首页> 外文OA文献 >A prototype recombinant-protein based chlamydia pecorum vaccine results in reduced chlamydial burden and less clinical disease in free-ranging koalas (Phascolarctos cinereus)
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A prototype recombinant-protein based chlamydia pecorum vaccine results in reduced chlamydial burden and less clinical disease in free-ranging koalas (Phascolarctos cinereus)

机译:一种基于重组蛋白的原型衣原体衣原体疫苗可减少散养考拉(Phascolarctos cinereus)的衣原体负担并减少临床疾病

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摘要

Diseases associated with infection are a major cause of decline in koala populations in Australia. While koalas in care can generally be treated, a vaccine is considered the only option to effectively reduce the threat of infection and disease at the population level. In the current study, we vaccinated 30 free-ranging koalas with a prototype vaccine consisting of a recombinant chlamydial MOMP adjuvanted with an immune stimulating complex. An additional cohort of 30 animals did not receive any vaccine and acted as comparison controls. Animals accepted into this study were either uninfected (Chlamydia PCR negative) at time of initial vaccination, or infected (C. pecorum positive) at either urogenital (UGT) and/or ocular sites (Oc), but with no clinical signs of chlamydial disease. All koalas were vaccinated/sampled and then re-released into their natural habitat before re-capturing and re-sampling at 6 and 12 months. All vaccinated koalas produced a strong immune response to the vaccine, as indicated by high titres of specific plasma antibodies. The incidence of new infections in vaccinated koalas over the 12-month period post-vaccination was slightly less than koalas in the control group, however, this was not statistically significant. Importantly though, the vaccine was able to significantly reduce the infectious load in animals that were Chlamydia positive at the time of vaccination. This effect was evident at both the Oc and UGT sites and was stronger at 6 months than at 12 months post-vaccination. Finally, the vaccine was also able to reduce the number of animals that progressed to disease during the 12-month period. While the sample sizes were small (statistically speaking), results were nonetheless striking. This study highlights the potential for successful development of a Chlamydia vaccine for koalas in a wild setting.
机译:与感染有关的疾病是澳大利亚考拉种群数量下降的主要原因。虽然护理中的考拉通常可以治疗,但疫苗被认为是在人群水平上有效减少感染和疾病威胁的唯一选择。在当前的研究中,我们用原型疫苗接种了30只自由放养的考拉疫苗,该疫苗由重组衣原体MOMP辅以免疫刺激复合物组成。另一组30只动物没有接受任何疫苗,并作为对照。接受本研究的动物在初次接种疫苗时未感染(衣原体PCR阴性),或在泌尿生殖道(UGT)和/或眼位(Oc)感染(C. pecorum阳性),但没有衣原体疾病的临床症状。对所有考拉进行了疫苗接种/采样,然后在释放之前进行了释放,并在6和12个月时重新采样。如高滴度的特异性血浆抗体所示,所有接种的考拉都对疫苗产生强烈的免疫反应。在接种疫苗后的12个月内,接种疫苗的考拉中新感染的发生率略低于对照组中的考拉,但是,这在统计学上没有统计学意义。但是重要的是,该疫苗能够显着降低接种疫苗时衣原体呈阳性的动物的感染量。这种效果在Oc和UGT部位均明显,并且在接种后6个月比在接种12个月时强。最后,该疫苗还能够减少在12个月内发展为疾病的动物数量。尽管样本量很小(从统计意义上来说),但结果仍然惊人。这项研究强调了在野生环境中成功开发用于考拉的衣原体疫苗的潜力。

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