A Viable Recombinant Rhabdovirus Lacking Its Glycoprotein Gene and Expressing Influenza Virus Hemagglutinin and Neuraminidase Is a Potent Influenza Vaccine

Ryder, Alex B.; Buonocore, Linda; Vogel, Leatrice; Nachbagauer, Raffael; Krammer, Florian; Rose, John K.

doi:10.1128/jvi.03246-14

Cited by 25 publications

(20 citation statements)

References 68 publications

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“…In contrast, the same intranasal inoculation with VSVΔG-CHIKV (n ϭ 8) and VLV (n ϭ 6) showed complete safety, with all mice surviving to the end of the experiment 42 days postinoculation. Although VSVΔG-H5N1 is nonpathogenic in adult mice outside the brain (45,46), here, we found it to be lethal after intranasal inoculation of P14 mice, with only a single survivor out of a large cohort (n ϭ 23) and almost all the mice succumbing to the virus within 4 to 10 days of inoculation (Fig. 4).…”

Section: Resultsmentioning

confidence: 84%

“…All the chimeric viruses discussed here have shown efficacy in acting in a vaccine capacity to protect against the respective virus antigens, including Nipah virus, chikungunya virus, and influenza virus (44,(46)(47)(48)(49). By virtue of their safety in both adult and developing brains, VSVΔG-CHIKV and VLV showed the least adverse neurotropism among the chimeric viruses tested; these viruses merit further investigation for potential applications, including vaccination.…”

Section: Discussionmentioning

confidence: 99%

“…The VSV glycoprotein gene was deleted (VSVΔG) in four of the viruses, VSVΔG-CHIKV, VSVΔG-H5N1, VSVΔG-Nipah F, and VSVΔG-Nipah G. VLV was generated from the Semliki Forest virus RNA replicon encoding VSV G and the four nonstructural proteins of SFV but none of the SFV structural proteins (37,39). All four recombinants have been tested as possible vaccine vectors (38,(44)(45)(46)(47)(48)(49). Three additional recombinant VSVs were used for control purposes; all three have been previously used to test intracranial safety (18,41,50).…”

Section: Resultsmentioning

confidence: 99%

“…The chimera incorporated functional CHIKV glycoproteins into the viral envelope in place of VSV G (44). VSVΔG-H5N1 has the VSV G gene deleted, and in its place were substituted the two influenza virus genes, H5 and N1, as described in detail previously (45,46). Genomic diagrams of the recombinant chimeric viruses are shown in Fig.…”

Section: Methodsmentioning

confidence: 99%

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Chikungunya, Influenza, Nipah, and Semliki Forest Chimeric Viruses with Vesicular Stomatitis Virus: Actions in the Brain

Pol

Mao

Chattopadhyay

et al. 2017

J Virol

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Recombinant vesicular stomatitis virus (VSV)-based chimeric viruses that include genes from other viruses show promise as vaccines and oncolytic viruses. However, the critical safety concern is the neurotropic nature conveyed by the VSV glycoprotein. VSVs that include the VSV glycoprotein (G) gene, even in most recombinant attenuated strains, can still show substantial adverse or lethal actions in the brain. Here, we test 4 chimeric viruses in the brain, including those in which glycoprotein genes from Nipah, chikungunya (CHIKV), and influenza H5N1 viruses were substituted for the VSV glycoprotein gene. We also test a virus-like vesicle (VLV) in which the VSV glycoprotein gene is expressed from a replicon encoding the nonstructural proteins of Semliki Forest virus. VSVΔG-CHIKV, VSVΔG-H5N1, and VLV were all safe in the adult mouse brain, as were VSVΔG viruses expressing either the Nipah F or G glycoprotein. In contrast, a complementing pair of VSVΔG viruses expressing Nipah G and F glycoproteins were lethal within the brain within a surprisingly short time frame of 2 days. Intranasal inoculation in postnatal day 14 mice with VSVΔG-CHIKV or VLV evoked no adverse response, whereas VSVΔG-H5N1 by this route was lethal in most mice. A key immune mechanism underlying the safety of VSVΔG-CHIKV, VSVΔG-H5N1, and VLV in the adult brain was the type I interferon response; all three viruses were lethal in the brains of adult mice lacking the interferon receptor, suggesting that the viruses can infect and replicate and spread in brain cells if not blocked by interferon-stimulated genes within the brain. IMPORTANCE Vesicular stomatitis virus (VSV) shows considerable promise both as a vaccine vector and as an oncolytic virus. The greatest limitation of VSV is that it is highly neurotropic and can be lethal within the brain. The neurotropism can be mostly attributed to the VSV G glycoprotein. Here, we test 4 chimeric viruses of VSV with glycoprotein genes from Nipah, chikungunya, and influenza viruses and nonstructural genes from Semliki Forest virus. Two of the four, VSVΔG-CHIKV and VLV, show substantially attenuated neurotropism and were safe in the healthy adult mouse brain. VSVΔG-H5N1 was safe in the adult brain but lethal in the younger brain. VSVΔG Nipah FϩG was even more neurotropic than wild-type VSV, evoking a rapid lethal response in the adult brain. These results suggest that while chimeric VSVs show promise, each must be tested with both intranasal and intracranial administration to ensure the absence of lethal neurotropism.

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Section: Resultsmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Chikungunya, Influenza, Nipah, and Semliki Forest Chimeric Viruses with Vesicular Stomatitis Virus: Actions in the Brain

Pol

Mao

Chattopadhyay

et al. 2017

J Virol

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“…In order to create a vaccination strategy that exploits the advantages of live viral vectors, while at the same time limiting exposure to a single viral vector system, vesicular stomatitis virus (VSV) vectors with different vesiculovirus envelope proteins (17) have been generated that can be used in primeboost vaccination. We have previously shown that VSV vectors can express influenza HA molecules and that these VSV-HA constructs protect against challenge with homologous influenza viruses (18)(19)(20). Here, we show that VSV-cHA vaccines administered by different routes (intramuscular [i.m.]…”

mentioning

confidence: 90%

Vaccination with Vesicular Stomatitis Virus-Vectored Chimeric Hemagglutinins Protects Mice against Divergent Influenza Virus Challenge Strains

Ryder

Nachbagauer

Buonocore

et al. 2016

J Virol

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Seasonal influenza virus infections continue to cause significant disease each year, and there is a constant threat of the emergence of reassortant influenza strains causing a new pandemic. Available influenza vaccines are variably effective each season, are of limited scope at protecting against viruses that have undergone significant antigenic drift, and offer low protection against newly emergent pandemic strains. "Universal" influenza vaccine strategies that focus on the development of humoral immunity directed against the stalk domains of the viral hemagglutinin (HA) show promise for protecting against diverse influenza viruses. Here, we describe such a strategy that utilizes vesicular stomatitis virus (VSV) as a vector for chimeric hemagglutinin (cHA) antigens. This vaccination strategy is effective at generating HA stalk-specific, broadly cross-reactive serum antibodies by both intramuscular and intranasal routes of vaccination. We show that prime-boost vaccination strategies provide protection against both lethal homologous and heterosubtypic influenza challenge and that protection is significantly improved with intranasal vaccine administration. Additionally, we show that vaccination with VSV-cHAs generates greater stalk-specific and cross-reactive serum antibodies than does vaccination with VSV-vectored full-length HAs, confirming that cHA-based vaccination strategies are superior at generating stalk-specific humoral immunity. VSV-vectored influenza vaccines that express chimeric hemagglutinin antigens offer a novel means for protecting against widely diverging influenza viruses. IMPORTANCEUniversal influenza vaccination strategies should be capable of protecting against a wide array of influenza viruses, and we have developed such an approach utilizing a single viral vector system. The potent antibody responses that these vaccines generate are shown to protect mice against lethal influenza challenges with highly divergent viruses. Notably, intranasal vaccination offers significantly better protection than intramuscular vaccination in a lethal virus challenge model. The results described in this study offer insights into the mechanisms by which chimeric hemagglutinin (HA)-based vaccines confer immunity, namely, that the invariant stalk of cHA antigens is superior to full-length HA antigens at inducing cross-reactive humoral immune responses and that VSV-cHA vaccine-induced protection varies by site of inoculation, and contribute to the further development of universal influenza virus vaccines. O n average, there are more than 200,000 hospitalizations due to influenza-associated complications each year in the United States (1), despite the widespread use of seasonal influenza vaccines. Many of these hospitalized patients had received the seasonal vaccine and yet developed disease (2). Recent meta-analysis suggests that the effectiveness of seasonal influenza vaccines is ca. 69% (3), although individual studies report much lower effectiveness for a given influenza season (3). This is in contrast ...

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R7A mutation in N protein renders temperature sensitive phenotype of VSV by affecting its replication and transcription in vitro

et al. 2019

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A Viable Recombinant Rhabdovirus Lacking Its Glycoprotein Gene and Expressing Influenza Virus Hemagglutinin and Neuraminidase Is a Potent Influenza Vaccine

Cited by 25 publications

References 68 publications

Chikungunya, Influenza, Nipah, and Semliki Forest Chimeric Viruses with Vesicular Stomatitis Virus: Actions in the Brain

Chikungunya, Influenza, Nipah, and Semliki Forest Chimeric Viruses with Vesicular Stomatitis Virus: Actions in the Brain

Vaccination with Vesicular Stomatitis Virus-Vectored Chimeric Hemagglutinins Protects Mice against Divergent Influenza Virus Challenge Strains

R7A mutation in N protein renders temperature sensitive phenotype of VSV by affecting its replication and transcription in vitro

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