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“增效策略”影响猫α疱疹病毒 1 的复制,以及感染细胞的代谢。

A "plus one" strategy impacts replication of felid alphaherpesvirus 1, and and the metabolism of coinfected feline cells.

机构信息

Asia-Pacific Centre for Animal Health, Melbourne Veterinary School, University of Melbourne, Melbourne, Victoria, Australia.

Metabolomics Australia, Bio21 Institute, University of Melbourne, Melbourne, Victoria, Australia.

出版信息

mSystems. 2024 Oct 22;9(10):e0085224. doi: 10.1128/msystems.00852-24. Epub 2024 Sep 24.

Abstract

Coinfections are known to play an important role in disease progression and severity. Coinfections are common in cats, but no coinfection studies have investigated the dynamics between feline viral and bacterial pathogens. In this study, we performed co-culture and invasion assays to investigate the ability of common feline bacterial respiratory pathogens, and , to replicate in and invade into Crandell-Rees feline kidney cells. We subsequently investigated how coinfection of these feline cells with each bacterium ( or ) and the common feline viral pathogen, felid alphaherpesvirus 1 (FHV-1), affects replication of each agent in this cell culture system. We also investigated the metabolic impact of each co-pathogen using metabolomic analysis of infected and coinfected cells. was able to invade and replicate in CRFKs, while had little capacity to invade. During coinfection, FHV-1 replication was minimally affected by the presence of either bacterial pathogen, but bacterial replication kinetics were more affected, particularly in . Both and replicated to higher levels in the presence of a secondary pathogen. Coinfections resulted in reprogramming of the glycolysis pathway, the pentose phosphate pathway, and the tricarboxylic acid cycle. The distinct metabolic profiles of coinfected cells compared to those of cells infected with just one of these three pathogens, as well as the impact of coinfections on viral or bacterial load, suggest strong interactions between these three pathogens and possible synergistic mechanisms enhancing virulence that need further investigation.IMPORTANCEIn the natural world, respiratory pathogens coexist within their hosts, but their dynamics and interactions remain largely unexplored. Herpesviruses, mycoplasmas, and chlamydias are common and significant causes of acute and chronic respiratory and system disease in animals and people, and these diseases are increasingly found to be polymicrobial. This study investigates how coinfection of feline cells between three respiratory pathogens of cats impact each other as well as the host innate metabolic response to infection. Each of these pathogens have been implicated in the induction of feline upper respiratory tract disease in cats, which is the leading cause of euthanasia in shelters. Understanding how coinfection impacts co-pathogenesis and host responses is critical for improving disease management.

摘要

共感染已知在疾病进展和严重程度中起重要作用。共感染在猫中很常见,但没有针对猫的病毒和细菌病原体之间共感染动态的共感染研究。在这项研究中,我们进行了共培养和侵袭测定,以研究常见的猫科细菌性呼吸道病原体和对 Crandell-Rees 猫肾细胞的复制和侵袭能力。随后,我们研究了这些猫科细胞与每种细菌(或)和常见的猫科病毒病原体,猫α疱疹病毒 1(FHV-1)共感染时如何影响该细胞培养系统中每种试剂的复制。我们还使用感染和共感染细胞的代谢组学分析研究了每种共病原体的代谢影响。能够入侵并在 CRFK 中复制,而则很少有能力入侵。在共感染期间,FHV-1 的复制受两种细菌病原体的存在影响很小,但细菌复制动力学受到的影响更大,特别是在。在次要病原体存在的情况下,和均以更高水平复制。共感染导致糖酵解途径、戊糖磷酸途径和三羧酸循环的重新编程。与仅感染这三种病原体之一的细胞相比,共感染细胞的代谢特征明显不同,以及共感染对病毒或细菌负荷的影响,表明这三种病原体之间存在强烈相互作用,并可能存在增强毒力的协同机制,需要进一步研究。

重要性
在自然界中,呼吸道病原体在宿主中共存,但它们的动态和相互作用在很大程度上仍未得到探索。疱疹病毒、支原体和衣原体是动物和人类急性和慢性呼吸道和系统疾病的常见且重要原因,并且这些疾病越来越多地被发现是多微生物的。这项研究调查了猫的三种呼吸道病原体之间的猫科细胞共感染如何相互影响以及宿主先天对感染的代谢反应。这些病原体中的每一种都被牵连到猫的上呼吸道疾病的诱导中,这是收容所中安乐死的主要原因。了解共感染如何影响共发病和宿主反应对于改善疾病管理至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06a2/11495031/57dbf3401c2d/msystems.00852-24.f001.jpg

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