Orthohantavirus

正坦病毒
  • 文章类型: Journal Article
    背景:肾综合征出血热(HFRS)是江西省严重的公共卫生问题,中国。先前的研究报道了汉坦正太病毒(Hantaan病毒,HTNV)在该地区的啮齿动物中。然而,HTNV变异与人类感染之间的关系尚待确认.本研究旨在确定患者的HTNV变异,并了解由这些变异引起的HFRS的临床特征。
    方法:从急性期住院的HFRS疑似病例中收集样本。使用定量实时RT-PCR确认HFRS病例。将来自HFRS患者的外周血单核细胞(PBMC)接种到Vero-E6细胞中进行病毒分离。通过基于扩增子的下一代测序获得来自患者的HTNV的基因组序列。对患者的临床特点进行回顾性分析。
    结果:在183例疑似HFRS患者中的53例检测到HTNVRNA。从HFRS病例的32个PBMC中分离出13个HTNVs。获得了14个HTNVs的全基因组序列,包括13名患者的细胞培养中的13个分离株,和一个来自致命病例的血浆,在细胞培养中没有成功分离。遗传分析显示,来自14名患者的HTNV序列与其他地区的HTNV菌株在核苷酸和氨基酸方面存在显着差异。发烧(100%,53/53),血小板减少症(100%,53/53),血清天冬氨酸转氨酶升高(100%,53/53),和乳酸脱氢酶增加(96.2%,51/53)是最常见的特征。在13.2%(7/53)的病例中观察到严重的急性肾损伤。临床症状,如疼痛,瘀斑,胃肠道或呼吸道症状并不常见。
    结论:HTNV遗传变异导致江西人感染。在急性期由HTNV遗传变异引起的HFRS的临床症状是不典型的。除了肾功能不全,应注意这些遗传变异引起的常见肝损伤。
    BACKGROUND: Hemorrhagic fever with renal syndrome (HFRS) is a severe public health problem in Jiangxi province, China. Previous studies reported genetic variants of Orthohantavirus hantanense (Hantaan virus, HTNV) in rodents in this area. However, the relationship between HTNV variants and human infection needs to be confirmed. This study aimed to identify the HTNV variants in patients and to understand the clinical characteristics of HFRS caused by these variants.
    METHODS: Samples were collected from hospitalized suspected cases of HFRS during the acute phase. HFRS cases were confirmed using quantitative real-time RT-PCR. Peripheral blood mononuclear cells (PBMC) from patients with HFRS were inoculated into Vero-E6 cells for viral isolation. The genomic sequences of HTNV from patients were obtained by amplicon-based next-generation sequencing. A retrospective analysis was conducted on the clinical characteristics of the patients.
    RESULTS: HTNV RNA was detected in 53 of 183 suspected HFRS patients. Thirteen HTNVs were isolated from 32 PBMCs of HFRS cases. Whole genome sequences of 14 HTNVs were obtained, including 13 isolates in cell culture from 13 patients, and one from plasma of the fatal case which was not isolated successfully in cell culture. Genetic analysis revealed that the HTNV sequence from the 14 patients showed significant variations in nucleotide and amino acid to the HTNV strains found in other areas. Fever (100%, 53/53), thrombocytopenia (100%, 53/53), increased serum aspartate aminotransferase (100%, 53/53), and increased lactate dehydrogenase (96.2%, 51/53) were the most common characteristics. Severe acute kidney injury was observed in 13.2% (7/53) of cases. Clinical symptoms, such as pain, petechiae, and gastrointestinal or respiratory symptoms were uncommon.
    CONCLUSIONS: The HTNV genetic variants cause human infections in Jiangxi. The clinical symptoms of HFRS caused by the HTNV genetic variant during the acute phase are atypical. In addition to renal dysfunction, attention should be paid to the common liver injuries caused by these genetic variants.
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  • 文章类型: Journal Article
    肾综合征出血热(HFRS)和蜱传脑炎(TBE)是俄罗斯最常见的病毒性疾病。HFRS由六种不同类型的汉坦病毒引起:汉坦病毒,阿穆尔,首尔,Puumala,Kurkino,还有索契,通过Muridae和Cricetidae家族的小型哺乳动物传播给人类。TBE由属于五种不同系统发育亚型的病毒引起。这里介绍了HFRS和TBE病原体的生态学相似性。感染汉坦病毒的小型哺乳动物可以将病毒传播给未感染的动物,蜱也可以将汉坦病毒传播给其他蜱和哺乳动物。汉坦病毒从蜱传播到人类只有在间接数据的基础上才有可能。在过去的23年里,在俄罗斯登记了164,582例HFRS(每105人4.9例)和71,579例TBE(每105人2.5例)。HFRS的死亡率为0.4%(668例),TBE的死亡率为1.6%(1136例)。14岁以下儿童有4030例(2.5%)和9414例TBE(13%)。HFRS和TBE病例在俄罗斯85个地区中的42个登记;仅在18个HFRS中,在13只TBE中,12人没有报告病例。本文对HFRS和TBE联合疫苗的应用前景进行了展望。
    Hemorrhagic fever with renal syndrome (HFRS) and tick-borne encephalitis (TBE) are the most common viral diseases in Russia. HFRS is caused by six different types of hantaviruses: Hantaan, Amur, Seoul, Puumala, Kurkino, and Sochi, which are transmitted to humans through small mammals of the Muridae and Cricetidae families. TBE is caused by viruses belonging to five different phylogenetic subtypes. The similarities in the ecology of HFRS and TBE pathogens is presented here. Hantavirus-infected small mammals can transmit the virus to uninfected animals, and ticks can also transmit hantavirus to other ticks and mammals. Hantavirus transmission from ticks to humans is possible only hypothetically based on indirect data. Over the past 23 years, 164,582 cases of HFRS (4.9 per 105 people) and 71,579 cases of TBE (2.5 per 105 people) were registered in Russia. The mortality rate was 0.4% (668 cases) in HFRS and 1.6% deaths (1136 cases) in TBE. There were 4030 HFRS (2.5%) and 9414 TBE (13%) cases in children under 14 years old. HFRS and TBE cases were registered in 42 out of 85 Russian regions; in 18-only HFRS, in 13-only TBE, and 12 had no reported cases. The prospects of applying a combined vaccine for HFRS and TBE prevention are shown in this paper.
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  • 文章类型: Journal Article
    正太病毒是人畜共患的病原体,在人类中引起急性和严重的综合征。进行这项审查是为了估计2010年至2022年之间南美人类正州病毒的发生。在对四个数据库进行系统的书目搜索后,对文章的资格和质量进行了仔细评估。使用随机效应模型荟萃分析计算了人类正畸病毒的合并频率。通过亚组分析和荟萃回归研究了估计值的异质性(由chi2检验和I2统计量产生)。在来自七个南美国家的35,548人中,诊断出了1,962例确诊的正坦病毒感染病例。基于来自32项研究的人类病例的一般汇集,估计正交病毒的一般发生率为4.4%(95%置信区间:2.9-6.2%)。在考虑研究设计和诊断方法的亚组分析中,确诊的正坦病毒感染的百分比有很大差异(I2=97.8%,p=0.00)在南美国家中。在阿根廷已经发现了四种正坦病毒的遗传变异,巴西,玻利维亚,智利,哥伦比亚,秘鲁。尽管在南美的许多国家中没有进行正交病毒的实验室诊断,有证据表明,四种不同的正州病毒在该地区传播。在超过一半的南美国家中,病毒感染的合并发生率约为4.0%。关于人类感染发生的最新信息对于监测领土传播和确定这种人畜共患病的频率至关重要。
    Orthohantaviruses are zoonotic pathogens that cause acute and severe syndromes in humans. This review was performed to estimate the occurrence of human orthohantaviruses in South America between 2010 and 2022. A careful evaluation of the eligibility and quality of the articles was carried out after a systematic bibliographic search of four databases. The pooled frequency of human orthohantaviruses was calculated using a random effects model meta-analysis. The heterogeneity of estimates (resulting from the chi2 test and I2 statistics) was investigated by subgroup analysis and meta-regression. 1,962 confirmed cases of orthohantavirus infections were diagnosed among 35,548 individuals from seven South American countries. The general occurrence of orthohantaviruses was estimated to be 4.4% (95% confidence interval: 2.9-6.2%) based on general pooling of human cases from 32 studies. In a subgroup analysis considering the study design and method of diagnosis, the percentages of diagnosed orthohantavirus infections differed substantially (I2 = 97.8%, p = 0.00) among South American countries. Four genetic variants of orthohantavirus have been identified circulating in Argentina, Brazil, Bolivia, Chile, Colombia, and Peru. Although laboratory diagnosis of orthohantaviruses is not performed in many countries in South America, there is evidence that four different orthohantaviruses are circulating in the region. The pooled occurrence of viral infection was approximately 4.0% in more than half of the South American countries. Updated information on the occurrence of human infections is essential for monitoring the territorial spread and determining the frequency of this zoonosis.
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  • 文章类型: Journal Article
    呼伦贝尔地区,以其多样的地形和丰富的野生动物而闻名,是各种自然流行疾病的热点。在2021年至2023年之间,我们从该地区收集了885个野生啮齿动物样本,代表三个家庭,七个属,11种。宏基因组分析确定了来自S,M,和汉塔病毒科的L段,与哈巴罗夫斯克病毒密切相关。S的核苷酸编码序列,M,和L(1392nt,3465nt,6491nt,分别)表现出82.34%的相似性,81.68%,和81.94%的已知序列,分别,而蛋白质水平分析表明94.92%的相似性更高,94.41%,和95.87%,分别。系统发育分析将这些序列置于与哈巴罗夫斯克相同的进化枝中,Puumala,Muju,北海道,Topografov,和塔特纳兰病毒,众所周知,所有这些都会导致人类发热性疾病。使用出血热和肾综合征患者的血清对核酸阳性啮齿动物肾脏样本进行免疫荧光检测证实了病毒颗粒的存在。基于这些发现,我们认为这种病毒代表了汉塔病毒科的新成员,暂定名为阿穆古朗病毒,在其主要分布区域之后。
    The Hulunbuir region, known for its diverse terrain and rich wildlife, is a hotspot for various natural epidemic diseases. Between 2021 and 2023, we collected 885 wild rodent samples from this area, representing three families, seven genera, and eleven species. Metagenomic analysis identified three complete nucleic acid sequences from the S, M, and L segments of the Hantaviridae family, which were closely related to the Khabarovsk virus. The nucleotide coding sequences for S, M, and L (1392 nt, 3465 nt, and 6491 nt, respectively) exhibited similarities of 82.34%, 81.68%, and 81.94% to known sequences, respectively, while protein-level analysis indicated higher similarities of 94.92%, 94.41%, and 95.87%, respectively. Phylogenetic analysis placed these sequences within the same clade as the Khabarovsk, Puumala, Muju, Hokkaido, Topografov, and Tatenalense viruses, all of which are known to cause febrile diseases in humans. Immunofluorescence detection of nucleic acid-positive rodent kidney samples using sera from patients with hemorrhagic fever and renal syndrome confirmed the presence of viral particles. Based on these findings, we propose that this virus represents a new member of the Hantaviridae family, tentatively named the Amugulang virus, after its primary distribution area.
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  • 文章类型: Case Reports
    汉坦病毒心肺综合征是一种由啮齿动物排泄物传播的严重疾病。我们描述了一个24岁男子咳嗽到急诊科就诊的案例,呼吸急促,发冷,肌痛,恶心,和腹泻。体格检查和实验室分析显示呼吸窘迫和血小板减少的迹象。他患病的轨迹导致急性呼吸窘迫综合征(ARDS)和血流动力学不稳定。血清检测汉坦病毒IgM和IgG抗体呈阳性。患者接受支持性治疗并得到改善。这个案例强调了在管理发生血小板减少症的患者时考虑汉坦病毒的重要性,ARDS,和血流动力学不稳定在适当的临床设置。
    Hantavirus cardiopulmonary syndrome is a severe illness transmitted by rodent excretions. We describe a case of a 24-year-old man who presented to the emergency department with cough, shortness of breath, chills, myalgias, nausea, and diarrhea. Physical examination and laboratory analysis revealed signs of respiratory distress and thrombocytopenia. The trajectory of his illness led to acute respiratory distress syndrome (ARDS) and hemodynamic instability. Serum testing was positive for hantavirus IgM and IgG antibodies. The patient was managed with supportive care and improved. This case highlights the importance of considering hantavirus when managing patients who develop thrombocytopenia, ARDS, and hemodynamic instability in the appropriate clinical setting.
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  • 文章类型: Journal Article
    肾综合征出血热(HFRS)和血小板减少综合征(SFTS)在农村地区都很流行,HFRS和SFTS之间的一些特征相似。这通常会导致误诊。在这项研究中,我们总结并比较了HFRS和SFTS的一些特征,这将为鉴别诊断提供科学信息。2011年至2022年,浙江省共报告43例HFRS和737例SFTS。与SFTS相比,HFRS病例中男性比例较高(72.46%[3142/4336]与50.88%[375/737],p=0.000)。所有4336例HFRS病例的中位年龄为49(39,59),而SFTS病例的中位年龄为66(57,74)。此外,HFRS涉及的县比SFTS多,但从2011年到2022年,受SFTS影响的县数量有所增加。大多数SFTS病例发生在夏季(5月至7月),但除了夏天,HFRS病例也在冬季出现高峰。最后,我们的结果表明,SFTS的病死率明显高于HFRS。尽管HFRS和SFTS之间有一些相似之处,我们的研究发现了它们之间的一些差异,比如性别分布,年龄分布,和季节性分布,这将为HFRS和SFTS的鉴别诊断提供科学信息。应该进行进一步的研究来探索这些差异的机制。
    Hemorrhagic fever with renal syndrome (HFRS) and severe fever with thrombocytopenia syndrome (SFTS) are both endemic in rural areas and some characteristics are similar between HFRS and SFTS, which usually lead to misdiagnosis. In this study, we summarized and compared some characteristics of HFRS and SFTS which will provide scientific information for differential diagnosis. From 2011 to 2022, a total of 4336 HFRS cases and 737 SFTS cases were reported in Zhejiang Province. Compared to SFTS, there was a higher proportion of males among HFRS cases (72.46% [3142/4336] vs. 50.88% [375/737], p = 0.000). The median age of all 4336 HFRS cases was 49 (39, 59), while the median age of SFTS cases was 66 (57, 74). In addition, the involved counties of HFRS were more than SFTS, but the number of counties affected by SFTS increased from 2011 to 2022. The majority of SFTS cases occurred in summer (from May to July), but besides summer, HFRS cases also showed a peak in winter. Finally, our results showed that the case fatality rate of SFTS was significantly higher than that of HFRS. Although there were some similarities between HFRS and SFTS, our study found several differences between them, such as gender distribution, age distribution, and seasonal distribution, which will provide scientific information for differential diagnosis of HFRS and SFTS. Further studies should be carried out to explore the mechanism of these differences.
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  • 文章类型: Journal Article
    在美国(美国),汉坦病毒肺综合征(HPS)和非HPS汉坦病毒感染是国家法定报告的疾病。识别人类病例的标准基于临床症状(HPS或非HPS)和急性诊断结果(IgM,IgG+滴度上升,RT-PCR+,或免疫组织化学(IHC)+)。在这里,我们提供了诊断测试的概述,并总结了2008年至2020年美国汉坦病毒病的发生和基因型分布。
    国家汉坦病毒登记处的流行病学数据与CDC进行的实验室诊断测试结果合并。对残留的汉坦病毒阳性标本进行测序,和可用的流行病学和遗传数据集进行了汉坦病毒病的基因组流行病学研究在美国
    从1993年到2020年,已经确定了833例人类汉坦病毒病例,从2008年到2020年,发生了335例人类病例。在CDC诊断实验室检测到的新世界(NW)汉坦病毒病例中(占总病例的29.2%),大多数(85.0%)是在急性疾病期间检测到的,然而,在传统上与汉坦病毒感染无关的州检测到一些恢复期病例(康涅狄格州,密苏里州,新泽西,宾夕法尼亚,田纳西州,和佛蒙特州)。从1993年到2020年,在密西西比州以西发现了94.9%(745/785)的美国汉坦病毒病例,在美国四角地区发现了45.7%(359/785)。从2008年到2020年,在3月至8月之间检测到67.7%的NW汉坦病毒病例。对RT-PCR阳性病例的测序表明,正坦病毒synnombreense种[SinNombre病毒(SNV),纽约病毒,和莫农加希拉病毒];然而,美国西北部和中部的病毒序列数据存在很大差距,这些数据表明,商业IgM测定与CDC开发的测定不一致,和“一致阳性”(即,商业IgM和CDCIgM结果)标本表现出汉坦病毒病的临床特征。
    汉塔病毒病广泛分布在美国病毒变体被定位到特定的地理区域,在大多数东南州很少发现汉坦病毒病。两种诊断检测方法之间的不一致结果凸显了美国汉坦病毒监测和检测将继续改进的标准化测试计划的必要性,系统报告方法,以及临床特征和诊断标准的明确指南。
    这项工作由提供给CDC病毒特殊病原体分支的核心资金资助。
    UNASSIGNED: In the United States (U.S.), hantavirus pulmonary syndrome (HPS) and non-HPS hantavirus infection are nationally notifiable diseases. Criteria for identifying human cases are based on clinical symptoms (HPS or non-HPS) and acute diagnostic results (IgM+, rising IgG+ titers, RT-PCR+, or immunohistochemistry (IHC)+). Here we provide an overview of diagnostic testing and summarize human Hantavirus disease occurrence and genotype distribution in the U.S. from 2008 to 2020.
    UNASSIGNED: Epidemiological data from the national hantavirus registry was merged with laboratory diagnostic testing results performed at the CDC. Residual hantavirus-positive specimens were sequenced, and the available epidemiological and genetic data sets were linked to conduct a genomic epidemiological study of hantavirus disease in the U.S.
    UNASSIGNED: From 1993 to 2020, 833 human hantavirus cases have been identified, and from 2008 to 2020, 335 human cases have occurred. Among New World (NW) hantavirus cases detected at the CDC diagnostic laboratory (representing 29.2% of total cases), most (85.0%) were detected during acute disease, however, some convalescent cases were detected in states not traditionally associated with hantavirus infections (Connecticut, Missouri, New Jersey, Pennsylvania, Tennessee, and Vermont). From 1993 to 2020, 94.9% (745/785) of U.S. hantaviruses cases were detected west of the Mississippi with 45.7% (359/785) in the Four Corners region of the U.S. From 2008 to 2020, 67.7% of NW hantavirus cases were detected between the months of March and August. Sequencing of RT-PCR-positive cases demonstrates a geographic separation of Orthohantavirus sinnombreense species [Sin Nombre virus (SNV), New York virus, and Monongahela virus]; however, there is a large gap in viral sequence data from the Northwestern and Central U.S. Finally, these data indicate that commercial IgM assays are not concordant with CDC-developed assays, and that \"concordant positive\" (i.e., commercial IgM+ and CDC IgM+ results) specimens exhibit clinical characteristics of hantavirus disease.
    UNASSIGNED: Hantaviral disease is broadly distributed in the contiguous U.S, viral variants are localised to specific geographic regions, and hantaviral disease infrequently detected in most Southeastern states. Discordant results between two diagnostic detection methods highlight the need for an improved standardised testing plan in the U.S. Hantavirus surveillance and detection will continue to improve with clearly defined, systematic reporting methods, as well as explicit guidelines for clinical characterization and diagnostic criteria.
    UNASSIGNED: This work was funded by core funds provided to the Viral Special Pathogens Branch at CDC.
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  • 文章类型: Journal Article
    啮齿动物传播的安第斯山脉病毒(ANDV)在人类中引起严重的疾病。我们开发了一种基于病毒基因组M片段的ANDVmRNA疫苗,与常规尿苷(U-mRNA)或N1-甲基假尿苷(m1kW-mRNA)。与U-mRNA免疫的小鼠相比,用m1Φ-mRNA免疫的雌性小鼠产生了更大的生发中心(GC)反应。GCB细胞的单细胞RNA和BCR测序显示了相似的活化水平,除了在接种了U-mRNA而不是m1btr-mRNA的动物中表现出干扰素反应的另外一簇细胞。在对疫苗的反应中观察到类似的免疫球蛋白类别转换和体细胞超突变。雌性叙利亚仓鼠通过初免方案免疫接种,每种疫苗接种两剂。U-mRNA构建体的糖蛋白结合抗体的滴度高于m1bps-mRNA构建体;然而,ANDV中和抗体的滴度相似.接种疫苗的动物用致死剂量的ANDV攻击,以及一个天真的对照组。所有对照动物和用较低剂量的m1btr-mRNA接种的两只动物都死于感染,而其他接种的动物存活而没有病毒复制的证据。数据表明开发了针对ANDV的保护性疫苗,并且缺乏m1Φ修饰对啮齿动物的免疫原性和保护作用的实质性影响。
    The rodent-borne Andes virus (ANDV) causes a severe disease in humans. We developed an ANDV mRNA vaccine based on the M segment of the viral genome, either with regular uridine (U-mRNA) or N1-methylpseudouridine (m1Ψ-mRNA). Female mice immunized by m1Ψ-mRNA developed slightly greater germinal center (GC) responses than U-mRNA-immunized mice. Single cell RNA and BCR sequencing of the GC B cells revealed similar levels of activation, except an additional cluster of cells exhibiting interferon response in animals vaccinated with U-mRNA but not m1Ψ-mRNA. Similar immunoglobulin class-switching and somatic hypermutations were observed in response to the vaccines. Female Syrian hamsters were immunized via a prime-boost regimen with two doses of each vaccine. The titers of glycoprotein-binding antibodies were greater for U-mRNA construct than for m1Ψ-mRNA construct; however, the titers of ANDV-neutralizing antibodies were similar. Vaccinated animals were challenged with a lethal dose of ANDV, along with a naïve control group. All control animals and two animals vaccinated with a lower dose of m1Ψ-mRNA succumbed to infection whereas other vaccinated animals survived without evidence of virus replication. The data demonstrate the development of a protective vaccine against ANDV and the lack of a substantial effect of m1Ψ modification on immunogenicity and protection in rodents.
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  • 文章类型: Journal Article
    汉坦病毒是在美洲引起汉坦病毒心肺综合症(HCPS)的人畜共患因子,巴西在南美确诊的HCPS病例数中排名第一。在这项研究中,我们通过将Kermack-McCormickSIR模型与细胞自动机模型(CA)结合来模拟高致死汉坦病毒在自然宿主中的每月传播,因此,同时评估宿主群体中的细胞内和细胞间感染动力学,使用最近汇编的主要宿主物种丰度和确认的汉坦病毒感染死亡数据。对于两种宿主物种来说,我们的模型预测感染面积会增加,迄今为止尚未确认病例的22个城市预计在未来十年内至少有一例病例,11个城市的感染率下降。我们的发现支持现有的研究,并揭示了汉坦病毒可能在公认的震中传播的新领域。突出时空趋势和潜在扩展,我们强调,由于普遍的栖息地碎片化和农业扩张,风险增加。持续的预防工作和“一个健康”行动至关重要,特别是在新确定的高风险城市。
    Hantaviruses are zoonotic agents responsible for causing Hantavirus Cardiopulmonary Syndrome (HCPS) in the Americas, with Brazil ranking first in number of confirmed HCPS cases in South America. In this study, we simulate the monthly spread of highly lethal hantavirus in natural hosts by conjugating a Kermack-McCormick SIR model with a cellular automata model (CA), therefore simultaneously evaluating both in-cell and between-cell infection dynamics in host populations, using recently compiled data on main host species abundances and confirmed deaths by hantavirus infection. For both host species, our models predict an increase in the area of infection, with 22 municipalities where no cases have been confirmed to date expected to have at least one case in the next decade, and a reduction in infection in 11 municipalities. Our findings support existing research and reveal new areas where hantavirus is likely to spread within recognized epicenters. Highlighting spatial-temporal trends and potential expansion, we emphasize the increased risk due to pervasive habitat fragmentation and agricultural expansion. Consistent prevention efforts and One Health actions are crucial, especially in newly identified high-risk municipalities.
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  • 文章类型: Journal Article
    Puumala原位病毒(PUUV)是欧洲和俄罗斯特有的一种新兴的人畜共患病毒,可引起肾病流行病,轻度肾综合征出血热(HFRS)。目前治疗和诊断正瘤病毒感染的选择有限,使得寻找潜在的免疫原性候选者至关重要。在目前的工作中,各种生物信息学工具被用来设计包含PUUV核衣壳蛋白多个表位的保守免疫原性肽。鉴定了PUUV核衣壳蛋白的11种保守肽(90%保守性)。使用共有表位预测算法选择含有多个T和B细胞表位的三个保守肽。使用HPEP对接服务器的分子对接证明了表位和HLA分子之间的强结合相互作用(每种I类和II类HLA的10个等位基因)。此外,使用IEDB数据库对人口覆盖率进行的分析显示,所鉴定的肽在六大洲的平均人口覆盖率超过90%。分子对接和模拟分析揭示了与所选免疫原性肽和Toll样受体-4的肽构建体的稳定相互作用。这些计算分析证明了选定的肽的免疫原性潜力,这需要在不同的实验系统中进行验证。
    Puumala orthohantavirus (PUUV) is an emerging zoonotic virus endemic to Europe and Russia that causes nephropathia epidemica, a mild form of hemorrhagic fever with renal syndrome (HFRS). There are limited options for treatment and diagnosis of orthohantavirus infection, making the search for potential immunogenic candidates crucial. In the present work, various bioinformatics tools were employed to design conserved immunogenic peptides containing multiple epitopes of PUUV nucleocapsid protein. Eleven conserved peptides (90% conservancy) of the PUUV nucleocapsid protein were identified. Three conserved peptides containing multiple T and B cell epitopes were selected using a consensus epitope prediction algorithm. Molecular docking using the HPEP dock server demonstrated strong binding interactions between the epitopes and HLA molecules (ten alleles for each class I and II HLA). Moreover, an analysis of population coverage using the IEDB database revealed that the identified peptides have over 90% average population coverage across six continents. Molecular docking and simulation analysis reveal a stable interaction with peptide constructs of chosen immunogenic peptides and Toll-like receptor-4. These computational analyses demonstrate selected peptides\' immunogenic potential, which needs to be validated in different experimental systems.
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