Engineering high fidelity mutations to increase safety of live-attenuated alphavirus vaccines
设计高保真突变以提高减毒甲病毒疫苗的安全性
基本信息
- 批准号:9925764
- 负责人:
- 金额:$ 53.83万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2016
- 资助国家:美国
- 起止时间:2016-06-20 至 2022-05-31
- 项目状态:已结题
- 来源:
- 关键词:AdultAdverse effectsAdverse eventAdverse reactionsAfricaAlphavirusAmericasAntigen-Presenting CellsArthralgiaArthritisAsiaAttenuatedAttenuated Live Virus VaccineBrainCellsChemicalsChikungunya virusClinicalClinical TrialsCulicidaeDevelopmentDiseaseDose-LimitingEncephalitisEngineeringFormulationGeneticGenetic VariationGenomeGoalsGoldHumanImmunityInfectionKineticsLaboratoriesLeadMeaslesMeasuresMorbidity - disease rateMusMuscleMutagensMutateMutationOrganPoint MutationRNA VirusesResourcesRiskSafetySyndromeTestingTravelTropismVaccinationVaccinesVariantVenezuelan Equine Encephalitis VirusVenezuelan Equine EncephalomyelitisViralViremiaVirulenceVirulentVirusVirus DiseasesVirus ReplicationYellow fever virusattenuationchikungunyacostdraining lymph nodeemerging human pathogenhuman modelhuman pathogenimmunogenicimmunogenicityimprovedlymph nodesmortalitymosquito-bornemouse modelneutralizing antibodypre-clinicalpreventprogenitorrecruittransmission processtreatment strategyvaccine candidatevaccine safetyvectorvector mosquitoviral RNAvirus geneticsvirus tropism
项目摘要
Project Summary
Live-attenuated vaccines are the gold standard for preventing viral illness but they can
revert to virulence, sometimes causing severe or fatal disease. The mosquito-borne
alphaviruses chikungunya (CHIKV) and Venezuelan equine encephalitis (VEEV) are
RNA viruses that produce a debilitating arthritic syndrome or encephalitis, respectively.
Both have repeatedly emerged to produce millions of human cases worldwide and
CHIKV has expanded into the Americas since 2013, indicating increasing need for
vaccines. Although live-attenuated candidate human vaccines have been developed for
both viruses, no licensed vaccines currently exist, in part due to adverse events in
clinical trials caused by revertant mutations. There is therefore a need to increase the
genetic stability of live-attenuated virus vaccine candidates to improve safety. The goal
of this project is to develop safe and effective CHIKV and VEEV vaccines to
prevent millions of human infections globally each year. Virus variants that mutate
less frequently would accrue fewer mutations that confer virulence, and may therefore
serve as safer live-attenuated vaccine candidates. This project will use high fidelity
variants we already identified and characterized inserted into candidate CHIKV and
VEEV vaccines to understand: 1) stability, infectivity, and potential for reversion; 2)
whether incorporation of high fidelity mutations improves vaccine safety while
maintaining or increasing immunogenicity in established mouse models; and 3)
mechanism(s) of attenuation. This approach represents the first use of fidelity
modulation to increase safety of live alphavirus vaccine candidates. If successful, this
strategy will potentially lead to a broader application of fidelity variants in improving
vaccine safety that can be used for other live-attenuated alphavirus vaccine platforms
and possibly other RNA viruses.
项目摘要
减毒活疫苗是预防病毒性疾病的金标准,但它们可以
恢复毒性,有时会导致严重或致命的疾病。蚊子传播的
基孔肯雅病毒(CHIKV)和委内瑞拉马脑炎(VEEV)是
分别产生使人衰弱的关节炎综合征或脑炎的RNA病毒。
这两种病毒都反复出现,在全世界造成数百万人感染,
自2013年以来,CHIKV已扩展到美洲,这表明对
疫苗。尽管已经开发了减毒活候选人疫苗用于
对于这两种病毒,目前还没有获得许可的疫苗,部分原因是
回复突变引起的临床试验因此,有必要增加
遗传稳定性的减毒活病毒候选疫苗,以提高安全性。目标
该项目的目的是开发安全有效的CHIKV和VEEV疫苗,
每年在全球范围内预防数百万人感染。变异的病毒变种
频率较低会产生较少的突变,赋予毒力,因此可能
作为更安全的减毒活疫苗候选物。这个项目将使用高保真
我们已经鉴定并表征了插入候选CHIKV的变体,
VEEV疫苗需要了解:1)稳定性、感染性和逆转的可能性; 2)
高保真突变的掺入是否提高了疫苗的安全性,
在建立的小鼠模型中维持或增加免疫原性;和3)
衰减机制。这种方法代表了保真度的第一次使用
调节以增加活甲病毒疫苗候选物的安全性。如果成功,这
战略将有可能导致更广泛的应用保真度的变种,以改善
可用于其他减毒活甲病毒疫苗平台的疫苗安全性
可能还有其他RNA病毒。
项目成果
期刊论文数量(2)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
Venezuelan Equine Encephalitis Virus V3526 Vaccine RNA-Dependent RNA Polymerase Mutants Increase Vaccine Safety Through Restricted Tissue Tropism in a Murine Model.
- DOI:10.15212/zoonoses-2021-0016
- 发表时间:2022-01-01
- 期刊:
- 影响因子:0
- 作者:Haines, Clint A;Campos, Rafael K;Rossi, Shannan L
- 通讯作者:Rossi, Shannan L
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Lark L Coffey其他文献
Role of non-human primate models in accelerating research and developing countermeasures against Zika virus infection
非人灵长类动物模型在加速寨卡病毒感染研究和制定对策中的作用
- DOI:
10.1016/j.lanmic.2024.101030 - 发表时间:
2025-06-01 - 期刊:
- 影响因子:20.400
- 作者:
Amanda Li;Lark L Coffey;Emma L Mohr;Jessica Raper;Ann Chahroudi;Karla K Ausderau;Matthew T Aliota;Thomas C Friedrich;Ann M Mitzey;Michelle R Koenig;Thaddeus G Golos;Hannah K Jaeger;Victoria H J Roberts;Jamie O Lo;Jessica L Smith;Alec J Hirsch;Daniel N Streblow;Christina M Newman;David H O’Connor;Eve M Lackritz;Jurai Wongsawat - 通讯作者:
Jurai Wongsawat
Lark L Coffey的其他文献
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{{ truncateString('Lark L Coffey', 18)}}的其他基金
Collaborative cross mice as a new model for diverse human outcomes of St. Louis encephalitis virus disease
协作杂交小鼠作为圣路易斯脑炎病毒病多种人类结果的新模型
- 批准号:
10726431 - 财政年份:2023
- 资助金额:
$ 53.83万 - 项目类别:
Transmission dynamics and fitness of reemerging St. Louis encephalitis virus
重新出现的圣路易斯脑炎病毒的传播动力学和适应度
- 批准号:
10645668 - 财政年份:2023
- 资助金额:
$ 53.83万 - 项目类别:
Engineering high fidelity mutations to increase safety of live-attenuated alphavirus vaccines
设计高保真突变以提高减毒甲病毒疫苗的安全性
- 批准号:
9160799 - 财政年份:2016
- 资助金额:
$ 53.83万 - 项目类别:
Engineering high fidelity mutations to increase safety of live-attenuated alphavirus vaccines
设计高保真突变以提高减毒甲病毒疫苗的安全性
- 批准号:
9300831 - 财政年份:2016
- 资助金额:
$ 53.83万 - 项目类别:
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