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微囊化疫苗增强对委内瑞拉马脑炎(VEE)病毒的保护性免疫反应。

Enhancement of protective immune responses to Venezuelan equine encephalitis (VEE) virus with microencapsulated vaccine.

作者信息

Greenway T E, Eldridge J H, Ludwig G, Staas J K, Smith J F, Gilley R M, Michalek S M

机构信息

Department of Microbiology, University of Alabama at Birmingham 35294, USA.

出版信息

Vaccine. 1995;13(15):1411-20. doi: 10.1016/0264-410x(95)00076-d.

Abstract

Venezuelan equine encephalomyelitis (VEE) virus is a mosquito-borne arbovirus of major human health significance in the New World. Currently two forms of VEE virus are used for immunization of humans and horses, i.e. a live attenuated and a formalin-inactivated vaccine. Clinical evidence suggests that these vaccines are not fully efficacious and may produce certain undesirable side-effects. In the present study, microspheres composed of biocompatible and biodegradable poly (DL-lactide-co-glycolide) (DL-PLG) were evaluated for their effectiveness as a delivery system of whole, inactivated VEE virus vaccine for the induction of protective immune responses. Mice receiving 50 micrograms VEE virus in microspheres composed of an equimolar ratio of DL-lactide and glycolide (50:50 DL-PLG) exhibited a primary circulating IgG antibody response which was approximately 32-times higher than the response induced with the same dose of unencapsulated (free) virus. A similar difference in responses was seen with antigen doses ranging from 3.1 to 50 micrograms. A rapid increase in antibody activity was seen after the secondary immunization (day 50). Formalin fixation of inactivated VEE virus was important for immunogenicity since the circulating anti-VEE virus antibody response induced with microencapsulated nonformalin-fixed virus vaccine was lower than that induced with microencapsulated formalin-fixed virus vaccine. Furthermore, at low antigen concentrations, DL-PLG microsphere vaccines prepared with the solvent methylene chloride induced higher antibody responses than those prepared using ethyl acetate as the solvent. Microencapsulated vaccine also induced higher VEE virus neutralization titers than did free virus vaccine. Finally, the microencapsulated virus was more effective than the free virus in inducing immune responses protective against systemic challenge with virulent VEE virus. These results demonstrate that DL-PLG microspheres containing formalin-fixed, inactivated VEE virus were effective in augmenting circulating IgG antibody levels and neutralization titers to the VEE virus following systemic immunization and in affording enhanced protection against systemic challenge with virulent VEE virus. The effects of antigen form and the microsphere processing solvent on the immunogenicity of the vaccine are discussed.

摘要

委内瑞拉马脑炎(VEE)病毒是一种由蚊子传播的虫媒病毒,在新大陆对人类健康具有重大意义。目前,两种形式的VEE病毒被用于人类和马匹的免疫接种,即减毒活疫苗和福尔马林灭活疫苗。临床证据表明,这些疫苗并非完全有效,且可能产生某些不良副作用。在本研究中,对由生物相容性和可生物降解的聚(DL-丙交酯-共-乙交酯)(DL-PLG)组成的微球作为全灭活VEE病毒疫苗的递送系统诱导保护性免疫反应的有效性进行了评估。接受由等摩尔比的DL-丙交酯和乙交酯(50:50 DL-PLG)组成的微球中50微克VEE病毒的小鼠表现出初次循环IgG抗体反应,该反应比相同剂量的未包封(游离)病毒诱导的反应高约32倍。在3.1至50微克的抗原剂量范围内也观察到类似的反应差异。二次免疫(第50天)后抗体活性迅速增加。灭活VEE病毒的福尔马林固定对免疫原性很重要,因为微囊化的非福尔马林固定病毒疫苗诱导的循环抗VEE病毒抗体反应低于微囊化福尔马林固定病毒疫苗诱导的反应。此外,在低抗原浓度下,用二氯甲烷作为溶剂制备的DL-PLG微球疫苗比用乙酸乙酯作为溶剂制备的疫苗诱导更高的抗体反应。微囊化疫苗也比游离病毒疫苗诱导更高的VEE病毒中和滴度。最后,微囊化病毒在诱导针对强毒VEE病毒全身攻击的保护性免疫反应方面比游离病毒更有效。这些结果表明,含有福尔马林固定的灭活VEE病毒的DL-PLG微球在全身免疫后有效提高循环IgG抗体水平和对VEE病毒的中和滴度,并能增强对强毒VEE病毒全身攻击的保护作用。讨论了抗原形式和微球加工溶剂对疫苗免疫原性的影响。

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