Protection of Rabbits from Viral Challenge by Gene Gun-Based Intracutaneous Vaccination with a Combination of Cottontail Rabbit Papillomavirus E1, E2, E6, and E7 Genes

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Journal of Virology, August 1999, p. 7039-7043, Vol. 73, No. 8
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

Protection of Rabbits from Viral Challenge by Gene Gun-Based Intracutaneous Vaccination with a Combination of Cottontail Rabbit Papillomavirus E1, E2, E6, and E7 Genes

Ricai Han,¹ Nancy M. Cladel,¹ Cynthia A. Reed,¹ Xuwen Peng,² and Neil D. Christensen¹^,³^,^*

Jake Gittlen Cancer Research Institute, Department of Pathology,¹ Department of Comparative Medicine,² and Department of Microbiology and Immunology,³ Pennsylvania State University College of Medicine, Hershey, Pennsylvania 17033

Received 4 February 1999/Accepted 12 May 1999

	ABSTRACT

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In this study, cottontail rabbit papillomavirus infection of domestic rabbits was used as an animal model to develop papillomavirusearly gene-based vaccines. Groups of rabbits were intracutaneouslyvaccinated with single papillomavirus early genes E1, E2, E6,and E7 or with a combination of these four genes. Only a fractionof rabbits were protected from subsequent viral challenge whenvaccinated with the E1 or E6 gene. Viral tumor growth in thoserabbits vaccinated with the E1 or E2 gene was suppressed comparedto that in controls. In contrast, seven of nine rabbits vaccinatedwith the combination of the E1, E2, E6, and E7 genes were completelyprotected against viral challenge. These data indicated that intracutaneousgenetic vaccination with the combination of the E1, E2, E6, andE7 genes can be an effective strategy for immunoprophylaxis ofpapillomavirusinfection.

	TEXT

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Human papillomavirus (HPV) infection induces mucosal and/or cutaneous hyperproliferative lesions which persist for monthsor years. Certain HPV types are linked to the development of skincancer (21), tumors of the head and neck (8), and anogenitalcarcinomas (30). Development and testing of papillomavirus vaccineshave been conducted extensively in animal models, such as bovinepapillomavirus (BPV) infection of cattle (3) and cottontailrabbit papillomavirus (CRPV) infection of domestic rabbits (16).Currently, several strategies have been utilized to develop papillomavirusvaccines. One strategy involves the induction of neutralizingantibodies by immunization with the viral structural protein L1or L2, particularly, virus-like particles (VLPs) assembled fromL1 or L1/L2. Another strategy involves the induction of cell-mediatedimmunity by papillomavirus early gene/protein-based vaccination.Recently, VLPs containing L1 and chimeric molecules of L1 andearly proteins were used as immunogens. This strategy has beenapplied to elicit concurrent viral neutralizing antibodies andcell-mediated immunity specific for viral early proteins (11).

A number of studies have demonstrated that VLP immunization protected animals against experimental virus challenge in theCRPV-infected rabbit model (2, 6, 13), in the BPV-infectedcow model (15), and in the canine oral papillomavirus (COPV)-infectedbeagle dog model (28). Furthermore, genetic vaccination withCRPV L1 (9, 26) or immunization with CRPV L1 proteins expressedas bacterial fusion proteins (18) also protected rabbits fromviral challenge. Protection has also been achieved by immunizationwith L2 proteins (5, 10, 19). One caveat of these animalmodel systems is that protection from natural papillomavirus infectionhas not been determined. In experimental infection models, sitesto be infected are vigorously scarified or wounded, resultingin damage to local blood vessels and the release of circulatingneutralizing antibodies at the sites of infection. In contrast,natural infection may occur following microtrauma to the epitheliumwithout significant damage to blood vessels and subsequent directexposure of virus to circulating neutralizing antibodies. Thus,circulating neutralizing antibodies may be unable to protect againstnatural papillomavirus infection. Protective vaccines targetingvirus-infected epithelium via cell-mediated immunity would overcomethese potentiallimitations.

Induction of protective cell-mediated immunity by immunization with papillomavirus early gene/proteins is expected to preventthe establishment of new lesions (immunoprophylaxis) as well asto eliminate existing lesions (immunotherapy). However, earlystudies disclosed variable results. In the CRPV-infected rabbitmodel, different papillomavirus early antigens and several methodsof antigen delivery have been applied in an attempt to elicitprotective antipapillomavirus immunity: (i) immunization withbacterial fusion proteins of CRPV E1 and/or E2 (24); (ii) immunizationwith recombinant Listeria monocytogenes expressing CRPV E1 (14);(iii) intracutaneous genetic vaccination of rabbits with CRPVE6 (27); and (iv) intramuscular injection of plasmid DNA encodingCRPV E1, E2, E6, or E7 (12). The immunity so induced stimulatedpapilloma regression in a fraction of vaccinated rabbits (14,24) and partially protected rabbits from subsequent virus challenge(27). However, none of these studies revealed complete protection.In the BPV-infected cow model, immunization with BPV E6 and E7proteins delayed papilloma formation, reduced papilloma size,and promoted papilloma regression but also did not lead to completeprotection (3, 4). BPV E2 immunizations were ineffective(4). In the present study, we immunized rabbits by gene gun-mediatedintracutaneous vaccination with individual CRPV E1, E2, E6, andE7 genes or with a combination of all four genes. We report thatvaccination with the combination of CRPV E1, E2, E6, and E7 genesprovided strong and complete protection of outbred rabbits againstCRPVchallenge.

Preparation of DNA vectors and gene gun-mediated immunization. CRPV E1, E2, E6, and E7 DNA genes were amplified by PCR and cloned into V1Jns expression vector (generous gift of M. A. Liu,Merck & Co, Westpoint, Pa.) at the BglII site individually (20).The resultant recombinant plasmids were referred to as V1JnsE1,V1JnsE2, V1JnsE6, and V1JnsE7, respectively. Plasmid DNA was precipitatedonto 1.6-µm-diameter gold microparticles at a ratio of 1 µg ofDNA/0.5 mg of gold particles as described by the manufacturer(Bio-Rad, Hercules, Calif.). Outbred New Zealand White rabbits(Covance Research Products Inc., Denver, Pa.) were immunized bygene gun-mediated intracutaneous delivery of DNA/gold particlesonto dorsal skin sites at 400 lb/in².

Protection of rabbits against challenge with cloned CRPV viral DNA. In our laboratory, we currently use a CRPV stock which was obtained originally from cottontail rabbit viral papillomas andthen expanded by using the nude mouse xenograft system. It ispossible that several CRPV variants exist in this virus stock(23). In this study, the E1, E2, E6, and E7 genes were clonedfrom a single clone or a variant. Theoretically, immunity to theseearly proteins will generate protection against the matching CRPVvariant but not to other variants if critical epitopes are antigenicallyunrelated. Rabbits were thus challenged with the same cloned viralDNA (17) from which the E1, E2, E6, and E7 genes were amplified.In the first experiment, 24 rabbits were divided into six groups(Table 1). For the groups vaccinated with a single gene or vector,rabbits received three immunizations at 3-week intervals: 20 µgof DNA for each of the first and the second immunizations, and10 µg of DNA for the final booster immunization. For the groupvaccinated with the combination of the four genes, rabbits receivedonly two immunizations at 3-week intervals, 10 µg of each E1-,E2-, E6-, and E7-encoding plasmid DNA. Numbers of challenged sitesin each rabbit that produced papillomas are shown in Table 1.Papillomas grew at all challenged sites in control rabbits thatwere vaccinated with V1Jns vector, indicating a high efficiencyof papilloma induction by viral DNA (100%) in this experiment.Among the groups vaccinated with single genes, 63% and 44% ofchallenged sites had no papilloma growth for E1-immunized rabbitsand for E6-immunized rabbits, respectively. In contrast, only13% of challenged sites for E2-vaccinated rabbits and 7% of sitesfor E7-vaccinated rabbits had no papilloma growth (Table 1).Two of four rabbits vaccinated with the E1 gene were completelyprotected, and one of four E6-vaccinated rabbits was also completelyprotected. These results demonstrated that individual E1 or E6vaccination provided protection in a subset of rabbits followinginfection with cloned viral DNA. In contrast, E2 and E7 vaccinationsdid not induce protective immunity. Among four rabbits vaccinatedwith the combination of E1, E2, E6, and E7 genes, two rabbitshad no papillomas, and on the remaining two rabbits, there wereonly small papillomas which completely regressed within threeweeks. Systemic regression of papillomas was not observed on rabbitsin the other groups, indicating that vaccination with all fourgenes induced the strongest protective antiviral immunity in thisexperiment. It is important to note that the rabbits in the combinationvaccine group received two immunizations with a total of 20 µgof DNA of each gene in contrast to the rabbits in the other groups,which received three immunizations with a total of 50 µg of DNAfor individual gene vaccination.

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TABLE 1. Papilloma growth in vaccinated and control rabbits

In the second experiment (Table 1), 10 rabbits were divided into two groups. One group was vaccinated with the combinationof the E1, E2, E6, and E7 genes. The second group received vectorDNA only as a control. In addition to the first and second immunizations,rabbits also received a third, booster immunization containing6 µg of DNA of each gene (Table 1). Papillomas grew at all challengedsites in all five control rabbits. In contrast, all five rabbitsvaccinated with the combination of E1, E2, E6, and E7 genes werecompletely protected (Table 1). These results demonstrated thatintracutaneous genetic vaccination with the combination of E1,E2, E6, and E7 protected all rabbits from challenge with clonedviralDNA.

Protection of rabbits against challenge with infectious virions. To investigate whether these protected rabbits were also resistant to challenge with virus particles, we infected all protectedrabbits with infectious virions (two E1-vaccinated, one E6-vaccinated,and nine combination gene-vaccinated rabbits; Table 1). Fiverabbits that were previously vaccinated with V1Jns vector werealso challenged with virus particles as a control. All controlrabbits grew papillomas at virion-challenged sites, and all protectedrabbits were resistant to the viral challenge except one rabbitwhich was vaccinated with the E1 gene alone. Papillomas on thelatter rabbit appeared at 4 weeks after virus challenge and persistedwithout regression until the termination of this experiment (4months). Vaccination with the combination of E1, E2, E6, and E7genes therefore completely protected rabbits from virus particleinfection.

Papilloma growth in nonprotected and partially protected rabbits. Papilloma size was measured for a total of 14 weeks following viral DNA challenge in those nonprotected and partially protectedrabbits. Mean papilloma sizes per site for rabbits vaccinatedwith the E1 or E2 genes were significantly smaller than thosein the vector-injected rabbits (vector group versus E1 group,t test, P < 0.05; vector group versus E2 group, t test, P < 0.05).Papilloma size per site for E6-vaccinated rabbits was somewhatsmaller than that for vector-vaccinated control rabbits, but sizedifferences were not statistically significant at 14 weeks postchallengewith virus (Fig. 1). E7 vaccination has little effect on papillomagrowth rates (Fig. 1).

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FIG. 1. Papilloma growth for nonprotected and control rabbits in the first experiment. Data represent the means ± standard errors of the means of papilloma areas that were calculated from the total numbers of papillomas, which are indicated in parentheses, for each group. Individual papilloma size was calculated by multiplying length (millimeters) and width (millimeters). Mean papilloma areas were significantly different in the V1Jns group and V1JnsE1 group (t test, P < 0.05) and in the V1Jns group and V1Jns group and V1JnsE2 group (t test, P < 0.05) but not in the V1Jns group and V1JnsE6 group and in the V1Jns group and V1JnsE7 group at 14 weeks postchallenge.

Systemic regression of papillomas was observed only for two rabbits that were vaccinated with the combination of the E1, E2,E6, and E7 genes in the first experiment (rabbits 1 and 2). Forone partially protected rabbit in the E2 group (rabbit 1; Table1), papillomas at one challenged site rapidly regressed and papillomagrowth at another site was significantly suppressed (9 mm² at 14 weeks) but did not regress. One papilloma on one E6-vaccinatedrabbit (rabbit 3; Table 1) appeared at week 4, then regressed,and reappeared at week 8. However, this papilloma regressed again,regrew at 14 weeks, and then became persistent. These observationsindicated that immunity induced by single gene vaccinations byusing the protocol described for the first experiment had an impacton papilloma growth but was insufficient to completely eliminateall viral papillomas. It is possible that additional booster vaccinationswith single genes prior to viral DNA challenge may have led toan increased level ofprotection.

T-cell-mediated immune responses. In vitro peripheral blood mononuclear cell (PBMC) proliferation assays were conducted to evaluate T-cell-mediated immune responses(12). PBMCs were isolated from ear arterial blood one week afterthe final booster immunization and stimulated with the specificantigens, CRPV E1, E2, E6 and E7, as histidine-tagged fusion proteins.Control antigens for all rabbits were CRPV L2 histidine-taggedfusion proteins. All fusion proteins were prepared by using recombinantbaculoviruses and purified by using nickel columns under denaturingconditions (Invitrogen, San Diego, Calif.) as previously described(12). All four E2-vaccinated rabbits showed strong antigen-specificproliferative responses (Table 2). Three of four rabbits in eachof the E1, E6, and E7 groups also showed antigen-specific proliferativeresponses (Table 2). These data indicated that genetic vaccinationwith CRPV E1, E2, E6, and E7 genes induced T-cell-mediated immunity.Interestingly, in vitro antigen-specific proliferative responseswere strongest in the E2- and E7-vaccinated rabbits despite alack of protection against viral DNA challenge in these two groups(Table 2). Furthermore, papilloma sizes in rabbits vaccinatedwith E7 were substantially larger than the papillomas of the E6-vaccinatedgroup (Fig. 1). These data suggest that in vitro antigen-specificproliferative responses do not correlate with in vivo protectiveimmunity.

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TABLE 2. PBMC proliferative responses to in vitro stimulation with antigens

Humoral immune responses. Rabbit serum was collected before vaccination and after the first, second, and third vaccinations (Fig. 1). Western blot analysisdid not detect specific anti-E1, -E2, -E6, or -E7 antibodies inthose vaccinated rabbits (data notshown).

Papillomavirus-induced lesions are maintained by hyperproliferation of virus-infected, undifferentiated cells in the basaland suprabasal layers of the epithelium. Immune-mediated cureof papillomavirus-induced lesions can be successful only whenthe latter cells are eliminated by effector cells, such as cytotoxicT lymphocytes. A potential vaccine candidate gene/protein(s) thereforemust be expressed in the infected, undifferentiated cells and,in addition, must be immunogenic. Experimental evidence for theviral proteins E1, E2, E6, and E7 in basal and suprabasal layersof infected epithelium has been indirectly established by RNA-RNAin situ hybridization studies (1, 25, 29). These four genestherefore are potential candidate vaccines. In the present study,E1 was the most effective of the four early genes for protectionby vaccination of animals against viral challenge. These resultsare consistent with the findings of Jensen and coworkers (14).Immunization with the E6 gene only provided partial protection.A similar result was obtained by other investigators (27). Unexpectedly,T-cell-mediated immune responses for the E2 immunization groupwere the strongest of any of the vaccinated groups as determinedby in vitro PBMC proliferation assays. However, none of the E2-vaccinatedrabbits were completely protected from viral challenge, althoughviral tumor growth was significantly suppressed. E7 vaccinationalso induced cell-mediated immunity but neither induced protectionof rabbits from viral challenge nor significantly suppressed viraltumor growth. In contrast, vaccination with the combination ofthe E1, E2, E6, and E7 genes provided complete protection of rabbitsagainst subsequent viral challenge. It is possible that the expressionlevels of the E1, E2, E6, and E7 proteins are low in the basaland suprabasal layers of the infected epithelium. Low expressionwould result in a low density of virus-derived peptide/major histocompatibilitycomplex (MHC) class I complexes on the cell surface. Efficientelimination of these virus-infected cells may be possible onlyif there is a pool of CD8⁺ T lymphocytes specific for E1, E2, E6, and E7 in certain MHCgenetic backgrounds. In this study, although the immunity inducedby E7 vaccination alone did not affect viral infection, E7 vaccinationmay still play a role in protection and/or suppression of viraltumor growth in some rabbits with certain MHC genotypes whichcan efficiently process and present E7 antigen to T cells. E7vaccination may also play a role in the prevention of cervicalcancer.

We have also immunized rabbits by (i) subcutaneous injection of recombinant baculovirus-expressed E1 and E2 proteins (unpublishedobservations), (ii) subcutaneous injection of recombinant retrovirusesexpressing E1 or E2 proteins (unpublished observations), and (iii)intramuscular injection of plasmid DNA encoding E1, E2, E6, orE7, respectively (12). Cell-mediated immunity was detectablein these vaccinated rabbits, but none of the above-listed vaccinationstrategies provided protection of rabbits against subsequent viralchallenge. Based on our observations, gene gun-mediated intracutaneousgenetic immunization is the most effective strategy for a papillomavirusearly-gene-based vaccine. It has been demonstrated that gene gun-mediatedintracutaneous inoculation of naked plasmid DNA directly deliveredthe DNA into skin-derived dendritic cells in vivo (7, 22).The proteins encoded by the plasmid DNA were expressed in thecytoplasm of dendritic cells in the draining lymph nodes. Theseprocedures produced potent, antigen-specific cytotoxic T-lymphocyte-mediatedprotective tumor immunity (7).

In vivo delivery of an oncogene-expressing plasmid DNA always raises safety concerns. Papillomavirus E6 and E7 are multifunctionaloncogenes based on in vitro assays. Gene gun-mediated deliverycan directly introduce E6- and E7-expressing plasmid into cells.Whether they can transform the in vivo transfected cells, suchas epithelial cells and Langerhans cells, is still an importantissue to be studied. Genetic engineering of E6 and E7 genes toinactivate their transforming functions may provide a solutionto this potentialproblem.

Our results provide two important considerations for HPV vaccine development. First, vaccination with a combination of severalearly genes was an effective strategy for achieving complete protectionin outbred populations. Second, gene gun-mediated intracutaneousgenetic vaccination induced protective antipapillomavirus immunity.This strategy has great potential for therapeutic approaches tothe treatment of HPVinfections.

	ACKNOWLEDGMENTS

This study was supported by grant RO1 CA47622 and the Jake Gittlen Memorial Golf Tournament. R. Han is the recipient of the1996-1998 American Social Health Association/Merck FoundationResearch Fellowship in sexually transmitteddiseases.

	FOOTNOTES

^* Corresponding author. Mailing address: Jake Gittlen Cancer Research Institute, Pennsylvania State University College of Medicine,500 University Dr., Hershey, PA 17033-2390. Phone: (717) 531-4700.Fax: (717) 531-5634. E-mail: ndc1{at}psu.edu.

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Christensen, N. D., Han, R., Cladel, N. M., Pickel, M. D. (2001). Combination Treatment with Intralesional Cidofovir and Viral-DNA Vaccination Cures Large Cottontail Rabbit Papillomavirus-Induced Papillomas and Reduces Recurrences. Antimicrob. Agents Chemother. 45: 1201-1209 [Abstract] [Full Text]
Han, R., Cladel, N. M., Reed, C. A., Peng, X., Budgeon, L. R., Pickel, M., Christensen, N. D. (2000). DNA Vaccination Prevents and/or Delays Carcinoma Development of Papillomavirus-Induced Skin Papillomas on Rabbits. J. Virol. 74: 9712-9716 [Abstract] [Full Text]
Leachman, S. A., Tigelaar, R. E., Shlyankevich, M., Slade, M. D., Irwin, M., Chang, E., Wu, T. C., Xiao, W., Pazhani, S., Zelterman, D., Brandsma, J. L. (2000). Granulocyte-Macrophage Colony-Stimulating Factor Priming plus Papillomavirus E6 DNA Vaccination: Effects on Papilloma Formation and Regression in the Cottontail Rabbit Papillomavirus-Rabbit Model. J. Virol. 74: 8700-8708 [Abstract] [Full Text]

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