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Título : Genetic diversity of the Junin virus in Argentina: geographic and temporal patterns
Autor : Garcia, Jorge 
Morzunov, Sergey P 
Levis, Silvana 
Rowe, Joan 
Calderón, Gladys 
Enria, Delia 
Sabattini, Marta S. 
Buchmeier, M J 
Bowen, M D 
St Jeor, S C 
Palabras clave : Animales;Argentina;Línea Celular;Análisis Mutacional de ADN;Genes Virales;Variación Genética;Glicoproteínas;Fiebre Hemorrágica Americana;Humanos;Virus Junin;Ratones;Datos de Secuencia Molecular;Muridae;Mutation;Nucleocápside;ARN Viral;Reacción en Cadena de la Polimerasa de Transcriptasa Inversa;Homología de Secuencia;Time Factors;Virulencia;Filogenia
Fecha de publicación : 20-jun-2000
Editorial : Elsevier
Academic Press
Proyecto: datasets
Journal: Virology 
Resumen : 
RNA was purified from 39 strains of cell-cultured Junin virus (JUN) from central Argentina, which included both human- and rodent-derived isolates (a total of 26 and 13, respectively), as well as from 2 laboratory JUN strains, XJ Cl3 and XJ #44. JUN-specific primers were used to amplify a 511-nucleotide (nt) fragment of the nucleocapsid protein gene and a 495-nt fragment of the glycoprotein 1 (GP1) gene. Genetic diversity among JUN strains studied was up to 13% at the nt level and up to 9% at the amino acid (aa) level for the GP1 gene and up to 9% (nt) and 4% (aa) for the NP gene. Phylogenetic analyses of both genes revealed three distinct clades. The first clade was composed of the JUN strains from the center of the endemic area and included the majority of JUN strains analyzed in the current study. The second clade contained 4 JUN strains isolated between 1963 and 1971 from Cordoba Province, the western-most edge of the known endemic area. The third clade contained 4 JUN strains that originated from Calomys musculinus trapped in Zarate, the northeastern edge of the known endemic area. Certain JUN sequences, which were obtained from GenBank and identified as XJ, XJ #44, and Candid #1 strains, appeared to form a separate clade. Over 400 nt of the GP1 and GP2 genes were additionally sequenced for 7 JUN strains derived from patients with different clinical presentations and outcomes of Argentine hemorrhagic fever. Analysis of the corresponding aa sequences did not allow us to attribute any particular genetic marker to the changing severity or clinical form of the human disease.
Descripción : 
Fil: García, Jorge B. ANLIS Dr.C.G.Malbrán. Instituto Nacional de Enfermedades Virales Humanas; Argentina.

Fil: Morzunov, Sergey P. University of Nevada at Reno. Department of Microbiology; Estados Unidos.

Fil: Levis, Silvana. ANLIS Dr.C.G.Malbrán. Instituto Nacional de Enfermedades Virales Humanas; Argentina.

Fil: Rowe, Joan. University of Nevada at Reno. Department of Microbiology; Estados Unidos.

Fil: Calderón, Gladys. ANLIS Dr.C.G.Malbrán. Instituto Nacional de Enfermedades Virales Humanas; Argentina.

Fil: Enría, Delia. ANLIS Dr.C.G.Malbrán. Instituto Nacional de Enfermedades Virales Humanas; Argentina.

Fil: Sabattini, Marta S. ANLIS Dr.C.G.Malbrán. Instituto Nacional de Enfermedades Virales Humanas; Argentina.

Fil: Buchmeier, M J. Scripps Research Institute. Department of Neuropharmacology; Estados Unidos.

Fil: Bowen, M D. Centers for Disease Control and Prevention. Special Pathogens Branch; Estados Unidos.

Fil: St Jeor, Stephen C. University of Nevada at Reno. Department of Microbiology; Estados Unidos.
URI : http://sgc.anlis.gob.ar/handle/123456789/2003
ISSN : 0042-6822
DOI: 10.1006/viro.2000.0345
Derechos: Open Access
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