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对引起人类管圆线虫病的 物种遗传多样性的见解及其对分子鉴定和诊断的意义。 (注:原文中“ spp.”表述不完整,这里按原样翻译)

Insights into the genetic diversity of spp. causing human angiostrongyliasis and implications for molecular identification and diagnosis.

作者信息

Chan Abigail Hui En, Kaenkaew Chanisara, Pakdee Wallop, Thaenkham Urusa

机构信息

Department of Helminthology, Faculty of Tropical Medicine, Mahidol University, Bangkok, Thailand.

出版信息

Food Waterborne Parasitol. 2024 May 22;35:e00230. doi: 10.1016/j.fawpar.2024.e00230. eCollection 2024 Jun.

Abstract

and are known human pathogens responsible for eosinophilic angiostrongyliasis and abdominal angiostrongyliasis, respectively. Humans are accidental hosts, where infection occurs through the consumption of the infective larva stage 3 in intermediate or paratenic hosts. The proven method for abdominal angiostrongyliasis diagnosis is the histological examination through tissue biopsy, while the diagnosis of eosinophilic angiostrongyliasis is the detection of larva in the cerebrospinal fluid. As there is molecular evidence of cryptic species within and lineages, along with morphological similarities within both lineages, accurate species identification and disease diagnosis may be challenging. Moreover, species within the lineages share similar intermediate and definitive hosts and geographic distribution. For example, both and (a closely related species in lineage) overlap in their geographic distribution in Southeast Asia. Additionally, variations in the molecular makeup of and lineages may impact the pathogenicity, infectivity, and disease severity of angiostrongyliasis. Understanding of the genetic diversity of both lineages is a cornerstone for improved diagnosis and disease intervention, especially in a changing global environment. To shed light and provide insights into the genetic diversity of the lineages causing human angiostrongyliasis, we aim to present an up-to-date review of the studies conducted and genetic markers used for and lineages. The implications for accurate molecular identification and diagnosis of human angiostrongyliasis are also discussed.

摘要

[物种名称1]和[物种名称2]分别是已知的导致嗜酸性粒细胞性血管圆线虫病和腹部血管圆线虫病的人类病原体。人类是偶然宿主,感染是通过食用中间宿主或转续宿主中的感染性三期幼虫而发生的。腹部血管圆线虫病诊断的已证实方法是通过组织活检进行组织学检查,而嗜酸性粒细胞性血管圆线虫病的诊断是检测脑脊液中的幼虫。由于在[物种名称1]和[物种名称2]谱系内存在隐存种的分子证据,以及两个谱系内的形态学相似性,准确的物种鉴定和疾病诊断可能具有挑战性。此外,谱系内的物种共享相似的中间宿主和终末宿主以及地理分布。例如,[物种名称1]和[物种名称2]([物种名称1]谱系中的一个近缘物种)在东南亚的地理分布上重叠。此外,[物种名称1]和[物种名称2]谱系的分子组成变化可能会影响血管圆线虫病的致病性、传染性和疾病严重程度。了解两个谱系的遗传多样性是改善诊断和疾病干预的基石,尤其是在不断变化的全球环境中。为了阐明并深入了解导致人类血管圆线虫病的[物种名称1]和[物种名称2]谱系的遗传多样性,我们旨在对已进行的研究以及用于[物种名称1]和[物种名称2]谱系的遗传标记进行最新综述。还讨论了对人类血管圆线虫病准确分子鉴定和诊断的意义。

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