Evaluation of two monkey species (Macaca mulatta and Macaca fascicularis) as possible models for human Helicobacter pylori disease

Euler, Arthur R.; Zurenko, Gary E.; Moe, James B.; Ulrich, Roger G.; Yagi, Yoshihiko

doi:10.1128/jcm.28.10.2285-2290.1990

Cited by 57 publications

(30 citation statements)

References 17 publications

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“…Experimental models of H pylori infection have been described using gnotobiotic piglets, 3 euthymic germ free mice, 4 athymic nude mice, 5 and monkeys. 6 The Mongolian gerbil also appears to be an appropriate animal model of H pylori infection. [7][8][9] Gastrointestinal diseases such as gastritis, gastric ulcer, and adenocarcinoma that mimic human H pylori infection can be studied in the Mongolian gerbil model.…”

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Helicobacter pylori infection induces duodenitis and superficial duodenal ulcer in mongolian gerbils

et al. 2003

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Background: There is no direct evidence for an animal model of Helicobacter pylori induced duodenal ulcer. Aim: In this study we evaluated the roles of bacterial strain and age of experimental animals in induction of duodenitis and duodenal ulcer in Mongolian gerbils after H pylori infection. Methods: Specific pathogen free Mongolian gerbils were inoculated orally with three bacterial strains (H pylori ATCC 43504, TN2GF4, and K-6, a clinical isolate from a patient with gastric cancer in our clinic). These strains have both the cagA gene and VacA. Five week old gerbils were used to emulate prematurity infection and 14 week old animals were used as mature test subjects. Animals were observed for 12 weeks after inoculation. Interleukin 8 (IL-8) production in gastric epithelial cells (MKN74) after coculture with the H pylori strains was measured by ELISA. Results: Gastritis and gastric ulcers were found in all gerbils infected with the three strains. However, duodenitis and gastric metaplasia were seen more frequently in gerbils infected with TN2GF4 and K-6 strains than in the ATCC 43504 infected or control groups (p<0.05). Superficial duodenal ulcers with severe duodenitis and gastric metaplasia were found in two gerbils inoculated at 14 weeks with the TN2GF4 strain but none at five weeks. The TN2GF4 strain stimulated significantly higher levels of IL-8 than ATCC 43504 and K6 strains (p=0.0039). Conclusions: When injected into adult Mongolian gerbils, a specific strain (TN2GF4) of H pylori can induce duodenitis with gastric metaplasia and superficial duodenal ulcers. Induction of duodenal ulcer in an animal model fulfills the requirements of Koch's postulates for establishing a role for H pylori as a causative agent.

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Helicobacter pylori infection induces duodenitis and superficial duodenal ulcer in mongolian gerbils

et al. 2003

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“…Several trials were done to establish animal models of H. pylon infection. The infection was successful in monkeys (9) and piglets (8, 22, 24) but unsuccessful in mice and rats (4, 6). These facts correlated well with our present data on H. pylon adhesion to the antral epithelial cells isolated from these anirpals.…”

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confidence: 99%

“…Other attempts were made to clarify the pathogenesis by establishing animal models of H. pylon infection. These studies revealed that, while establishment of H. pylon infection was unsuccessful in germfree rodents such as mice and rats (4,6), the bacteria could colonize the stomachs of monkeys (9), gnotobiotic piglets (8,22,24), gnotobiotic dogs (31), nude mice (21), and Mongolian gerbils (37) when the animals were orally challenged. However, these studies did not reveal why the bacteria colonized the stomachs of some * Corresponding author.…”

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Adhesion of Helicobacter pylori to gastric epithelial cells in primary cultures obtained from stomachs of various animals

1993

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Of 35 strains of Helicobacter pyloni tested, 5 were found to adhere well to HEp-2 cells. We selected three of these adhesive strains and four from the remaining strains to examine their ability to adhere to gastric epithelial cells in primary cultures obtained by collagenase digestion of stomachs from mice, rats, Mongolian gerbils, guinea pigs, pigs, and cynomolgus monkeys. The three adhesive strains adhered well to epithelial cells from monkey and pig gastric antra. The adhesion was inhibited by incubating the bacterial cells with fetuin, and this inhibition was further confirmed by the binding of gold-labeled fetuin to the surface of the adhesive strains. However, these adhesive strains only weakly adhered to fundic epithelial cells from monkeys and pigs and to gastric epithelial cells from the other animals. As for the four strains poorly adhesive to HEp-2 cells, they adhered weakly to gastric epithelial cells from all of the animals tested. They had higher hemagglutination titers than the adhesive strains, showing that there was no correlation between hemagglutination titers and the ability to adhere to gastric cells. Taking the similarities of human and monkey or pig stomachs into consideration, these results suggest that the primary target cell of H. pylon in colonization in human stomachs is the antral epithelial cell and that the putative adhesin involved in adhesion has affinity for fetuin.

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“…The primate model was described as a good model for human gastroduodenal diseases such as those induced by Helicobacter pylori (Euler et al 1990;Dubois et al 1996). Nevertheless, the ethical limitations linked to the use of primates, the cost to be supported and the difficulties to breed and to handle these species are limitations to carry out extensive investigations.…”

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Preclinical Assessment of Gastrooesophageal Tolerance of the New Antiosteoporotic Drug Strontium Ranelate: An Endoscopic Study in Monkeys

Fisch¹,

Attia²,

Dargent³

et al. 2006

Basic Clin Pharma Tox

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This study was aimed at evaluating the digestive tolerance of the new antiosteoporotic drug, strontium ranelate, and to compare it to that of another strontium salt, strontium chloride (SrCl 2 ). Strontium ranelate, SrCl 2 , or placebo were administered orally (capsules) to 3 groups of 2 male and 2 female cynomolgus monkeys (Macaca fascicularis) once a day for 7 days at a dose of 2 g/day, which is the recommended therapeutic dose in man. Endoscopic examination of the oesophagus, the stomach and the first part of the duodenum was performed on fasted animals approximately 3 hr after the first (Day 1) and last dosing (Day 7), and, on Day 8 and Day 14 in case of lesions on Day 7. Strontium ranelate did not induce any acute or subchronic toxic effect on the gastric mucosa, the oesophagus and the first part of the duodenum. On the contrary, acute and superficial damages were noted on all animals receiving SrCl 2 such as haemorrhagic and erosive lesions (formation of an ulcer in one male and a marked congestive antritis in one female). These effects were reversible after cessation of treatment. The microscopic examination of biopsies sampled at the site of gastric lesions revealed moderate granulocyte infiltration, indicating a local irritating origin of the lesions. Strontium ranelate by oral route is safe for the gastric mucosa while SrCl 2 induced superficial and reversible lesions.Safety and tolerance are particularly key issues with treatments against post-menopausal osteoporosis, which are mainly administered over a long period of time to elderly people. The currently available antiosteoporotic drugs, such as bisphosphonates, induce gastrointestinal side-effects when given by oral route, from abdominal pain (Maconi & Porro 1995;Sherman & Bini 1999) to gastric ulcer (Graham et al. 1997), which can affect a reliable compliance.Strontium ranelate is composed of two stable strontium atoms and of an organic moiety, ranelic acid. Strontium ranelate has been shown to prevent bone loss by decreasing osteoclast resorption and by inducing osteoblast formation in vivo (Marie et al. 1993) and in vitro (Canalis et al. 1996;Baron & Tsouderos 2002;Takahashi et al. 2003), and has therefore been developed for the treatment of post-menopausal osteoporosis.An endoscopic study was set up to assess in the cynomolgus monkey (Macaca fascicularis) the strontium ranelate tolerance on the gastrooesophageal tract, by comparison with strontium chloride (SrCl 2 ), a common strontium salt.Until now, the gastric tolerability of strontium chloride was not known. However, other chloride-containing chemicals, such as NaCl and KCl, when used as hypertonic solutions, have ulcerogenic activity in animals (Barkin et al.Author for correspondence: Isabelle Dupin-Roger, Servier, 6 place des Pléiades, 92415 Courbevoie Cedex, France (fax π33 1 5572 6436, e-mail philippe.halbout/fr.netgrs.com).1983; Takeuchi et al. 1986). This effect have raised the possibility of gastric intolerance with SrCl 2 .The primate model was described as a good model f...

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Evaluation of two monkey species (Macaca mulatta and Macaca fascicularis) as possible models for human Helicobacter pylori disease

Cited by 57 publications

References 17 publications

Helicobacter pylori infection induces duodenitis and superficial duodenal ulcer in mongolian gerbils

Helicobacter pylori infection induces duodenitis and superficial duodenal ulcer in mongolian gerbils

Adhesion of Helicobacter pylori to gastric epithelial cells in primary cultures obtained from stomachs of various animals

Preclinical Assessment of Gastrooesophageal Tolerance of the New Antiosteoporotic Drug Strontium Ranelate: An Endoscopic Study in Monkeys

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