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Candida albicans morphologies revealed by scanning electron microscopy analysis

机译:通过扫描电子显微镜分析揭示白色念珠菌的形态

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摘要

Scanning electron microscope (SEM) observations were used to analyze particular morphologies of Candida albicans clinical isolate (strain 82) and mutants defective in hyphae-promoting genes EFG1 (strain HLC52) and/or CPH1 (strains HLC54 and Can16). Transcription factors Efg1 and Cph1 play role in regulating filamentation and adhesion of C. albicans’ morphologies. Comparative analysis of such mutants and clinical isolate showed that Efg1 is required for human serum-induced cell growth and morphological switching. In the study, distinct differences between ultrastructural patterns of clinical strain’s and null mutants’ morphologies were observed (spherical vs tube-like blastoconidia, or solid and fragile constricted septa vs only the latter observed in strains with EFG1 deleted). In addition, wild type strain displayed smooth colonies of cells in comparison to mutants which exhibited wrinkled phenotype. It was observed that blastoconidia of clinical strain exhibited either polarly or randomly located budding. Contrariwise, morphotypes of mutants showed either multiple polar budding or a centrally located single bud scar (mother-daughter cell junction) distinguishing tube-like yeast/pseudohyphal growth (the length-to-width ratios larger than 1.5). In their planktonic form of growth, blastoconidia of clinical bloodstream isolate formed constitutively true hyphae under undiluted human serum inducing conditions. It was found that true hyphae are essential elements for developing structural integrity of conglomerate, as mutants displaying defects in their flocculation and conglomerate-forming abilities in serum. While filamentation is an important virulence trait in C. albicans the true hyphae are the morphologies which may be expected to play a role in bloodstream infections.
机译:扫描电子显微镜(SEM)观察用于分析白色念珠菌临床分离株(82株)的特殊形态以及在菌丝促进基因EFG1(HLC52株)和/或CPH1(HLC54和Can16株)中有缺陷的突变体。转录因子Efg1和Cph1在调节白色念珠菌形态的丝化和粘附中起作用。对此类突变体和临床分离株的比较分析表明,Efg1是人血清诱导的细胞生长和形态转换所必需的。在这项研究中,观察到临床菌株和无效突变体形态的超微结构模式之间存在明显差异(球形与管形的狂犬病,或实心和脆弱的收缩隔片,而在缺失EFG1的菌株中仅观察到后者)。另外,与表现出皱纹表型的突变体相比,野生型菌株显示出平滑的细胞集落。观察到临床菌株的芽孢杆菌显示出极性或随机定位的出芽。相反,突变体的形态型显示出多极萌芽或居中定位的单芽疤痕(母女细胞交界处),区别了管状酵母/假菌丝的生长(长宽比大于1.5)。在其浮游生物的生长形式中,临床血液分离物的胚球菌在未稀释的人血清诱导条件下组成性地形成了真正的菌丝。发现真正的菌丝是发展砾岩结构完整性的必要元素,因为突变体在其絮凝和在血清中形成砾岩的能力中显示出缺陷。尽管丝状化是白色念珠菌的重要毒力特性,但真正的菌丝是可以预期在血流感染中起作用的形态。

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