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用于评估免疫健全小鼠模型对宫本疏螺旋体感染的研究

Evaluation of Immunocompetent Mouse Models for Borrelia miyamotoi Infection.

作者信息

Armstrong Brittany A, Brandt Kevin S, Goodrich Irina, Gilmore Robert D

机构信息

Bacterial Diseases Branch, Division of Vector-Borne Diseases, National Center for Emerging and Zoonotic Infectious Diseases, Centers for Disease Control and Prevention, Fort Collins, Colorado, USA.

出版信息

Microbiol Spectr. 2023 Jan 30;11(2):e0430122. doi: 10.1128/spectrum.04301-22.

Abstract

Borrelia miyamotoi is a relapsing fever spirochete that is harbored by spp. ticks and is virtually uncharacterized, compared to other relapsing fever vectored by spp. ticks. There is not an immunocompetent mouse model for studying B. miyamotoi infection or for transmission in the vector-host cycle. Our goal was to evaluate B. miyamotoi infections in multiple mouse breeds/strains as a prelude to the ascertainment of the best experimental infection model. Two B. miyamotoi strains, namely, LB-2001 and CT13-2396, as well as three mouse models, namely, CD-1, C3H/HeJ, and BALB/c, were evaluated. We were unable to observe B. miyamotoi LB-2001 spirochetes in the blood via darkfield microscopy or to detect DNA via real-time PCR post needle inoculation in the CD-1 and C3H/HeJ mice. However, LB-2001 DNA was detected via real-time PCR in the blood of the BALB/c mice after needle inoculation, although spirochetes were not observed via microscopy. CD-1, C3H/HeJ, and BALB/c mice generated an antibody response to B. miyamotoi LB-2001 following needle inoculation, but established infections were not detected, and the I. scapularis larvae failed to acquire spirochetes from the exposed CD-1 mice. In contrast, B. miyamotoi CT13-2396 was visualized in the blood of the CD-1 and C3H/HeJ mice via darkfield microscopy and detected by real-time PCR post needle inoculation. Both mouse strains seroconverted. However, no established infection was detected in the mouse organs, and the I. scapularis larvae failed to acquire after feeding on CT13-2396 exposed CD-1 or C3H/HeJ mice. These findings underscore the challenges in establishing an experimental B. miyamotoi infection model in immunocompetent laboratory mice. Borrelia miyamotoi is a causative agent of hard tick relapsing fever, was first identified in the early 1990s, and was characterized as a human pathogen in 2011. Unlike other relapsing fever species, B. miyamotoi spread by means of ticks. The relatively recent recognition of this human pathogen means that B. miyamotoi is virtually uncharacterized, compared to other species. Currently there is no standard mouse-tick model with which to study the interactions of the pathogen within its vector and hosts. We evaluated two B. miyamotoi isolates and three immunocompetent mouse models to identify an appropriate model with which to study tick-host-pathogen interactions. With the increased prevalence of human exposure to ticks, having an appropriate model with which to study B. miyamotoi will be critical for the future development of diagnostics and intervention strategies.

摘要

宫本疏螺旋体是一种回归热螺旋体,由硬蜱属蜱虫携带,与其他由硬蜱属蜱虫传播的回归热相比,其特征几乎未被阐明。目前尚无用于研究宫本疏螺旋体感染或其在媒介-宿主循环中传播的免疫健全小鼠模型。我们的目标是评估多种小鼠品种/品系中的宫本疏螺旋体感染情况,以此作为确定最佳实验感染模型的前奏。我们评估了两种宫本疏螺旋体菌株,即LB-2001和CT13-2396,以及三种小鼠模型,即CD-1、C3H/HeJ和BALB/c。通过暗视野显微镜,我们未能在CD-1和C3H/HeJ小鼠经针刺接种后的血液中观察到宫本疏螺旋体LB-2001螺旋体,也未能通过实时PCR检测到其DNA。然而,在针刺接种后,虽然通过显微镜未观察到螺旋体,但在BALB/c小鼠的血液中通过实时PCR检测到了LB-2001 DNA。CD-1、C3H/HeJ和BALB/c小鼠在针刺接种后对宫本疏螺旋体LB-2001产生了抗体反应,但未检测到已建立的感染,肩胛硬蜱幼虫也未能从暴露的CD-1小鼠身上获取螺旋体。相比之下,通过暗视野显微镜在CD-1和C3H/HeJ小鼠经针刺接种后的血液中观察到了宫本疏螺旋体CT13-2396,并通过实时PCR检测到了该菌。两种小鼠品系均出现了血清转化。然而,在小鼠器官中未检测到已建立的感染,肩胛硬蜱幼虫在取食经CT13-2396暴露的CD-1或C3H/HeJ小鼠后也未能获取该菌。这些发现凸显了在免疫健全的实验室小鼠中建立宫本疏螺旋体实验感染模型的挑战。宫本疏螺旋体是硬蜱传播回归热的病原体,于20世纪90年代初首次被发现,并于2011年被确定为人类病原体。与其他回归热螺旋体物种不同,宫本疏螺旋体通过硬蜱传播。对这种人类病原体的认识相对较新,这意味着与其他物种相比,宫本疏螺旋体的特征几乎未被阐明。目前尚无标准的小鼠-蜱模型来研究该病原体在其媒介和宿主之间的相互作用。我们评估了两种宫本疏螺旋体分离株和三种免疫健全的小鼠模型,以确定一个合适的模型来研究蜱-宿主-病原体之间的相互作用。随着人类接触硬蜱的频率增加,拥有一个合适的模型来研究宫本疏螺旋体对于未来诊断和干预策略的发展至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45f0/10100797/b97efbde6d11/spectrum.04301-22-f001.jpg

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