Page 297 - Veterinary Immunology, 10th Edition
P. 297

project out of the ends. Because of this, MHC class I molecules only
  VetBooks.ir  bind peptides containing about nine amino acids. In order to do so,

               these peptides must bulge out in the middle. Overall, however, the
               antigen-binding sites on class II and class I molecules function in a

               similar manner.
                  The processing of endogenous peptides differs from the
               processing of exogenous peptides. Living cells continually break up
               and recycle the proteins they produce. As a result, abnormal

               proteins are removed, regulatory peptides do not accumulate, and
               amino acids are recycled. As a first step, the protein must be tagged.
               To do this, ubiquitin, a small protein found in all eukaryote cells,
               attaches to lysine residues in target proteins. Additional ubiquitins

               then attach to the protein-bound ubiquitin so that several ubiquitin
               molecules are linked like beads on a string. A chain of four
               ubiquitin molecules appears to be optimal for processing. These
               polyubiquinated proteins are marked for destruction since they are

               recognized by enzyme complexes called proteasomes.
                  Proteasomes are tubular molecular complexes whose function is
               to degrade ubiquinated proteins. They consist of an inner channel
               that contains the protease activity and two outer rings that regulate

               which proteins can enter and be destroyed. Ubiquitinated proteins
               bind to the outer rings, the tagged protein is unfolded, and the
               ubiquitin is released and reused. The unfolded protein is inserted
               into the inner channel, where it is broken into 8- to 15-amino acid

               long peptides (like a meat grinder). Most of these peptide fragments
               are recycled into new proteins. For about 1 in 1 million molecules,
               however, the peptides are rescued from further breakup by
               attachment to transporter proteins. Two transporter proteins are

               used: TAP-1 and TAP-2 (TAP stands for transporter for antigen
               processing). TAP-1 and TAP-2 form a heterodimer that binds
               peptide fragments and transports them into endosomes. Ideally, an
               8- to 10-amino acid peptide precisely fits the binding site on the

               heterodimer. In this case the peptide is loaded into the TAP dimer,
               carried to a newly formed MHC, and if it fits the MHC antigen-
               binding site, it is transferred. Once loaded on the MHC, the MHC-
               peptide complex is carried to the cell surface by its normal secretory
               pathway where it is displayed for many hours.

                                                      6
                  A cell can express about 10  MHC-peptide complexes at any one




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