Immunopathogenesis of vaccine-enhanced RSV disease

被引：125

作者：

Openshaw, PJM ^{[1
]}

Culley, FJ ^{[1
]}

Olszewska, W ^{[1
]}

机构：

[1] Univ London Imperial Coll Sci Technol & Med, Natl Heart & Lung Inst, Dept Resp Med, London W2 1PG, England

来源：

VACCINE | 2001年 / 20卷

关键词：

respiratory syncytial virus; Th1/Th2; review; immunopathology; animal models;

D O I：

10.1016/S0264-410X(01)00301-2

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Inducing a strong immune response is an essential aim of vaccination. Although immune responses to virus infections are usually protective, they can also be harmful. The best-documented examples of an immune response increasing disease severity are with dengue, measles and respiratory syncytial virus infections. In the 1960s, administration of formalin-inactivated, tissue culture grown RSV (FI-RSV) was found to induce strong ELISA binding but poor virus-neutralising antibody. Infants given this 'lot 100' vaccine appeared to exhibit an increased rate of RSV infection during subsequent natural RSV outbreaks, Although it has not been possible to exactly delineate the cause of disease enhancement in man, animal models strongly suggest that it was due to strong (and perhaps unbalanced) T cell priming rather than infection-enhancing or sensitising antibody. In animal models, enhanced disease can result from over-exuberant T cell priming which recruits an abundant inflammatory infiltrate in the lung (the nature of which depends on the patterns of cytokines and chemokines produced). Formalin-treated RSV vaccination has been linked specifically to the induction of Th2 cells, which make IL-4 and IL-5 and induce a strong pulmonary eosinophilic response. The vaccine dosing regime and the interval between vaccination and challenge can be critical to the induction of protection or pathology. Defining the correlates of protection and disease enhancement in man is critical to the rational development of effective and protective vaccines against RSV. (C) 2001 Published by Elsevier Science Ltd.

引用

页码：S27 / S31

页数：5

共 32 条

[1] DISTINCT TYPES OF LUNG-DISEASE CAUSED BY FUNCTIONAL SUBSETS OF ANTIVIRAL T-CELLS [J].

ALWAN, WH ;

KOZLOWSKA, WJ ;

OPENSHAW, PJM .

JOURNAL OF EXPERIMENTAL MEDICINE, 1994, 179 (01) :81-89

[2] CYTO-TOXIC T-CELLS CLEAR VIRUS BUT AUGMENT LUNG PATHOLOGY IN MICE INFECTED WITH RESPIRATORY SYNCYTIAL VIRUS [J].

CANNON, MJ ;

OPENSHAW, PJM ;

ASKONAS, BA .

JOURNAL OF EXPERIMENTAL MEDICINE, 1988, 168 (03) :1163-1168

[3] DEVELOPMENT OF CELL-MEDIATED CYTO-TOXIC IMMUNITY TO RESPIRATORY SYNCYTIAL VIRUS IN HUMAN INFANTS FOLLOWING NATURALLY ACQUIRED INFECTION [J].

CHIBA, Y ;

HIGASHIDATE, Y ;

SUGA, K ;

HONJO, K ;

TSUTSUMI, H ;

OGRA, PL .

JOURNAL OF MEDICAL VIROLOGY, 1989, 28 (03) :133-139

[4] PULMONARY HISTOPATHOLOGY INDUCED BY RESPIRATORY SYNCYTIAL VIRUS (RSV) CHALLENGE OF FORMALIN-INACTIVATED RSV-IMMUNIZED BALB/C MICE IS ABROGATED BY DEPLETION OF CD4+ T-CELLS [J].

CONNORS, M ;

KULKARNI, AB ;

FIRESTONE, CY ;

HOLMES, KL ;

MORSE, HC ;

SOTNIKOV, AV ;

MURPHY, BR .

JOURNAL OF VIROLOGY, 1992, 66 (12) :7444-7451

[5] COTTON RATS PREVIOUSLY IMMUNIZED WITH A CHIMERIC RSV FG GLYCOPROTEIN DEVELOP ENHANCED PULMONARY PATHOLOGY WHEN INFECTED WITH RSV, A PHENOMENON NOT ENCOUNTERED FOLLOWING IMMUNIZATION WITH VACCINIA RSV RECOMBINANTS OR RSV [J].

CONNORS, M ;

COLLINS, PL ;

FIRESTONE, CY ;

SOTNIKOV, AV ;

WAITZE, A ;

DAVIS, AR ;

HUNG, PP ;

CHANOCK, RM ;

MURPHY, BR .

VACCINE, 1992, 10 (07) :475-484

[6] CELLULAR-RESPONSE TO RESPIRATORY VIRUSES WITH PARTICULAR REFERENCE TO CHILDREN WITH DISORDERS OF CELL-MEDIATED-IMMUNITY [J].

FISHAUT, M ;

TUBERGEN, D ;

MCINTOSH, K .

JOURNAL OF PEDIATRICS, 1980, 96 (02) :179-186

[7] ALTERED REACTIVITY TO MEASLES VIRUS - ATYPICAL MEASLES IN CHILDREN PREVIOUSLY IMMUNIZED WITH INACTIVATED MEASLES VIRUS VACCINES [J].

FULGINITI, VA ;

ELLER, JJ ;

DOWNIE, AW ;

KEMPE, CH .

JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION, 1967, 202 (12) :1075-+

[8] RISK OF RESPIRATORY SYNCYTIAL VIRUS-INFECTION FOR INFANTS FROM LOW-INCOME FAMILIES IN RELATIONSHIP TO AGE, SEX, ETHNIC-GROUP, AND MATERNAL ANTIBODY LEVEL [J].

GLEZEN, WP ;

PAREDES, A ;

ALLISON, JE ;

TABER, LH ;

FRANK, AL .

JOURNAL OF PEDIATRICS, 1981, 98 (05) :708-715

[9] PROPHYLACTIC ADMINISTRATION OF RESPIRATORY SYNCYTIAL VIRUS IMMUNE GLOBULIN TO HIGH-RISK INFANTS AND YOUNG-CHILDREN [J].

GROOTHUIS, JR ;

SIMOES, EAF ;

LEVIN, MJ ;

HALL, CB ;

LONG, CE ;

RODRIGUEZ, WJ ;

ARROBIO, J ;

MEISSNER, HC ;

FULTON, DR ;

WELLIVER, RC ;

TRISTRAM, DA ;

SIBER, GR ;

PRINCE, GA ;

VANRADEN, M ;

HEMMING, VG .

NEW ENGLAND JOURNAL OF MEDICINE, 1993, 329 (21) :1524-1530

[10] TREATMENT AND PREVENTION OF SEVERE RESPIRATORY SYNCYTIAL VIRUS-INFECTION IN YOUNG-CHILDREN [J].

GROOTHUIS, JR .

CURRENT OPINION IN INFECTIOUS DISEASES, 1995, 8 (03) :206-208

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