首页> 外文期刊>Comparative Medicine >Establishing the Median Infectious Dose and Characterizing the Clinical Manifestations of Mouse, Rat, Cow, and Human Corynebacterium bovis Isolates in Select Immunocompromised Mouse Strains
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Establishing the Median Infectious Dose and Characterizing the Clinical Manifestations of Mouse, Rat, Cow, and Human Corynebacterium bovis Isolates in Select Immunocompromised Mouse Strains

机译:确定小鼠、大鼠、牛和人牛棒状杆菌分离株在特定免疫功能低下小鼠品系中的中位感染剂量并表征临床表现

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Corynebacterium bovis (Cb), the cause of hyperkeratotic dermatitis in various immunocompromised mouse strains, signifi-cantly impacts research outcomes if infected mice are used. Although Cb has been isolated from a variety of species, including mice, rats, cows, and humans, little is known about the differences in the infectivity and clinical disease that are associated with specific Cb isolates. The infectious dose that colonized 50 of the exposed population (ID50) and any associated clinical disease was determined in athymic nude mice (Hsd:Athymic Nude-Foxn1nu) inoculated with Cb isolates collected from mice (n = 5), rat (n = 1), cow (n = 1), and humans (n = 2) The same parameters were also determined for 2 of the mouse isolates in 2 furred immunocompromised mouse strains (NSG NOD.Cg-PrkdcscidIl2rgtm1Wjl/Sz and NSG-S NOD.Cg-PrkdcscidIl2rgtm1Wjl Tg(CMV-IL3,CSF2,KITLG)1Eav/MloySzJ). To determine the ID50, mice (n = 6/dose; 3 of each sex) were inoculated topically in 10-fold increments ranging from 1 to 108 bacteria. Mice were scored daily for 14 days for the severity of clinical signs. On days 7 and 14 after inoculation, buccal and dorsal skin swabs were evaluated by aerobic culture to determine infection status. The mouse isolates yielded lower ID50 values (58 to 1000 bacteria) than did the bovine (6460 to 7498 bacteria) and rat (10,000 bacteria) isolates. Human isolates did not colonize mice or cause disease. Mouse isolates produced clinical disease of vary-ing severity in nude mice. Despite significant immunodeficiency, furred NSG and NSG-S mice required a 1000-to 3000-fold higher inoculum for colonization than did athymic nude mice. Once colonized, clinically detectable hyperkeratosis did not develop in the haired strains until 18 to 22 d after inoculation, whereas athymic nude mice that developed clinically detect-able disease showed hyperkeratosis between 6 and 14 d after inoculation. In conclusion, there are significant differences in Cb's ID50, disease course, and severity of clinical signs between Cb isolates and among immunodeficient mouse strains.
机译:牛棒状杆菌 (Cb) 是各种免疫功能低下小鼠品系角化过度性皮炎的原因,如果使用受感染的小鼠,会显着影响研究结果。尽管已从多种物种(包括小鼠、大鼠、奶牛和人类)中分离出 Cb,但对与特定 Cb 分离株相关的传染性和临床疾病的差异知之甚少。在接种从小鼠 (n = 5)、大鼠 (n = 1)、牛 (n = 1) 和人类 (n = 2) 收集的 Cb 分离株的无胸腺裸鼠 (Hsd:Athymic Nude-Foxn1nu) 中测定定植于 50% 暴露人群 (ID50) 和任何相关临床疾病的感染剂量 2 种毛皮免疫功能低下小鼠品系 (NSG [NOD.Cg-PrkdcscidIl2rgtm1Wjl/Sz] 和 NSG-S [NOD.Cg-PrkdcscidIl2rgtm1Wjl Tg(CMV-IL3,CSF2,KITLG)1Eav/MloySzJ])。为了确定ID50,小鼠(n = 6 /剂量;每性别3只)以10倍的增量局部接种,范围为1至108个细菌。每天对小鼠进行临床症状严重程度评分,持续 14 天。接种后第 7 天和第 14 天,通过需氧培养评估颊侧和背部皮肤拭子以确定感染状态。小鼠分离株产生的ID50值(58至1000个细菌)低于牛(6460至7498个细菌)和大鼠(10,000个细菌)分离株。人类分离株不会定植小鼠或引起疾病。小鼠分离株在裸鼠中产生不同严重程度的临床疾病。尽管存在明显的免疫缺陷,但毛茸茸的NSG和NSG-S小鼠需要比无胸腺裸鼠高1000至3000倍的接种量进行定植。一旦定植,直到接种后 18 至 22 天,毛菌株中才出现临床可检测到的角化过度,而发生临床可检测疾病的无胸腺裸鼠在接种后 6 至 14 天之间表现出角化过度。总之,Cb分离株和免疫缺陷小鼠品系之间在Cb的ID50、病程和临床症状严重程度方面存在显著差异。

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