Vaccination of vampire bats using recombinant vaccinia-rabies virus

被引：44

作者：

Aguilar-Setién, A

Campos, YL

Cruz, ET

Kretschmer, R

Brochier, B

Pastoret, PP

机构：

[1] Ctr Med Nacl Siglo XXI, Hosp Pediat, Inst Mexicano Seguro Social, Unidad Invest Med Inmunol Coordinac Invest Med, Mexico City 06725, DF, Mexico

[2] Inst Pasteur Belgium, B-1180 Brussels, Belgium

[3] Univ Liege, Fac Vet Med, Dept Immunol Vaccinol, B-4000 Liege, Belgium

来源：

JOURNAL OF WILDLIFE DISEASES | 2002年 / 38卷 / 03期

关键词：

rabies; recombinant vaccinia-rabies; vaccination; vampire bats;

D O I：

10.7589/0090-3558-38.3.539

中图分类号：

S85 [动物医学（兽医学）];

学科分类号：

0906 ;

摘要：

Adult vampire bats (Desmodus rotundus) were vaccinated by intramuscular, scarification, oral, or aerosol routes (n=8 in each group) using a vaccinia-rabies glycoprotein recombinant virus. Sera were obtained before and 30 days after vaccination. All animals were then challenged intramuscularly with a lethal dose of rabies virus. Neutralizing antirabies antibodies were measured by rapid fluorescent focus inhibition test (RFFIT). Seroconversion was observed with each of the routes employed, but some aerosol and orally vaccinated animals failed to seroconvert. The highest antibody titers were observed in animals vaccinated by intramuscular and scarification routes. All animals vaccinated by intramuscular, scarification, and oral routes survived the viral challenge, but one of eight vampire bats receiving aerosol vaccination succumbed to the challenge. Of 31 surviving vaccinated and challenged animals, nine lacked detectable antirabies antibodies by RFFIT (five orally and four aerosol immunized animals). In contrast, nine of 10 non-vaccinated control bats succumbed to viral challenge. The surviving control bat had antiviral antibodies 90 days after viral challenge. These results suggest that the recombinant vaccine is an adequate and safe immunogen for bats by all routes tested.

引用

页码：539 / 544

页数：6

共 36 条

[1]

Acha PN., 1988, NATURAL HIST VAMPIRE, P208

[2]

ACHA PN, 1985, RABIES TROPICS, P780

[3]

ANDERSON RM, 1982, POPULATION DYNAMICS, P241

[4] POTENTIAL PATHOGENICITY FOR RODENTS OF VACCINES INTENDED FOR ORAL VACCINATION AGAINST RABIES - A COMPARISON [J].

ARTOIS, M ;

GUITTRE, C ;

THOMAS, I ;

LEBLOIS, H ;

BROCHIER, B ;

BARRAT, J .

VACCINE, 1992, 10 (08) :524-528

[5]

Baer G.M., 1991, P341

[6]

BLANCOU J, 1979, REV MED VET-TOULOUSE, V130, P1001

[7]

BOGEL K, 1981, B WORLD HEALTH ORGAN, V59, P269

[8] COMPARISON OF THE SUSCEPTIBILITY OF THE RED FOX (VULPES-VULPES) TO A VACCINIA-RABIES RECOMBINANT VIRUS AND TO COWPOX VIRUS [J].

BOULANGER, D ;

BROCHIER, B ;

CROUCH, A ;

BENNETT, M ;

GASKELL, RM ;

BAXBY, D ;

PASTORET, PP .

VACCINE, 1995, 13 (02) :215-219

[9] LARGE-SCALE ERADICATION OF RABIES USING RECOMBINANT VACCINIA RABIES VACCINE [J].

BROCHIER, B ;

KIENY, MP ;

COSTY, F ;

COPPENS, P ;

BAUDUIN, B ;

LECOCQ, JP ;

LANGUET, B ;

CHAPPUIS, G ;

DESMETTRE, P ;

AFIADEMANYO, K ;

LIBOIS, R ;

PASTORET, PP .

NATURE, 1991, 354 (6354) :520-522

[10] USE OF RECOMBINANT VACCINIA-RABIES GLYCOPROTEIN VIRUS FOR ORAL VACCINATION OF WILDLIFE AGAINST RABIES - INNOCUITY TO SEVERAL NON-TARGET BAIT CONSUMING SPECIES [J].

BROCHIER, B ;

BLANCOU, J ;

THOMAS, I ;

LANGUET, B ;

ARTOIS, M ;

KIENY, MP ;

LECOCQ, JP ;

COSTY, F ;

DESMETTRE, P ;

CHAPPUIS, G ;

PASTORET, PP .

JOURNAL OF WILDLIFE DISEASES, 1989, 25 (04) :540-547

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