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利用下一代测序技术阐明了美国东部宿主寻找的硬蜱幼虫和成虫中吞噬细胞无形体变体的地理分布变化。

Geographic variation in the distribution of Anaplasma phagocytophilum variants in host-seeking Ixodes scapularis nymphs and adults in the eastern United States elucidated using next generation sequencing.

机构信息

Division of Vector-Borne Diseases, Centers for Disease Control and Prevention, Fort Collins, CO, USA.

Division of Vector-Borne Diseases, Centers for Disease Control and Prevention, Fort Collins, CO, USA.

出版信息

Ticks Tick Borne Dis. 2024 Sep;15(5):102360. doi: 10.1016/j.ttbdis.2024.102360. Epub 2024 May 30.

Abstract

Human anaplasmosis cases, caused by Anaplasma phagocytophilum, are increasing in the United States. This trend is explained, in part, by expansion in the geographic range of the primary vector, Ixodes scapularis. Multiple variants of A. phagocytophilum have been identified in field collected ticks, but only a single variant (human active, or "Ap-ha," variant) has been shown to be pathogenic in humans. Until recently, laboratory methods used to differentiate variants were cumbersome and seldomly used in large scale assessments of the pathogen's geographic distribution. As a result, many surveys reported A. phagocytophilum without segregating variants. Lack of discrimination among A. phagocytophilum variants could lead to overestimation of anaplasmosis risk to humans. Next Generation Sequencing (NGS) assays were recently developed to efficiently detect multiple Ixodes scapularis-borne human pathogens including Ap-ha. In this study, we utilized NGS to detect and differentiate A. phagocytophilum variants (Ap-ha vs. non ha) in host-seeking I. scapularis nymphs and adults collected across 23 states in the eastern United States from 2012 to 2023 as part of national tick surveillance efforts and research studies. Many of the included ticks were tested previously using a TaqMan PCR assay that could detect A. phagocytophilum but could not differentiate variants. We retested A. phagocytophilum infected ticks with NGS to differentiate variants. Anaplasma phagocytophilum (any variant) was identified in 165 (35 %) of 471 counties from which ticks were tested, whereas Ap-ha was detected in 70 (15 %) of 469 counties where variants were differentiated. Both variants were identified in 32 % (n = 40) of 126 counties with either variant detected. Among states where A. phagocytophilum (any variant) was detected, prevalence ranged from 2 % to 19 % in unfed adults and from 0.2 % to 7.8 % in unfed nymphs; prevalence of Ap-ha variant ranged from 0.0 % to 16 % in adults, and 0.0 % to 4.6 % in nymphs.

摘要

人类粒细胞无形体病病例在美国不断增加,这主要是由主要传播媒介肩突硬蜱的地理范围扩大所致。在野外采集的蜱中已鉴定出多种粒细胞无形体变体,但只有一种变体(人类活动型或“Ap-ha”变体)已被证明对人类具有致病性。直到最近,用于区分变体的实验室方法都很繁琐,很少用于大规模评估病原体的地理分布。因此,许多调查报告都没有对粒细胞无形体病进行变体分类。不能区分粒细胞无形体变体可能导致对人类无形体病风险的高估。下一代测序 (NGS) 检测方法最近被开发出来,用于高效检测包括 Ap-ha 在内的多种由肩突硬蜱传播的人类病原体。在这项研究中,我们利用 NGS 检测和区分了在美国东部 23 个州的 2012 年至 2023 年期间宿主寻求的肩突硬蜱幼虫和成虫中的粒细胞无形体变体(Ap-ha 与非 ha),这是国家蜱监测工作和研究的一部分。许多包含的蜱之前都使用 TaqMan PCR 检测方法进行了测试,该方法可以检测到粒细胞无形体病,但无法区分变体。我们使用 NGS 对感染粒细胞无形体病的蜱进行了重新测试,以区分变体。在 471 个接受测试的县中,有 165 个(35%)县检测到任何变体的粒细胞无形体病,而在 469 个区分变体的县中,有 70 个(15%)县检测到 Ap-ha。在 32%(n=40)的同时检测到两种变体的县中发现了这两种变体。在检测到粒细胞无形体病(任何变体)的州中,未进食的成虫的流行率在 2%至 19%之间,未进食的幼虫的流行率在 0.2%至 7.8%之间;Ap-ha 变体的流行率在成虫中为 0.0%至 16%,在幼虫中为 0.0%至 4.6%。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe57/11774202/d7f47813b5f9/nihms-2048925-f0001.jpg

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