C. Veltkamp et al., Continuous stimulation by normal luminal bacteria is essential for the development and perpetuation of colitis in Tg is an element of 26 mice, GASTROENTY, 120(4), 2001, pp. 900-913
Background & Aims: Normal resident bacteria are required for development of
colitis in several rodent models. We determined whether bacterial stimulat
ion is necessary for both induction and perpetuation of mucosal inflammatio
n and T-cell activation in Tg epsilon 26 mice, in which transplantation of
wild-type bone marrow (BM double right arrow Tg epsilon 26) causes colitis
under specific pathogen-free (SPF) conditions. Methods: BM from (C57BL/6 X
CBA/J) Fl mice was transplanted into germfree (GF) or SPF Tg epsilon 26 mic
e. Mesenteric lymph node (MLN) cells from these mice were then transferred
into SPF or GF recipients. Colitis and activation of MLN cells were measure
d by histologic scores, membrane marker analysis, and intracellular cytokin
e staining. Cytokine secretion by MLN cells stimulated by anti-CD3 or by lu
minal or epithelial antigens was measured by ELISA. Results: Colitis did no
t develop when BM was transferred into GF recipient mice (BM double right a
rrow GF Tg epsilon 26). T lymphocytes that secreted interferon gamma upon a
ctivation were present in the MLN of BM double right arrow GF Tg epsilon 26
mice, albeit in lower frequency than in control BM double right arrow SPF
Tg epsilon 26 mice, Furthermore, transfer of MLN cells from BM double right
arrow SPF Tg epsilon 26 mice into SPF Tg epsilon 26 recipients induced act
ive colitis, but not if the same cells were transferred into GF Tg epsilon
26 recipients. Although CD4 T cells were detected in the colonic mucosa of
GF recipients, no inflammation was observed for at least 31 weeks. In a rec
iprocal experiment, MLN cells from BM double right arrow GF Tg epsilon 26 m
ice without colitis transferred disease to SPF Tge26 recipients within 2-4
weeks. Conclusions: Activated T cells are present in the mucosa of BM doubl
e right arrow GF Tg epsilon 26 mice but are incapable of inducing disease u
nless colonic bacteria are present. Moreover, pathogenic T cells require th
e continuous presence of colonic bacteria to sustain colitis.