| Primary Source |
[7] Reits, E. et al. Peptide diffusion, protection, and degradation in nuclear and cytoplasmic compartments before antigen presentation by MHC class I. Immunity 18, 97–108 (2003) [10] Neefjes, J. J., Momburg, F. & Hammerling, G. J. Selective and ATP-dependent translocation of peptides by the MHCencoded transporter. Science 261, 769–771 (1993) [66] Princiotta, M. F. et al. Quantitating protein synthesis, degradation, and endogenous antigen processing. Immunity 18, 343–354 (2003) [91] Gakamsky, D. M., Davis, D. M., Strominger, J. L. & Pecht, I. Assembly and dissociation of human leukocyte antigen (HLA)-A2 studied by real-time fluorescence resonance energy transfer. Biochemistry 39, 11163–11169 (2000)PubMed ID12530979, 8342042, 12648452, 10998256
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| Comments |
P.959 left column 2nd paragraph: "While each ribosome is producing a protein every 90 seconds, each proteasome is degrading 2.25 substrates per minute. Proteasomes are probably not working at full capacity though. Two independent
studies estimate that proteasomes are acting at ~20% of their total capacity in unstressed cells [refs 69, 70], indicating a Vmax of 11 substrates per proteasome per minute, or five seconds per substrate, which is 20 times faster
than the rate of protein synthesis (see table 2 for kinetics)." See note beneath table |