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成年小鼠的空肠弯曲菌实验性感染。

Experimental Campylobacter jejuni infection of adult mice.

作者信息

Blaser M J, Duncan D J, Warren G H, Wang W L

出版信息

Infect Immun. 1983 Feb;39(2):908-16. doi: 10.1128/iai.39.2.908-916.1983.

DOI:10.1128/iai.39.2.908-916.1983
PMID:6832823
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC348033/
Abstract

HA-ICR adult mice were studied to develop an animal model for Campylobacter jejuni enteritis in humans. Fecal and ileal cultures made by selective and nonselective methods showed that C. jejuni and related organisms are not bowel commensals. Intragastric feeding of 10(8) CFU of three different strains of C. jejuni produced infection in 100% of the animals, and infection rates were dose dependent. Pretreatment with antibiotics or opiates was not necessary to induce infection. Fresh isolates and strains passed on artificial media yielded similar infection rates. Infected mice did not show signs of illness, but transient bacteremia within 10 min of oral infection was observed in nearly 100%. The small intestine was the principal target organ, with epithelial inflammation seen 48 h after infection. Control mice of four species had undetectable serum immunoglobulin G antibody specific for the infecting strain, but infected mice showed peak titers at 1 week with rapid decline. Immunoglobulin M titers rose minimally, and immunoglobulin A titers did not rise. Infected mice uniformly became chronic asymptomatic excretors, shedding 10(4) to 10(6) CFU/g of feces; a minority were biliary carriers. Intestine carriage was most pronounced in the stomach and proximal small intestine. Because this experimental infection led to bacteremia, transient pathological changes, and immunoglobulin G titer rises, this model may be useful for evaluating the effects of prophylactic and therapeutic interventions.

摘要

对HA - ICR成年小鼠进行研究,以建立人类空肠弯曲菌肠炎的动物模型。通过选择性和非选择性方法进行的粪便和回肠培养表明,空肠弯曲菌及相关微生物并非肠道共生菌。给动物经胃投喂10⁸CFU的三种不同空肠弯曲菌菌株,100%的动物发生感染,且感染率呈剂量依赖性。诱导感染无需使用抗生素或阿片类药物进行预处理。新鲜分离株和在人工培养基上传代的菌株产生的感染率相似。受感染小鼠未表现出疾病迹象,但在口服感染后10分钟内,近100%的小鼠出现短暂菌血症。小肠是主要靶器官,感染后48小时可见上皮炎症。四种对照小鼠对感染菌株的血清免疫球蛋白G抗体检测不到,但受感染小鼠在1周时出现抗体滴度峰值,随后迅速下降。免疫球蛋白M滴度略有上升,免疫球蛋白A滴度未上升。受感染小鼠均成为慢性无症状排泄者,粪便中排出10⁴至10⁶CFU/g;少数为胆汁携带者。肠道携带在胃和近端小肠最为明显。由于这种实验性感染导致了菌血症、短暂的病理变化和免疫球蛋白G滴度升高,该模型可能有助于评估预防和治疗干预措施的效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe79/348033/cf8206d7575d/iai00143-0435-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe79/348033/cf8206d7575d/iai00143-0435-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe79/348033/cf8206d7575d/iai00143-0435-a.jpg

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本文引用的文献

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Experimental Shigella infections. II. Characteristics of a fatal enteric infection in guinea pigs following the subcutaneous inoculation of carbon tetrachloride.实验性志贺氏菌感染。II. 皮下接种四氯化碳后豚鼠发生致命性肠道感染的特征
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