure, Antiviral Agents pharmacology, Ribonucleases pharmacology, Virus Inactivation drug effects, Viruses drug effects

Abstract

Artificial ribonucleases (aRNases) are small compounds catalysing RNA cleavage. Recently we demonstrated that aRNases readily inactivate various viruses in vitro. Here, for three series of aRNases (1,4-diazabicyclo [2.2.2]octane-based and peptide-like compounds) we show that apart from ribonuclease activity the aRNases display chaotropic-like and membranolytic activities. The levels of membranolytic and chaotropic-like activities correlate well with the efficiency of various viruses inactivation (enveloped, non-enveloped, RNA-, DNA-containing). We evaluated the impact of these activities on the efficiency of virus inactivation and found: i) the synergism between membranolytic and chaotropic-like activities is sufficient for the inactivation of enveloped viruses (influenza A, encephalitis, vaccinia viruses) for 1,4-diazabicyclo [2.2.2]octane based aRNases, ii) the inactivation of non-enveloped viruses (encephalomyocarditis, acute bee paralysis viruses) is totally dependent on the synergism of chaotropic-like and ribonuclease activities, iii) ribonuclease activity plays a leading role in the inactivation of RNA viruses by aRNases Dp12F6, Dtr12 and K-D-1, iv) peptide-like aRNases (L2-3, K-2) being effective virus killers have a more specific mode of action. Obtained results clearly demonstrate that aRNases represent a new class of broad-spectrum virus-inactivating agents., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

2. Inactivation of a non-enveloped RNA virus by artificial ribonucleases: honey bees and acute bee paralysis virus as a new experimental model for in vivo antiviral activity assessment.

Author

Fedorova AA, Azzami K, Ryabchikova EI, Spitsyna YE, Silnikov VN, Ritter W, Gross HJ, Tautz J, Vlassov VV, Beier H, and Zenkova MA

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Bees drug effects, Bees growth & development, Cell Line, Tumor, Dicistroviridae physiology, Dose-Response Relationship, Drug, Electrophoresis, Polyacrylamide Gel, Larva drug effects, Larva growth & development, Microscopy, Electron, RNA, Viral metabolism, Reverse Transcriptase Polymerase Chain Reaction, Bees virology, Biological Assay, Dicistroviridae drug effects, Larva virology, Protein Engineering methods, RNA, Viral antagonists & inhibitors, Ribonucleases chemical synthesis, Ribonucleases pharmacology, Virus Inactivation drug effects

Abstract

RNA-containing viruses represent a global threat to the health and wellbeing of humans and animals. Hence, the discovery of new approaches for the design of novel vaccines and antiviral compounds attains high attention. Here we describe the potential of artificial ribonucleases (aRNases), low molecular weight compounds capable to cleave phosphodiester bonds in RNA under mild conditions, to act as antiviral compounds via destroying the genome of non-enveloped RNA viruses, and the potential of utilizing honey bee larvae and adult bees (Apis mellifera) as a novel experimental system for the screening of new antiviral compounds. Pre-incubation of an Acute bee paralysis virus (ABPV) suspension with aRNases D3-12, K-D-1 or Dp12F6 in a concentration-dependent manner increased the survival rate of bee larvae and adult bees subsequently infected with these preparations, whereas incubation of the virus with aRNases ABL3C3 or L2-3 had no effect at all. The results of RT-PCR analysis of viral RNA isolated from aRNase-treated virus particles confirmed that virus inactivation occurs via degradation of viral genomic RNA: dose-dependent inactivation of ABPV correlates well with the cleavage of viral RNA. Electron microscopy analysis revealed that the morphology of ABPV particles inactivated by aRNases remains unaffected as compared to control virus preparations. Altogether the obtained results clearly demonstrate the potential of aRNases as a new virus inactivation agents and bee larvae/ABPV as a new in vivo system for the screening of antiviral compounds., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011