TY - JOUR
T1 - Presentation of out-of-frame peptide/MHC class I complexes by a novel translation initiation mechanism
AU - Malarkannan, Subramaniam
AU - Horng, Tiffany
AU - Shih, Patty P.
AU - Schwab, Susan
AU - Shastri, Nilabh
N1 - Funding Information:
We thank Federico Gonzalez, Vu Nguyen, Minh Nguyen, Van Nguyen, and Hussein Hadeiba for their excellent technical support. This study was supported by National Institutes of Health grants (N. S.). S. M. was supported in part by the University of California Cancer Research Coordination Committee and T. H. by the Beckman undergraduate scholarship. T. H. and P. S. were also supported by the Undergraduate Biology Fellows Program of the Howard Hughes Medical Institute. S. S. is a predoctoral fellow of the National Science Foundation. We are grateful to U. Rajbhandary (MIT), A. Kaji (U. Pennsylvania), D. Peabody (Univ. New Mexico), R. Boeck (Univ. California), and other members of our laboratory for discussions.
PY - 1999/6
Y1 - 1999/6
N2 - Immune surveillance by CD8 T cells requires that peptides derived from intracellular proteins be presented by MHC class I molecules on the target cell surface. Interestingly, MHC molecules can also present peptides encoded in alternate translational reading frames, some even without conventional AUG initiation codons. Using T cells to measure expression of MHC bound peptides, we identified the non-AUG translation initiation codons and established that their activity was at the level of translational rather than DNA replication or transcription mechanisms. This translation mechanism decoded the CUG initiation codon not as the canonical methionine but as the leucine residue, and its activity was independent of upstream translation initiation events. Naturally processed peptide/MHC complexes can thus arise from 'noncoding' mRNAs via a novel translation initiation mechanism.
AB - Immune surveillance by CD8 T cells requires that peptides derived from intracellular proteins be presented by MHC class I molecules on the target cell surface. Interestingly, MHC molecules can also present peptides encoded in alternate translational reading frames, some even without conventional AUG initiation codons. Using T cells to measure expression of MHC bound peptides, we identified the non-AUG translation initiation codons and established that their activity was at the level of translational rather than DNA replication or transcription mechanisms. This translation mechanism decoded the CUG initiation codon not as the canonical methionine but as the leucine residue, and its activity was independent of upstream translation initiation events. Naturally processed peptide/MHC complexes can thus arise from 'noncoding' mRNAs via a novel translation initiation mechanism.
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U2 - 10.1016/S1074-7613(00)80067-9
DO - 10.1016/S1074-7613(00)80067-9
M3 - Article
C2 - 10403643
AN - SCOPUS:0033151592
SN - 1074-7613
VL - 10
SP - 681
EP - 690
JO - Immunity
JF - Immunity
IS - 6
ER -