Rabies virus

狂犬病病毒
  • 文章类型: Journal Article
    摘要狂犬病是一种威胁人类健康的致命的人畜共患疾病。作为唯一的病毒表面蛋白,狂犬病病毒(RABV)糖蛋白(G)诱导主要的中和抗体(Nab)应答;然而,Nab滴度与G的构象密切相关。通过共表达RABVG和基质蛋白(M)形成的病毒样颗粒(VLP)改善保留和抗原呈递,诱导广泛,持久的免疫反应。RABV核蛋白(N)可引起体液和细胞免疫应答。因此,我们开发了一系列核苷修饰的RABVmRNA疫苗,编码野生型G,由人工三聚体基序(tG-MTQ)形成的可溶性三聚体RABVG,膜锚定预融合稳定G(preG)。此外,我们还开发了共表达preG和M的RABVVLPmRNA疫苗以产生VLP,和VLP/NmRNA疫苗共表达preG,M,与灭活狂犬病疫苗相比,RABVmRNA疫苗诱导更高的体液和细胞反应,完全保护小鼠免受脑内攻击。此外,RABVpreG中的IgG和Nab滴度,VLP和VLP/NmRNA组明显高于G和tG-MTQ组。VLP或VLP/NmRNA疫苗的单次给药引发保护性Nab反应,在第7天,Nab滴度明显高于灭活疫苗组。此外,RABVVLP和VLP/NmRNA疫苗显示出优越的能力,以引起有效的生发中心,长寿命浆细胞和记忆B细胞反应,这与高滴度和持久的Nab反应有关。总之,我们的数据表明,RABVVLP和VLP/NmRNA疫苗可能是有希望的抗狂犬病候选疫苗.
    Rabies is a lethal zoonotic disease that threatens human health. As the only viral surface protein, the rabies virus (RABV) glycoprotein (G) induces main neutralizing antibody (Nab) responses; however, Nab titre is closely correlated with the conformation of G. Virus-like particles (VLP) formed by the co-expression of RABV G and matrix protein (M) improve retention and antigen presentation, inducing broad, durable immune responses. RABV nucleoprotein (N) can elicit humoral and cellular immune responses. Hence, we developed a series of nucleoside-modified RABV mRNA vaccines encoding wild-type G, soluble trimeric RABV G formed by an artificial trimer motif (tG-MTQ), membrane-anchored prefusion-stabilized G (preG). Furthermore, we also developed RABV VLP mRNA vaccine co-expressing preG and M to generate VLPs, and VLP/N mRNA vaccine co-expressing preG, M, and N. The RABV mRNA vaccines induced higher humoral and cellular responses than inactivated rabies vaccine, and completely protected mice against intracerebral challenge. Additionally, the IgG and Nab titres in RABV preG, VLP and VLP/N mRNA groups were significantly higher than those in G and tG-MTQ groups. A single administration of VLP or VLP/N mRNA vaccines elicited protective Nab responses, the Nab titres were significantly higher than that in inactivated rabies vaccine group at day 7. Moreover, RABV VLP and VLP/N mRNA vaccines showed superior capacities to elicit potent germinal centre, long-lived plasma cell and memory B cell responses, which linked to high titre and durable Nab responses. In summary, our data demonstrated that RABV VLP and VLP/N mRNA vaccines could be promising candidates against rabies.
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  • 文章类型: Journal Article
    狂犬病病毒(RABV)是狂犬病的病原体,哺乳动物的致命神经系统疾病。RABV菌株可分为固定菌株(实验室菌株)和街道菌株(现场/临床菌株),它们具有不同的特性,包括细胞嗜性和神经侵袭性。RABVToyohashi毒株是日本的街头毒株,从菲律宾的狂犬病狗咬伤的进口病例中分离出来。为了促进RABV的分子研究,我们建立了用于研究丰桥菌株的反向遗传学(RG)系统。重组病毒是从Toyohashi株的cDNA克隆获得的,在培养的细胞系中表现出与原始病毒相似的生长效率。原始菌株和重组菌株在小鼠中显示出相似的致病性,具有高神经侵袭性,受感染的小鼠发展了漫长而不一致的潜伏期,这是街头菌株的特征。我们还产生了表达与荧光蛋白mCherry融合的病毒磷蛋白(P蛋白)的重组Toyohashi菌株,并使用活细胞成像跟踪病毒P蛋白的细胞内动力学。提出的Toyohashi菌株的反向遗传系统将是探索RABV街道菌株复制的基本分子机制的有用工具。
    Rabies virus (RABV) is the causative agent of rabies, a lethal neurological disease in mammals. RABV strains can be classified into fixed strains (laboratory strains) and street strains (field/clinical strains), which have different properties including cell tropism and neuroinvasiveness. RABV Toyohashi strain is a street strain isolated in Japan from an imported case which had been bitten by rabid dog in the Philippines. In order to facilitate molecular studies of RABV, we established a reverse genetics (RG) system for the study of the Toyohashi strain. The recombinant virus was obtained from a cDNA clone of Toyohashi strain and exhibited similar growth efficiency as the original virus in cultured cell lines. Both the original and recombinant strains showed similar pathogenicity with high neuroinvasiveness in mice, and the infected mice developed a long and inconsistent incubation period, which is characteristic of street strains. We also generated a recombinant Toyohashi strain expressing viral phosphoprotein (P protein) fused with the fluorescent protein mCherry, and tracked the intracellular dynamics of the viral P protein using live-cell imaging. The presented reverse genetics system for Toyohashi strain will be a useful tool to explore the fundamental molecular mechanisms of the replication of RABV street strains.
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  • 文章类型: Journal Article
    泼妇是食虫动物,作为一系列人畜共患病毒的天然储库,包括最近于2018年在中国发现的狼牙网病毒(LayV)。重要的是要了解与泼妇有关的病毒,病毒多样性,和新的病毒。在目前的研究中,我们对从中国东部沿海捕获的398只shrew的肺样本进行了高通量测序,并具有6种常见的shrew种(Anourosorexsquamipes,Crociduralasiura,龙骨山,谷草,Sorexcaecutiens,和Suncusmurinus)。我们的分析揭示了包括54种已知病毒和72种新病毒的许多与泼妇相关的病毒,这些病毒显著增强了我们对哺乳动物病毒的理解。值得注意的是,34种鉴定的病毒具有潜在的溢出风险,6种是人类致病病毒:LayV,甲型流感病毒(H5N6)轮状病毒A,狂犬病病毒,禽副粘病毒1和大鼠戊型肝炎病毒。此外,在中国发现了10种以前未报告的病毒,其中六个具有溢出风险潜力。此外,所有54种已知病毒和12种新病毒都具有跨越物种界限的能力.我们的数据强调了与shrew相关的病毒的多样性,并为进一步研究追踪和预测源于shrew的新出现的传染病奠定了基础。
    Shrews being insectivores, serve as natural reservoirs for a wide array of zoonotic viruses, including the recently discovered Langya henipavirus (LayV) in China in 2018. It is crucial to understand the shrew-associated virome, viral diversity, and new viruses. In the current study, we conducted high-throughput sequencing on lung samples obtained from 398 shrews captured along the eastern coast of China, and characterized the high-depth virome of 6 common shrew species (Anourosorex squamipes, Crocidura lasiura, Crocidura shantungensis, Crocidura tanakae, Sorex caecutiens, and Suncus murinus). Our analysis revealed numerous shrew-associated viruses comprising 54 known viruses and 72 new viruses that significantly enhance our understanding of mammalian viruses. Notably, 34 identified viruses possess spillover-risk potential and six were human pathogenic viruses: LayV, influenza A virus (H5N6), rotavirus A, rabies virus, avian paramyxovirus 1, and rat hepatitis E virus. Moreover, ten previously unreported viruses in China were discovered, six among them have spillover-risk potential. Additionally, all 54 known viruses and 12 new viruses had the ability to cross species boundaries. Our data underscore the diversity of shrew-associated viruses and provide a foundation for further studies into tracing and predicting emerging infectious diseases originated from shrews.
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  • 文章类型: Case Reports
    本报告描述了狂犬病病毒在蒙特斯·克拉罗斯(MOC)市区的两种野生动物中的发生,米纳斯吉拉斯州,巴西,2023年5月。该病毒已在食肉性翼翅目(Artibeussp)和and猴(Callithrixpenicillata)中检测到。这是在MOC市区的C.penicillata物种中首次通报的狂犬病病毒病例。我们的发现表明,狂犬病病毒在MOC的城市地区传播;因此,必须采取永久性预防措施,以避免感染其他动物和人类。
    This report describes the occurrence of the rabies virus in two species of wild animals in the urban area of Montes Claros (MOC), Minas Gerais State, Brazil, in May 2023. The virus has been detected in frugivorous chiropterans (Artibeus sp) and marmosets (Callithrix penicillata). This is the first notified case of the rabies virus in the species C. penicillata in the urban area of MOC. Our findings show that the rabies virus is circulating in the urban area of MOC; therefore, permanent preventive measures must be adopted to avoid infection of other animals and humans.
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  • 文章类型: Journal Article
    狂犬病,主要由狗传播给人类(占病例的99%)。一旦发生狂犬病,其死亡率约为100%。暴露后预防(PEP)对于预防暴露于狂犬病动物后的狂犬病发作至关重要,疫苗接种是PEP的关键要素。然而,高昂的费用和复杂的免疫方案导致狂犬病疫苗接种依从性差。因此,迫切需要开发新的安全的狂犬病疫苗,高度免疫原性,和成本效益,以提高依从性和有效预防狂犬病。近年来,mRNA疫苗在递送系统的结构修饰和优化方面取得了重大进展。各种mRNA疫苗目前正在进行临床试验,将它们定位为传统狂犬病疫苗的可行替代品。在这篇文章中,我们讨论了一种目前正在进行临床和临床前测试的新型mRNA狂犬病疫苗,并评估其替代现有疫苗的潜力。
    Rabies, primarily transmitted to humans by dogs (accounting for 99% of cases). Once rabies occurs, its mortality rate is approximately 100%. Post-exposure prophylaxis (PEP) is critical for preventing the onset of rabies after exposure to rabid animals, and vaccination is a pivotal element of PEP. However, high costs and complex immunization protocols have led to poor adherence to rabies vaccinations. Consequently, there is an urgent need to develop new rabies vaccines that are safe, highly immunogenic, and cost-effective to improve compliance and effectively prevent rabies. In recent years, mRNA vaccines have made significant progress in the structural modification and optimization of delivery systems. Various mRNA vaccines are currently undergoing clinical trials, positioning them as viable alternatives to the traditional rabies vaccines. In this article, we discuss a novel mRNA rabies vaccine currently undergoing clinical and preclinical testing, and evaluate its potential to replace existing vaccines.
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  • 文章类型: Journal Article
    除了狂犬病病毒(RABV),世界上已经发现了16种Lyssavirus物种,导致类似于RABV的疾病。已经描述了与狂犬病无关的人类死亡,但病例数量未知,而这种病毒引起人类疾病的潜力是不可预测的。目前的狂犬病疫苗不能抵抗不同的裂解病毒,如莫科拉病毒(MOKV)或拉各斯蝙蝠病毒(LBV)。因此,需要一种更广泛的泛病毒疫苗。这里,我们评估了一种新型的Lyssavirus疫苗,该疫苗具有减毒的RABV载体,该载体带有嵌合RABV糖蛋白(G),其中MOKV的抗原位点I取代了狂犬病病毒的真实位点(RABVG-cAS1)。重组疫苗用于免疫小鼠并分析与同源疫苗相比的免疫应答。我们的发现表明,疫苗RABVG-cAS1具有免疫原性,并诱导了针对RABVG和MOKVG的高抗体滴度。对不同病毒的挑战研究表明,用MOKVG的相应位点替换RABVG的单个抗原位点提供了对同源RABV疫苗的显着改善,并防止RABV。Irkut病毒(IRKV),MOKV这种表位嵌合策略为一种泛病毒疫苗铺平了道路,以安全地对抗由这些病毒引起的疾病。
    In addition to the rabies virus (RABV), 16 more lyssavirus species have been identified worldwide, causing a disease similar to RABV. Non-rabies-related human deaths have been described, but the number of cases is unknown, and the potential of such lyssaviruses causing human disease is unpredictable. The current rabies vaccine does not protect against divergent lyssaviruses such as Mokola virus (MOKV) or Lagos bat virus (LBV). Thus, a more broad pan-lyssavirus vaccine is needed. Here, we evaluate a novel lyssavirus vaccine with an attenuated RABV vector harboring a chimeric RABV glycoprotein (G) in which the antigenic site I of MOKV replaces the authentic site of rabies virus (RABVG-cAS1). The recombinant vaccine was utilized to immunize mice and analyze the immune response compared to homologous vaccines. Our findings indicate that the vaccine RABVG-cAS1 was immunogenic and induced high antibody titers against both RABVG and MOKVG. Challenge studies with different lyssaviruses showed that replacing a single antigenic site of RABV G with the corresponding site of MOKV G provides a significant improvement over the homologous RABV vaccine and protects against RABV, Irkut virus (IRKV), and MOKV. This strategy of epitope chimerization paves the way towards a pan-lyssavirus vaccine to safely combat the diseases caused by these viruses.
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  • 文章类型: Journal Article
    狂犬病,一种引起致命脑炎的病毒性疾病,全世界每年杀害约59,000人,尽管有有效的对策。狂犬病在肯尼亚是地方病,主要通过狂犬病家犬的叮咬传播给人类。我们分析了从肯尼亚西部和东部的狂犬病动物中收集的164例脑干,并评估了来自两个地区的狂犬病病毒(RABV)的系统发育关系。与肯尼亚常用的RABV疫苗株相比,我们还分析了RABV基因组中核蛋白和糖蛋白疫苗抗原位点的潜在氨基酸变化。我们发现,来自肯尼亚东部的RABV基因组绝大多数与Africa-1b亚分化聚集在一起,来自肯尼亚西部的RABV与Africa-1a聚集在一起。我们注意到野生和疫苗病毒株之间的氨基酸差异最小。这些数据证实了两个地区之间的病毒迁移最小,并且狂犬病流行是疫苗覆盖率有限而不是疗效有限的结果。
    Rabies, a viral disease that causes lethal encephalitis, kills ≈59,000 persons worldwide annually, despite availability of effective countermeasures. Rabies is endemic in Kenya and is mainly transmitted to humans through bites from rabid domestic dogs. We analyzed 164 brain stems collected from rabid animals in western and eastern Kenya and evaluated the phylogenetic relationships of rabies virus (RABV) from the 2 regions. We also analyzed RABV genomes for potential amino acid changes in the vaccine antigenic sites of nucleoprotein and glycoprotein compared with RABV vaccine strains commonly used in Kenya. We found that RABV genomes from eastern Kenya overwhelmingly clustered with the Africa-1b subclade and RABV from western Kenya clustered with Africa-1a. We noted minimal amino acid variances between the wild and vaccine virus strains. These data confirm minimal viral migration between the 2 regions and that rabies endemicity is the result of limited vaccine coverage rather than limited efficacy.
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  • 文章类型: Journal Article
    背景:狂犬病是一种致命的人畜共患疾病,其发病机制尚未完全阐明,接种疫苗是预防狂犬病病毒感染的唯一有效方法。大多数灭活疫苗是使用Vero细胞生产的,非洲绿猴肾细胞,实现规模化生产。然而,由于非人类DNA污染,存在潜在的致癌风险。因此,用人二倍体细胞替代Vero细胞可能是更安全的策略。在这项研究中,我们开发了一种新的2BS细胞适应狂犬病病毒株,并分析了其序列,毒力和免疫原性,以确定其作为人二倍体细胞灭活疫苗的应用潜力。
    结果:通过传代40代并在2BS细胞中选择噬斑,建立了适应2BS细胞的狂犬病病毒株2aG4-B40。RNA序列分析揭示2BS细胞适应菌株中的突变不位于调节aG菌株中的中和抗体产生或毒力的关键位点(GQ412744.1)。毒力(从第40代到第55代保持在7.0logLD50/ml以上)和抗原的逐渐增加进一步表明,这些突变可以增加适应菌株对人二倍体细胞的亲和力。鉴定试验显示,抗狂犬病血清中和了适应2BS细胞的病毒株,中和指数为19,952。PrEP和PEP疫苗接种和NIH试验进一步表明,用2aG4-B40菌株制备的疫苗具有较高的中和抗体水平(2.24至46.67IU/ml),免疫原性(保护指数270)和效力(平均11.6IU/ml)。
    结论:在这项研究中,通过传代40代获得2aG4狂犬病病毒的2BS细胞适应株。适应株的测序分析和滴度测定结果表明,适应过程中的突变不位于病毒的关键序列区域,这些突变可以增强适应菌株对人二倍体细胞的亲和力。此外,由适应株2aG4-B40制成的疫苗具有较高的效力和免疫原性,可以作为灭活疫苗制备的理想候选狂犬病病毒株。
    BACKGROUND: Rabies is a fatal zoonotic disease whose pathogenesis has not been fully elucidated, and vaccination is the only effective method for protecting against rabies virus infection. Most inactivated vaccines are produced using Vero cells, which are African green monkey kidney cells, to achieve large-scale production. However, there is a potential carcinogenic risk due to nonhuman DNA contamination. Thus, replacing Vero cells with human diploid cells may be a safer strategy. In this study, we developed a novel 2BS cell-adapted rabies virus strain and analysed its sequence, virulence and immunogenicity to determine its application potential as a human diploid cell inactivated vaccine.
    RESULTS: The 2BS cell-adapted rabies virus strain 2aG4-B40 was established by passage for 40 generations and selection of plaques in 2BS cells. RNA sequence analysis revealed that mutations in 2BS cell-adapted strains were not located at key sites that regulate the production of neutralizing antibodies or virulence in the aG strain (GQ412744.1). The gradual increase in virulence (remaining above 7.0 logLD50/ml from the 40th to 55th generation) and antigen further indicated that these mutations may increase the affinity of the adapted strains for human diploid cells. Identification tests revealed that the 2BS cell-adapted virus strain was neutralized by anti-rabies serum, with a neutralization index of 19,952. PrEP and PEP vaccination and the NIH test further indicated that the vaccine prepared with the 2aG4-B40 strain had high neutralizing antibody levels (2.24 to 46.67 IU/ml), immunogenicity (protection index 270) and potency (average 11.6 IU/ml).
    CONCLUSIONS: In this study, a 2BS cell-adapted strain of the 2aG4 rabies virus was obtained by passage for 40 generations. The results of sequencing analysis and titre determination of the adapted strain showed that the mutations in the adaptive process are not located at key sequence regions of the virus, and these mutations may enhance the affinity of the adapted strain for human diploid cells. Moreover, vaccines made from the adapted strain 2aG4-B40 had high potency and immunogenicity and could be an ideal candidate rabies virus strain for inactivated vaccine preparation.
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  • 文章类型: Journal Article
    对纯化的狂犬病病毒(RABV)的蛋白质组学分析显示,病毒颗粒中有47种被包裹的宿主蛋白。在这些中,11种蛋白质高度无序。我们的研究特别集中在五种具有最高疾病水平的RABV捕获的小鼠蛋白质上:神经调节素,Chmp4b,DnaJB6,Vps37B,还有Wasl.我们广泛使用生物信息学工具,比如FuzDrop,D2P2,UniProt,RIDAO,STRING,AlphaFold,和ELM,全面分析这些蛋白质的内在紊乱倾向。我们的分析表明,这些无序的宿主蛋白可能在促进狂犬病病毒的致病性中起重要作用。免疫系统逃避,以及抗病毒药物耐药性的发展。我们的研究强调了病毒与其宿主的复杂相互作用,关注内在障碍如何在病毒致病过程中发挥关键作用,并表明这些内在无序蛋白(IDPs)和与疾病相关的宿主相互作用也可能是治疗策略的潜在靶标。
    A proteomics analysis of purified rabies virus (RABV) revealed 47 entrapped host proteins within the viral particles. Out of these, 11 proteins were highly disordered. Our study was particularly focused on five of the RABV-entrapped mouse proteins with the highest levels of disorder: Neuromodulin, Chmp4b, DnaJB6, Vps37B, and Wasl. We extensively utilized bioinformatics tools, such as FuzDrop, D2P2, UniProt, RIDAO, STRING, AlphaFold, and ELM, for a comprehensive analysis of the intrinsic disorder propensity of these proteins. Our analysis suggested that these disordered host proteins might play a significant role in facilitating the rabies virus pathogenicity, immune system evasion, and the development of antiviral drug resistance. Our study highlighted the complex interaction of the virus with its host, with a focus on how the intrinsic disorder can play a crucial role in virus pathogenic processes, and suggested that these intrinsically disordered proteins (IDPs) and disorder-related host interactions can also be a potential target for therapeutic strategies.
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  • 文章类型: Journal Article
    克罗地亚共和国已证明某些蝙蝠物种中的溶血病毒的血清流行率,但目前尚无证实的蝙蝠脑分离株阳性或与蝙蝠受伤/咬伤相关的人类死亡。这项研究包括对蝙蝠受伤/咬伤的回顾性分析,在萨格勒布反狂犬病诊所检查的人的暴露后预防(PEP)和蝙蝠伤害的地理分布,克罗地亚狂犬病参考中心。在1995-2020年期间,我们共检查了21,910名动物受伤患者,其中71例为蝙蝠相关(0.32%)。在上述患者中,4574人收到狂犬病PEP(20.87%)。然而,对于蝙蝠受伤,接受PEP的患者比例明显更高:71例患者中有66例(92.95%).其中,33只接种了狂犬病疫苗,而其他33名患者接受了人狂犬病免疫球蛋白(HRIG)疫苗。在五个案例中,没有进行PEP,因为没有治疗指征。35名受伤患者是生物学家或生物学学生(49.29%)。仅在一例暴露病例中确认了蝙蝠物种。这是一只血清型蝙蝠(Eptesicusserotinus),一种已知的汉堡病毒携带者。结果表明,与动物咬伤引起的其他人类伤害相比,蝙蝠咬伤是零星的。所有蝙蝠的伤害都应该被视为由狂犬病动物引起的,根据世卫组织的建议。强烈建议接触蝙蝠的人接种狂犬病疫苗。进入蝙蝠栖息地应谨慎行事,并符合目前的建议,全国范围的监测应由主管机构进行,并由蝙蝠专家密切合作,流行病学家和狂犬病专家。
    Seroprevalence of lyssaviruses in certain bat species has been proven in the Republic of Croatia, but there have been no confirmed positive bat brain isolates or human fatalities associated with bat injuries/bites. The study included a retrospective analysis of bat injuries/bites, post-exposure prophylaxis (PEP) and geographic distribution of bat injuries in persons examined at the Zagreb Antirabies Clinic, the Croatian Reference Centre for Rabies. In the period 1995-2020, we examined a total of 21,910 patients due to animal injuries, of which 71 cases were bat-related (0.32%). Of the above number of patients, 4574 received rabies PEP (20.87%). However, for bat injuries, the proportion of patients receiving PEP was significantly higher: 66 out of 71 patients (92.95%). Of these, 33 received only the rabies vaccine, while the other 33 patients received the vaccine with human rabies immunoglobulin (HRIG). In five cases, PEP was not administered, as there was no indication for treatment. Thirty-five of the injured patients were biologists or biology students (49.29%). The bat species was confirmed in only one of the exposure cases. This was a serotine bat (Eptesicus serotinus), a known carrier of Lyssavirus hamburg. The results showed that the bat bites were rather sporadic compared to other human injuries caused by animal bites. All bat injuries should be treated as if they were caused by a rabid animal, and according to WHO recommendations. People who come into contact with bats should be strongly advised to be vaccinated against rabies. Entering bat habitats should be done with caution and in accordance with current recommendations, and nationwide surveillance should be carried out by competent institutions and in close collaboration between bat experts, epidemiologists and rabies experts.
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