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曼氏血吸虫病的诊断:现有方法评估及单虫对检测研究

Diagnosis of schistosomiasis mansoni: an evaluation of existing methods and research towards single worm pair detection.

作者信息

Ogongo Paul, Kariuki Thomas M, Wilson R Alan

机构信息

Department of Tropical Infectious Diseases,Institute of Primate Research,P.O Box 24481,Karen 00502 Nairobi,Kenya.

Biology Department,Centre for Immunology and Infection, University of York,York YO10 5DD,UK.

出版信息

Parasitology. 2018 Sep;145(11):1355-1366. doi: 10.1017/S0031182018000240. Epub 2018 Mar 6.

DOI:10.1017/S0031182018000240
PMID:29506583
Abstract

The inadequacy of current diagnostics for the detection of low worm burdens in humans means that schistosomiasis mansoni is more widespread than previously acknowledged. With the inception of mass drug treatment programmes aimed at disease elimination and the advent of human vaccine trials, the need for more sensitive diagnostics is evident. In this review, we evaluate the merits and limitations of the principal diagnostic methods, namely detection of eggs in faeces; anti-schistosome antibodies in serum; parasite-derived proteins and glycans in serum or urine; parasite DNA in blood, faeces or urine. Only in the baboon model, where actual worm burden is determined by portal perfusion, have faecal smear and circulating antigen methods been calibrated, and shown to have thresholds of detection of 10-19 worm pairs. There is scope for improvement in all the four methods of detection, e.g. the identification of single targets for host antibodies to improve the specificity of enzyme linked immunosorbent assay. Despite recent advances in the definition of the schistosome secretome, there have been no comprehensive biomarker investigations of parasite products in the urine of infected patients. Certainly, the admirable goal of eliminating schistosomiasis will not be achieved unless individuals with low worm burdens can be diagnosed.

摘要

当前用于检测人体低虫负荷的诊断方法存在不足,这意味着曼氏血吸虫病的传播范围比之前公认的更广。随着旨在消除疾病的大规模药物治疗计划的启动以及人类疫苗试验的出现,对更敏感诊断方法的需求显而易见。在本综述中,我们评估了主要诊断方法的优缺点,即粪便中虫卵的检测;血清中抗血吸虫抗体的检测;血清或尿液中寄生虫衍生的蛋白质和聚糖的检测;血液、粪便或尿液中寄生虫DNA的检测。只有在通过门静脉灌注确定实际虫负荷的狒狒模型中,粪便涂片和循环抗原方法才得到校准,并显示检测阈值为10 - 19对虫体。这四种检测方法都有改进的空间,例如鉴定宿主抗体的单一靶点以提高酶联免疫吸附测定的特异性。尽管在血吸虫分泌蛋白组的定义方面最近取得了进展,但尚未对感染患者尿液中的寄生虫产物进行全面的生物标志物研究。当然,除非能够诊断出低虫负荷的个体,否则消除血吸虫病这一令人钦佩的目标将无法实现。

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