在感染波萨达斯球孢子菌的人类白细胞抗原表达转基因小鼠中对疫苗诱导的保护性相关因素进行临床前鉴定。
Preclinical identification of vaccine induced protective correlates in human leukocyte antigen expressing transgenic mice infected with Coccidioides posadasii.
作者信息
Hurtgen Brady J, Castro-Lopez Natalia, Jiménez-Alzate Maria Del Pilar, Cole Garry T, Hung Chiung-Yu
机构信息
Department of Biology and South Texas Center for Emerging Infectious Diseases, University of Texas, San Antonio, TX, USA; Department of Microbiology and Immunology, University of Texas Health Science Center at San Antonio, TX, USA.
Department of Biology and South Texas Center for Emerging Infectious Diseases, University of Texas, San Antonio, TX, USA.
出版信息
Vaccine. 2016 Oct 17;34(44):5336-5343. doi: 10.1016/j.vaccine.2016.08.078. Epub 2016 Sep 9.
There is an emerging interest to develop human vaccines against medically-important fungal pathogens and a need for a preclinical animal model to assess vaccine efficacies and protective correlates. HLA-DR4 (DRB1∗0401 allele) transgenic mice express a human major histocompatibility complex class II (MHC II) receptor in such a way that CD4 T-cell response is solely restricted by this human molecule. In this study HLA-DR4 transgenic mice were immunized with a live-attenuated vaccine (ΔT) and challenged by the intranasal route with 50-70 Coccidioides posadasii spores, a potentially lethal dose. The same vaccination regimen offers 100% survival for C57BL/6 mice. Conversely, ΔT-vaccinated HLA-DR4 mice displayed 3 distinct manifestations of Coccidioides infection including 40% fatal acute (FAD), 30% disseminated (DD) and 30% pulmonary disease (PD). The latter 2 groups of mice had reduced loss of body weight and survived to at least 50days postchallenge (dpc). These results suggest that ΔT vaccinated HLA-DR4 mice activated heterogeneous immunity against pulmonary Coccidioides infection. Vaccinated HLA-DR4 mice displayed early expansion of Th1 and Th17 cells and recruitment of inflammatory innate cells into Coccidioides-infected lungs during the first 9dpc. While contraction rates of Th cells and the inflammatory response during 14-35dpc significantly differed among the 3 groups of vaccinated HLA-DR4 mice. The FAD group displayed a sharply reduced Th1 and Th17 response, while overwhelmingly recruiting neutrophils into lungs during 9-14days. The FAD group approached moribund by 14dpc. In contrast, vaccinated HLA-DR4 survivors gradually contracted Th cells and inflammatory response with the greatest rate in the PD group. While vaccinated HLA-DR4 mice are susceptible to Coccidioides infection, they are useful for evaluation of vaccine efficacy and identification of immunological correlates against this mycosis.
开发针对具有医学重要性的真菌病原体的人类疫苗的兴趣日益浓厚,并且需要一种临床前动物模型来评估疫苗效力和保护性关联因素。HLA-DR4(DRB1∗0401等位基因)转基因小鼠以这样一种方式表达人类主要组织相容性复合体II类(MHC II)受体,即CD4 T细胞反应仅受该人类分子限制。在本研究中,用减毒活疫苗(ΔT)对HLA-DR4转基因小鼠进行免疫,并通过鼻内途径用50 - 70个波萨达斯球孢子菌孢子进行攻击,这是一个潜在的致死剂量。相同的疫苗接种方案能使C57BL/6小鼠100%存活。相反,用ΔT疫苗接种的HLA-DR4小鼠表现出球孢子菌感染的3种不同表现,包括40%的致命急性感染(FAD)、30%的播散性感染(DD)和30%的肺部疾病(PD)。后两组小鼠体重减轻减少,并且在攻击后至少存活50天(dpc)。这些结果表明,用ΔT疫苗接种的HLA-DR4小鼠激活了针对肺部球孢子菌感染的异质性免疫。接种疫苗的HLA-DR4小鼠在攻击后的前9天显示出Th1和Th17细胞的早期扩增以及炎性固有细胞募集到被球孢子菌感染的肺部。虽然在接种疫苗的3组HLA-DR4小鼠中,14 - 35天期间Th细胞的收缩率和炎症反应存在显著差异。FAD组的Th1和Th17反应急剧降低,而在9 - 14天期间大量募集嗜中性粒细胞到肺部。FAD组在14 dpc时接近濒死状态。相比之下,接种疫苗的HLA-DR4存活者逐渐收缩Th细胞和炎症反应,其中PD组的收缩率最大。虽然接种疫苗的HLA-DR4小鼠易受球孢子菌感染,但它们对于评估疫苗效力和确定针对这种真菌病的免疫关联因素很有用。
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