| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2031266 | Trends in Biochemical Sciences | 2007 | 6 Pages |
The enormous number of allelic MHC class II glycoproteins provides the immune system with a large set of heterodimeric receptors for the binding of pathogen-derived peptides. How do inherited allo- or isotypic subunits of MHC class II combine to produce such a variety of functional peptide receptors? We propose a new mechanism in which pairing of matched MHC class II α- and β-subunits is coordinated by the invariant chain chaperone. The assembly is proposed to occur in a sequential fashion, with a matched β-chain being selected by the α-chain–invariant chain ‘scaffold’ complex that is formed first. This sequential assembly is a prerequisite for subsequent intracellular transport of the α-chain–invariant chain–β-oligomer and its maturation into a functional peptide receptor.
