Rapid Emergence of Echinocandin Resistance during Candida kefyr Fungemia Treatment with Caspofungin

Fekkar, Arnaud; Meyer, I.; Brossas, Jean-Yves; Dannaoui, Éric; Palous, M.; Uzunov, Madalina; Nguyen, Su Minh Tuyet; Leblond, Veronique; Mazier, Dominique; Datry, A.

doi:10.1128/aac.02037-12

Cited by 51 publications

(46 citation statements)

References 15 publications

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“…More detailed study of these isolates (J. F. Staab, D. Neofytos, P. Rhee, C. Jimenez-Ortigosa, S. X. Zhang, D. S. Perlin, and K. A. Marr, submitted for publication) documented variable MICs to different echinocandins. Also, other investigators have observed C. kefyr resistance to echinocandins developing rapidly under treatment (37). Although our risk factor analysis identified administration of azoles or amphotericin B to be protective against C. kefyr colonization, it appears that C. kefyr has the propensity to develop resistance to all classes of antifungals, based on the MICs observed in the IC C. kefyr isolates in our study.…”

Section: Discussioncontrasting

confidence: 61%

Epidemiology of Candida kefyr in Patients with Hematologic Malignancies

et al. 2014

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g Candida kefyr is an emerging pathogen among patients with hematologic malignancies (HM). We performed a retrospective study at Johns Hopkins Hospital to evaluate the epidemiology of C. kefyr colonization and infection in HM patients between 2004 and 2010. Eighty-three patients were colonized and/or infected with C. kefyr, with 8 (9.6%) having invasive candidiasis (IC). The yearly incidence of C. kefyr colonization and candidemia increased over the study period (P < 0.01), particularly after 2009. In 2010, C. kefyr caused 16.7% of candidemia episodes. The monthly incidence of C. kefyr was higher during the summer throughout the study. In a cohort of patients with acute myelogenic leukemia receiving induction chemotherapy, risks for C. kefyr colonization included the summer season (odds ratio [OR], 3.1; P ‫؍‬ 0.03); administration of an azole (OR, 0.06; P < 0.001) or amphotericin B (OR, 0.35; P ‫؍‬ 0.05) was protective. Fingerprinting of 16 isolates by repetitive sequence-based PCR showed that all were different genotypes. The epidemiology of C. kefyr candidemia was evaluated in another hospital in Montreal, Canada; data confirmed higher rates of C. kefyr infection in the summer. C. kefyr appears to be increasing in HM patients, with prominent summer seasonality. These findings raise questions about the effect of antifungal agents and health care exposures (e.g., yogurt) on the epidemiology of this yeast.

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Section: Discussioncontrasting

confidence: 61%

Epidemiology of Candida kefyr in Patients with Hematologic Malignancies

et al. 2014

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“…Fifth, if multiple mutations were necessary for drug resistance, antifungal adaptation that required a particular combination of mutations would be expected to be extremely rare. Taken together, several lines of evidence besides our CFW study show that drug resistance based on protein function can emerge quickly given the appropriate selection pressure (11,13,33), consistent with single-gene mutations. In contrast, resistance to polyenes that target ergosterol distribution, rather than its synthesis, has been relatively durable, although even it has been overcome recently (33).…”

Section: Discussionsupporting

confidence: 63%

“…They did not identify the mutated genes, probably due to factors mentioned above. Second, echinocandin resistance mutations are typically at single sites in FKS1 (10)(11)(12). Third, single mutations in Erg11 lead to resistance to azoles (32).…”

Section: Discussionmentioning

confidence: 99%

“…The strong adaptation ability of fungi is well documented (13)(14)(15)(16), so it was not surprising to see antifungal drug resistance emerging quickly. Mutation hot spots in FKS1, which encodes beta-glucan synthase, were detected in some of the resistant strains but not in all (10)(11)(12). Our strategy can efficiently identify mutations in the latter group.…”

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confidence: 98%

“…Cowen (7) notes that the effectiveness of all existing antifungal drugs is reduced by resistant strains. Especially for echinocandins, clinically resistant strains were isolated shortly after their launch (11,12). The strong adaptation ability of fungi is well documented (13)(14)(15)(16), so it was not surprising to see antifungal drug resistance emerging quickly.…”

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Using Aspergillus nidulans To Identify Antifungal Drug Resistance Mutations

Kaminskyj

2014

Eukaryot Cell

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Systemic fungal infections contribute to at least 10% of deaths in hospital settings. Most antifungal drugs target ergosterol (polyenes) or its biosynthetic pathway (azoles and allylamines), or beta-glucan synthesis (echinocandins). Antifungal drugs that target proteins are prone to the emergence of resistant strains. Identification of genes whose mutations lead to targeted resistance can provide new information on those pathways. We used Aspergillus nidulans as a model system to exploit its tractable sexual cycle and calcofluor white as a model antifungal agent to cross-reference our results with other studies. Within 2 weeks from inoculation on sublethal doses of calcofluor white, we isolated 24 A. nidulans adaptive strains from sectoring colonies. Meiotic analysis showed that these strains had single-gene mutations. In each case, the resistance was specific to calcofluor white, since there was no cross-resistance to caspofungin (echinocandin). Mutation sites were identified in two mutants by next-generation sequencing. These were confirmed by reengineering the mutation in a wild-type strain using a gene replacement strategy. One of these mutated genes was related to cell wall synthesis, and the other one was related to drug metabolism. Our strategy has wide application for many fungal species, for antifungal compounds used in agriculture as well as health care, and potentially during protracted drug therapy once drug resistance arises. We suggest that our strategy will be useful for keeping ahead in the drug resistance arms race.

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Mechanisms of Resistance to Antifungal Agents

Perlin

2023

ClinMicroNow

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This chapter focuses on the epidemiologic, biological, and molecular nature of antifungal drug resistance. Antifungal drug action and the host immune system often must work synergistically to control and clear an infection. “Microbiological resistance” refers to decreased susceptibility of a fungal strain to an antifungal agent, which is reflected in standardized antifungal in vitro susceptibility testing relative to susceptible standard reference strains, as defined by the Clinical Laboratory Standards Institute and the European Committee on Antimicrobial Susceptibility Testing. The azole antifungal agents are the most prominent example of drug selection for less susceptible species. The polyene drug amphotericin is fungicidal, and resistance rarely occurs. Fungi encode numerous putative drug efflux transporters that have the potential to influence susceptibility to azole antifungal agents by reducing the effective cellular concentration of drugs below their inhibitory threshold. Biofilms are among the most prevalent forms of microbial growth in nature.

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Rapid Emergence of Echinocandin Resistance during Candida kefyr Fungemia Treatment with Caspofungin

Cited by 51 publications

References 15 publications

Epidemiology of Candida kefyr in Patients with Hematologic Malignancies

Epidemiology of Candida kefyr in Patients with Hematologic Malignancies

Using Aspergillus nidulans To Identify Antifungal Drug Resistance Mutations

Mechanisms of Resistance to Antifungal Agents

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