Influenza D

  • 文章类型: Journal Article
    背景:流感病毒可引起人畜共患感染,从而构成公共卫生风险。甲型和乙型流感病毒的监测是在全球范围内进行的;然而,关于流感C和D病毒的信息是有限的。几个国家已经对人类丙型流感病毒进行了纵向监测,但是没有对人类的D型流感病毒进行长期监测。因此,与D型流感病毒相关的公共卫生风险仍然未知。
    方法:我们建立了双重实时RT-PCR来检测C型和D型流感病毒,并分析了2018年1月至2023年3月期间从日本2144名患有呼吸道疾病的患者收集的呼吸道标本。我们分离了病毒并进行了血凝抑制试验,以检查抗原性和焦点减少试验,以确定对帽依赖性核酸内切酶抑制剂baloxavirmarboxil的敏感性。
    结果:我们检测到三种属于C/Kanagawa或C/圣保罗谱系的C型流感病毒,最近在全球流传。没有一个标本对D型流感病毒呈阳性。C/横滨/1/2022应变,从具有最高病毒RNA载量的标本中分离,属于C/神奈川谱系,显示出与参考C/神奈川谱系菌株相似的抗原性,并且对巴洛沙韦敏感。
    结论:我们的双重实时RT-PCR可用于从同一样本中同时检测C和D型流感病毒。将D型流感病毒添加到C型流感病毒的监测中,将有助于评估该病毒带来的公共卫生风险。
    BACKGROUND: Influenza viruses can cause zoonotic infections that pose public health risks. Surveillance of influenza A and B viruses is conducted globally; however, information on influenza C and D viruses is limited. Longitudinal monitoring of influenza C virus in humans has been conducted in several countries, but there has been no long-term monitoring of influenza D virus in humans. The public health risks associated with the influenza D virus therefore remain unknown.
    METHODS: We established a duplex real-time RT-PCR to detect influenza C and D viruses and analyzed respiratory specimens collected from 2144 patients in Japan with respiratory diseases between January 2018 and March 2023. We isolated viruses and conducted hemagglutination inhibition tests to examine antigenicity and focus reduction assays to determine susceptibility to the cap-dependent endonuclease inhibitor baloxavir marboxil.
    RESULTS: We detected three influenza C viruses belonging to the C/Kanagawa- or C/Sao Paulo-lineages, which recently circulated globally. None of the specimens was positive for the influenza D virus. The C/Yokohama/1/2022 strain, isolated from the specimen with the highest viral RNA load and belonging to the C/Kanagawa-lineage, showed similar antigenicity to the reference C/Kanagawa-lineage strain and was susceptible to baloxavir.
    CONCLUSIONS: Our duplex real-time RT-PCR is useful for the simultaneous detection of influenza C and D viruses from the same specimen. Adding the influenza D virus to the monitoring of the influenza C virus would help in assessing the public health risks posed by this virus.
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  • 文章类型: Journal Article
    已知狗对甲型流感病毒易感,尽管有关D型流感病毒(IDV)的信息有限。我们调查了2016年和2023年意大利普利亚地区426只狗的IDV血清阳性率。共有14份样本的IDV抗体呈阳性,提示狗接触IDV.
    Dogs are known to be susceptible to influenza A viruses, although information on influenza D virus (IDV) is limited. We investigated the seroprevalence of IDV in 426 dogs in the Apulia region of Italy during 2016 and 2023. A total of 14 samples were positive for IDV antibodies, suggesting exposure to IDV in dogs.
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  • 文章类型: Journal Article
    流感病毒D(IDV)在牛呼吸道疾病中的作用尚不清楚。体内实验导致临床症状增加,病变,以及与IDV和牛支原体共感染的小牛中的病原体复制(M.bovis),与单一感染的小牛相比。本研究旨在阐明宿主与病原体的相互作用,并描述这些小牛气道中脂质介质的动力学。在感染后2天(dpi)收集的支气管肺泡灌洗(BAL)样品用于通过液相色谱-串联质谱法(LC-MS/MS)进行蛋白质组学分析。此外,通过LC-MS/MS对在2、7和14dpi下收集的BAL样品进行脂质组学分析。而牛分枝杆菌诱导参与纤维蛋白形成的蛋白质的表达,IDV共感染抵消了这种凝血机制,并下调了其他急性期反应蛋白,如补体成分4(C4)和纤溶酶原(PLG)。针对牛分枝杆菌的炎症反应减少可能导致牛分枝杆菌复制增加和牛分枝杆菌清除延迟,这导致共感染的小牛体内的氧脂含量显着增加。鉴定出的诱导的氧脂主要来自花生四烯酸;可能被COX-1,COX-2和LOX-5氧化;并在7dpi达到峰值。本文介绍了牛对IDV和牛分枝杆菌感染的BAL蛋白质组和脂质介质动力学的第一个表征,并提出了有关IDV如何在牛呼吸道疾病中充当共同病原体的假设。
    The role of Influenza D virus (IDV) in bovine respiratory disease remains unclear. An in vivo experiment resulted in increased clinical signs, lesions, and pathogen replication in calves co-infected with IDV and Mycoplasma bovis (M. bovis), compared to single-infected calves. The present study aimed to elucidate the host-pathogen interactions and profile the kinetics of lipid mediators in the airways of these calves. Bronchoalveolar lavage (BAL) samples collected at 2 days post-infection (dpi) were used for proteomic analyses by liquid chromatography-tandem mass spectrometry (LC-MS/MS). Additionally, lipidomic analyses were performed by LC-MS/MS on BAL samples collected at 2, 7 and 14 dpi. Whereas M. bovis induced the expression of proteins involved in fibrin formation, IDV co-infection counteracted this coagulation mechanism and downregulated other acute-phase response proteins, such as complement component 4 (C4) and plasminogen (PLG). The reduced inflammatory response against M. bovis likely resulted in increased M. bovis replication and delayed M. bovis clearance, which led to a significantly increased abundance of oxylipids in co-infected calves. The identified induced oxylipids mainly derived from arachidonic acid; were likely oxidized by COX-1, COX-2, and LOX-5; and peaked at 7 dpi. This paper presents the first characterization of BAL proteome and lipid mediator kinetics in response to IDV and M. bovis infection in cattle and raises hypotheses regarding how IDV acts as a co-pathogen in bovine respiratory disease.
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  • 文章类型: Journal Article
    D型流感病毒(IDV)利用牛作为主要宿主,并定期溢出到其他宿主。我们先前已经证明IDV结合9-O-乙酰化N-乙酰神经氨酸(Neu5,9Ac2)和9-O-乙酰化N-羟乙酰神经氨酸(Neu5Gc9Ac)。牛生产Neu5,9Ac2和Neu5Gc9Ac,而人类在基因上无法合成Neu5Gc9Ac。唾液酸的9-O-乙酰化由CASDl通过共价乙酰基酶中间体催化。为了表征Neu5,9Ac2和Neu5Gc9Ac在IDV感染中的作用,并确定哪种形式的9-O-乙酰化唾液酸驱动IDV进入,我们利用CASD1敲除(KO)MDCK细胞系,并使用合成的9-O-乙酰唾液酸结合单轮和多轮IDV感染测定进行了饲养实验。来自我们研究的数据表明(i)CASD1KO细胞对IDV感染具有抗性,并且缺乏与细胞表面的IDV结合是导致IDV复制失败的原因;(ii)用Neu5,9Ac2或Neu5Gc9Ac饲喂CASD1KO细胞导致IDV感染性的剂量依赖性挽救;(iii)IDV在Neua9cfed的CASD1KO细胞中与Neu这些数据证明IDV可以利用含Neu5,9Ac2或非人Neu5Gc9Ac的聚糖受体进行感染。我们的发现提供了证据,表明IDV已经获得了在富含Neu5Gc9Ac的农业动物中感染和传播的能力,除了对仅表达Neu5,9Ac2的人类构成人畜共患病风险。IMPORTANCEAD型流感病毒(IDV)已成为一种多物种感染病原体,其中牛作为主要宿主。关于驱动IDV进入并促进其在不同宿主之间的跨物种溢出潜力的功能受体知之甚少。这里,我们证明IDV仅与9-O-乙酰化N-乙酰神经氨酸(Neu5,9Ac2)和非人9-O-乙酰化N-羟乙酰神经氨酸(Neu5Gc9Ac)结合,并同时用于进入和感染。有效参与两种9-O-乙酰化唾液酸作为感染的功能性受体的能力为IDV扩大其宿主范围提供了进化优势。这一发现还表明,IDV有可能在人类中出现,因为Neu5,9Ac2在人体组织中普遍表达,包括肺。因此,我们的研究结果强调了持续监测人类IDV的必要性,以及进一步研究其生物学和跨物种传播机制。
    Influenza D virus (IDV) utilizes bovines as a primary reservoir with periodical spillover to other hosts. We have previously demonstrated that IDV binds both 9-O-acetylated N-acetylneuraminic acid (Neu5,9Ac2) and 9-O-acetylated N-glycolylneuraminic acid (Neu5Gc9Ac). Bovines produce both Neu5,9Ac2 and Neu5Gc9Ac, while humans are genetically unable to synthesize Neu5Gc9Ac. 9-O-Acetylation of sialic acids is catalyzed by CASD1 via a covalent acetyl-enzyme intermediate. To characterize the role of Neu5,9Ac2 and Neu5Gc9Ac in IDV infection and determine which form of 9-O-acetylated sialic acids drives IDV entry, we took advantage of a CASD1 knockout (KO) MDCK cell line and carried out feeding experiments using synthetic 9-O-acetyl sialic acids in combination with the single-round and multi-round IDV infection assays. The data from our studies show that (i) CASD1 KO cells are resistant to IDV infection and lack of IDV binding to the cell surface is responsible for the failure of IDV replication; (ii) feeding CASD1 KO cells with Neu5,9Ac2 or Neu5Gc9Ac resulted in a dose-dependent rescue of IDV infectivity; and (iii) diverse IDVs replicated robustly in CASD1 KO cells fed with either Neu5,9Ac2 or Neu5Gc9Ac at a level similar to that in wild-type cells with a functional CASD1. These data demonstrate that IDV can utilize Neu5,9Ac2- or non-human Neu5Gc9Ac-containing glycan receptor for infection. Our findings provide evidence that IDV has acquired the ability to infect and transmit among agricultural animals that are enriched in Neu5Gc9Ac, in addition to posing a zoonotic risk to humans expressing only Neu5,9Ac2.IMPORTANCEInfluenza D virus (IDV) has emerged as a multiple-species-infecting pathogen with bovines as a primary reservoir. Little is known about the functional receptor that drives IDV entry and promotes its cross-species spillover potential among different hosts. Here, we demonstrated that IDV binds exclusively to 9-O-acetylated N-acetylneuraminic acid (Neu5,9Ac2) and non-human 9-O-acetylated N-glycolylneuraminic acid (Neu5Gc9Ac) and utilizes both for entry and infection. This ability in effective engagement of both 9-O-acetylated sialic acids as functional receptors for infection provides an evolutionary advantage to IDV for expanding its host range. This finding also indicates that IDV has the potential to emerge in humans because Neu5,9Ac2 is ubiquitously expressed in human tissues, including lung. Thus, results of our study highlight a need for continued surveillance of IDV in humans, as well as for further investigation of its biology and cross-species transmission mechanism.
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  • 文章类型: Journal Article
    C型流感病毒(ICV)与儿童社区获得性肺炎(CAP)的关系日益密切,其病情严重程度比B型流感病毒更为严重。但与甲型流感病毒相关的CAP相似。尽管ICV在人类中无处不在,对其在动物中的复制和病理生物学知之甚少。这项研究的目的是了解复制动力学,组织嗜性,与豚鼠中的猪D型流感病毒(swIDV)相比,人ICV(huICV)的发病机理。鼻内接种两种病毒均未引起临床症状,然而,受感染的动物在鼻洗液中释放病毒。在鼻甲复制的huICV,软腭,和气管,但不在肺中,而swIDV在所有四个组织中复制。对这两种相关的七段流感病毒的嗜性和发病机理的比较分析显示,与huICV相比,swIDV感染的动物表现出广泛的组织嗜性,在3、5和7dpi的脱落率和肺中的高病毒载量增加。huICV组在14dpi时出现血清转换,而感染swIDV的动物在7dpi时血清转化。感染huICV的豚鼠在软腭和气管的上皮中表现出轻度至中度的炎症变化,伴随着粘膜损伤和肺部多灶性肺泡炎。总之,豚鼠ICV的复制动力学和病理生物学特征与人类ICV感染的临床表现一致,因此,豚鼠可用于研究这些远缘相关的流感病毒。重要性类似于甲型和乙型流感,观察到ICV感染与细菌和病毒共感染相关,这使得对其实际临床意义的评估复杂化。Further,针对甲型和乙型流感病毒的抗病毒药物对ICV无效,这要求需要研究该病毒的病理生物学方面。在这里,我们证明了豚鼠的呼吸道具有ICV的特异性病毒受体。我们还比较了huICV和swIDV的复制动力学和发病机理,因为这些病毒共有50%的序列同一性。豚鼠与huICV相关的组织嗜性和病理学类似于人类由ICV引起的轻度呼吸道疾病,从而证明了豚鼠研究ICV的适用性。我们的比较分析表明,huICV和swIDV在豚鼠中的复制差异表明,特定类型的遗传差异可能导致病毒脱落和组织嗜性的差异。
    Influenza C virus (ICV) is increasingly associated with community-acquired pneumonia (CAP) in children and its disease severity is worse than the influenza B virus, but similar to influenza A virus associated CAP. Despite the ubiquitous infection landscape of ICV in humans, little is known about its replication and pathobiology in animals. The goal of this study was to understand the replication kinetics, tissue tropism, and pathogenesis of human ICV (huICV) in comparison to the swine influenza D virus (swIDV) in guinea pigs. Intranasal inoculation of both viruses did not cause clinical signs, however, the infected animals shed virus in nasal washes. The huICV replicated in the nasal turbinates, soft palate, and trachea but not in the lungs while swIDV replicated in all four tissues. A comparative analysis of tropism and pathogenesis of these two related seven-segmented influenza viruses revealed that swIDV-infected animals exhibited broad tissue tropism with an increased rate of shedding on 3, 5, and 7 dpi and high viral loads in the lungs compared to huICV. Seroconversion occurred late in the huICV group at 14 dpi, while swIDV-infected animals seroconverted at 7 dpi. Guinea pigs infected with huICV exhibited mild to moderate inflammatory changes in the epithelium of the soft palate and trachea, along with mucosal damage and multifocal alveolitis in the lungs. In summary, the replication kinetics and pathobiological characteristics of ICV in guinea pigs agree with the clinical manifestation of ICV infection in humans, and hence guinea pigs could be used to study these distantly related influenza viruses. IMPORTANCE Similar to influenza A and B, ICV infections are seen associated with bacterial and viral co-infections which complicates the assessment of its real clinical significance. Further, the antivirals against influenza A and B viruses are ineffective against ICV which mandates the need to study the pathobiological aspects of this virus. Here we demonstrated that the respiratory tract of guinea pigs possesses specific viral receptors for ICV. We also compared the replication kinetics and pathogenesis of huICV and swIDV, as these viruses share 50% sequence identity. The tissue tropism and pathology associated with huICV in guinea pigs are analogous to the mild respiratory disease caused by ICV in humans, thereby demonstrating the suitability of guinea pigs to study ICV. Our comparative analysis revealed that huICV and swIDV replicated differentially in the guinea pigs suggesting that the type-specific genetic differences can result in the disparity of the viral shedding and tissue tropism.
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  • 文章类型: Journal Article
    在牛呼吸道疾病(BRD)暴发中发现了D型流感病毒(IDV),和实验研究表明,这种病毒的能力,造成损伤的呼吸道。此外,在人血清中检测到IDV特异性抗体,这表明该病毒具有潜在的人畜共患作用。本研究旨在扩展我们对瑞典奶牛场IDV流行病学情况的了解,使用散装罐牛奶(BTM)样品检测IDV抗体。2019年和2020年共收集了461个和338个BTM样本,用内部间接ELISA进行分析。总的来说,在2019年和2020年,分别有147个(32%)和135个(40%)样本为IDV抗体阳性。总的来说,2/125(2%),11/157(7%)和269/517(52%)的样本在北部为IDV抗体阳性,瑞典中部和南部地区。在南方反复检出阳性样本比例最高,在哈兰郡,这是全国牛密度最高的县之一。为了了解IDV的流行病学,需要在不同的牛种群和人类中进行进一步的研究。
    Influenza D virus (IDV) has been detected in bovine respiratory disease (BRD) outbreaks, and experimental studies demonstrated this virus\'s capacity to cause lesions in the respiratory tract. In addition, IDV-specific antibodies were detected in human sera, which indicated that this virus plays a potential zoonotic role. The present study aimed to extend our knowledge about the epidemiologic situation of IDV in Swedish dairy farms, using bulk tank milk (BTM) samples for the detection of IDV antibodies. A total of 461 and 338 BTM samples collected during 2019 and 2020, respectively, were analyzed with an in-house indirect ELISA. In total, 147 (32%) and 135 (40%) samples were IDV-antibody-positive in 2019 and 2020, respectively. Overall, 2/125 (2%), 11/157 (7%) and 269/517 (52%) of the samples were IDV-antibody-positive in the northern, middle and southern regions of Sweden. The highest proportion of positive samples was repeatedly detected in the south, in the county of Halland, which is one of the counties with the highest cattle density in the country. In order to understand the epidemiology of IDV, further research in different cattle populations and in humans is required.
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  • 文章类型: Editorial
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  • 文章类型: Journal Article
    已在马匹中检测到D型流感病毒(IDV)的抗体,但是没有关于该领域疾病的证据。为了确定IDV是否具有传染性,免疫原性,和马的致病性,用6.25×107TCID50/动物D/牛/加利福尼亚/0363/2019(D/CA2019)病毒鼻内接种四匹对甲型(H3N8)和D病毒均呈血清阴性的2岁马,使用便携式马雾化器系统。每天观察马的临床症状,包括直肠温度,鼻腔分泌物,咳嗽,肺音,心动过速,和呼吸急促.没有马表现出疾病的临床症状。从感染后1-8天收集的鼻咽拭子通过qRT-PCR证明病毒脱落。马早在感染后13天(dpi)就显示出血清转化的证据,所有四匹马的抗体滴度(GMT)的几何平均值为16.82-160,如微中和测定所示。Further,在含胚鸡蛋中分离的病毒的深度RNA测序显示没有适应性突变,表明IDV可以在马中复制,表明IDV与牛水库在自然界中的种间传播的可能性。
    Antibodies to influenza D virus (IDV) have been detected in horses, but no evidence of disease in the field has been reported. To determine whether IDV is infectious, immunogenic, and pathogenic in horses, four 2-year-old horses seronegative for both influenza A (H3N8) and D viruses were intranasally inoculated with 6.25 × 107 TCID50/animal of D/bovine/California/0363/2019 (D/CA2019) virus, using a portable equine nebulizer system. Horses were observed daily for clinical signs including rectal temperature, nasal discharge, coughing, lung sounds, tachycardia, and tachypnea. No horses exhibited clinical signs of disease. Nasopharyngeal swabs collected from 1-8 days post-infection demonstrated virus shedding by qRT-PCR. The horses showed evidence of seroconversion as early as 13 days post-infection (dpi) and the geometric mean of the antibody titers (GMT) of all four horses ranged from 16.82-160 as demonstrated by the microneutralization assay. Further, deep RNA sequencing of the virus isolated in embryonated chicken eggs revealed no adaptive mutations indicating that IDV can replicate in horses, suggesting the possibility of interspecies transmission of IDV with bovine reservoir into equids in nature.
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  • 文章类型: Journal Article
    除了基因组结构,丙型流感(ICV),和D(IDV)病毒具有七个分段的基因组在生物学上与八个分段的甲型流感(IAV)不同,和B(IBV)病毒关于血凝素-酯酶融合蛋白的存在,它结合了负责受体结合的血凝素和神经氨酸酶的功能,聚变,和破坏受体的酶活性,分别。而以人类为主要宿主的ICV出现在近74年前,IDV,ICV的远亲,在2011年被隔离,牛作为主要宿主。尽管它最初出现在猪身上,IDV已被证明是一种跨界牛病原体,宿主范围更广,与甲型流感病毒(IAV)相似。ICV和IDV的受体特异性决定了宿主范围和物种特异性。人类呼吸道样本中存在IDV基因组的最新发现,高交通的人类环境表明了其公共卫生意义。相反,猪和牛中ICV的存在也增加了ICV和IDV之间基因片段相互作用/病毒重组的可能性,在这些病毒共存的地方.这篇综述是一个整体方法,通过关注迄今为止已知的宿主范围来讨论七段流感病毒的生态学,血清流行病学,生物学受体,系统动力学,物种特异性,以及ICV和IDV的跨物种传播。
    Other than genome structure, influenza C (ICV), and D (IDV) viruses with seven-segmented genomes are biologically different from the eight-segmented influenza A (IAV), and B (IBV) viruses concerning the presence of hemagglutinin-esterase fusion protein, which combines the function of hemagglutinin and neuraminidase responsible for receptor-binding, fusion, and receptor-destroying enzymatic activities, respectively. Whereas ICV with humans as primary hosts emerged nearly 74 years ago, IDV, a distant relative of ICV, was isolated in 2011, with bovines as the primary host. Despite its initial emergence in swine, IDV has turned out to be a transboundary bovine pathogen and a broader host range, similar to influenza A viruses (IAV). The receptor specificities of ICV and IDV determine the host range and the species specificity. The recent findings of the presence of the IDV genome in the human respiratory sample, and high traffic human environments indicate its public health significance. Conversely, the presence of ICV in pigs and cattle also raises the possibility of gene segment interactions/virus reassortment between ICV and IDV where these viruses co-exist. This review is a holistic approach to discuss the ecology of seven-segmented influenza viruses by focusing on what is known so far on the host range, seroepidemiology, biology, receptor, phylodynamics, species specificity, and cross-species transmission of the ICV and IDV.
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  • 文章类型: Journal Article
    The influenza D virus (IDV) uses a trimeric hemagglutinin-esterase fusion protein (HEF) for attachment to 9-O-acetylated sialic acid receptors on the cell surface of host species. So far research has revealed that farm animals such as cattle, domestic pigs, goats, sheep and horses contain the necessary receptors on the epithelial surface of the respiratory tract to accommodate binding of the IDV HEF protein of both worldwide clades D/Oklahoma (D/OK) and D/Oklahoma/660 (D/660). More recently, seroprevalence studies have identified IDV-seropositive wildlife such as wild boar, deer, dromedaries, and small ruminants. However, no research has thus far been conducted in wildlife to reveal the distribution of acetylated sialic acid receptors that accommodate binding of IDV. Using our previously developed tissue microarray (TMA) system, we developed TMAs containing respiratory tissues of various wild and domestic species including wild boar, deer, dromedary, springbok, water buffalo, tiger, hedgehog, and Asian elephant. Protein histochemical staining of these TMAs with HEF proteins showed no receptor binding for wild Suidae, Cervidae and tiger. However, receptors were present in dromedary, springbok, water buffalo, Asian elephant, and hedgehog. In contrast to previously tested farm animals, a difference in host tropism was observed between the D/OK and D/660 clade HEF proteins in Asian elephant, and water buffalo. These results show that IDV can attach to the respiratory tract of wildlife which might facilitate transmission of IDV between wildlife and domestic animals.
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