Publications
| Title | Abstract | Year Filter | PMID(sorted ascending) Filter |
|---|
| [Enhanced immune response of a novel T-cell immunogen in vaccine for foot-and-mouth disease]. | We investigated the enhanced immune response of a recombinant T cell immunogen as an effective cellular immune adjuvant. The T cell immunogen named TI contained several T cell epitopes from the VP1, VP4, 3A and 3D proteins of foot-and-mouth disease virus (FMDV) and two pan-T helper (T(H)) cell sites to broaden the immunogenicity of the protein. Meanwhile, another fusion protein named OA-VP1 was expressed in bacteria, which contained two VP1 proteins of O and Asia1 type FMDV. Mice were vaccinated ... | 2011 | 22117511 |
| serotype identification and vp1 coding sequence analysis of foot-and-mouth disease viruses from outbreaks in eastern and northern uganda in 2008/9. | in april 2008, foot-and-mouth disease (fmd) outbreaks were reported in kamuli district of the eastern region of uganda. soon after lifting the quarantines in this area, further fmd outbreaks were reported in northern uganda, which spread to more than 10 districts. the aim of this study was to identify the serotype and compare the variable protein (vp)1 coding sequences of the viruses responsible for fmd outbreaks during 2008 and 2009, to trace the transmission pathways of the disease in uganda. ... | 2011 | 22117844 |
| molecular characterization of amino acid deletion in vp1 (1d) protein and novel amino acid substitutions in 3d polymerase protein of foot and mouth disease virus subtype a/iran87. | the nucleotide sequence of the vp1 (1d) and partial 3d polymerase (3d(pol)) coding regions of the foot and mouth disease virus (fmdv) vaccine strain a/iran87, a highly passaged isolate (~150 passages), was determined and aligned with previously published fmdv serotype a sequences. overall analysis of the amino acid substitutions revealed that the partial 3d(pol) coding region contained four amino acid alterations. amino acid sequence comparison of the vp1 coding region of the field isolates reve ... | 2011 | 22122902 |
| Generation and genetic stability of tick-borne encephalitis virus mutants dependent on processing by FMDV 3C protease. | Mature capsid protein C of tick-borne encephalitis virus (TBEV) is cleaved from the polyprotein precursor by the viral NS2B/3 protease (NS2B/3pro). We showed previously that replacement of the NS2B/3pro cleavage site at the C-terminus of protein C by the foot-and-mouth disease virus (FMDV) 2A Stop/Go sequence leads to the production of infectious virions (Schrauf, S., Mandl, C.W., Bell-Sakyi, L. and Skern, T. 2009. J. Virol. 83: 11201-11210). Here, we show that infectious virions can also be pro ... | 2011 | 22131310 |
| inactivation of foot-and-mouth disease virus in various bovine tissues used for the production of natural sausage casings. | bovine intestines, bladders and oesophagus are used for the production of natural casings ("beef casings") as edible sausage containers. derived from cattle experimentally infected with fmdv (initial dosage 10(4) tcid(50)/ml, strain a iran 97), these beef casings were treated with sodium chloride (nacl) or phosphate supplemented salt (p-salt). in addition, different in-vitro experiments using beef casings were done on a small scale with other fmdv strains (a turkey 06, c-oberbayern and o(1) mani ... | 2011 | 22137684 |
| genetic characterization of vaccine and field strains of serotype a foot-and-mouth disease virus from india. | extreme antigenic and genetic heterogeneity of serotype a foot-and-mouth disease virus (fmdv) population has resulted in change of vaccine strains in india twice in the last decade. in such a situation, complete characterization of the vaccine strains is imperative. with regard to the frequent outbreaks of this disease, fmdv field strains are also of interest. therefore three vaccine strains and two field strains of type a fmdv from india were completely sequenced and the obtained sequences were ... | 2011 | 22149500 |
| Formation of higher-order FMDV 3Dpol complexes is dependent on elongation activity. | The replication of many viruses involves the formation of higher-order structures or replication 'factories'. We show that the key replication enzyme of foot-and-mouth disease virus (FMDV), the RNA-dependent-RNA polymerase, forms fibrils in vitro. Although there are similarities with previously characterised poliovirus polymerase fibrils, FMDV fibrils are narrower, composed of both protein and RNA and, importantly, are only seen when all components of an elongation assay are present. Furthermore ... | 2011 | 22156531 |
| fmd virus epitope dominance in the antibody response of vaccinated animals. | five neutralising antigenic sites have been identified on the surface of serotype o foot-and-mouth disease virus. a set of mab neutralisation escape mutant viruses were used for the first time to evaluate the relative use of known binding sites by polyclonal antibodies from three target species, cattle, sheep and pigs. antibodies to all the five neutralising antigenic sites were detected in all the three species, with most antibodies directed against antigenic site 2, followed by antigenic site ... | 2011 | 22158876 |
| the infectivity and pathogenicity of a foot-and-mouth disease virus persistent infection strain from oesophageal-pharyngeal fluid of a chinese cattle in 2010. | abstract: background: foot-and mouth disease (fmd) is an acute, febrile, and contagious vesicular disease affecting cloven-hoofed animals. some animals may become persistent infected carriers when they contact fmd virus (fmdv), and persistent infected animals are a dangerous factor to cause fmd outbreak. findings: 300 op (oesophageal-pharyngeal) fluid samples were collected from cattle without clinic symptom after one month fmd circulated in 2010 in china. a fmdv strain was isolated when a posi ... | 2011 | 22166050 |
| a rapid molecular strategy for early detection and characterization of vietnamese foot-and-mouth disease virus serotypes o, a, and asia 1. | a one-step rt-pcr method using newly designed primers vn-vp1f/vn-vp1r targeting the full vp1 capsid protein-coding gene, combined with direct sequencing of its pcr product, has been developed successfully for universal detection and characterization of vietnamese fmdv serotypes o, a, and asia 1 directly from clinical samples. the one-step rt-pcr amplified 821-bp dsdna products covering the entire vp1 gene of fmdv serotypes o, a, and asia 1. the obtained dsdna products were suitable for direct se ... | 2011 | 22172973 |
| an elisa based on the repeated foot-and-mouth disease virus 3b epitope peptide can distinguish infected and vaccinated cattle. | to develop a strategy of differentiating infected from vaccinated animals (diva) with foot-and-mouth disease virus (fmdv), a short (27aa) peptide containing three conserved linear b cell epitopes of the fmdv 3b nonstructural protein was designed. this novel bf peptide was synthesized using a gene splicing by overlap extension protocol with preferred codons for escherichia coli. the resultant eight tandem repeat multimer (1, 2, 4, 6, 8, 16, 24, and 32bf) were expressed as soluble fusion proteins ... | 2011 | 22207215 |
| detection and genetic characterization of foot-and-mouth disease viruses in samples from clinically healthy animals in endemic settings. | a total of 1501 oral swab samples from pakistan, afghanistan and tajikistan were collected from clinically healthy animals between july 2008 and august 2009 and assayed for the presence of foot-and-mouth disease virus (fmdv) rna. the oral swab samples from two (of four) live animal markets in pakistan (n = 245), one (of three) live animal market in afghanistan (n=61) and both the live animal markets in tajikistan (n=120) all tested negative. however, 2 of 129 (∼2%) samples from gondal and 11 of ... | 2011 | 22212855 |
| comparison of ires and f2a-based locus-specific multicistronic expression in stable mouse lines. | efficient and stoichiometric expression of genes concatenated by bi- or multi-cistronic vectors has become an invaluable tool not only in basic biology to track and visualize proteins in vivo, but also for vaccine development and in the clinics for gene therapy. to adequately compare, in vivo, the effectiveness of two of the currently popular co-expression strategies - the internal ribosome entry site (ires) derived from the picornavirus and the 2a peptide from the foot-and-mouth disease virus ( ... | 2011 | 22216134 |
| a survey on the frequency of foot-and-mouth disease virus carriers in cattle in north-east of iran by rt-pcr: implications for revising disease control strategy. | foot-and-mouth disease (fmd) is endemic in iran. it is essential to timely evaluate the current disease control programme in iran. here, we report the frequency of fmd virus (fmdv) carrier state in cattle slaughtered in mashhad abattoir, mashhad, khorasan razavi, north-east of iran, which contains long common borders with afghanistan and turkmenistan. soft palate samples were collected immediately after slaughter for the detection of fmdv by rt-pcr. the results show that 37.7% of cattle (96 of 2 ... | 2012 | 22222047 |
| virus survival in slurry: analysis of the stability of foot-and-mouth disease, classical swine fever, bovine viral diarrhoea and swine influenza viruses. | farm slurry can be highly contaminated with viral pathogens. the survival of these pathogens within slurry is important since this material is often distributed onto farm land either directly or after heat treatment. there is clearly some risk of spreading pathogens in the early stages of an outbreak of disease before it has been recognized. the survival of foot-and-mouth disease virus, classical swine fever virus, bovine viral diarrhoea virus and swine influenza virus, which belong to three dif ... | 2011 | 22226541 |
| early detection and visualization of human adenovirus serotype 5-viral vectors carrying foot-and-mouth disease virus or luciferase transgenes in cell lines and bovine tissues. | recombinant replication-defective human adenovirus type 5 (ad5) vaccines containing capsid-coding regions from foot-and-mouth disease virus (fmdv) have been demonstrated to induce effective immune responses and provide homologous protective immunity against fmdv in cattle. however, basic mechanisms of ad5-fmdv vaccine function including virus tropism, transgene expression, and antigen presentation, remain incompletely understood. the current study characterized the dynamics of ad5 viral vector ( ... | 2012 | 22227230 |
| 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 |
| serosurveillance for foot-and-mouth disease in mongolian gazelles (procapra gutturosa) and livestock on the eastern steppe of mongolia. | foot-and-mouth disease (fmd) is a highly contagious, viral disease that affects most ruminant and porcine species, and periodic outbreaks on mongolia's eastern steppe affect mongolian gazelles (procapra gutturosa) and livestock. during 2005-08, we collected sera from 36 and 57 calf and adult gazelles, respectively, and from adult domestic animals sympatric with the gazelles, including 138 sheep (ovis aries), 140 goats (capra aegagrus hircus), 139 bactrian camels (camelus bactrianus), and 138 cat ... | 2012 | 22247371 |
| immunogenicity of foot-and-mouth disease virus structural polyprotein p1 expressed in transgenic rice. | transgenic plants have become developed as bioreactors for producing heterologous proteins and may even form edible vaccines. in the present study, a transgenic rice expressing the capsid precursor polypeptide (p1) gene of foot-and-mouth disease virus (fmdv), under the control of a dual cauliflower mosaic virus (camv 35s) promoter, was generated by agrobacterium-mediated transformation. southern blot, northern blot, western blot, and elisa analyses confirmed that the p1 gene was integrated into ... | 2012 | 22274594 |
| immune response in goats to different payloads of fmdv monovalent vaccine: protection against virulent challenge and development of carrier status. | the relationship of foot-and-mouth disease virus antigen payload and number of dose of vaccine conferring protection against virus challenge in goats was studied. goats vaccinated with oil adjuvant foot-and-mouth disease vaccines containing different antigen payloads with or without booster resisted virulent challenge at 21 days post-vaccination or 7 days after booster respectively. however, localized sub-clinical infection was observed in two vaccinated goats on 35 days post-challenge. rna coul ... | 2011 | 22282634 |
| correlation between efficacy and structure of recombinant epitope vaccines against bovine type o foot and mouth disease virus. | to develop recombinant epitope vaccines against foot-and-mouth disease virus (fmdv), genes coding for six recombinant proteins (rp1–rp6) consisting of different combinations of b cell and t cell epitope from vp1 capsid protein (vp1) of type o fmdv were constructed and the 3d structure of these proteins analyzed. this revealed a surface-exposed rgd sequence of b cell epitopes in all six recombinant proteins as that in vp1 of fmdv and rp1, rp2 and rp4 globally mimicked the backbone conformation of ... | 2012 | 22286179 |
| bovine type iii interferon significantly delays and reduces the severity of foot-and-mouth disease in cattle. | interferons (ifns) are the first line of defense against viral infections. although type i and ii ifns have proven effective to inhibit foot-and-mouth disease virus (fmdv) replication in swine, a similar approach had only limited efficacy in cattle. recently, a new family of ifns, type iii ifn or ifn-λ, has been identified in human, mouse, chicken, and swine. we have identified bovine ifn-λ3 (boifn-λ3), also known as interleukin 28b (il-28b), and demonstrated that expression of this molecule usi ... | 2012 | 22301155 |
| promotion of viral internal ribosomal entry site-mediated translation under amino acid starvation. | cap-dependent and internal ribosomal entry site (ires)-mediated translation are regulated differently within cells. viral ires-mediated translation often remains active when cellular cap-dependent translation is severely impaired under cellular stresses induced by virus infection. to investigate how cellular stresses influence the efficiency of viral ires-mediated translation, we used a bicistronic luciferase reporter construct harbouring ires elements from the following viruses: encephalomyocar ... | 2012 | 22302880 |
| chimeric calicivirus-like particles elicit specific immune responses in pigs. | virus-like particles (vlps) have received considerable attention due to their potential application in veterinary vaccines and, in particular, vlps from rabbit haemorrhagic disease virus (rhdv) have successfully shown to be good platforms for inducing immune responses against an inserted foreign epitope in mice. the aim of this study was to assess the immunogenicity of chimeric rhdv-vlps as vaccine vectors in pigs. for this purpose, we have generated chimeric vlps containing a well-known t epito ... | 2012 | 22306796 |
| bacterial toxin fusion proteins elicit mucosal immunity against a foot-and-mouth disease virus antigen when administered intranasally to guinea pigs. | peptides corresponding to the foot-and-mouth disease virus vp1 g-h loop are capable of inducing neutralizing antibodies in some species but are considered relatively poor immunogens, especially at mucosal surfaces. however, intranasal administration of antigens along with the appropriate delivery vehicle/adjuvant has been shown to induce mucosal immune responses, and bacterial enterotoxins have long been known to be effective in this regard. in the current study, two different carrier/adjuvant a ... | 2011 | 22312350 |
| xenoepitope substitution avoids deceptive imprinting and broadens the immune response to foot-and-mouth disease virus. | many rna viruses encode error-prone polymerases which introduce mutations into b and t cell epitopes, providing a mechanism for immunological escape. when regions of hypervariability are found within immunodominant epitopes with no known function, they are referred to as "decoy epitopes," which often deceptively imprint the host's immune response. in this work, a decoy epitope was identified in the foot-and-mouth disease virus (fmdv) serotype o vp1 g-h loop after multiple sequence alignment of 1 ... | 2012 | 22323558 |
| adenovirus-vectored shrnas targeted to the highly conserved regions of vp1 and 2b in tandem inhibits replication of foot-and-mouth disease virus both in vitro and in vivo. | foot-and-mouth disease is a highly contagious and economically important disease of cloven-hoofed animals. rna interference (rnai) can be used as a rapid and specific antiviral approach. it was shown that treatment with recombinant adenovirus (ad(vp1-2b)) carrying shrnas targeted to the vp1 and 2b genes of fmdv expressed in tandem had marked antiviral effects against fmdv both in ibrs-2 cells and guinea pigs. treatment with ad(vp1-2b) both before and after fmdv infection was most effective in ib ... | 2012 | 22327142 |
| a dna vaccination regime including protein boost and electroporation protects cattle against foot-and-mouth disease. | protection against foot-and-mouth disease (fmd) using dna technology has been documented for sheep and pigs but not for the highly susceptible species of cattle. twenty-five holstein friesian cross-bred cattle were vaccinated twice, 21 days apart, with a dna vaccine containing the capsid coding region (p1) along with the non-structural proteins 2a, 3c and 3d (pcdna3.1/p1-2a3c3d) of o(1) kaufbeuren alone or coated onto plg (d,l-lactide-co-glycolide) microparticles. in some pcdna3.1/p1-2a3c3d was ... | 2012 | 22330893 |
| direct contact transmission of three different foot-and-mouth disease virus strains in swine demonstrates important strain-specific differences. | a novel direct contact transmission model for the study of foot-and-mouth disease virus (fmdv) infection of swine was utilized to investigate transmission characteristics of three fmdv strains belonging to serotypes a, o and asia1. each strain demonstrated distinct transmission characteristics and required different exposure times to achieve successful contact transmission. while a 4h exposure was sufficient for strain a24 cruzeiro (a24cru), both o1 manisa and asia1 shamir transmission required ... | 2012 | 22342891 |
| genotypic and phenotypic changes of bhk-21 cells grown in suspension cultures. | the propagation of foot-and-mouth disease virus on bhk-21 suspension cells, although economically convenient, may yield a scarcely immunizing antigen. helpful insights were obtained by investigating a few genotypic and phenotypic features of the cell cultures. the appearance of polyploid populations, higher cell concentrations at the end of culturing, the progressive reduction of spreading on surfaces and an abnormal expression of the α5β1 integrin were found to be correlated with the number of ... | 1993 | 22358669 |
| strong buffering capacity of insect cells. implications for the baculovirus expression system. | insect cells are widely used for expression of a variety of different proteins by using the baculovirus expression system. the applicability of this system depends on production of proteins which have biological properties similar to their native counterparts. one application has been the expression of viral capsid proteins and their assembly into empty capsid structures to provide new viral immunogens which retain complex antigenic sites. an important parameter for efficient folding and assembl ... | 1995 | 22359206 |
| gemin5 proteolysis reveals a novel motif to identify l protease targets. | translation of picornavirus rna is governed by the internal ribosome entry site (ires) element, directing the synthesis of a single polyprotein. processing of the polyprotein is performed by viral proteases that also recognize as substrates host factors. among these substrates are translation initiation factors and rna-binding proteins whose cleavage is responsible for inactivation of cellular gene expression. foot-and-mouth disease virus (fmdv) encodes two proteases, l(pro) and 3c(pro). widespr ... | 2012 | 22362733 |
| modelling the influence of foot-and-mouth disease vaccine antigen stability and dose on the bovine immune response. | foot and mouth disease virus causes a livestock disease of significant global socio-economic importance. advances in its control and eradication depend critically on improvements in vaccine efficacy, which can be best achieved by better understanding the complex within-host immunodynamic response to inoculation. we present a detailed and empirically parametrised dynamical mathematical model of the hypothesised immune response in cattle, and explore its behaviour with reference to a variety of ex ... | 2012 | 22363437 |
| southeast asian foot-and-mouth disease viruses in eastern asia. | foot-and-mouth disease (fmd) outbreaks recently affected 2 countries (japan and south korea) in eastern asia that were free of fmd without vaccination. analysis of viral protein 1 nucleotide sequences indicated that fmd serotype a and o viruses that caused these outbreaks originated in mainland southeast asia to which these viruses are endemic. | 2012 | 22377196 |
| application of the ceditest® fmdv type o and fmdv-ns enzyme-linked immunosorbent assays for detection of antibodies against foot-and-mouth disease virus in selected livestock and wildlife species in uganda. | diagnosis and control of foot-and-mouth disease virus (fmdv) requires rapid and sensitive diagnostic tests. two antibody enzyme-linked immunosorbent assay (elisa) kits, ceditest® fmdv-ns for the detection of antibodies against the nonstructural proteins of all fmdv serotypes and ceditest® fmdv type o for the detection of antibodies against serotype o, were evaluated under african endemic conditions where the presence of multiple serotypes and the use of nonpurified vaccines complicate serologica ... | 2012 | 22379044 |
| acute bovine viral diarrhea associated with extensive mucosal lesions, high morbidity, and mortality in a commercial feedlot. | in 2008, a northwest texas feedlot underwent an outbreak of bovine viral diarrhea virus (bvdv) causing high morbidity and mortality involving 2 lots of calves (lots a and b). severe mucosal surface lesions were observed grossly in the oral cavity, larynx, and esophagus. mucosal lesions varied from small (1-3 mm) infrequent mucosal ulcerations to large (5 mm to 1 cm) and coalescing ulcerations. necrotic debris was present in ulcerations of some mortalities with some having plaque-like debris, but ... | 2012 | 22379057 |
| an alternate delivery system improves vaccine performance against foot-and-mouth disease virus (fmdv). | foot-and-mouth disease virus (fmdv) causes vesicular disease of cloven-hoofed animals with severe agricultural and economic implications. one of the most highly infectious and contagious livestock pathogens known, the disease spreads rapidly in naïve populations making it critical to have rapidly acting vaccines. needle inoculation of killed virus vaccine is an efficient method of swiftly vaccinating large numbers of animals, either in eradication efforts or in outbreak situations in disease fre ... | 2012 | 22387223 |
| foot-and-mouth disease virus causes a decrease in spleen dendritic cells and the early release of ifn-α in the plasma of mice. differences between infectious and inactivated virus. | foot-and-mouth disease (fmd) is a highly contagious and acute viral disease of cloven-hoofed animals. from an economical point of view, it is the most important disease of livestock worldwide. it is known that the virus interacts with dendritic cells, both in the natural host and in mice, but the impact of this interaction on the adaptive immune response is controversial. currently available vaccines are based on inactivated forms of the fmd virus. little is known about the differences between i ... | 2012 | 22387627 |
| recombinant viral capsid protein vp1 suppresses migration and invasion of human cervical cancer by modulating phosphorylated prohibitin in lipid rafts. | recombinant capsid protein vp1 (rvp1) of foot-and-mouth disease virus inhibits invasion/metastasis of cancer cells. here we studied its mechanism of action on human cervical cancer cells. the inhibition of cell invasion by rvp1 was accompanied with reduction in phosphatidylinositol (3,4,5)-triphosphate (pip3), phospho-akt s473, phosphorylated prohibitin (phospho-phb) t258 in lipid rafts, dissociation of phospho-phb t258 with raf-1 and the inactivation of raf-1/erk. addition of pip3 or overexpres ... | 2012 | 22388104 |
| molecular epidemiology of foot-and-mouth disease virus type a in south america. | a databank of 78 vp(1) complete sequences of type a foot-and-mouth disease virus (fmdv) from south american isolates was constructed. forty-nine samples corresponded to fmdv that circulated between the years 1999-2008, mainly in venezuela, where most type a outbreaks have occurred lately and twenty-nine to strains historically relevant for the continent. the phylogenetic analysis showed that all south american fmdv belonged to the euro-sa topotype. sixteen subgenotypes could be identified, based ... | 2012 | 22397938 |
| inclusion of a specific t cell epitope increases the protection conferred against foot-and-mouth disease virus in pigs by a linear peptide containing an immunodominant b cell site. | foot-and-mouth disease virus (fmdv) causes an economically important and highly contagious disease of cloven-hoofed animals. fmd control in endemic regions is implemented using chemically inactivated whole-virus vaccines. currently, efforts are directed to the development of safe and marked vaccines. we have previously reported solid protection against fmdv conferred by branched structures (dendrimeric peptides) harbouring virus-specific b and t-cell epitopes. in order to gain insights into the ... | 2012 | 22416886 |
| structure, assembly, and dna packaging of the bacteriophage t4 head. | the bacteriophage t4 head is an elongated icosahedron packed with 172 kb of linear double-stranded dna and numerous proteins. the capsid is built from three essential proteins: gp23*, which forms the hexagonal capsid lattice; gp24*, which forms pentamers at 11 of the 12 vertices; and gp20, which forms the unique dodecameric portal vertex through which dna enters during packaging and exits during infection. intensive work over more than half a century has led to a deep understanding of the phage ... | 2012 | 22420853 |
| quantitative trait loci associated with the immune response to a bovine respiratory syncytial virus vaccine. | infectious disease is an important problem for animal breeders, farmers and governments worldwide. one approach to reducing disease is to breed for resistance. this linkage study used a charolais-holstein f2 cattle cross population (n = 501) which was genotyped for 165 microsatellite markers (covering all autosomes) to search for associations with phenotypes for bovine respiratory syncytial virus (brsv) specific total-igg, igg1 and igg2 concentrations at several time-points pre- and post-brsv va ... | 2012 | 22438944 |
| mutagenesis-mediated virus extinction: virus-dependent effect of viral load on sensitivity to lethal defection. | lethal mutagenesis is a transition towards virus extinction mediated by enhanced mutation rates during viral genome replication, and it is currently under investigation as a potential new antiviral strategy. viral load and virus fitness are known to influence virus extinction. here we examine the effect or the multiplicity of infection (moi) on progeny production of several rna viruses under enhanced mutagenesis. | 2012 | 22442668 |
| emergence of antigenic variants with in serotype a foot and mouth disease virus in india and evaluation of a new vaccine candidate panel. | emergence of genetically and antigenically divergent lineages/genotypes and poor intergenotypic antigenic coverage is a major concern in serotype a foot-and-mouth-disease virus (fmdv) in india. in 2009, to cover antigenic diversity emerged in serotype a virus field isolates, ind40/2000 was selected as the new vaccine strain for incorporation in the trivalent fmd vaccine formulation used in india. although current vaccine strain (ind40/2000) covers most isolates antigenically, a few vp3(59)-delet ... | 2012 | 22445197 |
| [construction and functional characterization of a monocistronic replicon based on the hcv genotype 2a promotor]. | to construct a hepatitis c virus (hcv) genotype 2a monocistronic replicon and investigate its replication capabilities in the human hepatocarcinoma cell lines, huh7.5 and huh7.1, in order to determine its potential as a molecular tool for future in vitro studies of hcv replication and selection studies for putative anti-hcv drugs. site-directed mutagenesis was used to delete the core-e1-e2-p7-ns2 fragment (about 3090 bp) from plasmid pj6jfh1blarl. the resultant trianglepj6jfh1blarl plasmid was d ... | 2012 | 22464780 |
| evolutionary trend of foot-and-mouth disease virus in hong kong. | foot-and-mouth disease is an endemic animal disease in hong kong. in this study, a total of 70 clinical specimens were collected from locally infected pigs from 2001 to 2010. phylogenetic analysis of vp1 sequences reveal that all hong kong fmdv serotype o isolates are classified into three lineages: hk-a and hk-b in cathay topotype, and hk-c in sea topotype. regression analysis projects that the time of divergence from the most recent common ancestor of hk-a and hk-b are 1964 ± 12 and 1987 ± 9 y ... | 2012 | 22472703 |
| upconversion nanoparticles modified with aminosilanes as carriers of dna vaccine for foot-and-mouth disease. | the potential of the upconversion nanoparticles nayf(4):yb/er@silica(ucps)/plasmid dna (pcdna3.1/vp1-gfp) complex in inducing immune responses was evaluated using the ucps as carriers of the foot-and-mouth disease virus (fmdv asiai/jiangsu2005) dna vaccine. the ucps protection against dnasei degradation was measured using an in vitro inhibition assay. the expression of the plasmid in vivo was determined via confocal microscopy. its biocompatibility was evaluated through cytotoxicity assay. based ... | 2012 | 22476264 |
| [construction of a full-length infectious cdna clone of inter-genotypic chimeric foot-and-mouth disease virus]. | a series of type o foot-and-mouth disease (fmd) outbreaks occurred in china seriously affect development of chinese husbandry. its causative agent-type o foot-and-mouth disease virus (fmdv) has been evolved three topotypes: cathay, middle east-south asia and southeast asia, specifically, the viruses of cathay topotype are highly adapted to pig, representing the biggest threat on chinese pig industry. the available fmd vaccine in china provides insufficient protection against some arising viruses ... | 2012 | 22489468 |
| experimental infection of wild boar and domestic pigs with a foot and mouth disease virus strain detected in the southeast of bulgaria in december of 2010. | foot and mouth disease (fmd) was detected in a wild boar in southeastern bulgaria in december 2010. the occurrence and spread of the disease in wild cloven-hoofed animals may pose an unexpected and significant threat to fmd virus (fmdv)-free areas within and outside the european union. so far, only one well documented experimental infection with fmd in wild boar has been published. in order to obtain more epidemiologically relevant data regarding the disease in wild boar we conducted an experime ... | 2012 | 22503391 |
| insertion of type o-conserved neutralizing epitope into the foot-and-mouth disease virus type asia1 vp1 g-h loop: effect on viral replication and neutralization phenotype. | previously, we finely mapped the neutralizing epitopes recognized by foot-and-mouth disease virus (fmdv) type asia1-specific mab 3e11 and fmdv type o-specific mab 8e8. in this study, we engineered recombinant fmdvs of the serotype asia1 (rfmdvs) displaying the type o-neutralizing epitope recognized by the mab 8e8. these epitope-inserted viruses were genetically stable and exhibited growth properties that were similar to those of their parental virus. importantly, the recombinant virus rfmdv-c sh ... | 2012 | 22513388 |
| experimental foot-and-mouth disease virus infection in white tailed deer. | white tailed deer (odocoileus virginianus) were inoculated with foot-and-mouth disease virus (fmdv) o ukg 11/2001 and monitored for the development of clinical signs, histopathological changes and levels of virus replication. all fmdv-infected deer developed clinical signs starting at 2 days post inoculation and characterized by an increase in body temperature, increased salivation and lesions in the mouth and on the feet. virus spread to various tissues was determined by quantifying the amount ... | 2012 | 22520809 |
| coordinate lentiviral expression of cre recombinase and rfp/egfp mediated by fmdv 2a and analysis of cre activity. | the site-specific recombination mediated by cre recombinase has been utilized extensively in genetic engineering and gene function studies. efficient delivery of a cre enzyme with enzymatic activity and the ability to monitor the enzyme expression are required in applications, and lentiviral constructs with a fluorescent protein (fp) to report the cre expression are suitable for most studies. however, the current lentiviral vector systems have some deficiencies in precise reporting the cre expre ... | 2012 | 22532014 |
| [erratum: the following article was subsequently withdrawn by the authors. yarim gf, ciftci g (2011): investigation of serum protein profiles in sheep naturally infected with foot-and-mouth disease virus berl munch tierarztl wochenschr (5/6):194-197]. | 2012 | 22550766 | |
| evaluation of the solid phase competition elisa for detecting antibodies against the six foot-and-mouth disease virus non-o serotypes. | the solid-phase competition elisa (spce) has been evaluated in both screening and titration assay formats for detecting antibodies against foot-and-mouth disease virus (fmdv) for the six non-o serotypes a, c, sat 1, sat 2, sat 3 and asia 1. cut-off values were determined as a percentage inhibition of 40 for the sat serotypes and 50 for serotypes a, c and asia 1, which gave rise to specificity values ranging from 99.41% to 99.9% for the different serotypes. the relative sensitivity between the sp ... | 2012 | 22561986 |
| evaluation of a genetically modified foot-and-mouth disease virus vaccine candidate generated by reverse genetics. | foot-and-mouth disease (fmd) is the most economically important and highly contagious disease of cloven-hoofed animals worldwide. control of the disease has been mainly based on large-scale vaccinations with whole-virus inactivated vaccines. in recent years, a series of outbreaks of type o fmd occurred in china (including chinese taipei, chinese hong kong) posed a tremendous threat to chinese animal husbandry. its causative agent, type o fmdv, has evolved into three topotypes (east-south asia (m ... | 2012 | 22591597 |
| mechanism of nucleic acid unwinding by sars-cov helicase. | the non-structural protein 13 (nsp13) of severe acute respiratory syndrome coronavirus (sars-cov) is a helicase that separates double-stranded rna (dsrna) or dna (dsdna) with a 5' → 3' polarity, using the energy of nucleotide hydrolysis. we determined the minimal mechanism of helicase function by nsp13. we showed a clear unwinding lag with increasing length of the double-stranded region of the nucleic acid, suggesting the presence of intermediates in the unwinding process. to elucidate the natur ... | 2012 | 22615777 |
| capsid coding sequences of foot-and-mouth disease viruses are determinants of pathogenicity in pigs. | the surface exposed capsid proteins, vp1, vp2 and vp3, of foot-and-mouth disease virus (fmdv) determine its antigenicity and the ability of the virus to interact with host-cell receptors. hence, modification of these structural proteins may alter the properties of the virus.in the present study we compared the pathogenicity of different fmdvs in young pigs. in total 32 pigs, 7-weeks-old, were exposed to virus, either by direct inoculation or through contact with inoculated pigs, using cell cultu ... | 2012 | 22624592 |
| diagnosis and control measures of the 2010 outbreak of foot-and-mouth disease a type in the republic of korea. | in january 2010, foot-and-mouth disease (fmd) occurred for the first time in 8 years in korea. the outbreaks were because of a serotype, different from the o type, which had occurred previously in 2000 and 2002. the fmd outbreaks were identified in seven farms, consisting of six cattle farms where viruses were detected and one deer farm where only fmdv antibody was detected. the seven farms were within 9.3 km of each other. all susceptible animals within 10 km radius of the outbreak farms were p ... | 2013 | 22630568 |
| modelling the within-host dynamics of the foot-and-mouth disease virus in cattle. | in this paper we investigate the within-host dynamics of the foot-and-mouth disease virus (fmdv) in cattle using previously published data for 8 experimentally infected cows. an 8-compartment, 14-parameter differential equation model was fitted to data collected from each cow every 24 h over the course of an infection on: (i) the concentration of fmdv genomes in the blood, (ii) the concentration of infectious virus in the blood, (iii) antibody levels, and (iv) interferon levels. model parameters ... | 2012 | 22664068 |
| investigation of foot and mouth disease hotspots in northern lao pdr. | foot and mouth disease (fmd) is an endemic transboundary disease in the mekong region, and fmd records of reports to animal health authorities in lao pdr between 2009 and 2011 were reviewed. fmd outbreaks occurred in 2 of 3 years in eight districts in three of the eight northern lao pdr provinces, locations suggested as fmd 'hotspots'. the relatively higher risk of recurrence of fmd in these districts was likely due to the presence of a dense large ruminant population, extensive animal trading i ... | 2013 | 22690839 |
| mapping of antigenic determinants on a sat2 foot-and-mouth disease virus using chicken single-chain antibody fragments. | recombinant single-chain variable fragments (scfvs) of antibodies make it possible to localize antigenic and immunogenic determinants, identify protective epitopes and can be exploited for the design of improved diagnostic tests and vaccines. a neutralizing epitope, as well as other potential antigenic sites of a sat2 foot-and-mouth disease virus (fmdv) were identified using phage-displayed scfvs. three unique zim/7/83-specific scfvs, designated scfv1, scfv2 and scfv3, were isolated. further cha ... | 2012 | 22698877 |
| sindbis virus replicase-based dna vaccine construct encoding fmdv-specific multivalent epitope gene: studies on its immune responses in guinea pigs. | foot-and-mouth disease (fmd) is still a perennial global menace affecting livestock health and production. it is imperative to figure out new ways to curb this disease. in this study, a sindbis virus replicase-based dna vaccine, psincmv-vac-meg990, encoding a multivalent epitope gene (representing tandemly linked vp1 c-terminal halves of three foot-and-mouth disease virus (fmdv) serotypes) was constructed. in vitro transfection studies in bhk-21 cells revealed that the construct was able to expr ... | 2012 | 22702835 |
| field outbreak strains of serotype o foot-and-mouth disease virus from india with a deletion in the immunodominant βg-βh loop of the vp1 protein. | foot-and-mouth disease virus serotype o accounts for around 80 % of the outbreaks in india. although indian serotype o isolates belongs to the me-sa topotype, circulation of different lineages has been noted. after its emergence in the year 2001, the 'ind2001' lineage outcompeted the panasia lineage in causing serotype o outbreaks in the year 2009. three isolates had an amino acid deletion at position 139 in the vp1 coding region and grouped with the 'ind2001' lineage. the currently used indian ... | 2012 | 22707045 |
| foot-and-mouth disease virus 3c protease cleaves nemo to impair innate immune signaling. | foot-and-mouth disease is a highly contagious viral illness of wild and domestic cloven-hoofed animals. the causative agent, foot-and-mouth disease virus (fmdv), replicates rapidly, efficiently disseminating within the infected host and being passed on to susceptible animals via direct contact or the aerosol route. to survive in the host, fmdv has evolved to block the host interferon (ifn) response. previously, we and others demonstrated that the leader proteinase (l(pro)) of fmdv is an ifn anta ... | 2012 | 22718831 |
| expression of vp1 protein of serotype a and o of foot-and-mouth disease virus in transgenic sunnhemp plants and its immunogenicity for guinea pigs. | recently, transgenic plants expressing immunogenic proteins of foot-and-mouth disease virus (fmdv) have been used as oral or parenteral vaccines against foot-and-mouth disease (fmd). they exhibit advantages like cost effectiveness, absence of processing, thermostability, and easy oral application. fmdv vp1 protein of single serotype has been mostly used as immunogen. here we report the development of a bivalent vaccine with tandem-linked vp1 proteins of two serotypes, a and o, present in transge ... | 2012 | 22720698 |
| a dna vaccine encoding the fmdv capsid precursor polypeptide p1 and the enhancing effect of bovine herpesvirus 1 vp22 protein as molecular adjuvant. | dna vaccines containing the capsid precursor polypeptide p1 gene of foot-and-mouth disease virus (fmdv) alone or combined with the vp22 gene of bovine herpesvirus 1 (bvp22) as molecular adjuvant were constructed and used for immunization of balb/c mice. the latter were challenged with fmdv and their humoral as well as cell-mediated immune responses and virus clearance capacity were assayed. both dna vaccines elicited specific immune responses, however, the dna vaccine with the bvp22 adjuvant sho ... | 2012 | 22720700 |
| gegenees: fragmented alignment of multiple genomes for determining phylogenomic distances and genetic signatures unique for specified target groups. | the rapid development of next generation sequencing technologies leads to the accumulation of huge amounts of sequencing data. the scientific community faces an enormous challenge in how to deal with this explosion. here we present a software tool, 'gegenees', that uses a fragmented alignment approach to facilitate the comparative analysis of hundreds of microbial genomes. the genomes are fragmented and compared, all against all, by a multithreaded blast control engine. ready-made alignments can ... | 2012 | 22723939 |
| ns2b/3 proteolysis at the c-prm junction of the tick-borne encephalitis virus polyprotein is highly membrane dependent. | the replication of tick-borne encephalitis virus (tbev), like that of all flaviviruses, is absolutely dependent on proteolytic processing. production of the mature proteins c and prm from their common precursor requires the activity of the viral ns2b/3 protease (ns2b/3(pro)) at the c-terminus of protein c and the host signal peptidase i (spasei) at the n-terminus of protein prm. recently, we have shown in cell culture that the cleavage of protein c and the subsequent production of tbev particles ... | 2012 | 22727684 |
| bola-drb3 gene polymorphism and fmd resistance or susceptibility in wanbei cattle. | for the further characterization of foot-and-mouth disease virus (fmdv)-induced foot-and-mouth disease, we investigated the association between polymorphism of bola-drb3 gene and fmd resistance/susceptibility of wanbei cattle challenged with fmdv. one hundred cattle were challenged with fmdv and exon 2 of bola-drb3 genes was amplified by hemi-nested polymerase chain reaction from asymptomatic animals and from animals with fmd. pcr products were characterized by the rflp technique using restricti ... | 2012 | 22744423 |
| increased plasma cardiac troponin i concentration in lambs with myocarditis. | cardiac troponin i (ctni) is a blood biomarker of myocardial injury. a human ctni assay may be useful for measuring ctni concentrations in lambs with naturally occurring myocarditis. | 2012 | 22747688 |
| the integration of molecular tools into veterinary and spatial epidemiology. | at the interface of molecular biology and epidemiology, the emerging discipline of molecular epidemiology offers unique opportunities to advance the study of diseases through the investigation of infectious agents at the molecular level. molecular tools can increase our understanding of the factors that shape the spatial and temporal distribution of pathogens and disease. both spatial and molecular aspects have always been important to the field of infectious disease epidemiology, but recently n ... | 2011 | 22748175 |
| connecting network properties of rapidly disseminating epizoonotics. | to effectively control the geographical dissemination of infectious diseases, their properties need to be determined. to test that rapid microbial dispersal requires not only susceptible hosts but also a pre-existing, connecting network, we explored constructs meant to reveal the network properties associated with disease spread, which included the road structure. | 2012 | 22761900 |
| mutagenesis-mediated decrease of pathogenicity as a feature of the mutant spectrum of a viral population. | rna virus populations are heterogeneous ensembles of closely related genomes termed quasispecies. this highly complex distribution of variants confers important properties to rna viruses and influences their pathogenic behavior. it has been hypothesized that increased mutagenesis of viral populations, by treatment with mutagenic agents, can induce alterations in the pathogenic potential of a virus population. in this work we investigate whether mutagenized foot-and-mouth disease virus (fmdv) pop ... | 2012 | 22761933 |
| improved neutralising antibody response against foot-and-mouth-disease virus in mice inoculated with a multi-epitope peptide vaccine using polyinosinic and poly-cytidylic acid as an adjuvant. | a peptide-based vaccine for foot-and-mouth disease (fmd) was designed. the peptide immunogen had a g-h loop domain optimised for immunogenicity and broad-spectrum antigenicity to different lineages of serotype-o fmd viruses (fmdvs). polyinosinic and poly-cytidylic acid [poly (i:c)] was used as the adjuvant to overcome the low humoral antibody levels often observed in association with peptide-based vaccines. the multi-epitope peptide alone induced the secretion of a certain level of neutralising ... | 2012 | 22766183 |
| acquiring transgenic tobacco plants with insect resistance and glyphosate tolerance by fusion gene transformation. | the advantages of gene 'stacking' or 'pyramiding' are obvious in genetically modified (gm) crops, and several different multi-transgene-stacking methods are available. using linker peptides for multiple gene transformation is considered to be a good method to meet a variety of needs. in our experiment, the bt cry1ah gene, which encodes the insect-resistance protein, and the mg ( 2 ) -epsps gene, which encodes the glyphosate-tolerance protein, were connected by a 2a or lp4/2a linker. linker 2a is ... | 2012 | 22777591 |
| mutations that hamper dimerization of foot-and-mouth disease virus 3a protein are detrimental for infectivity. | foot-and-mouth disease virus (fmdv) nonstructural protein 3a plays important roles in virus replication, virulence, and host range. in other picornaviruses, homodimerization of 3a has been shown to be relevant for its biological activity. in this work, fmdv 3a homodimerization was evidenced by an in situ protein fluorescent ligation assay. a molecular model of the fmdv 3a protein, derived from the nuclear magnetic resonance (nmr) structure of the poliovirus 3a protein, predicted a hydrophobic in ... | 2012 | 22787230 |
| double candida antarctica lipase b co-display on pichia pastoris cell surface based on a self-processing foot-and-mouth disease virus 2a peptide. | to develop a high efficiency candida antarctica lipase b (calb) yeast display system, we linked two calb genes fused with sacchromyces cerevisiae cell wall protein genes, the sed1 and the 3'-terminal half of sag1, separately by a 2a peptide of foot-and-mouth disease virus (fmdv) in a single open reading frame. the calb copy number of recombinant strain kcse2acsa that harbored the orf was identified, and the quantity of calb displayed on the cell surface and the enzyme activity of the strain were ... | 2012 | 22797600 |
| synergistic effects of 2a-mediated polyproteins on the production of lignocellulose degradation enzymes in tobacco plants. | cost-effective bioethanol production requires a supply of various low-cost enzymes that can hydrolyse lignocellulosic materials consisting of multiple polymers. because plant-based enzyme expression systems offer low-cost and large-scale production, this study simultaneously expressed β-glucosidase (bglb), xylanase (xylii), exoglucanase (e3), and endoglucanase (cel5a) in tobacco plants, which were individually fused with chloroplast-targeting transit peptides and linked via the 2a self-cleaving ... | 2012 | 22798663 |
| characterization of epitope-tagged foot-and-mouth disease virus. | foot-and-mouth disease (fmd) is a highly contagious and economically devastating disease of cloven-hoofed animals with an almost-worldwide distribution. conventional fmd vaccines consisting of chemically inactivated viruses have aided in the eradication of fmd from europe and remain the main tool for control in endemic countries. although significant steps have been made to improve the quality of vaccines, such as improved methods of antigen concentration and purification, manufacturing processe ... | 2012 | 22815275 |
| exploring ires region accessibility by interference of foot-and-mouth disease virus infectivity. | translation initiation of picornavirus rna is driven by an internal ribosome entry site (ires) element located upstream of the initiator codon. rna structure organization as well as rna-protein interaction plays a fundamental role in internal initiation. ires activity has been mainly analyzed in the context of reporter genes, lacking regions of the viral genome potentially affecting translation efficiency. with the aim to understand the vulnerability of the ires and translation start region to s ... | 2012 | 22815996 |
| characteristics of serology-based vaccine potency models for foot-and-mouth disease virus. | foot-and-mouth disease (fmd) vaccine potency testing involves hundreds of animals each year. despite considerable efforts during the past decades, a challenge-free alternative vaccine potency test to replace the european protective dose 50% test (pd(50)) has not been implemented yet. the aim of the present study was to further characterize the properties of serological vaccine potency models. | 2012 | 22824343 |
| genome sequences of sat 2 foot-and-mouth disease viruses from egypt and palestinian autonomous territories (gaza strip). | two foot-and-mouth disease virus (fmdv) genome sequences have been determined for isolates collected from recent field outbreaks in north africa (egypt) and the middle east (palestinian autonomous territories). these data represent the first examples of complete genomic sequences for the fmdv sat 2 topotype vii, which is thought to be endemic in countries immediately to the south of the sahara desert. further studies are now urgently required to provide insights into the epidemiological links be ... | 2012 | 22843860 |
| foot-and-mouth disease virus serotype o phylodynamics: genetic variability associated with epidemiological factors in pakistan. | one of the most challenging aspects of foot-and-mouth disease (fmd) control is the high genetic variability of the fmd virus (fmdv). in endemic settings such as the indian subcontinent, this variability has resulted in the emergence of pandemic strains that have spread widely and caused devastating outbreaks in disease-free areas. in countries trying to control and eradicate fmd using vaccination strategies, the constantly evolving and wide diversity of field fmdv strains is an obstacle for iden ... | 2013 | 22846206 |
| expression and stability of foreign epitopes introduced into 3a nonstructural protein of foot-and-mouth disease virus. | foot-and-mouth disease virus (fmdv) is an aphthovirus that belongs to the picornaviridae family and causes one of the most important animal diseases worldwide. the capacity of other picornaviruses to express foreign antigens has been extensively reported, however, little is known about fmdv. to explore the potential of fmdv as a viral vector, an 11-amino-acid (aa) hsv epitope and an 8 aa flag epitope were introduced into the c-terminal different regions of 3a protein of fmdv full-length infectio ... | 2012 | 22848509 |
| modulation of foot-and-mouth disease virus ph threshold for uncoating correlates with differential sensitivity to inhibition of cellular rab gtpases and decreases infectivity in vivo. | the role of cellular rab gtpases that govern traffic between different endosome populations was analysed on foot-and-mouth disease virus (fmdv) infection. changes of viral receptor specificity did not alter rab5 requirement for infection. however, a correlation between uncoating ph and requirement of rab5 for infection was observed. a mutant fmdv with less acidic uncoating ph threshold was less sensitive to inhibition of rab5, whereas another mutant with more acidic requirements was more sensiti ... | 2012 | 22875255 |
| the effect of uniform capture molecule orientation on biosensor sensitivity: dependence on analyte properties. | uniform orientation of capture molecules on biosensors has been reported to increase sensitivity. here it is investigated which analyte properties contribute to sensitivity by orientation. orientation of capture molecules on biosensors was investigated using variable domains of llama heavy-chain antibodies (vhhs) as capture molecule, and a surface plasmon resonance (spr) chip as biosensor. two vhhs were tested in this study: one recognizing foot-and-mouth disease virus (fmdv) and another recogni ... | 2013 | 22878083 |
| human adenovirus-vectored foot-and-mouth disease vaccines: establishment of a vaccine product profile through in vitro testing. | next generation, foot-and-mouth disease (fmd) molecular vaccines based on replication deficient human adenovirus serotype 5 viral vectored delivery of fmd capsid genes (adfmd) are being developed by the united states dept. of homeland security and industry partners. the strategic goal of this program is to develop adfmd licensed vaccines for the usa national veterinary stockpile for use, if needed, as emergency response tools during an fmd outbreak. this vaccine platform provides a unique opport ... | 2012 | 22888605 |
| identification of short hairpin rna targeting foot-and-mouth disease virus with transgenic bovine fetal epithelium cells. | although it is known that rna interference (rnai) targeting viral genes protects experimental animals, such as mice, from the challenge of foot-and-mouth disease virus (fmdv), it has not been previously investigated whether shrnas targeting fmdv in transgenic dairy cattle or primary transgenic bovine epithelium cells will confer resistance against fmdv challenge. | 2012 | 22905125 |
| a safe foot-and-mouth disease vaccine platform with two negative markers for differentiating infected from vaccinated animals. | vaccination of domestic animals with chemically inactivated foot-and-mouth disease virus (fmdv) is widely practiced to control fmd. currently, fmd vaccine manufacturing requires the growth of large volumes of virulent fmdv in biocontainment-level facilities. here, two marker fmdv vaccine candidates (a(24)ll3d(yr) and a(24)ll3b(pvkv)3d(yr)) featuring the deletion of the leader coding region (l(pro)) and one of the 3b proteins were constructed and evaluated. these vaccine candidates also contain e ... | 2012 | 22915802 |
| [early steps of picornavirus infection]. | picornaviridae is a large family of viruses that cause a variety of infectious diseases in humans and animals. it includes important viruses such as poliovirus, hepatisis a virus and foot and mouth disease virus. early steps of infection play important roles in determining the host range and the target organs for each virus. here, i review the recent advances in the studies of cellular receptors for picornaviruses, mechanisms of cell entry and viral uncoating. | 2011 | 22916565 |
| novel antiviral therapeutics to control foot-and-mouth disease. | foot-and-mouth disease virus (fmdv) causes a highly contagious disease of cloven-hoofed animals. vaccines require ∼7 days to induce protection; thus, before this time, vaccinated animals are still susceptible to the disease. our group has previously shown that swine inoculated with 1×10(11) focus forming units (ffu) of a replication-defective human adenovirus containing the gene for porcine interferon alpha (adt-pifn-α) are sterilely protected from fmdv serotypes a24, o1 manisa, or asia 1 when t ... | 2012 | 22924938 |
| foot-and-mouth disease virus nonstructural protein 2c interacts with beclin1, modulating virus replication. | foot-and-mouth disease virus (fmdv), the causative agent of foot-and-mouth disease, is an apthovirus within the picornaviridae family. replication of the virus occurs in association with replication complexes that are formed by host cell membrane rearrangements. the largest viral protein in the replication complex, 2c, is thought to have multiple roles during virus replication. however, studies examining the function of fmdv 2c have been rather limited. to better understand the role of 2c in the ... | 2012 | 22933281 |
| interplay of foot-and-mouth disease virus, antibodies and plasmacytoid dendritic cells: virus opsonization under non-neutralizing conditions results in enhanced interferon-alpha responses. | foot-and-mouth disease virus (fmdv) is a highly infectious member of the picornaviridae inducing an acute disease of cloven-hoofed species. vaccine-induced immune protection correlates with the presence of high levels of neutralizing antibodies but also opsonising antibodies have been proposed as an important mechanism of the immune response contributing to virus clearance by macrophages and leading to the production of type-i interferon (ifn) by plasmacytoid dendritic cells (pdc). the present s ... | 2012 | 22934974 |
| robust expression and secretion of xylanase1 in chlamydomonas reinhardtii by fusion to a selection gene and processing with the fmdv 2a peptide. | microalgae have recently received attention as a potential low-cost host for the production of recombinant proteins and novel metabolites. however, a major obstacle to the development of algae as an industrial platform has been the poor expression of heterologous genes from the nuclear genome. here we describe a nuclear expression strategy using the foot-and-mouth-disease-virus 2a self-cleavage peptide to transcriptionally fuse heterologous gene expression to antibiotic resistance in chlamydomon ... | 2012 | 22937037 |
| homology modeling and analysis of structure predictions of the bovine rhinitis b virus rna dependent rna polymerase (rdrp). | bovine rhinitis b virus (brbv) is a picornavirus responsible for mild respiratory infection of cattle. it is probably the least characterized among the aphthoviruses. brbv is the closest relative known to foot and mouth disease virus (fmdv) with a ~43% identical polyprotein sequence and as much as 67% identical sequence for the rna dependent rna polymerase (rdrp), which is also known as 3d polymerase (3d(pol)). in the present study we carried out phylogenetic analysis, structure based sequence a ... | 2012 | 22942748 |
| development of a foot-and-mouth disease virus serotype a empty capsid subunit vaccine using silkworm (bombyx mori) pupae. | foot-and-mouth disease (fmd) is a highly contagious disease of cloven-hoofed animals that inflicts severe economic losses in the livestock industry. in 2009, fmdv serotype a caused outbreaks of fmd in cattle in china. although an inactivated virus vaccine has proven effective to control fmd, its use may lead to new disease outbreaks due to a possible incomplete inactivation of the virus during the manufacturing process. here, we expressed the p1-2a and the 3c coding regions of a serotype a fmdv ... | 2012 | 22952788 |
| effectiveness of vaccines and vaccination programs for the control of foot-and-mouth disease in uganda, 2001-2010. | foot-and-mouth disease (fmd) is a highly contagious disease of cloven-hoofed animals. in uganda, fmd outbreaks are mainly controlled by ring vaccination and restriction of animal movements. vaccination stimulates immunity and prevents animals from developing clinical signs which include lameness, inappetence, and decreased production. ring vaccination and restriction of animal movements have, however, not successfully controlled fmd in uganda and outbreaks reoccur annually. the objective of this ... | 2013 | 22956440 |
| development and evaluation of a real-time reverse transcription-loop-mediated isothermal amplification assay for rapid serotyping of foot-and-mouth disease virus. | a one-step, real-time reverse transcription-loop-mediated isothermal amplification assay (rt-lamp) for rapid detection and serotyping of indian foot-and-mouth disease virus (fmdv) is described. the rt-lamp assay was found to be 10(3)-10(5) fold more sensitive in comparison with rt-pcr, with a detection limit ranging from 10(-3) to 10(-5) tcid(50) of virus samples of all three serotypes. the rt-lamp assay and qrt-pcr could detect 100 percent of clinical samples of three serotypes, whereas the rt- ... | 2013 | 22960423 |
| effects of amino acid substitutions in the vp2 b-c loop on antigenicity and pathogenicity of serotype asia1 foot-and-mouth disease virus. | foot-and-mouth disease virus (fmdv) exhibits a high degree of antigenic variability. studies of the antigenic diversity and determination of amino acid changes involved in this diversity are important to the design of broadly protective new vaccines. although extensive studies have been carried out to explore the molecular basis of the antigenic variation of serotype o and serotype a fmdv, there are few reports on asia1 serotype fmdv. | 2012 | 22963009 |