Non-peptidic HIV vaccine
非肽HIV疫苗
基本信息
- 批准号:7852915
- 负责人:
- 金额:$ 50万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2009
- 资助国家:美国
- 起止时间:2009-09-30 至 2011-08-31
- 项目状态:已结题
- 来源:
- 关键词:AIDS/HIV problemAcquired Immunodeficiency SyndromeAddressAdjuvantAnimalsAntibody FormationAntigensAttenuatedBiological AssayBlood CellsBlood specimenCD4 Positive T LymphocytesCD8B1 geneCXCR4 geneCell CountCellsColorControl GroupsDiphosphatesDiseaseEffector CellEnzyme-Linked Immunosorbent AssayFlow CytometryGaggingGenetic VariationHIV vaccineHIV-1Humoral ImmunitiesImmuneImmune responseImmunityImmunologic AdjuvantsInfectionInterleukin-2IntravenousLactococcus lactisListeriaLymphoidLymphoid TissueMacacaMacaca mulattaMeasuresMemoryMethodsMucous MembraneMycobacterium tuberculosisOutcomePeptidesPlasmaRecombinantsResistanceSIVStaining methodStainsSystemT-LymphocyteTestingTimeVaccinatedVaccinationVaccinesViral Load resultVirusVirus Replicationcytokineenzyme linked immunospot assayimmunogenicimprovedmucosal sitenovel strategiesnovel vaccinesparticleprotective effectpublic health relevancereceptorresponsesimian human immunodeficiency virussuccesstraffickingvaccine deliveryvector vaccineviral RNA
项目摘要
DESCRIPTION (provided by applicant): HIV-caused AIDS is a potentially lethal disease with no vaccine or cure available at the moment. The obstacles to overcome when developing an effective HIV vaccine include devising a strategy that would generate cellular and humoral immunity with sufficient a) strength to be 'virus- replication-clobbering' and b) breadth to address the extraordinary genetic diversity of the virus. Our proposal is focused specifically on increasing the 'immunizing strength' of HIV vaccines. For this purpose we have developed highly immunogenic recombinant attenuated Listeria vaccine vectors and recombinant Lactococcus lactis vaccine particles. Antigenic priming and boosting with these new vaccine-delivery systems elicits remarkable T-cell and Ab responses. In addition, we have demonstrated that a nonpeptidic phosphoantigen (E)-4-hydroxy-3-methyl-but-2-enyl pyrophosphate (HMBPP) together with interleukin-2 stimulate prolonged expansion of V32V42 T effector cells in the lymphoid and mucosal compartments and enhance 12 T-cell and antibody responses. Here we propose studies to ascertain whether or not the strong immunoadjuvant effect of V32V42 T-cell stimulation can be utilized in increasing the 'immunizing strength' of HIV vaccines. Specifically, we propose to test our hypothesis that V32V42 T effector cells generated after HMBPP/IL-2 treatment can readily traffic to the lymphoid tissues and mucosae and upregulate the breadth and magnitude of HIV vaccine-elicited T-cell and antibody responses and ultimately increase the vaccine's protective effects against HIV/AIDS. Thus, our main specific aim is to determine whether the V32V42 T-cell-activating/expanding treatment with HMBPP plus IL-2 can augment the anti-SHIV89.6P potency of our attenuated Listeria ?actA prfA* vaccine vectors expressing HIV-1 Env and SIV gag in SHIV89.6P-challenged rhesus macaques.
PUBLIC HEALTH RELEVANCE: There is no vaccine or cure for HIV/AIDS, which is a potentially lethal disease. The main focus of this application is to test a novel strategy for boosting the capacity of HIV vaccines to induce protective responses against HIV/AIDS. Even partial success may have worldwide beneficial effect.
描述(由申请人提供):艾滋病毒引起的艾滋病是一种潜在的致命疾病,目前没有疫苗或治疗方法。在开发有效的HIV疫苗时要克服的障碍包括设计一种策略,该策略将产生具有足够的a)“病毒复制-击倒”的强度和B)针对病毒的非凡遗传多样性的广度的细胞和体液免疫。我们的建议特别侧重于提高艾滋病毒疫苗的“免疫强度”。为此,我们开发了高免疫原性的重组减毒李斯特菌疫苗载体和重组乳酸乳球菌疫苗颗粒。用这些新的疫苗递送系统进行的抗原引发和加强激发了显著的T细胞和Ab应答。此外,我们已经证明,非肽磷酸化抗原(E)-4-羟基-3-甲基-丁-2-烯焦磷酸(HMBPP)与白细胞介素-2刺激淋巴和粘膜隔室中的V32 V42 T效应细胞的长期扩增,并增强12 T细胞和抗体应答。在这里,我们提出的研究,以确定是否可以利用V32 V42 T细胞刺激的强免疫佐剂作用,以增加“免疫强度”的HIV疫苗。具体地说,我们建议测试我们的假设,即HMBPP/IL-2治疗后产生的V32 V42 T效应细胞可以容易地运输到淋巴组织和粘膜,并上调HIV疫苗引起的T细胞和抗体应答的广度和幅度,并最终增加疫苗对HIV/AIDS的保护作用。因此,我们的主要具体目标是确定用HMBPP加IL-2的V32 V42 T细胞活化/扩增处理是否可以增强我们的减毒李斯特菌的抗SHIV 89.6P效力?在SHIV89.6P攻击的恒河猴中表达HIV-1 Env和SIV gag的actA prfA* 疫苗载体。
公共卫生相关性:艾滋病毒/艾滋病是一种潜在的致命疾病,没有疫苗或治愈方法。这项申请的主要重点是测试一种新的策略,以提高艾滋病毒疫苗诱导对艾滋病毒/艾滋病的保护性反应的能力。即使是部分成功也可能产生世界性的有益影响。
项目成果
期刊论文数量(0)
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MIROSLAV MALKOVSKY其他文献
MIROSLAV MALKOVSKY的其他文献
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{{ truncateString('MIROSLAV MALKOVSKY', 18)}}的其他基金
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- 资助金额:
$ 50万 - 项目类别:
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6213966 - 财政年份:2000
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6751654 - 财政年份:2000
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