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巴西副球孢子菌 60kDa 热休克蛋白编码 DNA 疫苗对实验性巴西副球孢子菌病的治疗作用。

Therapeutic effect of DNA vaccine encoding the 60-kDa-heat shock protein from Paracoccidoides brasiliensis on experimental paracoccidioidomycosis in mice.

机构信息

Ribeirão Preto Medical School, University of São Paulo, 14049-900 Ribeirão Preto, SP, Brazil.

Paulista University, 14024-270 Ribeirão Preto, SP, Brazil.

出版信息

Vaccine. 2019 Sep 3;37(37):5607-5613. doi: 10.1016/j.vaccine.2019.07.090. Epub 2019 Aug 6.

DOI:10.1016/j.vaccine.2019.07.090
PMID:31399276
Abstract

Paracoccidioidomycosis (PCM) is a systemic mycosis autochthonous to Latin America and endemic to Brazil, which has the majority of the PCM cases. PCM is acquired through the inhalation of propagules of fungi from genus Paracoccidioides spp. and mainly affects the lungs. We have previously shown that P. brasiliensis-infected mice treated with single-dose of recombinant 60-kDa-heat shock protein from P. brasiliensis (rPbHsp60) had a worsening infection in comparison to animals only infected. In this study, we investigate whether the treatment of infected mice with PB_HSP60 gene cloned into a plasmid (pVAX1-PB_HSP60) would result in efficient immune response and better control of the disease. The harmful impact of single-dose therapy with protein was not seen with plasmid preparations. Most importantly, three doses of pVAX1-PB_HSP60 and protein induced a beneficial effect in experimental PCM with a reduction in fungal load and lung injury when compared with infected mice treated with pVAX1 or PBS. The increase of the cytokines IFN-γ, TNF, and IL-17 and the decrease of IL-10 observed after treatment with three doses of pVAX1-PB_HSP60 appears to be responsible for the control of infection. These results open perspectives of the therapeutic use of Hsp60 in PCM.

摘要

副球孢子菌病(PCM)是一种源于拉丁美洲的系统性真菌病,在巴西流行,该国有大多数 PCM 病例。PCM 通过吸入副球孢子菌属真菌的繁殖体而获得,主要影响肺部。我们之前已经表明,与仅受感染的动物相比,用重组 60kDa 热休克蛋白(rPbHsp60)单次治疗感染 P. brasiliensis 的小鼠会使感染恶化。在这项研究中,我们研究了将克隆到质粒(pVAX1-PB_HSP60)中的 PB_HSP60 基因治疗感染小鼠是否会导致有效的免疫反应并更好地控制疾病。单一剂量蛋白治疗的有害影响在质粒制剂中没有看到。最重要的是,与用 pVAX1 或 PBS 治疗的感染小鼠相比,三剂 pVAX1-PB_HSP60 和蛋白可降低真菌负荷和肺部损伤,对实验性 PCM 产生有益作用。与感染小鼠相比,用三剂 pVAX1-PB_HSP60 治疗后观察到细胞因子 IFN-γ、TNF 和 IL-17 的增加和 IL-10 的减少,这似乎是控制感染的原因。这些结果为 PCM 中 Hsp60 的治疗用途开辟了前景。

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