Jelocnik Martina, Forshaw David, Cotter Jennifer, Roberts Danny, Timms Peter, Polkinghorne Adam
Institute for Health and Biomedical Innovation, Queensland University of Technology, Kelvin Grove, Queensland 4059, Australia.
BMC Vet Res. 2014 May 29;10:121. doi: 10.1186/1746-6148-10-121.
Despite its global recognition as a ruminant pathogen, cases of Chlamydia pecorum infection in Australian livestock are poorly documented. In this report, a C. pecorum specific Multi Locus Sequence Analysis scheme was used to characterise the C. pecorum strains implicated in two cases of sporadic bovine encephalomyelitis confirmed by necropsy, histopathology and immunohistochemistry. This report provides the first molecular evidence for the presence of mixed infections of C. pecorum strains in Australian cattle.
Affected animals were two markedly depressed, dehydrated and blind calves, 12 and 16 weeks old. The calves were euthanized and necropsied. In one calf, a severe fibrinous polyserositis was noted with excess joint fluid in all joints whereas in the other, no significant lesions were seen. No gross abnormalities were noted in the brain of either calf. Histopathological lesions seen in both calves included: multifocal, severe, subacute meningoencephalitis with vasculitis, fibrinocellular thrombosis and malacia; diffuse, mild, acute interstitial pneumonia; and diffuse, subacute epicarditis, severe in the calf with gross serositis. Immunohistochemical labelling of chlamydial antigen in brain, spleen and lung from the two affected calves and brain from two archived cases, localised the antigen to the cytoplasm of endothelium, mesothelium and macrophages. C. pecorum specific qPCR, showed dissemination of the pathogen to multiple organs. Phylogenetic comparisons with other C. pecorum bovine strains from Australia, Europe and the USA revealed the presence of two genetically distinct sequence types (ST). The predominant ST detected in the brain, heart, lung and liver of both calves was identical to the C. pecorum ST previously described in cases of SBE. A second ST detected in an ileal tissue sample from one of the calves, clustered with previously typed faecal bovine isolates.
This report provides the first data to suggest that identical C. pecorum STs may be associated with SBE in geographically separated countries and that these may be distinct from those found in the gastrointestinal tract. This report provides a platform for further investigations into SBE and for understanding the genetic relationships that exist between C. pecorum strains detected in association with other infectious diseases in livestock.
尽管衣原体作为反刍动物病原体已得到全球公认,但澳大利亚家畜中感染鹦鹉热衣原体的病例记录甚少。在本报告中,采用了一种鹦鹉热衣原体特异性多位点序列分析方案,对两例经尸检、组织病理学和免疫组织化学确诊的散发性牛脑脊髓炎病例中涉及的鹦鹉热衣原体菌株进行了特征分析。本报告首次提供了澳大利亚牛群中存在鹦鹉热衣原体菌株混合感染的分子证据。
患病动物为两头12周龄和16周龄的犊牛,表现为极度抑郁、脱水和失明。犊牛实施安乐死后进行了尸检。其中一头犊牛出现严重的纤维素性多浆膜炎,所有关节均有过多的关节液,而另一头犊牛未发现明显病变。两头犊牛的脑部均未发现明显异常。两头犊牛的组织病理学病变包括:多灶性、严重、亚急性脑膜脑炎伴血管炎、纤维细胞性血栓形成和软化;弥漫性、轻度、急性间质性肺炎;以及弥漫性、亚急性心外膜炎,在有明显浆膜炎的犊牛中较为严重。对两头患病犊牛的脑、脾和肺以及两例存档病例的脑进行衣原体抗原免疫组织化学标记,将抗原定位在内皮细胞、间皮细胞和巨噬细胞的细胞质中。鹦鹉热衣原体特异性定量PCR显示病原体扩散到多个器官。与来自澳大利亚、欧洲和美国的其他鹦鹉热衣原体牛菌株进行系统发育比较,发现存在两种基因不同的序列类型(ST)。在两头犊牛的脑、心、肺和肝中检测到的主要ST与先前在散发性牛脑脊髓炎病例中描述的鹦鹉热衣原体ST相同。在其中一头犊牛的回肠组织样本中检测到的第二种ST与先前分型的粪便牛分离株聚集在一起。
本报告首次提供数据表明,相同的鹦鹉热衣原体ST可能与地理上分隔的国家中的散发性牛脑脊髓炎有关,并且这些ST可能与在胃肠道中发现的ST不同。本报告为进一步研究散发性牛脑脊髓炎以及了解与家畜其他传染病相关的鹦鹉热衣原体菌株之间存在的遗传关系提供了一个平台。