Date

2013-8

Type

Article

Journal title

PUBMed

Issue

Vol. 32 No. 0

Author(s)

Hanedi A

Pages

5563 - 5573

Abstract

The classical nuclear factor-kappaB (NF-kB) signaling pathway has been shown to be important in a number of models of inflammation-associated cancer. In a mouse model of Helicobacter-induced gastric cancer, impairment of classical NF-kB signaling in the gastric epithelium led to the development of increased preneoplastic pathology, however the role of specific NF-kB proteins in Helicobacter-associated gastric cancer development remains poorly understood. To investigate this C57BL/6, Nfkb1/, Nfkb2/ and c-Rel/ mice were infected with Helicobacter felis for 6 weeks or 12 months. Bacterial colonization, gastric atrophy and preneoplastic changes were assessed histologically and cytokine expression was assessed by qPCR. Nfkb1/ mice developed spontaneous gastric atrophy when maintained for 12 months in conventional animal house conditions. They also developed more pronounced gastric atrophy after short-term H. felis colonization with a similar extent of preneoplasia to wild-type (WT) mice after 12 months. c-Rel/ mice developed a similar degree of gastric atrophy to WT mice; 3 of 6 of these animals also developed lymphoproliferative lesions after 12 months of infection. Nfkb2/ mice developed minimal gastric epithelial pathology even 12 months after H. felis infection. These findings demonstrate that NF-kB1- and NF-kB2-mediated signaling pathways differentially regulate the epithelial consequences of H. felis infection in the stomach, while c-Rel-mediated signaling also appears to modulate the risk of lymphomagenesis in gastric mucosa-associated lymphoid tissue.

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