scholarly journals Genome Analysis and Replication Studies of the African Green Monkey Simian Foamy Virus Serotype 3 Strain FV2014

Viruses ◽  
2020 ◽  
Vol 12 (4) ◽  
pp. 403
Author(s):  
Sandra M. Fuentes ◽  
Eunhae H. Bae ◽  
Subhiksha Nandakumar ◽  
Dhanya K. Williams ◽  
Arifa S. Khan
Keyword(s):  
Nucleotide Sequence ◽  
Cell Line ◽  
Kidney Cell ◽  
Foamy Virus ◽  
African Green Monkey ◽  
Nucleotide Sequence Analysis ◽  
Cell Tropism ◽  
Kidney Cell Line ◽  
Virus Serotype ◽  
Green Monkey

African green monkey (AGM) spumaretroviruses have been less well-studied than other simian foamy viruses (SFVs). We report the biological and genomic characterization of SFVcae_FV2014, which was the first foamy virus isolated from an African green monkey (AGM) and was found to be serotype 3. Infectivity studies in various cell lines from different species (mouse, dog, rhesus monkey, AGM, and human) indicated that like other SFVs, SFVcae_FV2014 had broad species and cell tropism, and in vitro cell culture infection resulted in cytopathic effect (CPE). In Mus dunni (a wild mouse fibroblast cell line), MDCK (Madin-Darby canine kidney cell line), FRhK-4 (a fetal rhesus kidney cell line), and MRC-5 (a human fetal lung cell line), SFVcae_FV2014 infection was productive resulting in CPE, and had delayed or similar replication kinetics compared with SFVmcy_FV21 and SFVmcy_FV34[RF], which are two Taiwanese macaque isolates, designated as serotypes 1 and 2, respectively. However, in Vero (AGM kidney cell line) and A549 (a human lung carcinoma cell line), the replication kinetics of SFVcae_FV2014 and the SFVmcy viruses were discordant: In Vero, SFVcae_FV2014 showed rapid replication kinetics and extensive CPE, and a persistent infection was seen in A549, with delayed, low CPE, which did not progress even upon extended culture (day 55). Nucleotide sequence analysis of the assembled SFVcae_FV2014 genome, obtained by high-throughput sequencing, indicated an overall 80–90% nucleotide sequence identity with SFVcae_LK3, the only available full-length genome sequence of an AGM SFV, and was distinct phylogenetically from other AGM spumaretroviruses, corroborating previous results based on analysis of partial env sequences. Our study confirmed that SFVcae_FV2014 and SFVcae_LK3 are genetically distinct AGM foamy virus (FV) isolates. Furthermore, comparative infectivity studies of SFVcae_FV2014 and SFVmcy isolates showed that although SFVs have a wide host range and cell tropism, regulation of virus replication is complex and depends on the virus strain and cell-specific factors.

scholarly journals VIRAL SUSCEPTIBILITY OF AN AFRICAN GREEN MONKEY KIDNEY CELL LINE-Vero

Uirusu ◽  
1968 ◽  
Vol 18 (3) ◽  
pp. 214-228 ◽  
Author(s):  
Heihachi ITOH ◽  
Yoshio MORIMOTO ◽  
Yutaka DOI ◽  
Tsuneo SANPE ◽  
Hiroshi TSUNODA
Keyword(s):  
Cell Line ◽  
Kidney Cell ◽  
African Green Monkey ◽  
Monkey Kidney ◽  
Kidney Cell Line ◽  
Monkey Kidney Cell ◽  
African Green Monkey Kidney ◽  
Viral Susceptibility ◽  
Green Monkey

Glycosphingolipids of a green monkey kidney cell line (GMK AH-1)

1982 ◽  
Vol 711 (3) ◽  
pp. 466-477 ◽  
Author(s):  
Jonas Blomberg ◽  
Michael E. Breimer ◽  
Karl-Anders Karlsson
Keyword(s):  
Cell Line ◽  
Kidney Cell ◽  
Monkey Kidney ◽  
Kidney Cell Line ◽  
Monkey Kidney Cell ◽  
Green Monkey

Nucleotide sequence analysis and enhancer function of long terminal repeats associated with an endogenous African green monkey retroviral DNA

1985 ◽  
Vol 5 (6) ◽  
pp. 1335-1342
Author(s):  
M Kessel ◽  
A S Khan
Keyword(s):  
Nucleotide Sequence ◽  
Repeat Unit ◽  
African Green Monkey ◽  
Nucleotide Sequence Analysis ◽  
Direct Repeats ◽  
Long Terminal Repeats ◽  
Enhancer Activity ◽  
Enhancer Element ◽  
Green Monkey ◽  
Terminal Repeats

The nucleotide sequence and enhancer activity of the long terminal repeats (LTRs) associated with a cloned endogenous African green monkey (AGM) retroviral DNA designated as lambda-AGM-1 was studied. A unique feature of the endogenous AGM proviral LTRs was the presence of multiple copies of two types of directly repeating units in the U3 region: 16 8-base-pair (bp) repeats were present in the 5' LTR and 12 were present in the 3' LTR which were bound by a 6-bp perfect direct repeat; tandem duplication of a 32-bp sequence resulted in 3.5 copies in the 5' LTR and 2.5 copies in the 3' LTR. Nucleotide sequence homology was seen between the 8-bp direct repeats located in the AGM proviral LTRs and a 10-bp repeat unit of the deca-satellite present in AGM cellular DNA. The 32-bp repeats of the AGM proviral LTRs contained sequences which were related to the SV40 21-bp repeats and to the "core" of the SV40 72-bp enhancer element. Furthermore, the AGM provirus was distinct from known infectious retroviruses due to the presence of a primer-binding sequence complementary to the 3' terminus of mammalian tRNAGly. Functional analysis of the 3' LTR present in lambda-AGM-1 DNA by chloramphenicol acetyltransferase assay demonstrated enhancer activity associated with the 32-bp direct repeats. Sequences outside the 32-bp unit were necessary for full activator function, suggesting the presence of multiple enhancer domains in the AGM provirus.

scholarly journals Complete Genome Sequence of the African Green Monkey Simian Foamy Virus Serotype 3 Strain FV2014 (SFVcae_FV2014)

2018 ◽  
Vol 6 (3) ◽  
Author(s):  
Subhiksha Nandakumar ◽  
Eunhae H. Bae ◽  
Arifa S. Khan
Keyword(s):  
High Throughput Sequencing ◽  
Genomic Organization ◽  
Foamy Virus ◽  
African Green Monkey ◽  
Simian Foamy Virus ◽  
Monkey Species ◽  
Chlorocebus Aethiops ◽  
Virus Serotype ◽  
Green Monkey ◽  
Full Length Sequence

ABSTRACTThe full-length sequence of simian foamy virus serotype 3 (SFV-3) strain FV2014, an African green monkey (Chlorocebus aethiops) isolate, was obtained using high-throughput sequencing. SFVcae_FV2014 consisted of 13,127 bp and had a genomic organization similar to those of other SFVs but was distinct from SFV strain LK3, isolated from the same monkey species.

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