TY - JOUR
T1 - A point mutation in HLA-A*0201 results in failure to bind the TAP complex and to present virus-derived peptides to CTL
AU - Peace-Brewer, Amy L.
AU - Tussey, Lynda G.
AU - Matsui, Masanori
AU - Li, Guoxuan
AU - Quinn, Daniel G.
AU - Frelinger, Jeffrey A.
N1 - Funding Information:
The authors would like to thank A. J. Zajac for critical reading of the manuscript and Dr. F. Brodsky, Dr. B. Koppelman, and Dr. P. Cresswell for the gifts of UCSF2 and R.RING4C, respectively. D. G. Q. is supported by National Institutes of Health training grant AI 07273. This work was supported by National Institutes of Health grants AI 20288 and AI 28324.
PY - 1996/5
Y1 - 1996/5
N2 - Mutating the HLA-A*0201 heavy chain from threonine to lysine at position 134 (T134K) results in a molecule that presents exogenous peptide, but cannot present endogenously derived antigen. This is reflected in diminished cell surface expression and altered intracellular trafficking of T134K. The failure of T134K to present endogenous antigen can be overcome by using an ER targeting sequence, suggesting that the antigen presentation defect is restricted to TAP-dependent peptide loading. The ability of T134K to load peptide in a TAP-dependent manner is dramatically reduced compared with HLA-A*0201. By coimmunoprecipitation there is no detectable association of the T134K molecule with the TAP complex. Thus, T134K selectively affects TAP association and peptide loading, suggesting a requirement for the direct interaction of MHC class I heavy chain and the TAP complex for efficient presentation of endogenous antigen.
AB - Mutating the HLA-A*0201 heavy chain from threonine to lysine at position 134 (T134K) results in a molecule that presents exogenous peptide, but cannot present endogenously derived antigen. This is reflected in diminished cell surface expression and altered intracellular trafficking of T134K. The failure of T134K to present endogenous antigen can be overcome by using an ER targeting sequence, suggesting that the antigen presentation defect is restricted to TAP-dependent peptide loading. The ability of T134K to load peptide in a TAP-dependent manner is dramatically reduced compared with HLA-A*0201. By coimmunoprecipitation there is no detectable association of the T134K molecule with the TAP complex. Thus, T134K selectively affects TAP association and peptide loading, suggesting a requirement for the direct interaction of MHC class I heavy chain and the TAP complex for efficient presentation of endogenous antigen.
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U2 - 10.1016/S1074-7613(00)80416-1
DO - 10.1016/S1074-7613(00)80416-1
M3 - Article
C2 - 8630735
AN - SCOPUS:0030152620
VL - 4
SP - 505
EP - 514
JO - Immunity
JF - Immunity
SN - 1074-7613
IS - 5
ER -