Paneth's disease.

Jan Wehkamp, Eduard F Stange

Robert-Bosch-Krankenhaus Stuttgart, Auerbachstr 110, 7076 Stuttgart, Germany.

Journal Article: Journal of Crohn s and Colitis (impact factor: 1.73). 11/2010; 4(5):523-31. DOI: 10.1016/j.crohns.2010.05.010

Abstract

In about 70% of patients Crohn's disease (CD) affects the small intestine. This disease location is stable over time and associated with a genetic background different from isolated colonic disease. A characteristic feature of small intestinal host defense is the presence of Paneth cells at the bottom of the crypts of Lieberkühn. These cells produce different broad spectrum antimicrobial peptides (AMPs) most abundantly the α-defensins HD-5 and -6 (DEFA5 und DEFA6). In small intestinal Crohn's disease both these PC products are specifically reduced. As a functional consequence, ileal extracts from Crohn's disease patients are compromised in clearing bacteria and enteroadherent E. coli colonize the mucosa. Mechanisms for defective antimicrobial Paneth cell function are complex and include an association with a NOD2 loss of function mutation, a disturbance of the Wnt pathway transcription factor TCF7L2 (also known as TCF4), the autophagy factor ATG16L1, the endosomal stress protein XBP1, the toll-like receptor TLR9, the calcium mediated potassium channel KCNN4 as well as mutations or inactivation of HD5. Thus we conclude that small intestinal Crohn's disease is most likely a complex disease of the Paneth cell: Paneth's disease.

Source: PubMed

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Keywords

characteristic feature
 
colonic disease
 
complex disease
 
Crohn's disease patients
 
different broad spectrum antimicrobial peptides
 
endosomal stress protein XBP1
 
enteroadherent E. coli colonize
 
function mutation
 
functional consequence
 
genetic background different
 
mutations
 
Paneth's disease
 
patients Crohn's disease
 
PC products
 
potassium channel KCNN4
 
small intestinal Crohn's disease
 
small intestinal host defense
 
small intestine
 
toll-like receptor TLR9
 
α-defensins HD-5