Publications
| Title | Abstract | Year(sorted descending) Filter | PMID Filter |
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| development and laboratory evaluation of two lateral flow devices for the detection of vesicular stomatitis virus in clinical samples. | two lateral flow devices (lfd) for the detection of vesicular stomatitis (vs) virus (vsv), types indiana (vsv-ind) and new jersey (vsv-nj) were developed using monoclonal antibodies c1 and f25vsvnj-45 to the respective vsv serotypes. the performance of the lfds was evaluated in the laboratory on suspensions of vesicular epithelia and cell culture passage derived supernatants of vsv. the collection of test samples included 105 positive for vsv-ind (92 vesicular epithelial suspensions and 13 cell ... | 2011 | 22230813 |
| a mutant of asia 1 serotype of foot-and-mouth disease virus with the deletion of an important antigenic epitope in the 3a protein. | foot-and-mouth disease is a highly contagious viral disease of cloven-hoofed animals. the availability of a vaccine for differentiating infected from vaccinated animals (diva) is crucial for the control and eradication of foot-and-mouth disease virus (fmdv). because traditional inactivated vaccines may contain trace nonstructural proteins interfering with the diva, we hypothesized that mutant fmdv with deletion of immunodominant epitopes may be valuable. our previous study has generated a full-l ... | 2011 | 21358757 |
| rt-pcr evaluation for identification and sequence analysis of foot-and-mouth disease serotype o from 2006 to 2007 in punjab, pakistan. | fmd clinically positive 250 tissue samples (mouth and hoof epithelium and vesicle swabs, tongue tissue) and 175 secretion samples (milk, saliva, serum, plasma) were evaluated by rt-pcr for the diagnosis of fmd with different pair of universal and serotype-specific primers from 2006 to 2007 in punjab, pakistan. universal primer pair p1/p2 from vp1 gene detected fmd in 182 out of 250 (72.8%) tissues and 92 out of 175 (52.6%) secretion samples, while universal primer 1f/1r from 5'utr region detecte ... | 2011 | 20031216 |
| low diversity of foot-and-mouth disease serotype c virus in kenya: evidence for probable vaccine strain re-introductions in the field. | most viruses are maintained by complex processes of evolution that enable them to survive but also complicate efforts to achieve their control. in this paper, we study patterns of evolution in foot-and-mouth disease (fmd) serotype c virus isolates from kenya, one of the few places in the world where serotype c has been endemic and is suspected to remain. the nucleotide sequences encoding the capsid protein vp1 from eight isolates collected between 1967 and 2004 were analysed for patterns of sequ ... | 2011 | 20334728 |
| foot-and-mouth disease: the question of implementing vaccinal control during an epidemic. | the question of whether or not to use vaccines during an epidemic of foot-and-mouth disease (fmd) has interested veterinary administrators for many decades. this review assesses the historical uses, successes and failures of vaccinal control, and addresses the questions of where, how, and when to use vaccination against fmd. approaching the problem in this manner can aid in identifying which tools are likely to be most effective during an epidemic, and how successful a given contingency plan mig ... | 2011 | 20350828 |
| difference in the level of interferon gamma mrna transcripts on stimulation of cattle and buffalo mononuclear cells with foot and mouth disease virus-antigen: a possible role of sequence variation in promoter region. | in an attempt to resolve the claim that buffaloes differ from cattle in disease progression, this study was undertaken to compare the mitogen (cona) or antigen (foot and mouth disease virus) induced expression levels of interferon gamma (ifn-γ mrna in peripheral blood mononuclear cells (pbmcs) by real-time quantitative pcr. in general, the levels of ifn-γ mrna were lower in buffaloes than in crossbred cattle. significantly higher levels of ifn-γ mrna were also observed in crossbred cattle when i ... | 2011 | 20541234 |
| direct typing and molecular evolutionary analysis of field samples of foot-and-mouth disease virus collected in viet nam between 2006 and 2007. | in this study, we used universal or duplex serotype-specific (o and asia 1) rt-pcr to analyze clinical field samples of foot-and-mouth disease virus (fmdv) or virus isolates collected in viet nam between 2006 and 2007. we found viral serotypes o and asia 1 circulating concurrently during this period. direct sequencing of type-specific rt-pcr products revealed the existence of three different topotypes of serotype o: southeast asia (sea), middle east-south asia (me-sa), and cathay. of these, sea ... | 2011 | 20667669 |
| multiple invasions of o1 fmdv serotype into israel revealed by genetic analysis of vp1 genes of israeli's isolates from 1989 to 2007. | foot-and-mouth disease virus (fmdv), one of the most dangerous viruses affecting cloven-hoofed animals, comprises seven serotypes that do not mutually cross-protect, with a total of about 80 subtypes. the middle east is an fmd-endemic region, with repeated fmd outbreaks and in spite of its compulsory vaccination policy in israel, outbreaks occur repeatedly. in order to compare the israeli isolates, the complete viral vp1 genes of representative viruses isolated during the major outbreaks from 19 ... | 2011 | 20702050 |
| modelling foot-and-mouth disease virus dynamics in oral epithelium to help identify the determinants of lysis. | foot-and-mouth disease virus (fmdv) causes an economically important disease of cloven-hoofed livestock; of interest here is the difference in lytic behaviour that is observed in bovine epithelium. on the skin around the feet and tongue, the virus rapidly replicates, killing cells, and resulting in growing lesions, before eventually being cleared by the immune response. in contrast, there is usually minimal lysis in the soft palate, but virus may persist in tissue long after the animal has recov ... | 2011 | 20725794 |
| meta-analysis on the efficacy of foot-and-mouth disease emergency vaccination. | the objectives of this study were to provide a summary quantification of the efficacy of fmd emergency vaccination based on a systematic review and a meta-analysis of available literature, and to further discuss the suitability of this review and meta-analysis to summarize and further interpret the results. peer-reviewed, symposium, and unpublished studies were considered in the analysis. clinical protection and virological protection against fmd were used as parameters to assess the efficacy of ... | 2011 | 20869130 |
| porcine type i interferon rapidly protects swine against challenge with multiple serotypes of foot-and-mouth disease virus. | foot-and-mouth disease virus (fmdv) causes a highly contagious disease of cloven-hoofed animals. current inactivated vaccines require approximately 7 days to induce protection, but before this time vaccinated animals remain susceptible to disease. previously, we demonstrated that intramuscular (im) inoculation of a replication-defective human adenovirus type 5 (ad5) vector containing a porcine interferon α gene (pifnα) can protect swine challenged 1 day later by intradermal (id) injection with f ... | 2010 | 20874428 |
| improved immune response by id-pvac: a secretory dna vaccine construct delivered by plg micro particles against foot and mouth disease in guinea pigs. | foot and mouth disease (fmd) outbreaks usually have devastating effects on the economy of countries were disease is endemic due to direct and indirect cost; most of them related to international trade embargoes of animals and animal products. although currently used inactivated vaccine provides protection, it has several drawbacks like short duration of immunity, and the requirement for containment facilities. a dna vaccine construct which expresses the secretary antigens, delivered through micr ... | 2010 | 20884037 |
| recombinant pseudorabies virus expressing p12a and 3c of fmdv can partially protect piglets against fmdv challenge. | one of the crucial factors for evaluation of an effective genetically engineered vaccine is whether susceptible animals are protected from virus challenge after vaccination. in this study, a recombinant pseudorabies virus (prv-p12a3c) that expressed capsid precursor polypeptide p12a and nonstructural protein 3c of foot-and-mouth disease virus (fmdv) was used as a vaccine. the expression of p12a3c and its immunogenicity and protective efficacy against fmdv challenge were measured. humoral and cel ... | 2010 | 20947111 |
| development and validation of a lateral flow immunoassay using colloidal gold for the identification of serotype-specific foot-and-mouth disease virus o, a and asia 1. | a lateral flow immunoassay (lfi) was developed to identify and diagnose foot-and-mouth disease virus (fmdv) serotypes o, a and asia 1. antibodies obtained from rabbits and guinea pigs immunized with cell-culture-adapted virus strains (o/cha/99, a/gs/lx/66, asia 1/chn/05) and suckling-mouse adapted virus strains (o/av99(l), a/av88(l), asia 1/ynbs/58) were used as capture antibodies. the diagnostic kit included three immunochromatographic strips of types o, a and asia 1, and the type-specific resu ... | 2010 | 20951743 |
| b cell epitopes within vp1 of type o foot-and-mouth disease virus for detection of viral antibodies. | in this study, the coding region of type o fmdv capsid protein vp1 and a series of codon optimized dna sequences coding for vp1 amino acid residues 141-160 (epitope1), tandem repeat 200-213 (epitope2 (+2)) and the combination of two epitopes (epitope1-2) was genetically cloned into the prokaryotic expression vector pp(ro)exhtb and pgex4t-1, respectively. vp1 and the fused epitopes gst-e1, gst-e2 (+2) and gst-e1-2 were successfully solubly expressed in the cytoplasm of escherichia coli and wester ... | 2010 | 20960280 |
| identification of a conformational epitope on the vp1 g-h loop of type asia1 foot-and-mouth disease virus defined by a protective monoclonal antibody. | although neutralizing antigenic sites of foot-and-mouth disease virus (fmdv) can be defined by selection of monoclonal antibody (mab) escape mutants, no conformational neutralizing epitope on the major antigenic site located on the g-h loop of type asia1 fmdv has been precisely mapped. in this study, we generated a potent neutralizing mab 3e11, which recognized a conformation-dependent epitope and neutralized fmdv asia1/ys/cha/05 in vitro. importantly, a dose of 5.5 nt(50) of the mab 3e11 comple ... | 2010 | 20961714 |
| identification of a conserved linear epitope on the vp1 protein of serotype o foot-and-mouth disease virus by neutralising monoclonal antibody 8e8. | foot-and-mouth disease virus (fmdv) serotype o remains an important threat to animal husbandry worldwide, and the variability of the virus presents a major problem for fmdv vaccine design. high-affinity neutralising antibodies against a conserved epitope could provide protective immunity against diverse subtypes of fmdv serotype o and protect against future pandemics. we generated a novel monoclonal antibody (mab) 8e8 that potently neutralised infection of fmdv o/ys/cha/05 both in vitro and in v ... | 2010 | 20974198 |
| phylogenetic analyses of the polyprotein coding sequences of serotype o foot-and-mouth disease viruses in east africa: evidence for interserotypic recombination. | foot-and-mouth disease (fmd) is endemic in east africa with the majority of the reported outbreaks attributed to serotype o virus. in this study, phylogenetic analyses of the polyprotein coding region of serotype o fmd viruses from kenya and uganda has been undertaken to infer evolutionary relationships and processes responsible for the generation and maintenance of diversity within this serotype. fmd virus rna was obtained from six samples following virus isolation in cell culture and in one ca ... | 2010 | 20731826 |
| competition-colonization dynamics: an ecology approach to quasispecies dynamics and virulence evolution in rna viruses. | a single and purified clone of foot-and-mouth disease virus diversified in cell culture into two subpopulations that were genetically distinct. the subpopulation with higher virulence was a minority and was suppressed by the dominant but less virulent one. these two populations follow the competitioncolonization dynamics described in ecology. virulent viruses can be regarded as colonizers because they killed the cells faster and they spread faster. the attenuated subpopulation resembles competit ... | 2010 | 20798818 |
| genetic characterization of the cell-adapted panasia strain of foot-and-mouth disease virus o/fujian/cha/5/99 isolated from swine. | according to office international des epizooties (oie) bulletin, the panasia strain of foot-and-mouth disease virus (fmdv) was invaded into the people's republic of china in may 1999. it was confirmed that the outbreaks occurred in tibet, hainan and fujian provinces. in total, 1280 susceptible animals (68 cattle, 1212 swine) were destroyed for the epidemic control.to investigate the distinct biological properties, we performed plaque assay, estimated the pathogenicity in suckling mice and determ ... | 2010 | 20807416 |
| study of a chimeric foot-and-mouth disease virus dna vaccine containing structural genes of serotype o in a genome backbone of serotype asia 1 in guinea pigs. | since foot-and-mouth disease virus (fmdv) serotypes display a great genetic and antigenic diversity, there is a constant requirement to monitor the performance of fmdv vaccines in the field with respect to their antigenic coverage. to avoid possible antigenic changes in field fmdv isolates during their adaptation to bhk-21 cells, a standard step used in production of conventional fmdv vaccines, the custom-made chimeric conventional or dna vaccines, in which antigenic determinants are replaced wi ... | 2010 | 20822311 |
| alternative way to test the efficacy of swine fmd vaccines: measurement of pigs median infected dose (pid50) and regulation of live virus challenge dose. | foot-and -mouth disease to pigs is serious recently around the world. "vaccination prevention" is still an important policy. oie specifies 10,000 tcid50(0.2 ml) of virulent virus for challenge test in pigs to test the potency of fmd vaccine by intradermal route inoculating the virus in the heel bulbs of one foot or by intramuscular route administering into one site of the neck behind the ear. convenience and speediness are available in the process of potency test of commercial fmd vaccine. we se ... | 2010 | 20822547 |
| two-dimensional heteronuclear saturation transfer difference nmr reveals detailed integrin αvβ6 protein-peptide interactions. | we report the first example of peptide-protein heteronuclear two-dimensional (2d) saturation transfer difference nuclear magnetic resonance (std nmr). this method, resulting in dramatically reduced overlap, was applied to the interaction of the integrin αvβ6 with a known peptide ligand and highlights novel contact points between the substrate and target protein. | 2010 | 20838674 |
| specific detection of rinderpest virus by real-time reverse transcription-pcr in preclinical and clinical samples from experimentally infected cattle. | a highly sensitive detection test for rinderpest virus (rpv), based on a real-time reverse transcription-pcr (rrt-pcr)system, was developed. five different rpv genomic targets were examined, and one was selected and optimized to detect viral rna in infected tissue culture fluid with a level of detection ranging from 0.59 to 87.5 50% tissue culture infectious doses (tcid(50)) per reaction depending on the viral isolate. the strain sensitivity of the test was validated on 16 rpv strains belonging ... | 2010 | 20844216 |
| a mutant of infectious asia 1 serotype foot-and-mouth disease virus with the deletion of 10-amino-acid in the 3a protein. | foot-and-mouth disease virus (fmdv) serotype asia 1 is one of the most predominant endemic serotypes in china. our previous study has generated a full-length cdna clone (pbsas) of an asia 1 serotype fmdv (as1/cha/05) isolated from bovine. to further study the properties of this virus, a mutant in the 3a region of the cdna clone (pbsas-3a10d), containing the deletion at position 93-102 of the 3a protein of as1/cha/05, was generated by pcr and cloning. after synthesis of rna in vitro and transfect ... | 2010 | 20844943 |
| development of a foot-and-mouth disease infection model in severe combined immunodeficient mice for the preliminary evaluation of antiviral drugs. | recent european guidelines facilitate the use of emergency vaccines during outbreaks of foot-and-mouth disease. antiviral drugs could be used as a complementary measure. this study aimed at developing a small animal model to assess the in vivo activity of early antiviral lead molecules with anti-foot-and-mouth disease virus (fmdv) activity in vitro. in a first attempt, several fmdv strains were titrated in balb/c mice. inoculations with o₁ manisa or c₁ noville did not induce clinical disease, wh ... | 2010 | 21029400 |
| multiplex pcr for rapid detection of serotype a foot-and-mouth disease virus variants with amino acid deletion at position 59 of the capsid protein vp3. | in india, there has been co-circulation, extinction and emergence of genotypes/lineages within serotype a foot-and-mouth disease (fmd) virus. at present an antigenically heterogeneous, unique lineage within genotype vii dominates the field outbreaks. this genetic cluster has amino acid deletion at position 59 of vp3 (vp3(59)-deletion group), considered to be critical antigenically. the emergence of this group warrants rapid and accurate detection to facilitate early planning and implementation o ... | 2010 | 21029752 |
| enhancement of dna vaccine (p12a3c-pcdna) efficacy against foot-and-mouth disease by coadministration of interleukin-18-expressing (il18 pcdna) plasmid in guinea-pigs. | foot-and-mouth disease (fmd) is a highly contagious disease of cloven-hoofed animals causing considerable economic loss in the affected countries. the presently used tissue-cultured inactivated vaccine protects the vaccinated animals for a short duration of immunity. as one of the approaches to develop alternative vaccines, p12a3c-pcdna (containing p12a and 3c coding sequences of foot-and-mouth disease virus) and bovine il18 pcdna plasmids were constructed and the immune response of these constr ... | 2010 | 21039923 |
| preparation and characterization of neutralizing monoclonal antibodies against fmdv serotype o with synthetic peptide antigen. | a short linear peptide was designed according to the antigenic site analysis of vp1 protein of foot-and-mouth virus (fmdv) serotype o and synthesized as the peptide immunogen. the peptide, which covers the region from amino acid 133 to 160 of vp1 of fmdv, was linked to the n-terminal cysteine and conjugated with the carrier protein of keyhole limpet hemocyanin (klh). normal 6- to 8-week-old balb/c mice were immunized with the 20 μg dose conjugated peptide antigen four times. the splenocytes from ... | 2010 | 21050041 |
| structural analysis provides insights into the modular organization of picornavirus ires. | picornavirus rna translation is driven by the internal ribosome entry site (ires) element. the impact of rna structure on the foot-and-mouth disease virus (fmdv) ires activity has been analyzed using selective 2'hydroxyl acylation analyzed by primer extension (shape) and high throughput analysis of rna conformation by antisense oligonucleotides printed on microarrays. shape reactivity revealed the self-folding capacity of domain 3 and evidenced a change of rna structure in a defective gnra mutan ... | 2010 | 21056890 |
| risk evaluation of nonvaccinated, weaned calves transported through areas under systematic foot and mouth disease (fmd) vaccination. | the recurrence and persistence of foot and mouth disease (fmd) could be the consequence of cyclic and massive transportation of calves. for this reason, in south america, vaccination strategies related to livestock dynamic are being promoted. in order to aid the evaluation of such strategies, a method for predicting the risk of transportation of nonvaccinated weaned calves was developed; this method combines expert opinion and empirical evidence using bayesian estimators. it was applied through ... | 2010 | 21071104 |
| regulation of iga responses in cattle, humans and mice. | secretory iga (siga) constitutes the largest component of the humoral immune system of the body with gram quantities of this isotype produced by mammals on a daily basis. secretory iga (siga) antibodies function by both blocking pathogen/commensal entry at mucosal surfaces and virus neutralization. several pathways of induction of iga responses have been described which depend on t cells (t cell dependent or td) pathways or are independent of t cells (t-independent or ti) and are mediated by den ... | 2010 | 21074276 |
| the epidemiological characteristics of the 2007 foot-and-mouth disease epidemic in sarpang and zhemgang districts of bhutan. | this study was undertaken to compare the epidemiological characteristics of the 2007 foot-and-mouth disease outbreak in two districts of sarpang and zhemgang in bhutan. zhemgang district recorded a significantly higher cumulative incidence in all species (26.9%) as well as for cattle (29.3%) compared to sarpang (6.5% and 7.4%, respectively). the case fatality for cattle in zhemgang (14.1%) was significantly higher than in sarpang (3.3%). a total of 404 cattle and 73 pigs died of fmd in zhemgang, ... | 2010 | 21078083 |
| promising multiple-epitope recombinant vaccine against foot-and-mouth disease virus type o in swine. | in order to develop a completely safe immunogen to replace the traditional inactivated vaccine, a tandem-repeat multiple-epitope recombinant vaccine against foot-and-mouth disease (fmd) virus (fmdv) type o was developed. it contained three copies each of residues 141 to 160 and 200 to 213 of vp1 of the o/china/99 strain of fmdv coupled with a swine immunoglobulin g heavy-chain constant region (scigg). the data showed that the multiple-epitope recombinant vaccine elicited high titers of anti-fmdv ... | 2010 | 21084463 |
| development of a dot immunoblot method for differentiation of animals infected with foot-and-mouth disease virus from vaccinated animals using non-structural proteins expressed prokaryotically. | five non-structural proteins (nsps) of foot-and-mouth disease virus (fmdv) were expressed in e. coli to develop a dot immunoblot (dot blot) assay for the differentiation of fmdv infected animals from vaccinated animals (diva). the five nsps were 3a (24 kda), 3b (15 kda), major b-cell epitope regions of 2c (23 kda), partial 3d (44 kda) and 3abc (59 kda). the criteria for the dot blot were determined and are described as follows: a test sample is considered positive if four or more nsps demonstrat ... | 2010 | 21087638 |
| phylogeography of foot-and-mouth disease virus types o and a in malaysia and surrounding countries. | foot-and-mouth disease (fmd) is endemic in the countries of mainland southeast asia where it represents a major obstacle to the development of productive animal industries. the aim of this study was to use genetic data to determine the distribution of fmd virus (fmdv) lineages in the southeast asia region, and in particular identify possible sources of fmdv causing outbreaks in malaysia. complete vp1 sequences, obtained from 214 samples collected between 2000 and 2009, from fmd outbreaks in six ... | 2010 | 21093614 |
| fmd subunit vaccine produced using a silkworm-baculovirus expression system: protective efficacy against two type asia1 isolates in cattle. | cattle vaccinated with a single dose of subunit vaccine containing the capsid and 3c proteinase coding regions of foot-and-mouth disease virus (fmdv) asia i/hnk/cha/05 strain were protected when challenged 28 days later with a homologous virus. here, the 50% bovine protective dose (pd(50)) test was performed to assess the potency of the subunit vaccine. when challenged with two chinese isolates, the subunit vaccine could achieve 6.5 pd(50) (challenged with asia i/hnk/cha/05 strain) and 5.2 pd(50 ... | 2010 | 21109368 |
| foot-and-mouth disease virus utilizes an autophagic pathway during viral replication. | foot-and-mouth disease virus (fmdv) is the type species of the aphthovirus genus within the picornaviridae family. infection of cells with positive-strand rna viruses results in a rearrangement of intracellular membranes into viral replication complexes. the origin of these membranes remains unknown; however induction of the cellular process of autophagy is beneficial for the replication of poliovirus, suggesting that it might be advantageous for other picornaviruses. by using confocal microscop ... | 2010 | 21112602 |
| evolutionary analysis of foot-and-mouth disease virus serotype sat 1 isolates from east africa suggests two independent introductions from southern africa. | in east africa, foot-and-mouth disease virus serotype sat 1 is responsible for occasional severe outbreaks in livestock and is known to be maintained within the buffalo populations. little is known about the evolutionary forces underlying its epidemiology in the region. to enhance our appreciation of the epidemiological status of serotype sat 1 virus in the region, we inferred its evolutionary and phylogeographic history by means of genealogy-based coalescent methods using 53 vp1 coding sequence ... | 2010 | 21118525 |
| an induced hypersensitive-like response limits expression of foreign peptides via a recombinant tmv-based vector in a susceptible tobacco. | by using tobacco mosaic virus (tmv)-based vectors, foreign epitopes of the vp1 protein from food-and-month disease virus (fmdv) could be fused near to the c-terminus of the tmv coat protein (cp) and expressed at high levels in susceptible tobacco plants. previously, we have shown that the recombinant tmv vaccines displaying fmdv vp1 epitopes could generate protection in guinea pigs and swine against the fmdv challenge. recently, some recombinant tmv, such as tmvfn20 that contains an epitope fn20 ... | 2010 | 21124743 |
| immune responses to the oral administration of recombinant bacillus subtilis expressing multi-epitopes of foot-and-mouth disease virus and a cholera toxin b subunit. | bacillus subtilis has been engineered successfully to express heterologous antigens for use as a vaccine vehicle that can elicit mucosal and systemic immunity response. in this study, a recombinant b. subtilis expressing the b subunit of cholera toxin (ct-b) and an epitope box constituted with antigen sites from foot-and-mouth disease virus (fmdv) type asia 1 was constructed and named 1a751/ctb-tepias. its capability to induce mucosal, humoral, and cellular responses in mice and guinea pigs was ... | 2010 | 21129406 |
| quantitative trait loci for variation in immune response to a foot-and-mouth disease virus peptide. | infectious disease of livestock continues to be a cause of substantial economic loss and has adverse welfare consequences in both the developing and developed world. new solutions to control disease are needed and research focused on the genetic loci determining variation in immune-related traits has the potential to deliver solutions. however, identifying selectable markers and the causal genes involved in disease resistance and vaccine response is not straightforward. the aims of this study we ... | 2010 | 21138580 |
| the role of african buffalos (syncerus caffer) in the maintenance of foot-and-mouth disease in uganda. | to study the role of african buffalos (syncerus caffer) in the maintenance of foot-and-mouth disease in uganda, serum samples were collected from 207 african buffalos, 21 impalas (aepyceros melampus), 1 giraffe (giraffa camelopardalis), 1 common eland (taurotragus oryx), 7 hartebeests (alcelaphus buselaphus) and 5 waterbucks (kobus ellipsiprymnus) from four major national parks in uganda between 2005 and 2008. serum samples were screened to detect antibodies against foot-and-mouth disease virus ... | 2010 | 21143994 |
| characterisation and epitope mapping of neutralising monoclonal antibodies to a24 cruzeiro strain of fmdv. | characterisation of seven neutralising monoclonal antibodies (mabs) produced against foot-and-mouth disease virus a(24) cruzeiro revealed three reactivity groups. gr-i recognised linear epitopes where as gr-ii was conformation-dependent and trypsin-insensitive. the gr-iii was also conformation-dependent, but trypsin-sensitive. mar (mab neutralisation resistant)-mutants could only be produced against gr-i and gr-iii mabs. capsid sequence comparison of gr-i mar-mutants with parent virus revealed c ... | 2010 | 21144677 |
| efficient and stable expression of gfp through wheat streak mosaic virus-based vectors in cereal hosts using a range of cleavage sites: formation of dense fluorescent aggregates for sensitive virus tracking. | a series of wheat streak mosaic virus (wsmv)-based expression vectors were developed by engineering a cycle 3 gfp (gfp) cistron between p1 and hc-pro cistrons with several catalytic/cleavage peptides at the c-terminus of gfp. wsmv-gfp vectors with the foot-and-mouth disease virus 1d/2a or 2a catalytic peptides cleaved gfp from hc-pro but expressed gfp inefficiently. wsmv-gfp vectors with homologous nia-pro heptapeptide cleavage sites did not release gfp from hc-pro, but efficiently expressed gfp ... | 2010 | 21145088 |
| sequence-based prediction for vaccine strain selection and identification of antigenic variability in foot-and-mouth disease virus. | identifying when past exposure to an infectious disease will protect against newly emerging strains is central to understanding the spread and the severity of epidemics, but the prediction of viral cross-protection remains an important unsolved problem. for foot-and-mouth disease virus (fmdv) research in particular, improved methods for predicting this cross-protection are critical for predicting the severity of outbreaks within endemic settings where multiple serotypes and subtypes commonly co- ... | 2010 | 21151576 |
| beyond the consensus: dissecting within-host viral population diversity of foot-and-mouth disease virus by using next-generation genome sequencing. | the diverse sequences of viral populations within individual hosts are the starting material for selection and subsequent evolution of rna viruses such as foot-and-mouth disease virus (fmdv). using next-generation sequencing (ngs) performed on a genome analyzer platform (illumina), this study compared the viral populations within two bovine epithelial samples (foot lesions) from a single animal with the inoculum used to initiate experimental infection. genomic sequences were determined in duplic ... | 2010 | 21159860 |
| sequence and phylogenetic analysis of the non-structural 3a and 3b protein-coding regions of foot-and-mouth disease virus subtype a iran 05. | the a iran 05 foot-and-mouth disease virus (fmdv) subtype was detected in iran during 2005 and has proven to be highly virulent. this study was undertaken to focus on molecular and phylogenetic analysis of 3a and 3b coding-regions in the a iran 05 field isolate. to assess the genetic relatedness of a iran 05 isolate the nucleotide and predicted amino acid sequences of the 3ab region of type a fmdv isolates were compared with twenty previously described type a fmdv isolates. the phylogenetic tree ... | 2010 | 20706032 |
| molecular cloning and phylogenetic analysis of integrins alphavbeta1 and alphavbeta6 of one-humped camel (camelus dromedarius). | bactrian camels can relatively easily be infected with fmdv, but dromedary camels remain resistant even to high doses of the virus. to understand the different susceptibility between the two camel species from the standpoint of viral receptors, this work reports the sequences of the dromedary camel integrin cdnas encoding alphavbeta1 and alphavbeta6 and compare them to those of other species, especially to bactrian camels. the complete coding sequences for the dromedary camel alphav, beta1 and b ... | 2010 | 20015555 |
| design and optimization of a novel reverse transcription linear-after-the-exponential pcr for the detection of foot-and-mouth disease virus. | a novel molecular assay for the detection of foot-and-mouth disease virus (fmdv) was developed using linear-after-the-exponential polymerase chain reaction (late-pcr). | 2010 | 20028437 |
| coexpression of double or triple copies of the rabies virus glycoprotein gene using a 'self-cleaving' 2a peptide-based replication-defective human adenovirus serotype 5 vector. | rabies virus glycoprotein (rvg) is a major structural protein and antigen of rabies virus that induces a highly immunogenic response. in the present study, we have used 2a self-cleaving sequence of the foot-and-mouth disease virus (fmdv) to express double or triple copies of the rvg from a single open reading frame derived from human adenovirus 5 (adhu5). the recombinant adenoviruses produce similar virus titers, indicating that the insertion of double or triple copies of the rvg gene linked wit ... | 2010 | 20682459 |
| development of an in process control filtration-assisted chemiluminometric immunoassay to quantify foot and mouth disease virus (fmdv) non-capsid proteins in vaccine-antigen batches. | in many countries, foot and mouth disease (fmd) is controlled by vaccination and surveillance against non-capsid proteins (ncp); therefore vaccines are required not to induce antibodies against ncp. vaccine purity is evaluated by repeated inoculation of naïve cattle, an expensive and time consuming protocol that raises several animal welfare concerns. we have developed an in process control filtration-assisted chemiluminometric immunoassay (fal-elisa), to detect and quantify ncp in vaccine-antig ... | 2010 | 20685600 |
| antibodies to pathogenic livestock viruses in a wild vicuña (vicugna vicugna) population in the argentinean andean altiplano. | serum samples from 128 wild vicuñas (vicugna vicugna) were tested for antibodies (ab) to rotavirus (rv), bovine parainfluenza virus 3 (bpiv-3), bovine herpesvirus-1 (bhv-1), bovine viral diarrhea virus (bvdv-1), foot-and-mouth disease virus (fmdv), bluetongue virus (btv), equine herpesvirus-1 (ehv-1), and influenza a virus equine (eiv). samples were collected in cieneguillas province of jujuy, in northern argentina. feces from 44 vicuñas were also collected to investigate rv shedding. llamas (la ... | 2010 | 20688660 |
| survey for foot-and-mouth disease in the endangered marsh deer (blastocerus dichotomus) from marshlands of the parana river basin, brazil. | habitat fragmentation and diseases have resulted in a decline of the marsh deer (blastocerus dichotomus) throughout its south american range. our objectives were to determine whether marsh deer intended for translocation from a region of the rio paraná basin had been infected previously by foot-and-mouth disease virus (fmdv) and whether they were carrying virus. we captured marsh deer from june to october 1998 and collected blood from 108 animals and esophageal-pharyngeal fluid from 53. serum wa ... | 2010 | 20688701 |
| serotype specificity of antibodies against foot-and-mouth disease virus in cattle in selected districts in uganda. | uganda had an unusually large number of foot-and-mouth disease (fmd) outbreaks in 2006, and all clinical reports were in cattle. a serological investigation was carried out to confirm circulating antibodies against foot-and-mouth disease virus (fmdv) by elisa for antibodies against non-structural proteins and structural proteins. three hundred and forty-nine cattle sera were collected from seven districts in uganda, and 65% of these were found positive for antibodies against the non-structural p ... | 2010 | 20696028 |
| genetic characterization of indian type o fmd virus 3a region in context with host cell preference. | the 3a region of foot-and-mouth disease virus has been implicated in host range and virulence. for example, amino acid deletions in the porcinophilic strain (o/taw/97) at 93-102aa of the 153 codons long 3a protein have been recognized as the determinant of species specificity. in the present study, 18 type o fmdv isolates from india were adapted in different cell culture systems and the 3a sequence was analyzed. these isolates had complete 3a coding sequence (153aa) and did not exhibit growth re ... | 2010 | 20302973 |
| an indirect elisa for serodiagnosis of cattle footrot caused by fusobacterium necrophorum. | a serodiagnostic elisa (rl-elisa) using recombinant truncated leukotoxin protein pl2 (aa 311-644) of fusobacterium necrophorum as antigen was developed for detection of antibodies against f. necrophorum from cattle footrot. in rl-elisa, the recombinant diagnostic antigen showed no cross-reaction with antisera against bovine foot and mouth disease virus, bovine rhinotracheitis virus, bovine viral diarrhea virus, bovine rotavirus type a, bovine escherichia coli, and bovine salmonella. the rl-elisa ... | 2010 | 20304080 |
| [transmission risk for foot-and-mouth-disease in an animal-densed region in germany--results from an expert survey]. | due to its strong impact on economics and trading the foot-and-mouth-disease (fmd) is one of the most important animal diseases within animal husbandry. because no recent specific field observation for fmd exists in germany, the risk assessment needs validated epidemiological models to prepare decision tools for fmd-outbreak management. the aim of this investigation was therefore to prepare a risk assessment for different transmission pathways to use for fmd-models in future. to prepare a fmd-tr ... | 2010 | 20329640 |
| development of tobacco necrosis virus a as a vector for efficient and stable expression of fmdv vp1 peptides. | plant virus-based expression systems provide attractive alternatives for production of animal virus-originated antigenic peptides. in the present study, an infectious cdna clone of tobacco necrosis virus a chinese isolate (tnv-a(c)) was used for expression of different peptides derived from foot and mouth disease virus (fmdv) serotype o vp1 fused downstream of the coat protein (cp) open reading frame (orf). chenopodium amaranticolor inoculated with in vitro transcripts of the chimaeras developed ... | 2010 | 20331532 |
| effect of foot-and-mouth disease virus capsid precursor protein and 3c protease expression on bovine herpesvirus 1 replication. | several reports have previously shown that expression of the foot-and-mouth disease virus (fmdv) capsid precursor protein encoding region p1-2a together with the 3c protease (p1-2a/3c) results in correct processing of the capsid precursor into vp0, vp1 and vp3 and formation of fmdv capsid structures that are able to induce a protective immune response against fmdv challenge after immunization using naked dna constructs or recombinant viruses. to elucidate whether bovine herpesvirus 1 (bhv-1) mig ... | 2010 | 20333533 |
| the efficacy of fmd vaccine reduced non-structural proteins with a mab against 3b protein. | a monoclonal antibody, 3bigg, against the prokaryotically expressed foot-and-mouth disease virus (fmdv) non-structural protein (nsp) 3b was obtained. the 3bigg-sepharose conjugant (3bmab-6bff) was prepared by adding the purified 3bigg into epoxy-activated sepharose 6bff, incubating with the inactivated fmdv, and then removing the sepharose by centrifugation. the vaccine was made from the supernatant emulsified with oil-adjuvant isa206. ten guinea pigs, 26 pigs and six cattle were vaccinated, and ... | 2010 | 20512625 |
| functional expression of secreted proteins from a bicistronic retroviral cassette based on foot-and-mouth disease virus 2a can be position dependent. | the expression of two or more genes from a single viral vector has been widely used to label or select for cells containing the transgenic element. identification of the foot-and-mouth disease virus (fmdv) 2a cleavage peptide as a polycistronic linker capable of producing equivalent levels of transgene expression has greatly improved this approach in the field of gene therapy. however, as a consequence of 2a posttranslational cleavage the upstream protein is left with a residual 19 amino acids f ... | 2010 | 20528679 |
| foot and mouth disease in animals in sharkia governorate - egypt. | this study was carried out to determine the current state of foot and mouth disease (fmd) in different animal species in sharkia governorate in egypt. in addition, we investigated the spreading of the virus through water and soil in the animal environment as well as by rodents. the isolation rates of fmd virus in tissue culture were 39.6%, 11.4%, 41.2% and 100% for cattle, buffalo, sheep and goat respectively. all animals did not show any clinical signs for fmd. in addition, the virus was isolat ... | 2010 | 20537095 |
| chitosan can stop or postpone the death of the suckling mice challenged with foot-and-mouth disease virus. | in the study, a method called "hardening in liquid phase" for preparing chitosan granules with glutaraldehyde as crosslinker and tween 80 as surfactant and paraffin liquid as dispersant was established. the chitosan granules were light yellow and insoluble in water or oil, but they swelled in acid solution and narrowed in neutral or alkaline solution. furthermore, some of characteristics of the chitosan granules were revealed. (a) stability: their shapes were stable at ph 7.0 and ph 8.0 and -30 ... | 2010 | 20540780 |
| antibodies against foot-and-mouth disease (fmd) virus in african buffalos (syncerus caffer) in selected national parks in uganda (2001-2003). | in east africa, the foot-and-mouth disease (fmd) virus (fmdv) isolates have over time included serotypes o, a, c, southern african territories (sat) 1 and sat 2, mainly from livestock. sat 3 has only been isolated in a few cases and only in african buffalos (syncerus caffer). to investigate the presence of antibodies against fmdv serotypes in wildlife in uganda, serological studies were performed on buffalo serum samples collected between 2001 and 2003. thirty-eight samples from african buffalos ... | 2010 | 20561289 |
| multiple shrnas driven by u6 and cmv promoter enhances efficiency of antiviral effects against foot-and-mouth disease virus. | foot-and-mouth disease (fmd) is an economically significant animal disease because of the speed of its transmission. the current vaccine for fmd provides no protection until 7 days post-vaccination, thus reducing its effectiveness in the case of an outbreak. small interfering rna (sirna) is a promising antiviral approach because it can induce a protective response much more rapidly. this study is the first report to apply multiple short hairpin rna (shrna) expression systems to inhibit foot-and- ... | 2010 | 20561543 |
| letter to the editor. loss of plasmacytoid dendritic cell function coincides with lymphopenia and viremia during foot-and-mouth disease virus infection. | 2010 | 20565298 | |
| qualitative assessment of the commodity risk for spread of foot-and-mouth disease associated with international trade in deboned beef. | the risk of importing foot-and-mouth disease virus (fmdv) restricts trade in livestock and their products from parts of the world where the virus is present. this reduces trade opportunities and investment in the livestock sector of many developing countries and constrains global food supply. this review focuses on the risks associated with trade in deboned beef (db) from foot-and-mouth disease (fmd)-infected cattle, countries or zones. a definition of db is provided along with a description of ... | 2010 | 20569417 |
| status of foot-and-mouth disease in pakistan. | the present study reports the distribution of different serotypes of foot-and-mouth disease virus (fmdv) in pakistan during the period 1952-2007. during this time, a total of 1,543 epithelial samples out of 2,484 tested were found positive for various serotypes of fmdv. serotype o was found to be the most prevalent (p < 0.001) followed by serotype asia-1 and a. serotype c was detected only in 1954, 1963 and 1995. the disease was found to be more prevalent (p < 0.0001) in cattle than buffaloes. t ... | 2010 | 20571838 |
| [fusion expression of asia i type fmdv neutralizing epitope with heavy chain constant region of sheep igg and the assessment of its immunogenicity]. | vp1 is a major antigenic protein of foot-and-mouth disease virus(fmdv), which induces the immune response against fmdv infection, and contains several epitopes of the virus. we designed and chemically synthesized a dna fragment which encoding a tandem repeat protein of 136-160aa and 198-211aa of a strain of type asia i fmdv, and cloned the gene of heavy chain constant region of sheep igg. by using the bamh i, ecor i and xho i sites, both genes were cloned into pproexhtb vector in turn to form a ... | 2010 | 20575432 |
| a simulation model for the potential spread of foot-and-mouth disease in the castile and leon region of spain. | a spatial stochastic model was used to simulate the spread of a foot-and-mouth disease (fmd) epidemic in the castile-and-leon (cyl) region of spain. the model was fitted using information available on premises demographics and on assumptions for animal movements, indirect contacts, and airborne exposure. control measures dictated by spanish and european union regulations constituted a reference strategy to which six alternative control strategies were compared. for the reference strategy, the me ... | 2010 | 20579754 |
| domain disruptions of individual 3b proteins of foot-and-mouth disease virus do not alter growth in cell culture or virulence in cattle. | picornavirus rna replication is initiated by a small viral protein primer, 3b (also known as vpg), that is covalently linked to the 5' terminus of the viral genome. in contrast to other picornaviruses that encode a single copy of 3b, foot-and-mouth disease virus (fmdv) encodes three copies of 3b. viruses containing disrupted native sequence or deletion of one of their three 3b proteins were derived from a fmdv a24 cruzeiro full-length cdna infectious clone. mutant viruses had growth characterist ... | 2010 | 20580394 |
| baculovirus treatment fully protects mice against a lethal challenge of fmdv. | foot-and-mouth disease virus (fmdv) causes a highly contagious and economically devastating disease that affects cattle, swine, goat and sheep among others. fmdv is able to overcome the initial host innate immune response by inhibiting the induction of antiviral molecules at both the transcriptional and the translational levels. it has been demonstrated that fmdv a/arg/2001 causes the death of adult c57bl/6 mice within 72h. we evaluated the capacity of autographa californica nuclear polyhedrosis ... | 2010 | 20580746 |
| the early pathogenesis of foot-and-mouth disease in cattle after aerosol inoculation. identification of the nasopharynx as the primary site of infection. | to characterize the early events of foot-and-mouth disease virus (fmdv) infection in cattle subsequent to simulated natural exposure, 16 steers were aerosol inoculated with fmdv and euthanized at various times. samples were collected from each steer antemortem (serum, nasal swabs, and oral swabs) and postmortem (up to 40 tissues per animal) and screened for fmdv by virus isolation and for fmdv rna by real-time reverse transcription polymerase chain reaction. tissues that tested positive for fmdv ... | 2010 | 20587691 |
| foot-and-mouth disease virus replicates only transiently in well-differentiated porcine nasal epithelial cells. | three-dimensional (3d) porcine nasal mucosal and tracheal mucosal epithelial cell cultures were developed to analyze foot-and-mouth disease virus (fmdv) interactions with mucosal epithelial cells. the cells in these cultures differentiated and polarized until they closely resemble the epithelial layers seen in vivo. fmdv infected these cultures predominantly from the apical side, primarily by binding to integrin alphav beta6, in an arg-gly-asp (rgd)-dependent manner. however, fmdv replicated onl ... | 2010 | 20592089 |
| a recombinant humanized monoclonal antibody completely protects mice against lethal challenge with venezuelan equine encephalitis virus. | a recombinant humanized antibody to venezuelan equine encephalitis virus (veev) was constructed in a monocistronic adenoviral expression vector with a foot-and-mouth-disease virus-derived 2a self-cleavage oligopeptide inserted between the antibody heavy and light chains. after expression in mammalian cells, the heavy and light chains of the humanized antibody (hu1a4a1igg1-2a) were completely cleaved and properly dimerized. the purified hu1a4a1igg1-2a retained veev binding affinity and neutralizi ... | 2010 | 20600509 |
| co-circulation of two extremely divergent serotype sat 2 lineages in kenya highlights challenges to foot-and-mouth disease control. | amongst the sat serotypes of foot-and-mouth disease virus (fmdv), the sat 2 serotype is the most widely distributed throughout sub-saharan africa. kenyan serotype sat 2 viruses have been reported to display the highest genetic diversity for the serotype globally. this complicates diagnosis and control, and it is essential that patterns of virus circulation are known in order to overcome these difficulties. this study was undertaken to establish patterns of evolution of fmdv serotype sat 2 in ken ... | 2010 | 20614146 |
| [prokaryotic expression, protein purification and reactivity analysis of the vp1 and its c terminus of a south african isolate of fmdv serotype sat2]. | to induce the expression of structure protein vp1 and its c terminus of foot-and-mouth disease virus (fmdv) serotype sat2 in e.coli and analyze their reactivities with fmdv positive antiserum. | 2010 | 20619084 |
| diversity and transboundary mobility of serotype o foot-and-mouth disease virus in east africa: implications for vaccination policies. | foot-and-mouth disease (fmd) virus serotype o has been responsible for most reported outbreaks of the disease in east africa. a sustained campaign for the past 40 years to control fmd mainly by vaccination, combined with quarantine and zoosanitary measures has been undertaken with limited success. we investigated the genetic relationships among serotype o strains in eastern africa using complete vp1 coding region sequences obtained from 46 fmd virus isolates collected in kenya in the years 1964- ... | 2010 | 20619358 |
| molecular characterization of foot-and-mouth disease viruses collected from sudan. | the aim of this study was to characterize foot-and-mouth disease (fmd) viruses collected between 2004 and 2008 from sudan, a country where fmd is endemic. using virus isolation and antigen elisa, three fmd virus serotypes (o, a and sat2) were detected in 24 samples that were submitted to the fao world reference laboratory for fmd. pan-serotypic real-time rt-pcr assays targeting the 5' untranslated region (5'utr) and 3d genes of fmd virus were also used to contribute to the laboratory diagnosis o ... | 2010 | 20626708 |
| high-resolution in vivo imaging of breast cancer by targeting the pro-invasive integrin alphavbeta6. | the integrin alphavbeta6 is expressed only on epithelia and then usually only during processes of tissue remodelling including cancer, where its high expression correlates with reduced survival. thus, alphavbeta6 represents an important target for imaging and therapy of cancer and new molecular-specific targeting agents are required. we have developed a20fmdv2, a peptide derived from the vp1 coat protein of foot-and-mouth-disease virus that binds specifically and stably to alphavbeta6. using a n ... | 2010 | 20629113 |
| adjuvant effect of cliptox on the protective immune response induced by an inactivated vaccine against foot and mouth disease virus in mice. | foot and mouth disease (fmd) is an acute disease caused by foot and mouth disease virus (fmdv) which causes important economy losses, this is why it is necessary to obtain a vaccine that stimulates a rapid and long-lasting protective immune response. cliptox is a mineral microparticle that in earlier studies has shown adjuvant activity against different antigens. in this study we have examined the effects of cliptox on the magnitude and type of immunity elicited in response to inactivated fmdv ( ... | 2010 | 20637310 |
| mapping of amino acid residues responsible for adhesion of cell culture-adapted foot-and-mouth disease sat type viruses. | foot-and-mouth disease virus (fmdv) infects host cells by adhering to the alpha(v) subgroup of the integrin family of cellular receptors in a arg-gly-asp (rgd) dependent manner. fmd viruses, propagated in non-host cell cultures are reported to acquire the ability to enter cells via alternative cell surface molecules. sequencing analysis of sat1 and sat2 cell culture-adapted variants showed acquisition of positively charged amino acid residues within surface-exposed loops of the outer capsid stru ... | 2010 | 20637812 |
| foot-and-mouth disease virus leader proteinase inhibits dsrna-induced type i interferon transcription by decreasing interferon regulatory factor 3/7 in protein levels. | the leader proteinase (l(pro)) of foot-and-mouth disease virus (fmdv) has been identified as an interferon-beta (ifn-beta) antagonist that disrupts the integrity of transcription factor nuclear factor kappab (nf-kappab). in this study, we showed that the reduction of double stranded rna (dsrna)-induced ifn-alpha1/beta expression caused by l(pro) was also associated with a decrease of interferon regulatory factor 3/7 (irf-3/7) in protein levels, two critical transcription factors for activation o ... | 2010 | 20638368 |
| confidence in indirect assessment of foot-and-mouth disease vaccine potency and vaccine matching carried out by liquid phase elisa and virus neutralization tests. | the necessity of avoiding the use of animals in vaccine potency testing has been widely recognized. the repeatability and reproducibility of the expected percentage of protection (epp) as a serological potency surrogate for a24 cruzeiro foot-and-mouth disease virus (fmdv) strain was assessed, and compared with the results obtained with challenge in the protection against podal generalization (ppg) test. to determine the epps, the serum titers obtained by liquid phase blocking competitive elisa ( ... | 2010 | 20643090 |
| translation driven by picornavirus ires is hampered from sindbis virus replicons: rescue by poliovirus 2a protease. | alphavirus replicons are very useful for analyzing different aspects of viral molecular biology. they are also useful tools in the development of new vaccines and highly efficient expression of heterologous genes. we have investigated the translatability of sindbis virus (sv) subgenomic mrna bearing different 5'-untranslated regions, including several viral internal ribosome entry sites (iress) from picornaviruses, hepatitis c virus, and cricket paralysis virus. our findings indicate that all th ... | 2010 | 20643140 |
| application of two bicistronic systems involving 2a and ires sequences to the biosynthesis of carotenoids in rice endosperm. | coordination of multiple transgenes is essential for metabolic engineering of biosynthetic pathways. here, we report the utilization of two bicistronic systems involving the 2a sequence from the foot-and-mouth disease virus and the internal ribosome entry site (ires) sequence from the crucifer-infecting tobamovirus to the biosynthesis of carotenoids in rice endosperm. two carotenoid biosynthetic genes, phytoene synthase (psy) from capsicum and carotene desaturase (crti) from pantoea, were linked ... | 2010 | 20649940 |
| degradation of foot-and-mouth disease virus during composting of infected pig carcasses. | the objective of this study was to investigate the inactivation and degradation of foot-and-mouth disease (fmd) virus during composting of infected pig carcasses as measured by virus isolation in tissue culture and by real-time reverse transcriptase polymerase chain reaction (rrt-pcr). three fmd-infected pig carcasses were composted in a mixture of chicken manure and wood shavings in a biocontainment level 3 facility. compost temperatures had reached 50 degrees c and 70 degrees c by days 10 and ... | 2010 | 20357957 |
| genetic and antigenic characterization of foot-and-mouth disease viruses isolated in taiwan between 1998 and 2009. | a devastating outbreak of foot-and-mouth disease (fmd), caused by a porcinophilic serotype o virus, occurred in taiwan in march 1997. this outbreak was brought under control by means of a stamping-out policy and vaccination. although mandatory vaccination was conducted in taiwan between 1997 and 2007, sporadic outbreaks of fmd occurred between 1998 and 2009; however, the viruses that caused these outbreaks remain uncharacterized. this article reports the genetic and antigenic characterization of ... | 2010 | 20362404 |
| cell entry of the aphthovirus equine rhinitis a virus is dependent on endosome acidification. | equine rhinitis a virus (erav) is genetically closely related to foot-and-mouth disease virus (fmdv), and both are now classified within the genus aphthovirus of the family picornaviridae. for disease security reasons, fmdv can be handled only in high-containment facilities, but these constraints do not apply to erav, making it an attractive alternative for the study of aphthovirus biology. here, we show, using immunofluorescence, pharmacological agents, and dominant negative inhibitors, that er ... | 2010 | 20375159 |
| structure of foot-and-mouth disease virus mutant polymerases with reduced sensitivity to ribavirin. | passage of poliovirus (pv) or foot-and-mouth disease virus (fmdv) in the presence of ribavirin selected for viruses with decreased sensitivity to r, which included different mutations in their polymerase (3d): g64s located in the finger subdomain in the case of pv and m296i located within loop beta9-alpha11 at the active site in the case of fmdv. to investigate why disparate substitutions were selected in two closely related 3ds, we constructed fmdvs with a 3d that included either g62s (the equi ... | 2010 | 20392853 |
| characteristics of codon usage bias in two regions downstream of the initiation codons of foot-and-mouth disease virus. | the mechanism of utilization of alternative two augs in foot-and-mouth disease virus (fmdv) is still unknown to date. in this study, the characteristics of codon usage bias (cub) of the region between the two augs (the region-la) and of the same-sized region behind the second aug (the region-lb) in 94 different fmdv rna sequences were analyzed using relative synonymous codon usage (rscu) values. the results indicated that many codons with negative cub were preferentially used in the region-la. t ... | 2010 | 20398725 |
| assessment of gold nanoparticles as a size-dependent vaccine carrier for enhancing the antibody response against synthetic foot-and-mouth disease virus peptide. | to assess the ability of gold nanoparticles (gnps) to act as a size-dependent carrier, a synthetic peptide resembling foot-and-mouth disease virus (fmdv) protein was conjugated to gnps ranging from 2 to 50 nm in diameter (2, 5, 8, 12, 17, 37, and 50 nm). an extra cysteine was added to the c-terminus of the fmdv peptide (pfmdv) to ensure maximal conjugation to the gnps, which have a high affinity for sulfhydryl groups. the resultant pfmdv-gnp conjugates were then injected into balb/c mice. immuni ... | 2010 | 20400818 |
| no between-pen transmission of foot-and-mouth disease virus in vaccinated pigs. | many studies have shown transmission of foot-and-mouth disease virus (fmdv) within groups of pigs, even when vaccinated, but only limited information is available on transmission between pens. three new experiments were carried out in two replicates, which consisted of infectious pigs housed in a central pen surrounded by four separate pens. first, all pigs were non-vaccinated and pens were separated by a walkway of 40-70 cm. second, all pigs were non-vaccinated again but pens were adjacent. thi ... | 2010 | 20416264 |
| analysis of synonymous codon usage in foot-and-mouth disease virus. | in this study, we calculate the relative synonymous codon usage (rscu) values and codon usage bias (cub) values to carry out a comparative analysis of codon usage pattern for open reading frames (orfs) among 85 samples which belong to all seven serotypes of foot-and-mouth disease virus (fmdv). although the degree of cub for orfs is a relatively slight, there is a significant variation for cub among different serotypes, which is mainly determined by codon usage pattern depending on rscu. by compa ... | 2010 | 20425142 |
| crystal structure of equine rhinitis a virus in complex with its sialic acid receptor. | equine rhinitis a virus (erav) shares many features with foot-and-mouth disease virus (fmdv) and both are classified within the genus aphthovirus of the family picornaviridae. erav is used as a surrogate for fmdv research as it does not require high-level biosecurity. in contrast to fmdv, which uses integrins as cellular receptors, the receptor for erav has been reported to involve the sugar moiety sialic acid. this study confirmed the importance of sialic acid for cell entry by erav and reports ... | 2010 | 20427563 |
| pan-serotypic detection of foot-and-mouth disease virus by rt linear-after-the-exponential pcr. | a reverse transcription linear-after-the-exponential polymerase chain reaction (rt late-pcr) assay was evaluated for detection of foot-and-mouth disease virus (fmdv). this pan-serotypic assay targets highly conserved sequences within the 3d (rna polymerase) region of the fmdv genome, and uses end-point hybridisation analysis of a single mismatch-tolerant low temperature probe to confirm the identity of the amplicons. an armored rna served as an internal control to validate virus negative results ... | 2010 | 20433917 |
| recent spread of foot-and-mouth disease in the far east. | 2010 | 20435988 | |
| molecular characterization and expression analysis of porcine integrins alphavbeta3, alphavbeta6 and alphavbeta8 that are potentially involved in fmdv infection. | in the present study, we report the sequences and characterization of the porcine integrin cdnas encoding alphav, beta3, beta6 and beta8 subunits and compare them to those of other species. the coding sequences for the porcine alphav, beta3, beta6 and beta8 subunits were found to be 3141, 2289, 2367 and 2304 nucleotides in length, encoding 1046, 762, 788 and 767-amino-acid-residue protein, respectively. the porcine integrin alphav, beta3, beta6 and beta8 subunit shares common structural and func ... | 2010 | 20438833 |
| nmr solution structure of poliovirus uridylyated peptide linked to the genome (vpgpu). | picornaviruses have a 22-24 amino acid peptide, vpg, bound covalently at the 5' end of their rna, that is essential for replication. vpgs are uridylylated at a conserved tyrosine to form vpgpu, the primer of rna synthesis by the viral polymerase. this first complete structure for any uridylylated vpg, of poliovirus type 1 (pv1)-vpgpu, shows that conserved amino acids in vpg stabilize the bound ump, with the uridine atoms involved in base pairing and chain elongation projected outward. comparing ... | 2010 | 20441784 |