The Immunodominant, L super(d)-Restricted T Cell Response to Hepatitis B Surface Antigen (HBsAg) Efficiently Suppresses T Cell Priming to Multiple D super(d)-, K super(d)-, and K super(b)-Restricted HBsAg Epitopes

MHC-I-restricted CTL responses of H-2 super(d) (L super(d+) or L super(d-)) and F sub(1) H-2 super(dxb) mice to hepatitis B surface Ag (HBsAg) are primed by either DNA vaccines or HBsAg particles. The D super(d)/S sub(201 209) and K super(d)/S sub(199 208) epitopes are generated by processing endoge...

Full description

Saved in:
Bibliographic Details
Published inThe Journal of immunology (1950) Vol. 168; no. 12; pp. 6253 - 6262
Main Authors Schirmbeck, R, Stober, D, Kholy, SE, Riedl, P, Reimann, J
Format Journal Article
LanguageEnglish
Published 15.06.2002
Online AccessGet full text

Cover

More Information
Summary:MHC-I-restricted CTL responses of H-2 super(d) (L super(d+) or L super(d-)) and F sub(1) H-2 super(dxb) mice to hepatitis B surface Ag (HBsAg) are primed by either DNA vaccines or HBsAg particles. The D super(d)/S sub(201 209) and K super(d)/S sub(199 208) epitopes are generated by processing endogenous HBsAg; the K super(b)/S sub(208 215) epitope is generated by processing exogenous HbsAg; and the L super(d)/S sub(28 39) epitope is generated by exogenous as well as endogenous processing of HBsAg. DNA vaccination primed high numbers of CTL specific for the L super(d)/S sub(28 39) HBsAg epitope, low numbers of CTL specific for the D super(d)/S sub(201 209) or K super(d)/S sub(199 208) HBsAg epitopes in BALB/c mice, and high numbers of D super(d)/S sub(201 209)- and K super(d)/S sub(199 208)-specific CTL in congenic H-2 super(d)/L super(d-) dm2 mice. In F sub(1) super(dxb) mice, the K super(d)-, D super(d)-, and K super(b)-restricted CTL responses to HBsAg were strikingly suppressed in the presence but efficiently elicited in the absence of L super(d)/S sub(28 39)-specific CTL. Once primed, the K super(d)- and D super(d)-restricted CTL responses to HBsAg were resistant to suppression by immunodominant L super(d)/S sub(28 39)-specific CTL. The L super(d)-restricted immunodominant CTL reactivity to HBsAg can thus suppress priming to multiple alternative epitopes of HBsAg, independent of the processing pathway that generates the epitope, of the background of the mouse strain used, and of the presence/absence of different allelic variants of the K and D MHC class I molecules.
Bibliography:ObjectType-Article-2
SourceType-Scholarly Journals-1
content type line 23
ObjectType-Feature-1
ISSN:0022-1767