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Role of Tec1 in the Development Architecture and Integrity of Sexual Biofilms of Candida albicans

机译:Tec1在白色念珠菌性生物膜的发育结构和完整性中的作用

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摘要

MTL-homozygous (>a/>a or α/α) white cells form a complex sexual biofilm that exhibits the same architecture as that of MTL-heterozygous (>a/α) pathogenic biofilms. However, the former is regulated by the mitogen-activated protein (MAP) kinase pathway, while the latter is regulated by the Ras1/cyclic AMP (cAMP) pathway. We previously demonstrated that in the formation of an MTL-homozygous, mature (48 h) sexual biofilm in RPMI 1640 medium, the MAP kinase pathway targets Tec1 rather than Cph1, the latter of which is the target of the same pathway, but for the opaque cell mating response. Here we continued our analysis of the role of Tec1 by comparing the effects of deleting TEC1 on initial adhesion to silicone elastomer, high-resolution confocal microscopy assessments of the stages and cellular phenotypes during the 48 h of biofilm development, human white cell penetration, and biofilm fragility. We show that although Tec1 plays only a minor role in initial adhesion to the silicone elastomer, it does play a major role in the growth of the basal yeast cell polylayer, vertical extension of hyphae and matrix deposition in the upper portion of the biofilm, final biofilm thickness, penetrability of human white blood cells, and final biofilm integrity (i.e., resistance to fluid flow). These results provide a more detailed description of normal biofilm development and architecture and confirm the central role played by the transcription factor Tec1 in the biofilm model employed here.
机译:MTL纯合子(> a / > a 或α/α)白细胞形成复杂的有性生物膜,其结构与MTL杂合子(> a < / strong> /α)致病生物膜。但是,前者受有丝分裂原活化蛋白(MAP)激酶途径调控,而后者受Ras1 /环AMP(cAMP)途径调控。我们先前证明,在RPMI 1640培养基中形成MTL-纯合,成熟(48小时)的有性生物膜时,MAP激酶途径靶向Tec1而不是Cph1,后者是同一途径的靶标,但针对不透明的细胞交配反应。在这里,我们通过比较删除TEC1对初始粘附于有机硅弹性体的影响,高分辨率共聚焦显微镜评估生物膜发育48小时内的阶段和细胞表型,人类白细胞穿透以及生物膜的脆弱性。我们显示,尽管Tec1在与有机硅弹性体的初始黏附中仅起次要作用,但在基础酵母细胞多层的生长,菌丝的垂直延伸和生物膜上部的基质沉积,最终形成中确实起主要作用生物膜的厚度,人类白细胞的渗透性以及最终的生物膜完整性(即对流体流动的抵抗力)。这些结果提供了正常生物膜发育和结构的更详细描述,并证实了转录因子Tec1在此处采用的生物膜模型中所起的核心作用。

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