Fungal Quorum-Sensing Molecules: A Review of Their Antifungal Effect against Candida Biofilms

Kovács, Renátó; Majoros, László

doi:10.3390/jof6030099

Cited by 57 publications

(49 citation statements)

References 111 publications

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“…In the present paper, we explored the efficacy of the peptide towards the dualspecies Candida/Klebsiella biofilm, showing its ability of both inhibiting and eradicating in vitro the biofilm at sub-MIC concentrations. The low antimicrobial activity of the peptide used in this work towards C. albicans and K. pneumoniae was very low and was similar to that of other previously tested membranotropic peptides [14,15]; nevertheless, these characteristics may represent an advantageous property in the prevention of the possible development of resistances in the entire microbial consortium, a feature typical of several compounds proposed as anti-biofilms molecules [11]. The mechanism of action of gH625-M against C. albicans monospecies biofilm, as shown by a CSLM analysis previously reported [15], is initially directed towards the esopolymeric matrix of the biofilm and then penetrates across cell membranes, producing a local and temporary destabilization of membranes, which nonetheless has scarce effects on cell viability.…”

Section: Discussionsupporting

confidence: 68%

“…The potential use of antimicrobial peptides (AMPs) as a valid alternative to conventional antibiotics has been acknowledged and widely studied. In fact, their fast and strong antimicrobial activity, their antibiofilm action, and their reduced induction of resistance compared to conventional antibiotics make AMPs relevant compounds for controlling infections due to multi-drug resistant microorganisms embedded in a biofilm [10][11][12]. Among AMPs, there is a particularly relevant class of peptides, known as membranotropic peptides, which, apart from their eventual antimicrobial activity, present a high ability to disrupt the biofilm and thus may have an action both in the inhibition and in the eradication of the biofilm [13].…”

Section: Introductionmentioning

confidence: 99%

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The Membranotropic Peptide gH625 to Combat Mixed Candida albicans/Klebsiella pneumoniae Biofilm: Correlation between In Vitro Anti-Biofilm Activity and In Vivo Antimicrobial Protection

Maione

Alteriis

Carraturo

et al. 2021

JoF

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The antibiofilm activity of a gH625 analogue was investigated to determine the in vitro inhibition and eradication of a dual-species biofilm of Candida albicans and Klebsiella pneumoniae, two leading opportunistic pathogens responsible for several resistant infections. The possibility of effectively exploiting this peptide as an alternative anti-biofilm strategy in vivo was assessed by the investigation of its efficacy on the Galleria mellonella larvae model. Results on larvae survival demonstrate a prophylactic efficacy of the peptide towards the infection of each single microorganism but mainly towards the co-infection. The expression of biofilm-related genes in vivo showed a possible synergy in virulence when these two species co-exist in the host, which was effectively prevented by the peptide. These findings provide novel insights into the treatment of medically relevant bacterial–fungal interaction.

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Section: Discussionsupporting

confidence: 68%

Section: Introductionmentioning

confidence: 99%

The Membranotropic Peptide gH625 to Combat Mixed Candida albicans/Klebsiella pneumoniae Biofilm: Correlation between In Vitro Anti-Biofilm Activity and In Vivo Antimicrobial Protection

Maione

Alteriis

Carraturo

et al. 2021

JoF

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“…Alternative treatments interfering with quorum-sensing have recently become attractive therapeutic strategies, particularly against difficult-to-treat multidrug-resistant pathogens such as C. auris (9,(21)(22). Previous studies have reported that fungal quorum-sensing molecules may have a remarkable antifungal effect and/or a potent adjuvant effect in combination with traditional antifungal agents (7,10,23-26).…”

Section: Discussionmentioning

confidence: 99%

“…Although farnesol does not affect the growth rate of C. albicans when growing in planktonic form, it significantly decreased the growth of C. auris regarding both planktonic cells and also 1-dayold biofilms of this organism (7). Recently, alternative therapeutic approaches designed to disturb quorum-sensing have become an attractive treatment strategy (8)(9). The usage of farnesol and traditional antifungal drugs in combination may provide new insights into the management of newly emerged fungal species, such as C. auris, which poses a global threat to the nosocomial environment (7,10).…”

Section: Introductionmentioning

confidence: 99%

Transcriptional profiling of the Candida auris response to exogenous farnesol exposure

Jakab

Balla

Ragyák

et al. 2021

Preprint

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The antifungal resistance threat posed by Candida auris necessitates bold and innovative therapeutic options. Farnesol, a quorum-sensing molecule with a potential antifungal and/or adjuvant effect; it may be a promising candidate in alternative treatment regimens. To gain further insights into the farnesol-related effect on C. auris, genome-wide gene expression analysis was performed using RNA-Seq. Farnesol exposure resulted in 1,766 differentially expressed genes. Of these, 447 and 304 genes with at least 1.5-fold increase or decrease in expression, respectively, were selected for further investigation. Genes involved in morphogenesis, biofilm events (maturation and dispersion), gluconeogenesis, iron metabolism, and regulation of RNA biosynthesis showed down-regulation, whereas those related to antioxidative defense, transmembrane transport, glyoxylate cycle, fatty acid β-oxidation, and peroxisome processes were up-regulated. In addition, farnesol treatment increased the expression of certain efflux pump genes, including MDR1, CDR1, and CDR2. Growth, measured by change in CFU number, was significantly inhibited within 2 hours of the addition of farnesol (5.8×107±1.1×107 and 1.1×107±0.3×107 CFU/ml for untreated control and farnesol-exposed cells, respectively) (p<0.001). In addition, farnesol treatment caused a significant reduction in intracellular iron (152.2±21.1 vs. 116.0±10.0 mg/kg), manganese (67.9±5.1 vs. 18.6±1.8 mg/kg), and zinc (787.8±22.2 vs. 245.8±34.4 mg/kg) (p<0.05–0.001) compared to untreated control cells, whereas the level of cooper was significantly increased (274.6±15.7 vs. 828.8±106.4 mg/kg) (p<0.001). Our data demonstrate that farnesol significantly influences the growth, intracellular metal ion contents, and gene expression related to fatty acid metabolism, which could open new directions in developing alternative therapies against C. auris.ImportanceCandida auris is a dangerous fungal pathogen that causes outbreaks in health care facilities, with infections associated with high mortality rate. As conventional antifungal drugs have limited effects against the majority of clinical isolates, new and innovative therapies are urgently needed. Farnesol is a key regulator molecule of fungal morphogenesis, inducing phenotypic adaptations and influencing biofilm formation as well as virulence. Alongside these physiological modulations, it has a potent antifungal effect alone or in combination with traditional antifungals, especially at supraphysiological concentrations. However, our knowledge about the mechanisms underlying this antifungal effect against C. auris is limited. This study has demonstrated that farnesol enhances the oxidative stress and reduces the fungal survival strategies. Furthermore, it inhibits manganese, zinc transport, and iron metabolism as well as increases fungal intracellular copper content. In addition, metabolism was modulated towards β-oxidation. These results provide definitive explanations for the observed antifungal effects.

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“…The reviews in this Special Issue covered recent developments in the area of Candida albicans sexual biofilms specifically focusing on how they are formed, their physical characteristics, and their role in Candida biology [13], the properties of the quorum sensing molecules farnesol and tyrosol secreted by Candida and their effect as anti-biofilm agents [14], and an extensive compilation of plant derived compounds with activities against biofilms of distinct Candida species [15]. Overall, this Special Issue is a great resource highlighting novel work on fungal biofilms.…”

mentioning

confidence: 99%

Fungal Biofilms 2020

Rodrigues

Romo

2021

JoF

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Fungal Quorum-Sensing Molecules: A Review of Their Antifungal Effect against Candida Biofilms

Cited by 57 publications

References 111 publications

The Membranotropic Peptide gH625 to Combat Mixed Candida albicans/Klebsiella pneumoniae Biofilm: Correlation between In Vitro Anti-Biofilm Activity and In Vivo Antimicrobial Protection

The Membranotropic Peptide gH625 to Combat Mixed Candida albicans/Klebsiella pneumoniae Biofilm: Correlation between In Vitro Anti-Biofilm Activity and In Vivo Antimicrobial Protection

Transcriptional profiling of the Candida auris response to exogenous farnesol exposure

Fungal Biofilms 2020

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