Your search keyword '"Artuso MC"' showing total 6 results

1. Inhibition of Junin virus replication by small interfering RNAs

Author

Artuso, MC, Ellenberg, PC, Scolaro, LA, Damonte, EB, Garcia, CC, Artuso, MC, Ellenberg, PC, Scolaro, LA, Damonte, EB, and Garcia, CC

Abstract

Junín virus (JUNV), the etiological agent of the Argentine hemorrhagic fever, has a single-stranded RNA genome with ambisense expression which encodes for five proteins. In previous works we have demonstrated that the Z arenavirus matrix protein represents an attractive target for antiviral therapy. With the aim of studying a new alternative therapeutic mechanism, four Z-specific siRNAs (Z1- to Z4-siRNAs) were tested showing variable efficacy. The most effective inhibitor was Z2-siRNA targeted at the region encompassed by nt 179-197 of Z gene. The efficacy of this Z2-siRNA against JUNV was also demonstrated in virus-infected cells, by testing infectious virus plaque formation (92.8% JUNV yield reduction), viral RNA level or antigen expression, as well as in cells transfected with Z-specific reporter plasmids (91% reduction in expression of Z-EGFP fusion protein). Furthermore, the lack of effect of this Z-siRNA on the expression of other JUNV proteins, such as N and GPC, confirmed the specificity of action exerted by Z2-siRNA on Z transcript. Thus, the present study represents the first report of virus inhibition mediated by RNA interference for a New World arenavirus.

Published

2009

2. Detection and characterization of highly pathogenic avian influenza A (H5N1) clade 2.3.4.4b virus circulating in Argentina in 2023.

Author

Artuso MC, Marchione VD, Benedetti E, Bonastre P, Alvarez AM, Piccini L, Ponde A, Barrios Benito E, Fabeiro M, Waisman K, Coppola L, Poklepovich T, Chamorro A, Avaro M, Riva DA, Pontoriero A, Ferrer ME, Marcos A, Dassa L, Caria D, Melon X, Balzano Parodi RE, and Nicola AM

Abstract

In 2021, avian influenza A (H5N1) clade 2.3.4.4b virus spread to North America and then to Central and South America in October 2022, extending from Colombia to Chile in three months. During 2023, several countries, mostly in the Americas, reported outbreaks in poultry, wild birds and mammals, as well as the emergence of two cases in humans (one in Ecuador in January and one in Chile in March). As of September 20th, 2023, 17 countries in the Americas Region have recorded cases of A (H5N1) in birds and mammals. On February 14th, 2023, Argentina confirmed the first case of avian influenza in wild birds, which was later detected in backyard and commercial poultry, and in the South-American sea lion (Otaria flavescens) in Tierra del Fuego, in the south of the country. So far, 21 suspected cases have been recorded in humans; however, all of them tested negative for Influenza A virus. Hemagglutinin sequence data of animal viruses analyzed in this report showed that Argentinian viruses clustered together with those isolated in other countries of the region. Epidemiological data suggested the possibility of multiple simultaneous entries of the avian virus, highlighting the role of migratory avian populations in the introduction and dissemination of the disease in Argentina. Continued comprehensive surveillance of these viruses in animals and people worldwide, along with ongoing preparedness efforts, are critical to determine the public health risk., (Copyright © 2024 The Author(s). Publicado por Elsevier España, S.L.U. All rights reserved.)

Published

2024

3. Viruses: As mediators in "Élan vital" of the "creative" evolution.

Author

Artuso MC, Roldán JS, Scolaro LA, and Carlucci MJ

Subjects

Animals, Gene Transfer, Horizontal, Life, Mice, Polysaccharides, Simplexvirus, Sulfates, Evolution, Molecular, Viruses

Abstract

The understanding of the processes occurring in Nature has been a continuing concern throughout the history of mankind. Intellectual tools employed towards this goal were specific for each period and have been largely based on the prevailing paradigms that reigned in the past. In this work we present evidence that supports the idea of viruses as key agents mediating natural processes linked to the evolution of organisms, particularly those involved in the flux of genes in the environment. This point of view tinges our perception of Nature and prompts us to include "viral" creativity and plasticity among the tools we employ to analyze those processes far beyond actual paradigms. Experimental data to support this proposal arose during the study of the interaction of the human pathogen, herpes simplex virus (HSV) with sulfated polysaccharides during multiplication of the virus in vitro. Sulfated polysaccharides are the main chemical structures found in carrageenans (CGNs) that are natural products obtained from seaweeds, which proved to be strong inhibitors for the virus. Here we describe the interaction between virus and CGNs as a suitable scenario for the emergence of viral variants which proved to be markedly attenuated for mice. A striking feature of these variants is that they showed changes at the level of conserved regions of the genome such as the DNA polymerase and thymidine kinase genes. In view of these findings, the importance of HSV evolution towards attenuated variants by the action of polysaccharides is also discussed. Attenuation may be considered part of a natural evolutionary process enabling the virus to contribute with valuable information for the host., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

4. Emergence of herpes simplex virus-1 syncytial variants with altered virulence for mice after selection with a natural carrageenan.

Author

Mateu CG, Recalde MP, Artuso MC, Hermida G, Linero FN, Scolaro LA, Damonte EB, Pujol CA, and Carlucci MJ

Subjects

Animals, Chlorocebus aethiops, Female, Herpes Genitalis pathology, Herpes Genitalis virology, Herpes Simplex pathology, Herpes Simplex virology, Herpesvirus 1, Human classification, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human genetics, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Microbial Sensitivity Tests, Rhodophyta chemistry, Seaweed chemistry, Vero Cells, Virulence, Antiviral Agents pharmacology, Carrageenan pharmacology, Genetic Variation, Giant Cells physiology, Herpesvirus 1, Human pathogenicity, Selection, Genetic

Abstract

Background: Antiviral therapy against herpes simplex virus based on sulfated polysaccharides, like carrageenans, represents a new alternative for genital herpes infections treatment and arises the concern about the appearance of resistant viral populations., Methods: We characterized the F strain of herpes simplex virus-1 passaged in the presence of a natural carrageenan isolated from the red seaweed Gigartina skottbergii in view of the virulence for mice of isolated viral clones., Results: Viral clones (syn14-1 and syn17-2) showed a syncytial phenotype and a mild resistance to carrageenan, heparin, acyclovir, and brivudine. Both clones were avirulent for BALB/c mice when inoculated intravaginally, whereas F strain produced high mortality. Attenuation correlated with low levels of TNF-[alpha], interleukin-6, and IFN-[gamma] in vaginal lavages although virus titers were similar to those obtained for F strain. On the contrary, they showed a marked virulence when inoculated intranasally leading to a generalized spreading of virus., Conclusions: Results confirm the hypothesis that selection of herpes simplex virus-1 with a carrageenan in vitro leads to the emergence of variants with a differential virulence when compared to the original virus. This finding should be addressed when an antiviral therapy against genital herpes infection employing a natural carrageenan is under consideration.

Published

2011

5. Inhibition of Junín virus replication by small interfering RNAs.

Author

Artuso MC, Ellenberg PC, Scolaro LA, Damonte EB, and García CC

Subjects

Animals, Base Sequence, Cell Line, Chlorocebus aethiops, Cricetinae, Junin virus chemistry, Junin virus physiology, Molecular Sequence Data, RNA, Small Interfering chemistry, RNA, Small Interfering metabolism, Sequence Alignment, Vero Cells, Arenaviridae Infections virology, Down-Regulation, Junin virus genetics, RNA Interference, RNA, Small Interfering genetics, Virus Replication

Abstract

Junín virus (JUNV), the etiological agent of the Argentine hemorrhagic fever, has a single-stranded RNA genome with ambisense expression which encodes for five proteins. In previous works we have demonstrated that the Z arenavirus matrix protein represents an attractive target for antiviral therapy. With the aim of studying a new alternative therapeutic mechanism, four Z-specific siRNAs (Z1- to Z4-siRNAs) were tested showing variable efficacy. The most effective inhibitor was Z2-siRNA targeted at the region encompassed by nt 179-197 of Z gene. The efficacy of this Z2-siRNA against JUNV was also demonstrated in virus-infected cells, by testing infectious virus plaque formation (92.8% JUNV yield reduction), viral RNA level or antigen expression, as well as in cells transfected with Z-specific reporter plasmids (91% reduction in expression of Z-EGFP fusion protein). Furthermore, the lack of effect of this Z-siRNA on the expression of other JUNV proteins, such as N and GPC, confirmed the specificity of action exerted by Z2-siRNA on Z transcript. Thus, the present study represents the first report of virus inhibition mediated by RNA interference for a New World arenavirus.

Published

2009

6. Characterization of Junín virus particles inactivated by a zinc finger-reactive compound.

Author

García CC, Ellenberg PC, Artuso MC, Scolaro LA, and Damonte EB

Subjects

Animals, Anti-HIV Agents pharmacology, Arenaviridae Infections metabolism, Carrier Proteins biosynthesis, Carrier Proteins genetics, Chlorocebus aethiops, Green Fluorescent Proteins, Junin virus genetics, Microscopy, Electron, Transmission, Nucleocapsid Proteins metabolism, Recombinant Fusion Proteins biosynthesis, Vero Cells, Virion ultrastructure, Virus Inactivation, Arenaviridae Infections drug therapy, Azo Compounds pharmacology, Disulfides pharmacology, Guanidines pharmacology, Junin virus drug effects, Virion drug effects, Zinc Fingers

Abstract

Our previous studies reported the inhibitory action against arenaviruses of antiretroviral zinc finger-reactive compounds provided by the National Cancer Institute (USA). These compounds were able to inactivate virions as well as to reduce virus yields from infected cells. Here, the inactivation of the arenavirus Junín (JUNV), agent of Argentine hemorrhagic fever, by the aromatic disulfide NSC20625 was analyzed. The treatment of purified JUNV with this compound eliminated infectivity apparently through irreversible modifications in the matrix Z protein detected by: (a) alterations in the electrophoretic migration profile of Z under non-reducing conditions; (b) an electrodense labeling in the internal layer beneath the envelope and around the matrix Z protein, in negatively stained preparations; (c) changes in the subcellular localization of Z in cells transfected with a recombinant fusion protein JUNVZ-eGFP. The infection of Vero cells with JUNV inactivated particles was blocked at the uncoating of viral nucleocapsid from endosomes, providing new evidence for a functional role of Z in this stage of arenavirus cycle. Furthermore, the inactivated JUNV particles retained the immunoreactivity of the surface glycoprotein GP1 suggesting that this disulfide may be useful in the pursuit of an inactivating agent to obtain a vaccine antigen or diagnostic tool.

Published

2009