Salmonella enterica subspecies 1 serovar Typhimurium is a principal cause of human enterocolitis. For unknown reasons, in mice serovar Typhimurium does not provoke intestinal inflammation but rather targets the gut-associated lymphatic tissues and causes a systemic typhoid-like infection. The lack of a suitable murine model has limited the analysis of the pathogenetic mechanisms of intestinal salmonellosis. We describe here how streptomycin-pretreated mice provide a mouse model for serovar Typhimurium colitis. Serovar Typhimurium colitis in streptomycin-pretreated mice resembles many aspects of the human infection, including epithelial ulceration, edema, induction of intercellular adhesion molecule 1, and massive infiltration of PMN/ CD18 ؉ cells. This pathology is strongly dependent on protein translocation via the serovar Typhimurium SPI1 type III secretion system. Using a lymphotoxin -receptor knockout mouse strain that lacks all lymph nodes and organized gut-associated lymphatic tissues, we demonstrate that Peyer's patches and mesenteric lymph nodes are dispensable for the initiation of murine serovar Typhimurium colitis. Our results demonstrate that streptomycin-pretreated mice offer a unique infection model that allows for the first time to use mutants of both the pathogen and the host to study the molecular mechanisms of enteric salmonellosis.Salmonella spp. are gram-negative enterobacteria that cause diseases ranging from a self-limiting enterocolitis to systemic infection (typhoid fever). Salmonella enterica serovar Typhimurium evokes a common form of nonsystemic enterocolitis in humans and cattle, whereas mice are intrinsically resistant to serovar Typhimurium enterocolitis (68,81). Although resistant to intestinal salmonellosis, certain susceptible mouse strains that carry mutations in the NRAMP gene develop a disease similar to typhoid fever (30,75).After oral infection of susceptible mice, serovar Typhimurium does not replicate efficiently in the intestine but penetrates the epithelial barrier by invasion of M cells (12,41,64) or (less efficiently) by transport via CD18 ϩ /dendritic cells (67, 80) and possibly by penetration of enterocytes (72). After penetration of the epithelial barrier, Salmonella spp. colonize Peyer's patches and mesenteric lymph nodes and then spread to the liver and spleen, and the mice finally succumb to systemic infection (10,35,75,81). However, mice show few signs of the intestinal inflammation observed in cattle or humans.Due to the lack of a versatile animal model, much less is known about the mechanisms of the enteric salmonellosis (21,33,62,75,81). To overcome these limitations, the pathogenesis of enteric salmonellosis has been studied by extrapolating data from tissue culture (review by Galan [26]) or from intestinal organ culture (1) or by infection of ligated murine and rabbit ileal loops (11,12,20,41,63,64). However, it remains unclear how these results relate to enteric salmonellosis.For this reason, bovine infection models with serovar Typhimurium (and serovar D...
