Cathepsin V is involved in the degradation of invariant chain in human thymus and is overexpressed in myasthenia gravis.

نویسندگان

  • Eva Tolosa
  • Weijie Li
  • Yoshiyuki Yasuda
  • Wolfgang Wienhold
  • Lisa K Denzin
  • Alfred Lautwein
  • Christoph Driessen
  • Petra Schnorrer
  • Ekkehard Weber
  • Stefan Stevanovic
  • Raffael Kurek
  • Arthur Melms
  • Dieter Bromme
چکیده

Stepwise degradation of the invariant chain (Ii) is required for the binding of antigenic peptides to MHC class II molecules. Cathepsin (Cat) L in the murine thymus and Cat S in peripheral APCs have both been implicated in the last step of Ii degradation that gives rise to the class II-associated invariant chain peptides (CLIP). Cat V has been recently described as highly homologous to Cat L and exclusively expressed in human thymus and testis, but with no mouse orthologue. We report that Cat V is the dominant cysteine protease in cortical human thymic epithelial cells, while Cat L and Cat S seem to be restricted to dendritic and macrophage-like cells. Active Cat V in thymic lysosomal preparations was demonstrated by active-site labeling. Recombinant Cat V was capable of converting Ii into CLIP efficiently, suggesting that Cat V is the protease that controls the generation of alphabeta-CLIP complexes in the human thymus, in analogy to Cat L in mouse. Comparison of Cat V expression between thymi from patients with myasthenia gravis and healthy controls revealed a significantly higher expression level in the pathological samples, suggesting a potential involvement of this protease in the immunopathogenesis of myasthenia gravis, an autoimmune disease almost invariably associated with thymic pathology.

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عنوان ژورنال:
  • The Journal of clinical investigation

دوره 112 4  شماره 

صفحات  -

تاریخ انتشار 2003