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一种使用家蚕(Bombyx mori)的与人类相关的毛霉病替代感染模型。

A human-relevant alternative infection model for mucormycosis using the silkworm Bombyx mori.

作者信息

Ishii Masaki, Mikami Kazuhiro, Tabuchi Fumiaki, Maruyama Naho, Miyashita Atsushi

机构信息

Research Institute of Pharmaceutical Sciences, Faculty of Pharmacy, Musashino University, Tokyo, Japan.

Institute of Medical Mycology, Teikyo University, Tokyo, Japan.

出版信息

PLoS One. 2025 Sep 25;20(9):e0333476. doi: 10.1371/journal.pone.0333476. eCollection 2025.

Abstract

Mucorales fungi cause life-threatening mucormycosis in patients with clinical risk factors, such as immunodeficiency. Moreover, they are resistant to several antifungal drugs, highlighting the urgent need for novel therapies. Traditional mammalian models are expensive and raise ethical concerns, thereby limiting their suitability for large-scale studies. We established a silkworm (Bombyx mori) infection model to investigate the pathogenicity of Mucorales and evaluated its relevance to human infection. Strains of Rhizopus arrhizus, Mucor circinelloides, and Cunninghamella bertholletiae induced fatal infections in the silkworm. Grocott-stained silkworm tissue sections revealed hyphal invasion patterns closely resembling those observed in human mucormycosis. In addition, experimental simulation of clinical risk factors (steroid use and iron overload) significantly reduced the median lethal dose (LD50). Treatment with the antifungal drug isavuconazonium prolonged the survival of R. arrhizus-infected silkworms, suggesting the potential use of this model for novel antifungal screening. LD50 estimation for four R. arrhizus strains revealed up to a 100-fold difference in pathogenicity to the silkworm among the tested strains, corresponding to variations in cell surface characteristics. Interestingly, the presence of high-molecular weight (50-100 kDa) cell surface proteins was associated with high pathogenicity among R. arrhizus strains. In conclusion, the silkworm is a viable, human-relevant alternative model to investigate Mucorales infections, with potential for large-scale antimucormycosis drug screening.

摘要

毛霉目真菌可在患有免疫缺陷等临床风险因素的患者中引发危及生命的毛霉病。此外,它们对多种抗真菌药物具有抗性,这凸显了对新型疗法的迫切需求。传统的哺乳动物模型成本高昂且引发伦理问题,因此限制了它们在大规模研究中的适用性。我们建立了家蚕(Bombyx mori)感染模型来研究毛霉目的致病性,并评估其与人类感染的相关性。米根霉、卷枝毛霉和伯氏小克银汉霉菌株在家蚕中引发了致命感染。Grocott染色的家蚕组织切片显示,菌丝侵袭模式与在人类毛霉病中观察到的模式极为相似。此外,对临床风险因素(使用类固醇和铁过载)的实验模拟显著降低了半数致死剂量(LD50)。抗真菌药物艾沙康唑治疗可延长米根霉感染家蚕的存活时间,这表明该模型在新型抗真菌药物筛选方面具有潜在用途。对四种米根霉菌株的LD50估计显示,在所测试的菌株中,它们对家蚕的致病性差异高达100倍,这与细胞表面特征的变化相对应。有趣的是,高分子量(50 - 100 kDa)细胞表面蛋白的存在与米根霉菌株的高致病性相关。总之,家蚕是一种可行的、与人类相关的替代模型,可用于研究毛霉目感染,具有进行大规模抗毛霉病药物筛选的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8020/12463241/e6bfc1a8a927/pone.0333476.g001.jpg

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