Induction of mucosal immune responses and protection of cattle against direct-contact challenge by intranasal delivery with foot-and-mouth disease virus antigen mediated by nanoparticles

Pan, Li; Zhang, Zhongwang; Lv, Jing; Zhou, Peng; Hu, Wenfa; Fang, Yuqi; Chen, Hao-tai; Liu, Xinsheng; Shao, Jing; Zhao, Furong; Ding, Yongsheng; Lin, Tong; Chang, Huiyun; Zhang, Jie; Zhang, Yongguang; Wang, Yonglu

doi:10.2147/ijn.s72318

Cited by 42 publications

(17 citation statements)

References 55 publications

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“…A single study in cattle assessed two types of nanoparticle nasal vaccines against serotype A FMDV: i) chitosan‐coated polylactic‐co‐glycolic acid (PLGA) loaded with plasmid DNA encoding sections of P1, 2A and 3C; and ii) chitosan–trehalose loaded with inactivated FMDV. The DNA‐based vaccine was the more promising of the two, inducing specific IgA production in the nasal mucosa from 4 days post‐immunization and protecting three out of four animals from challenge (Pan et al., ). Continued investigation of needle‐free vaccination is needed.…”

Section: Literature Reviewmentioning

confidence: 99%

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 3 - Vaccines

Robinson

Knight-Jones

Charleston

et al. 2016

Transbound Emerg Dis

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SummaryThis study assessed research knowledge gaps in the field of FMDV (foot-andmouth disease virus) vaccines. The study took the form of a literature review combined with research updates collected in 2014 from 33 institutes from across the world. Findings were used to identify priority areas for future FMD vaccine research. Vaccines play a vital role in FMD control, used both to limit the spread of the virus during epidemics in FMD-free countries and as the mainstay of disease management in endemic regions, particularly where sanitary controls are difficult to apply. Improvements in the performance or cost-effectiveness of FMD vaccines will allow more widespread and efficient disease control. FMD vaccines have changed little in recent decades, typically produced by inactivation of whole virus, the quantity and stability of the intact viral capsids in the final preparation being key for immunogenicity. However, these are exciting times and several promising novel FMD vaccine candidates have recently been developed. This includes the first FMD vaccine licensed for manufacture and use in the USA; this adenovirus-vectored FMD vaccine causes in vivo expression of viral capsids in vaccinated animals. Another promising vaccine candidate comprises stabilized empty FMDV capsids produced in vitro in a baculovirus expression system. Recombinant technologies are also being developed to improve otherwise conventionally produced inactivated vaccines, for example, by creating a chimeric vaccine virus to increase capsid stability and by inserting sequences into the vaccine virus for desired antigen expression. Other important areas of ongoing research include enhanced adjuvants, vaccine quality control procedures and predicting vaccine protection from immune correlates, thus reducing dependency on animal challenge studies. Globally, the degree of independent vaccine evaluation is highly variable, and this is essential for vaccine quality. Previously neglected, the importance of evaluating vaccination programme effectiveness and impact is increasingly being recognized.

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Section: Literature Reviewmentioning

confidence: 99%

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 3 - Vaccines

Robinson

Knight-Jones

Charleston

et al. 2016

Transbound Emerg Dis

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“…Intranasal delivery of cationic PLGA nano/microparticles loaded with various FMDV DNA vaccine formulations encoding IL-6 as a molecular adjuvant enhanced protective immunity against infection by aerosolized FMDV [20]. Another study also suggested that intranasal delivery of Chi-PLGA-DNA nanoparticles with FMDV antigen resulted in high levels of mucosal, systemic and cell-mediated immunity and could reduce disease severity and virus excretion as well as delay clinical symptoms [23]. .…”

Section: Discussionmentioning

confidence: 99%

Protection against Foot-and-Mouth Disease Virus in Guinea Pigs via Oral Administration of Recombinant Lactobacillus plantarum Expressing VP1

et al. 2015

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Mucosal vaccination is an effective strategy for generating antigen-specific immune responses against mucosal infections of foot-and-mouth disease virus (FMDV). In this study, Lactobacillus plantarum strains NC8 and WCFS1 were used as oral delivery vehicles containing a pSIP411-VP1 recombinant plasmid to initiate mucosal and systemic immune responses in guinea pigs. Guinea pigs were orally vaccinated (three doses) with NC8-pSIP411, NC8-pSIP411-VP1, WCFS1-pSIP411, WCFS1-pSIP411-VP1 or milk. Animals immunized with NC8-pSIP411-VP1 and WCFS1-pSIP411-VP1 developed high levels of antigen-specific serum IgG, IgA, IgM, mucosal secretory IgA (sIgA) and neutralizing antibodies, and revealed stronger cell-mediated immune responses and enhanced protection against FMDV challenge compared with control groups. The recombinant pSIP411-VP1 effectively improved immunoprotection against FMDV in guinea pigs.

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“…To the best of our knowledge, this is the first study that utilizes chitosan nanoparticles as carriers for an intranasal vaccine against fungi, although chitosan nanoparticles have already been used in intranasal vaccines against viral infections [ 32 , 33 , 34 , 35 ].…”

Section: Discussionmentioning

confidence: 99%

Intranasal Vaccine Using P10 Peptide Complexed within Chitosan Polymeric Nanoparticles as Experimental Therapy for Paracoccidioidomycosis in Murine Model

Santos

Silva

Dias

et al. 2020

JoF

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Paracoccidioidomycosis (PCM) is a granulomatous fungal disease caused by the dimorphic fungal species of Paracoccidioides, which mainly affects the lungs. Modern strategies for the treatment and/or prevention of PCM are based on a Th1-type immune response, which is important for controlling the disease. One of the most studied candidates for a vaccine is the P10 peptide, derived from the 43 kDa glycoprotein of Paracoccidioides brasiliensis. In order to improve its immune modulatory effect, the P10 peptide was associated with a chitosan-conjugated nanoparticle. The nanoparticles presented 220 nm medium size, poly dispersion index (PDI) below 0.5, zeta potential of +20 mV and encapsulation efficiency around 90%. The nanoparticles’ non-toxicity was verified by hemolytic test and cell viability using murine macrophages. The nanoparticles were stable and presented physicochemical characteristics desirable for biological applications, reducing the fungal load and the usual standard concentration of the peptide from 4 to 20 times.

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Induction of mucosal immune responses and protection of cattle against direct-contact challenge by intranasal delivery with foot-and-mouth disease virus antigen mediated by nanoparticles

Cited by 42 publications

References 55 publications

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 3 - Vaccines

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 3 - Vaccines

Protection against Foot-and-Mouth Disease Virus in Guinea Pigs via Oral Administration of Recombinant Lactobacillus plantarum Expressing VP1

Intranasal Vaccine Using P10 Peptide Complexed within Chitosan Polymeric Nanoparticles as Experimental Therapy for Paracoccidioidomycosis in Murine Model

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