Human cytotoxic T cells stimulated by antigen on dendritic cells recognize the N, SH, F, M, 22K, and 1b proteins of respiratory syncytial virus.

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J Virol. 1992 April; 66(4): 2102-2110

Human cytotoxic T cells stimulated by antigen on dendritic cells recognize the N, SH, F, M, 22K, and 1b proteins of respiratory syncytial virus.

A H Cherrie, K Anderson, G W Wertz and P J Openshaw

Department of Medicine, St. Mary's Hospital Medical School, London, United Kingdom.

ABSTRACT

We examined the human cytotoxic T-cell repertoire of nine adultsto 9 of the 10 proteins of respiratory syncytial (RS) virus.Peripheral blood mononuclear cells from normal adults were stimulatedwith RS virus in vitro. The resulting polyclonal cultures weretested for lysis of B-lymphoblastoid cell lines infected withrecombinant vaccinia viruses expressing each of nine individualRS virus proteins. The use of peripheral blood dendritic cellsto present antigen gave more easily reproducible results overa shorter culture period than conventional methods. The sixRS virus proteins most strongly recognized were the nucleoproteinN (nine of nine donors with greater than 10% above backgroundlysis; P = 0.0004), the surface proteins SH (six of nine donors;P = 0.002) and F (five of nine donors; P = 0.008), the matrixproteins M (five of nine donors; P = 0.004) and 22K (three ofnine donors; P = 0.01) and the nonstructural protein 1b (sixof nine donors; P = 0.004). There was no significant recognitionof the major surface glycoprotein G (two of nine donors), theinternal phosphoprotein P (one of nine donors), or the nonstructuralprotein 1c (one of nine donors). Recognition was major histocompatibilitycomplex class I restricted, but no association between majorhistocompatibility complex phenotype and protein specificityof T cells was seen. Recognition of F and 22K appeared to beassociated with recent infection indicated by increased levelsof anti-RS virus immunoglobulin G antibody in serum measuredby enzyme-linked immunosorbent assay. Since cytotoxic T-cellrecognition of RS virus proteins has been demonstrated to beimportant in the clearance of virus from infected hosts, theN, M, SH, 1b, F, and 22K proteins should be considered potentialvaccine components.

J Virol. 1992 April; 66(4): 2102-2110

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