感染O104:H4疫情菌株和肠出血性大肠杆菌O157:H7的悉生仔猪的临床和免疫学发现比较
Comparison of clinical and immunological findings in gnotobiotic piglets infected with O104:H4 outbreak strain and EHEC O157:H7.
作者信息
Wöchtl Bettina, Gunzer Florian, Gerner Wilhelm, Gasse Hagen, Koch Michaela, Bagó Zoltán, Ganter Martin, Weissenböck Herbert, Dinhopl Nora, Coldewey Sina M, von Altrock Alexandra, Waldmann Karl-Heinz, Saalmüller Armin, Zimmermann Kurt, Steinmann Jörg, Kehrmann Jan, Klein-Hitpass Ludger, Blom Jochen, Ehricht Ralf, Engelmann Ines, Hennig-Pauka Isabel
机构信息
University Clinic for Swine, Department for Farm Animals and Veterinary Public Health, University of Veterinary Medicine Vienna, Veterinärplatz 1, 1220 Vienna, Austria.
Institute of Medical Microbiology and Hygiene, Faculty of Medicine Carl Gustav Carus, TU Dresden, Fetscherstrasse 74, 01307 Dresden, Germany.
出版信息
Gut Pathog. 2017 May 25;9:30. doi: 10.1186/s13099-017-0179-8. eCollection 2017.
BACKGROUND
Shiga toxin (Stx) producing () (STEC) is the most frequent cause of diarrhoea-positive haemolytic uraemic syndrome (D + HUS) in humans. In 2011, a huge outbreak with an STEC O104:H4 strain in Germany highlighted the limited possibilities for causative treatment of this syndrome. The responsible STEC strain was found to combine Stx production with adherence mechanisms normally found in enteroaggregative (EAEC). Pathotypes of evolve and can exhibit different adhesion mechanisms. It has been shown previously that neonatal gnotobiotic piglets are susceptible for infection with STEC, such as STEC O157:H7 as well as for EAEC, which are considered to be the phylogenetic origin of O104:H4. This study was designed to characterise the host response to infection with the STEC O104:H4 outbreak strain in comparison to an STEC O157:H7 isolate by evaluating clinical parameters (scoring) and markers of organ dysfunction (biochemistry), as well as immunological (flow cytometry, assessment of cytokines/chemokines and acute phase proteins) and histological alterations (light- and electron microscopy) in a gnotobiotic piglet model of haemolytic uraemic syndrome.
RESULTS
We observed severe clinical symptoms, such as diarrhoea, dehydration and neurological disorders as well as attaching-and-effacing lesions (A/E) in the colon in STEC O157:H7 infected piglets. In contrast, STEC O104:H4 challenged animals exhibited only mild clinical symptoms including diarrhoea and dehydration and HUS-specific/severe histopathological, haematological and biochemical alterations were only inconsistently presented by individual piglets. A specific adherence phenotype of STEC O104:H4 could not be observed. Flow cytometric analyses of lymphocytes derived from infected animals revealed an increase of natural killer cells (NK cells) during the course of infection revealing a potential role of this subset in the anti-bacterial activity in STEC disease.
CONCLUSIONS
Unexpectedly, O104:H4 infection caused only mild symptoms and minor changes in histology and blood parameters in piglets. Outcome of the infection trial does not reflect O104:H4 associated human disease as observed during the outbreak in 2011. The potential role of cells of the innate immune system for STEC related disease pathogenesis should be further elucidated.
背景
产志贺毒素大肠杆菌(STEC)是人类腹泻阳性溶血尿毒综合征(D + HUS)最常见的病因。2011年,德国爆发的一起由STEC O104:H4菌株引起的大规模疫情凸显了该综合征病因治疗方法的局限性。人们发现,引发疫情的STEC菌株既能产生志贺毒素,又具备通常在肠集聚性大肠杆菌(EAEC)中发现的黏附机制。大肠杆菌的致病型会发生演变,并可能表现出不同的黏附机制。此前研究表明,新生无菌仔猪易感染STEC,如STEC O157:H7,也易感染EAEC,而EAEC被认为是O104:H4的系统发育起源。本研究旨在通过评估临床参数(评分)和器官功能障碍标志物(生化指标),以及免疫指标(流式细胞术、细胞因子/趋化因子评估和急性期蛋白)和组织学改变(光学显微镜和电子显微镜观察),在溶血尿毒综合征的无菌仔猪模型中,比较STEC O104:H4疫情菌株与STEC O157:H7分离株感染后的宿主反应。
结果
我们观察到,感染STEC O157:H7的仔猪出现了严重的临床症状,如腹泻、脱水和神经紊乱,以及结肠中的紧密黏附性损伤(A/E)。相比之下,感染STEC O104:H4的动物仅表现出轻度临床症状,包括腹泻和脱水,且个别仔猪仅偶尔出现HUS特异性/严重的组织病理学、血液学和生化改变。未观察到STEC O104:H4的特定黏附表型。对感染动物的淋巴细胞进行流式细胞术分析发现,感染过程中自然杀伤细胞(NK细胞)数量增加,这表明该细胞亚群在STEC疾病的抗菌活性中可能发挥作用。
结论
出乎意料的是,O104:H4感染在仔猪中仅引起轻微症状以及组织学和血液参数的微小变化。感染试验的结果并未反映出2011年疫情期间观察到的与O104:H4相关的人类疾病情况。固有免疫系统细胞在STEC相关疾病发病机制中的潜在作用有待进一步阐明。
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