Ovine rotavirus strain LLR-85-based bovine rotavirus candidate vaccines: Construction, characterization and immunogenicity evaluation

Chang, Jitao; Li, Xin; Liu, Haijun; Yu, Li

doi:10.1016/j.vetmic.2010.04.016

Cited by 5 publications

(4 citation statements)

References 55 publications

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“…For the confirmation of bovine rotavirus, amplification of both the VP4 and VP6 gene was carried out using primer sets given in Table 1 as mentioned in (4,16,17). For the desired amplification of VP4 gene (880 bp) and VP6 gene (250 bp) of bovine rotavirus, optimization of PCR conditions was done by using the varying concentrations of cDNA, primers and Taq polymerase in PCR reaction mixture.…”

Section: Amplification Of Vp4 and Vp6 Gene Through Pcrmentioning

confidence: 99%

“…The genome is a double stranded RNA having 11 segments, which encodes six structural viral proteins (VP1-4, VP6, and VP7) and six non-structural proteins (NSP1-6) (2, 3). The structural viral proteins VP4, VP6 and VP7 are important as they are used for serological characterization of rotaviruses (4). In reference to the immunity development, VP4 and VP7 are helpful, so information of these genotypes is necessary to develop a vaccine (5).…”

Section: Introductionmentioning

confidence: 99%

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Molecular Characterization of Bovine Rotaviruses in Pakistan

Mukhtar

Yaqub

Masood

et al. 2016

Jundishapur J Microbiol

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Section: Amplification Of Vp4 and Vp6 Gene Through Pcrmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Molecular Characterization of Bovine Rotaviruses in Pakistan

Mukhtar

Yaqub

Masood

et al. 2016

Jundishapur J Microbiol

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“…Although it is too early to know whether and to what extent the widespread use of HRV will lead to immune selection of new strains, there is the potential for vaccine-associated collateral infections especially in immunocompromised individuals [ 10 ]. In contrast to attenuated-live vaccines, the use of inactivated or non-replicative virus like particles (VLPs) as vaccine candidates, coupled with new strategies for boosting mucosal immunity, [ 9 , 11 , 12 , 13 , 14 ], and/or direct competition with virus-host cell binding using a dietary nutriceutical approach, may have the greatest potential to provide stable, long-term protection against rotavirus disease in both animals and people. This approach also reduces the possibility of emergence of virus P and G types not represented in the vaccine strains since non-replicative virus particles will not reassort with wild type rotaviruses.…”

Section: Introductionmentioning

confidence: 99%

“…Despite remarkable progress in rotavirus vaccine development for both animals [ 12 , 13 , 15 , 16 , 17 ] and humans [ 2 , 18 , 19 , 20 , 21 , 22 ], there are no effective commercial vaccines or licensed rotavirus-specific antiviral agents for animals in wide clinical use and no practical method of preventing rotavirus infection in swine herds. In this report, we provide proof of concept that an orally administered, synthetic, neoglycolipid can be used as a therapeutic receptor mimetic for the prevention of Group A rotavirus disease in neonatal piglets.…”

Section: Introductionmentioning

confidence: 99%

Inhibition of Rotavirus Infectivity by a Neoglycolipid Receptor Mimetic

et al. 2011

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Group A rotaviruses are a major cause of diarrhea in the young of many mammalian species. In rotavirus infected piglets mortality can be as high as 60%. Previous research in this laboratory has identified a porcine intestinal GM3 ganglioside receptor that is required for sialic acid-dependent rotavirus recognition of host cells. In addition, we previously demonstrated exogenously added GM3 can competitively inhibit porcine rotavirus binding and infectivity of host cells in vitro. Sialyllactose, the carbohydrate moiety of GM3, is approximately 3 orders of magnitude less effective than GM3 at inhibiting rotavirus binding to cells. Furthermore, production of therapeutic quantities of GM3 ganglioside for use as an oral carbomimetic in swine is cost prohibitive. In an effort to circumvent these problems, a sialyllactose-containing neoglycolipid was synthesized and evaluated for its ability to inhibit rotavirus binding and infectivity of host cells. Sialyllactose was coupled to dipalmitoylphosphatidylethanolamine (PE) by reductive amination and the product (SLPE) purified by HPLC. Characterization of the product showed a single primulin (lipid) and resorcinol (sialic acid) positive band by thin layer chromatography and quantification of phosphate and sialic acid yielded a 1:1 molar ratio. Mass spectroscopy confirmed a molecular weight coinciding with SLPE. Concentration-dependent binding of rotavirus to SLPE was demonstrated using a thin-layer overlay assay. Using concentrations comparable to GM3, SLPE was also shown to inhibit rotavirus binding to host cells by 80%. Furthermore, SLPE was shown to decrease rotavirus infection of host cells by over 90%. Finally, preliminary results of in vivo animal challenge studies using newborn piglets in their natural environment, demonstrated SLPE afforded complete protection from rotavirus disease. The efficacy of SLPE in inhibiting rotavirus binding and infection in vitro and in vivo, coupled with its relatively low-cost, large-scale production capabilities make SLPE a promising candidate for further exploration as a possible prophylactic or therapeutic nutriceutical for combating rotavirus disease in animals. Most importantly, the results presented here provide proof of concept that the nutriceutical approach of providing natural or synthetic dietary receptor mimetics for protection against gastrointestinal virus infectious disease in all species is plausible.

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