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Enterococcus faecalis Inhibits Hyphal Morphogenesis and Virulence of Candida albicans

机译:粪肠球菌抑制白色念珠菌的菌丝形态发生和毒力

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摘要

The Gram-positive bacterium Enterococcus faecalis and the fungus Candida albicans are both found as commensals in many of the same niches of the human body, such as the oral cavity and gastrointestinal (GI) tract. However, both are opportunistic pathogens and have frequently been found to be coconstituents of polymicrobial infections. Despite these features in common, there has been little investigation into whether these microbes affect one another in a biologically significant manner. Using a Caenorhabditis elegans model of polymicrobial infection, we discovered that E. faecalis and C. albicans negatively impact each other's virulence. Much of the negative effect of E. faecalis on C. albicans was due to the inhibition of C. albicans hyphal morphogenesis, a developmental program crucial to C. albicans pathogenicity. We discovered that the inhibition was partially dependent on the Fsr quorum-sensing system, a major regulator of virulence in E. faecalis. Specifically, two proteases regulated by Fsr, GelE and SerE, were partially required. Further characterization of the inhibitory signal revealed that it is secreted into the supernatant, is heat resistant, and is between 3 and 10 kDa. The substance was also shown to inhibit C. albicans filamentation in the context of an in vitro biofilm. Finally, a screen of an E. faecalis transposon mutant library identified other genes required for suppression of C. albicans hyphal formation. Overall, we demonstrate a biologically relevant interaction between two clinically important microbes that could affect treatment strategies as well as impact our understanding of interkingdom signaling and sensing in the human-associated microbiome.
机译:革兰氏阳性菌粪肠球菌和真菌白色念珠菌在人体的许多相同壁ni(例如口腔和胃肠道)中均被发现是共有的。然而,这两种都是机会病原体,并且经常被发现是微生物感染的共同组成部分。尽管有这些共同特征,但很少有研究关于这些微生物是否以生物学上重要的方式相互影响。使用多虫微生物秀丽隐杆线虫模型,我们发现屎肠球菌和白色念珠菌对彼此的毒力产生负面影响。粪肠球菌对白色念珠菌的大部分负面影响是由于抑制白色念珠菌菌丝形态发生,这对白色念珠菌的致病性至关重要。我们发现抑制作用部分取决于Fsr群体感应系统,粪肠球菌的主要毒力调节剂。具体而言,部分需要受Fsr调节的两种蛋白酶GelE和SerE。抑制信号的进一步表征表明,它被分泌到上清液中,具有耐热性,在3至10 kDa之间。在体外生物膜的背景下,该物质还显示出抑制白色念珠菌丝状化的作用。最后,粪肠球菌转座子突变体文库的筛选确定了抑制白色念珠菌菌丝形成所需的其他基因。总体而言,我们证明了两种临床上重要的微生物之间的生物学相关相互作用,这可能会影响治疗策略,并影响我们对与人类相关的微生物组中信号传导和感知的理解。

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