Publikation

Role for cathepsin F in invariant chain processing and major histocompatibility complex class II peptide loading by macrophages

Wissenschaftlicher Artikel/Review - 03.04.2000

Bereiche
PubMed

Zitation
Shi G, Bryant R, Riese R, Verhelst S, Driessen C, Li Z, Bromme D, Ploegh H, Chapman H. Role for cathepsin F in invariant chain processing and major histocompatibility complex class II peptide loading by macrophages. The Journal of experimental medicine 2000; 191:1177-86.
Art
Wissenschaftlicher Artikel/Review (Englisch)
Zeitschrift
The Journal of experimental medicine 2000; 191
Veröffentlichungsdatum
03.04.2000
ISSN (Druck)
0022-1007
Seiten
1177-86
Kurzbeschreibung/Zielsetzung

The major histocompatibility complex (MHC) class II-associated invariant chain (Ii) regulates intracellular trafficking and peptide loading of MHC class II molecules. Such loading occurs after endosomal degradation of the invariant chain to a approximately 3-kD peptide termed CLIP (class II-associated invariant chain peptide). Cathepsins L and S have both been implicated in degradation of Ii to CLIP in thymus and peripheral lymphoid organs, respectively. However, macrophages from mice deficient in both cathepsins S and L can process Ii and load peptides onto MHC class II dimers normally. Both processes are blocked by a cysteine protease inhibitor, indicating the involvement of an additional Ii-processing enzyme(s). Comparison of cysteine proteases expressed by macrophages with those found in splenocytes and dendritic cells revealed two enzymes expressed exclusively in macrophages, cathepsins Z and F. Recombinant cathepsin Z did not generate CLIP from Ii-MHC class II complexes, whereas cathepsin F was as efficient as cathepsin S in CLIP generation. Inhibition of cathepsin F activity and MHC class II peptide loading by macrophages exhibited similar specificity and activity profiles. These experiments show that cathepsin F, in a subset of antigen presenting cells (APCs), can efficiently degrade Ii. Different APCs can thus use distinct proteases to mediate MHC class II maturation and peptide loading.