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机会性人类致病黑酵母出芽短梗霉菌丝和分生孢子发育过程中微管和F-肌动蛋白结构的分析

Analysis of microtubules and F-actin structures in hyphae and conidia development of the opportunistic human pathogenic black yeast Aureobasidium pullulans.

作者信息

Kopecká Marie, Gabriel Miroslav, Takeo Kanji, Yamaguchi Masashi, Svoboda Augustin, Hata Kunihiko

机构信息

Research Center for Pathogenic Fungi and Microbial Toxicoses, Chiba University, 1-8-1 Inohana, Chuo-ku, Chiba 260-8673, Japan.

Department of Biology, Faculty of Medicine, Masaryk University, Joštova 10, Brno 66243, Czech Republic.

出版信息

Microbiology (Reading). 2003 Apr;149(Pt 4):865-876. doi: 10.1099/mic.0.26006-0.

Abstract

Organization of the cytoskeleton was studied in the ascomycetous black yeast Aureobasidium pullulans, an opportunistic human pathogen, in an effort to present it as a potential target of antifungal therapy. Long cytoplasmic microtubules, extending along the hyphae from the base to the growing apex, were the dominant structures in multinucleate interphase cells. Before mitosis these microtubules disappeared and were replaced by intranuclear spindles. This reorganization of microtubules occurred along the whole length of hypha before synchronous division of the nuclei. Actin cytokinetic rings were rarely seen. Cortical actin in the form of patches accumulated in areas of cell wall growth, i.e. in the hyphal apex and near the occasionally formed septum. Actin cables were not seen. During synchronous conidiogenesis, the cytoplasmic microtubules extended along developing conidia, and actin patches lined their subcortical areas. Actin rings were formed regularly at the base of uninuclear conidia. Microtubule inhibitor methyl benzimidazol-2-ylcarbamate disintegrated the microtubules, and inhibited nuclear division, development of hyphae and conidiogenesis. Actin inhibitor Cytochalasin D induced swelling of hyphal apexes and developing conidia. This inhibitory activity ceased after 5 to 12 h when the occasional septa appeared and conidiogenesis was completed. The lack of unicellular organization in multinucleate hyphae of A. pullulans seems be related to a rarity of F-actin structures: i.e. absence of actin cables, the lack of actin cytokinetic rings in particular, resulting in the uncoupling of the nuclear division from cytokinesis; the association of both processes is, however, retained during conidiogenesis.

摘要

为了将其作为抗真菌治疗的潜在靶点,我们对机会性人类病原体——子囊菌黑酵母出芽短梗霉的细胞骨架组织进行了研究。多核间期细胞中的主要结构是长的细胞质微管,它们沿着菌丝从基部延伸至生长顶端。在有丝分裂之前,这些微管消失并被核内纺锤体取代。在细胞核同步分裂之前,微管的这种重组发生在菌丝的整个长度上。很少能看到肌动蛋白细胞分裂环。斑块状的皮质肌动蛋白聚集在细胞壁生长的区域,即菌丝顶端和偶尔形成的隔膜附近。未观察到肌动蛋白束。在同步产孢过程中,细胞质微管沿着发育中的分生孢子延伸,并在其亚皮质区域排列着肌动蛋白斑块。在单核分生孢子的基部规则地形成肌动蛋白环。微管抑制剂甲基苯并咪唑-2-基氨基甲酸酯使微管解体,并抑制核分裂、菌丝发育和产孢。肌动蛋白抑制剂细胞松弛素D诱导菌丝顶端和发育中的分生孢子肿胀。当偶尔出现隔膜且产孢完成后,这种抑制活性在5至12小时后停止。出芽短梗霉多核菌丝中缺乏单细胞组织似乎与F-肌动蛋白结构的稀少有关:即缺乏肌动蛋白束,特别是缺乏肌动蛋白细胞分裂环;这导致核分裂与胞质分裂解偶联;然而,在产孢过程中这两个过程的关联得以保留。

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