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首页> 外文期刊>Molecular Immunology >Gliotoxin as putative virulence factor and immunotherapeutic target in a cell culture model of cerebral aspergillosis.
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Gliotoxin as putative virulence factor and immunotherapeutic target in a cell culture model of cerebral aspergillosis.

机译:胶质毒素是脑曲霉病细胞培养模型中的假定毒力因子和免疫治疗靶标。

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The mycotoxin gliotoxin is an important metabolite produced by Aspergillus fumigatus, but its precise role in the pathogenesis of cerebral aspergillosis is not yet determined. We could demonstrate that growth in cerebrospinal fluid (CSF) induced the production and secretion of significant amounts of gliotoxin by A. fumigatus. These concentrations of 590-720nM were sufficient to reduce the viability of astrocytes and neurons, as well as of primary microglia, already after few hours of incubation. Annexin staining and electron microscopy revealed the induction of apoptosis rather than necrosis as the relevant mode of gliotoxin action in the brain. Furthermore, even a low gliotoxin concentration of 100nM, which was subtoxic for astrocytes, was able to significantly down-modulate the phagocytic capacity of astrocytes. In order to improve the current antimycotic therapy of cerebral aspergillosis by supporting innate immunity in the fight against Aspergillus, we aimed to neutralize the toxic potency of gliotoxin towards different brain cell types. Compounds such as dithiothreitol (DTT) or glutathione that reduce the internal disulfide bond of gliotoxin were shown here to be able to interfere with the gliotoxin-induced decrease of cell viability and to save the cells from induction of apoptosis. Thus, exploration of these substances may lead to novel approaches for adjunctive treatment of cerebral aspergillosis.
机译:霉菌毒素gliotoxin是烟曲霉产生的重要代谢产物,但其在脑曲霉病发病机理中的确切作用尚未确定。我们可以证明,脑脊液(CSF)的生长会诱导烟曲霉产生和分泌大量的胶质毒素。孵育数小时后,这些590-720nM的浓度足以降低星形胶质细胞和神经元以及原代小胶质细胞的活力。膜联蛋白染色和电子显微镜检查显示,诱导凋亡而不是坏死是脑中胶质毒素作用的相关模式。此外,即使对于星形胶质细胞而言亚毒性的低胶质毒素浓度为100nM,也能够显着下调星形胶质细胞的吞噬能力。为了通过支持抗曲霉菌的先天免疫力来改善当前的脑曲霉病抗真菌治疗,我们旨在中和胶质毒素对不同脑细胞类型的毒性。此处显示的化合物(例如二硫苏糖醇(DTT)或谷胱甘肽)可减少胶体毒素的内部二硫键,从而能够干扰胶体毒素诱导的细胞活力降低,并使细胞免于凋亡诱导。因此,对这些物质的探索可能会导致新的方法来辅助治疗脑曲霉病。

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