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乌干达伊丽莎白女王国家公园周边牛群中未被识别的SAT 1型口蹄疫病毒传播情况。

Unrecognized circulation of SAT 1 foot-and-mouth disease virus in cattle herds around Queen Elizabeth National Park in Uganda.

作者信息

Dhikusooka Moses Tefula, Ayebazibwe Chrisostom, Namatovu Alice, Belsham Graham J, Siegismund Hans Redlef, Wekesa Sabenzia Nabalayo, Balinda Sheila Nina, Muwanika Vincent B, Tjørnehøj Kirsten

机构信息

National Animal Disease Diagnostics and Epidemiology Centre, Ministry of Agriculture Animal Industry and Fisheries, P. O. Box 513, Entebbe, Uganda.

Department of Biotechnical and Diagnostic Sciences, College of Veterinary Medicine, Animal Resources and Biosecurity, Makerere University, P. O. Box 7062, Kampala, Uganda.

出版信息

BMC Vet Res. 2016 Jan 6;12:5. doi: 10.1186/s12917-015-0616-1.

Abstract

BACKGROUND

Foot-and-mouth disease (FMD) is endemic in Uganda in spite of the control measures used. Various aspects of the maintenance and circulation of FMD viruses (FMDV) in Uganda are not well understood; these include the role of the African buffalo (Syncerus caffer) as a reservoir for FMDV. To better understand the epidemiology of FMD at the livestock-wildlife-interface, samples were collected from young, unvaccinated cattle from 24 pastoral herds that closely interact with wildlife around Queen Elizabeth National Park in Uganda, and analysed for evidence of FMDV infection.

RESULTS

In total, 37 (15%) of 247 serum samples had detectable antibodies against FMDV non-structural proteins (NSPs) using a pan-serotypic assay. Within these 37 sera, antibody titres ≥ 80 against the structural proteins of serotypes O, SAT 1, SAT 2 and SAT 3 were detected by ELISA in 5, 7, 4 and 3 samples, respectively, while neutralizing antibodies were only detected against serotype O in 3 samples. Two FMDV isolates, with identical VP1 coding sequences, were obtained from probang samples from clinically healthy calves from the same herd and are serotype SAT 1 (topotype IV (EA-I)). Based on the VP1 coding sequences, these viruses are distinct from previous cattle and buffalo SAT 1 FMDV isolates obtained from the same area (19-30% nucleotide difference) and from the vaccine strain (TAN/155/71) used within Uganda (26% nucleotide difference). Eight herds had only one or a few animals with antibodies against FMDV NSPs while six herds had more substantial evidence of prior infection with FMDV. There was no evidence for exposure to FMDV in the other ten herds.

CONCLUSIONS

The two identical SAT 1 FMDV VP1 sequences are distinct from former buffalo and cattle isolates from the same area, thus, transmission between buffalo and cattle was not demonstrated. These new SAT 1 FMDV isolates differed significantly from the vaccine strain used to control Ugandan FMD outbreaks, indicating a need for vaccine matching studies. Only six herds had clear serological evidence for exposure to O and SAT 1 FMDV. Scattered presence of antibodies against FMDV in other herds may be due to the occasional introduction of animals to the area or maternal antibodies from past infection and/or vaccination. The evidence for asymptomatic FMDV infection has implications for disease control strategies in the area since this obstructs early disease detection that is based on clinical signs in FMDV infected animals.

摘要

背景

尽管采取了防控措施,但口蹄疫在乌干达仍呈地方性流行。口蹄疫病毒(FMDV)在乌干达的维持和传播的各个方面尚未得到充分了解;其中包括非洲水牛(非洲草原水牛)作为FMDV储存宿主的作用。为了更好地了解家畜-野生动物界面处口蹄疫的流行病学,从乌干达伊丽莎白女王国家公园周边与野生动物密切互动的24个游牧牛群中未接种疫苗的幼牛采集样本,并分析FMDV感染的证据。

结果

使用泛血清型检测方法,在247份血清样本中,共有37份(15%)检测到针对FMDV非结构蛋白(NSPs)的可检测抗体。在这37份血清中,通过ELISA分别在5份、7份、4份和3份样本中检测到针对O型、SAT 1型、SAT 2型和SAT 3型结构蛋白的抗体滴度≥80,而仅在3份样本中检测到针对O型的中和抗体。从同一牛群临床健康犊牛的探咽样本中获得了两个具有相同VP1编码序列的FMDV分离株,它们为SAT 1型(拓扑型IV(EA-I))。基于VP1编码序列,这些病毒与之前从同一地区获得的牛和水牛SAT 1 FMDV分离株不同(核苷酸差异为19 - 30%),也与乌干达使用的疫苗株(TAN/155/71)不同(核苷酸差异为26%)。8个牛群中只有一两只动物具有针对FMDV NSPs的抗体,而6个牛群有更确凿的FMDV既往感染证据。其他10个牛群没有接触FMDV的证据。

结论

两个相同的SAT 1 FMDV VP1序列与同一地区以前的水牛和牛分离株不同,因此,未证明水牛和牛之间存在传播。这些新的SAT 1 FMDV分离株与用于控制乌干达口蹄疫疫情的疫苗株有显著差异,表明需要进行疫苗匹配研究。只有6个牛群有明确的血清学证据表明接触过O型和SAT 1型FMDV。其他牛群中FMDV抗体的零星存在可能是由于偶尔有动物进入该地区,或者是过去感染和/或接种疫苗产生的母源抗体所致。无症状FMDV感染的证据对该地区的疾病控制策略具有影响,因为这阻碍了基于FMDV感染动物临床症状的早期疾病检测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0728/4704403/e556e4de09f7/12917_2015_616_Fig1_HTML.jpg

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