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152. Multicentre validation of a EUCAST method for the antifungal susceptibility testing of microconidia-forming dermatophytes

Author

Arendrup, Maiken Cavling, primary, Jørgensen, Karin Meinike, primary, Guinea, Jesus, primary, Lagrou, Katrien, primary, Chryssanthou, Erja, primary, Hayette, Marie-Pierre, primary, Barchiesi, Francesco, primary, Lass-Flörl, Cornelia, primary, Hamal, Petr, primary, Dannaoui, Eric, primary, Chowdhary, Anuradha, primary, and Meletiadis, Joseph, primary

Published
2020
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154. Invasive pulmonary aspergillosis treatment duration in haematology patients in Europe: An EFISG, IDWP‐EBMT, EORTC‐IDG and SEIFEM survey

Author

Lanternier, Fanny, primary, Seidel, Danila, additional, Pagano, Livio, additional, Styczynski, Jan, additional, Mikulska, Malgorzata, additional, Pulcini, Celine, additional, Maertens, Johan, additional, Munoz, Patricia, additional, Garcia‐Vidal, Carol, additional, Rijnders, Bart, additional, Arendrup, Maiken Cavling, additional, Sabino, Raquel, additional, Verissimo, Cristina, additional, Gaustad, Peter, additional, Klimko, Nikolay, additional, Arikan‐Akdagli, Sevtap, additional, Arsic, Valentina, additional, Barac, Aleksandra, additional, Skiada, Anna, additional, Klingspor, Lena, additional, Herbrecht, Raoul, additional, Donnelly, Peter, additional, Cornely, Oliver A., additional, Lass‐Flörl, Cornelia, additional, and Lortholary, Olivier, additional

Published
2020
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157. Collateral consequences of agricultural fungicides on pathogenic yeasts: A One Health perspective to tackle azole resistance.

Author

Castelo‐Branco, Débora, Lockhart, Shawn R., Chen, Yee‐Chun, Santos, Daniel Assis, Hagen, Ferry, Hawkins, Nichola Jane, Lavergne, Rose‐Anne, Meis, Jacques F., Le Pape, Patrice, Rocha, Marcos Fabio Gadelha, Sidrim, José Julio Costa, Arendrup, Maiken, and Morio, Florent

Subjects
AZOLES, FUNGICIDES, YEAST, ASPERGILLUS fumigatus, ROAD maps, ANTIFUNGAL agents
Abstract

Candida and Cryptococcus affect millions of people yearly, being responsible for a wide array of clinical presentations, including life‐threatening diseases. Interestingly, most human pathogenic yeasts are not restricted to the clinical setting, as they are also ubiquitous in the environment. Recent studies raise concern regarding the potential impact of agricultural use of azoles on resistance to medical antifungals in yeasts, as previously outlined with Aspergillus fumigatus. Thus, we undertook a narrative review of the literature and provide lines of evidence suggesting that an alternative, environmental route of azole resistance, may develop in pathogenic yeasts, in addition to patient route. However, it warrants sound evidence to support that pathogenic yeasts cross border between plants, animals and humans and that environmental reservoirs may contribute to azole resistance in Candida or other yeasts for humans. As these possibilities could concern public health, we propose a road map for future studies under the One Health perspective. [ABSTRACT FROM AUTHOR]

Published
2022
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158. In Vitro Activity of Ibrexafungerp (SCY-078) against Candida auris Isolates as Determined by EUCAST Methodology and Comparison with Activity against C. albicans and C. glabrata and with the Activities of Six Comparator Agents

Author

Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Hare, Rasmus Krøger, and Chowdhary, Anuradha

Subjects
Experimental Therapeutics, bacterial infections and mycoses
Abstract

Ibrexafungerp (SCY-078) is a novel first-in-class antifungal agent targeting glucan synthase. Candida auris is an emerging multidrug-resistant species that has caused outbreaks on five continents. We investigated the in vitro activity of ibrexafungerp against C. auris by applying EUCAST E.Def 7.3.1 methodology. C. albicans and C. glabrata, as well as anidulafungin, micafungin, amphotericin B, fluconazole, voriconazole, and isavuconazole, were included as comparators. Three C. auris reference strains (CBS12372, CBS12373, and CBS10913) and 122 C. auris, 16 C. albicans, and 16 C. glabrata isolates were evaluated. C. albicans ATCC 64548, C. parapsilosis ATCC 22019, and C. krusei ATCC 6258 served as quality control strains. Echinocandin-resistant isolates were fks sequenced. MIC ranges and modal MIC and MIC(50) values were determined. Wild-type upper limits (the upper MIC value where the wild-type distribution ends) were determined according to EUCAST principles for setting ECOFFs. Nine repetitions of three QC strains and MICs for C. albicans and C. glabrata yielded narrow MIC ranges with modal MICs in agreement with established EUCAST modal MICs, confirming a robust test performance. The ibrexafungerp MICs against C. auris isolates displayed a Gaussian distribution with a modal MIC (range) of 0.5 mg/liter (0.06 to 2 mg/liter), suggesting uniform susceptibility. Of 122 isolates, 8 were echinocandin resistant and harbored the S639F Fks1 alteration. All but one were fluconazole resistant, and the MIC distributions for voriconazole and isavuconazole were multimodal confirming variable susceptibility. Ibrexafungerp demonstrated promising activity against C. auris, including isolates resistant to echinocandins and/or other agents. The MICs were similar to those reported for the Clinical and Laboratory Standards Institute method, suggesting that a common clinical breakpoint may be appropriate.

Published
2020

159. Toward Harmonization of Voriconazole CLSI and EUCAST Breakpoints for Candida albicans Using a Validated In Vitro Pharmacokinetic/Pharmacodynamic Model

Author

Beredaki, Maria-Ioanna Georgiou, Panagiota-Christina Siopi, Maria Kanioura, Lamprini Andes, David Arendrup, Maiken Cavling Mouton, Johan W. Meletiadis, Joseph

Abstract

CLSI and EUCAST susceptibility breakpoints for voriconazole and Candida albicans differ by one dilution (95% PTA values were found for EUCAST/CLSI MICs of

Published
2020

160. ECMM Candi Reg—A ready to use platform for outbreaks and epidemiological studies

Author

Koehler, Philipp, Arendrup, Maiken Cavling, Arikan‐akdagli, Sevtap, Bassetti, Matteo, Bretagne, Stéphane, Klingspor, Lena, Lagrou, Katrien, Meis, Jacques F., Rautemaa‐richardson, Riina, Schelenz, Silke, Hamprecht, Axel, Koehler, Felix C., Kurzai, Oliver, Salmanton‐garcía, Jon, Vehreschild, Jörg‐janne, Alanio, Alexandre, Alastruey‐izquierdo, Ana, Arsic Arsenijevic, Valentina, Gangneux, Jean‐pierre, Gow, Neil A. R., Hadina, Suzana, Hamal, Petr, Klimko, Nikolay, Lass‐flörl, Cornelia, Mares, Mihai, Özenci, Volkan, Papp, Tamas, Roilides, Emmanuel, Sabino, Raquel, Segal, Esther, Talento, Alida Fe, Tortorano, Anna Maria, Verweij, Paul E., Hoenigl, Martin, and Cornely, Oliver A.

Abstract

BackgroundRecent outbreaks of Candida auris further exemplify that invasive Candida infections are a substantial threat to patients and healthcare systems. Even short treatment delays are associated with higher mortality rates. Epidemiological shifts towards more resistant Candida spp. require careful surveillance.ObjectivesTriggered by the emergence of C auris and by increasing antifungal resistance rates the European Confederation of Medical Mycology developed an international Candida Registry (FungiScope™ CandiReg) to allow contemporary multinational surveillance.MethodsCandiReg serves as platform for international cooperation to enhance research regarding invasive Candida infections. CandiReg uses the General Data Protection Regulation compliant data platform ClinicalSurveys.net that holds the electronic case report forms (eCRF). Data entry is supported via an interactive macro created by the software that can be accessed via any Internet browser.ResultsCandiReg provides an eCRF for invasive Candida infections that can be used for a variety of studies from cohort studies on attributable mortality to evaluations of guideline adherence, offering to the investigators of the 28 ECMM member countries the opportunity to document their cases of invasive Candida infection. CandiReg allows the monitoring of epidemiology of invasive Candida infections, including monitoring of multinational outbreaks. Here, we describe the structure and management of the CandiReg platform.ConclusionCandiReg supports the collection of clinical information and isolates to improve the knowledge on epidemiology and eventually to improve management of invasive Candida infections. CandiReg promotes international collaboration, improving the availability and quality of evidence on invasive Candida infection and contributes to improved patient management.

Published
2019
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161. Ibrexafungerp:A novel oral triterpenoid antifungal in development for the treatment of candida auris infections

Author

Ghannoum, Mahmoud, Arendrup, Maiken Cavling, Chaturvedi, Vishnu P., Lockhart, Shawn R., McCormick, Thomas S., Chaturvedi, Sudha, Berkow, Elizabeth L., Juneja, Deven, Tarai, Bansidhar, Azie, Nkechi, Angulo, David, Walsh, Thomas J., Ghannoum, Mahmoud, Arendrup, Maiken Cavling, Chaturvedi, Vishnu P., Lockhart, Shawn R., McCormick, Thomas S., Chaturvedi, Sudha, Berkow, Elizabeth L., Juneja, Deven, Tarai, Bansidhar, Azie, Nkechi, Angulo, David, and Walsh, Thomas J.

Abstract

Candida auris is an emerging multidrug-resistant fungal pathogen reported worldwide. Infections due to C. auris are usually nosocomial and associated with high rates of fluconazole resistance and mortality. Echinocandins are utilized as the first-line treatment. However, echinocandins are only available intravenously and are associated with increasingly higher rates of resistance by C. auris. Thus, a need exists for novel treatments that demonstrate potent activity against C. auris. Ibrexafungerp is a first-in-class triterpenoid antifungal agent. Similar to echinocandins, ibrexafungerp inhibits (1→3)-β-D-glucan synthase, a key component of the fungal cell wall, resulting in fungicidal activity against Candida spp. Ibrexafungerp demonstrates broad in vitro activity against various Candida spp. including C. auris and C. auris isolates with fks mutations. Minimum inhibitory concentration (MIC50 and MIC90) values in >400 C. auris isolates were 0.5 µg/mL and 1.0 µg/mL, respectively. Clinical results were reported for two patients with invasive candidiasis or candidemia due to C. auris treated during the CARES (Candidiasis Caused by Candida Auris) trial, an ongoing open-label study. These patients experienced a complete response after treatment with ibrexafungerp. Thus, ibrexafungerp represents a promising new antifungal agent for treating C. auris infections.

Published
2020

162. Azole-Resistant Aspergillus fumigatus Among Danish Cystic Fibrosis Patients:Increasing Prevalence and Dominance of TR34/L98H

Author

Risum, Malene, Hare, Rasmus Kroger, Gertsen, Jan Berg, Kristensen, Lise, Johansen, Helle Krogh, Helweg-Larsen, Jannik, Abou-Chakra, Nissrine, Pressler, Tacjana, Skov, Marianne, Jensen-Fangel, Soren, Arendrup, Maiken Cavling, Risum, Malene, Hare, Rasmus Kroger, Gertsen, Jan Berg, Kristensen, Lise, Johansen, Helle Krogh, Helweg-Larsen, Jannik, Abou-Chakra, Nissrine, Pressler, Tacjana, Skov, Marianne, Jensen-Fangel, Soren, and Arendrup, Maiken Cavling

Abstract

Azole-resistant (azole-R) Aspergillus is an increasing challenge worldwide. Patients with cystic fibrosis (CF) are at risk of Aspergillus colonization and disease due to a favorable lung environment for microorganisms. We performed a nationwide study in 2018 of azole-non-susceptible Aspergillus in CF patients and compared with data from two prior studies. All airway samples with mold isolates from patients monitored at the two CF centers in Denmark (RH, Jan–Sept and AUH, Jan–Jun) were included. Classical species identification (morphology and thermo-tolerance) was performed and MALDI-TOF/β-tubulin sequencing was performed if needed. Susceptibility was determined using EUCAST E.Def 10.1, and E.Def 9.3.2. cyp51A sequencing and STRAf genotyping were performed for azole-non-susceptible isolates and relevant sequential isolates. In total, 340 mold isolates from 159 CF patients were obtained. The most frequent species were Aspergillus fumigatus (266/340, 78.2%) and Aspergillus terreus (26/340, 7.6%). Azole-R A. fumigatus was cultured from 7.3% (10/137) of patients, including 9.5% (9/95) of patients at RH and 2.4% at AUH (1/42), respectively. In a 10-year perspective, azole-non-susceptibility increased numerically among patients at RH (10.5% in 2018 vs 4.5% in 2007–2009). Cyp51A resistance mechanisms were found in nine azole-R A. fumigatus from eight CF patients. Five were of environmental origin (TR34/L98H), three were human medicine-driven (two M220K and one M220R), and one was novel (TR343/L98H) and found in a patient who also harbored a TR34/L98H isolate. STRAf genotyping identified 27 unique genotypes among 45 isolates and ≥2 genotypes in 8 of 12 patients. This included one patient carrying two unique TR34/L98H isolates, a rare phenomenon. Genotyping of sequential TR343/L98H and TR34/L98H isolates from the same patient showed only minor differences in 1/9 markers. Finally, azole-R A. terreus was found in three patients including two with Cyp51A alterations (M217I and

Published
2020

163. Introduction of a Comprehensive Diagnostic and Interdisciplinary Management Approach in Haematological Patients with Mucormycosis : A Pre and Post-Intervention Analysis

Author

Risum, Malene, Helweg-Larsen, Jannik, Petersen, Soren Lykke, Kampmann, Peter, Overgaard, Ulrik Malthe, El Fassi, Daniel, Nielsen, Ove Juul, Brabrand, Mette, Rubek, Niclas, Munksgaard, Lars, Severinsen, Marianne Tang, Nielsen, Bendt, Gertsen, Jan Berg, Gylfe, Åsa, Hjort, Ulla, Vourtsi, Angeliki, Hare, Rasmus Kroger, Arendrup, Maiken Cavling, Risum, Malene, Helweg-Larsen, Jannik, Petersen, Soren Lykke, Kampmann, Peter, Overgaard, Ulrik Malthe, El Fassi, Daniel, Nielsen, Ove Juul, Brabrand, Mette, Rubek, Niclas, Munksgaard, Lars, Severinsen, Marianne Tang, Nielsen, Bendt, Gertsen, Jan Berg, Gylfe, Åsa, Hjort, Ulla, Vourtsi, Angeliki, Hare, Rasmus Kroger, and Arendrup, Maiken Cavling

Abstract

Mucormycosis is a life threatening infection in patients with haematological disease. We introduced a Mucorales-PCR and an aggressive, multidisciplinary management approach for mucormycosis during 2016-2017 and evaluated patient outcomes in 13 patients diagnosed and treated in 2012-2019. Management principle: repeated surgical debridement until biopsies from the resection margins were clean as defined by negative Blankophor microscopy, Mucorales-PCR (both reported within 24 h), and cultures. Cultured isolates underwent EUCAST E.Def 9.3.1 susceptibility testing. Antifungal therapy (AFT) (mono/combination) combined with topical AFT (when possible) was given according to the minimal inhibitory concentration (MIC), severity of the infection, and for azoles, specifically, it was guided by therapeutic drug monitoring. The outcome was evaluated by case record review. All patients underwent surgery guided by diagnostic biopsies from tissue and resection margins (195 samples in total). Comparing 2012-2015 and 2016-2019, the median number of patients of surgical debridements was 3 and 2.5 and of diagnostic samples: microscopy/culture/PCR was 3/3/6 and 10.5/10/10.5, respectively. The sensitivity of microscopy (76%) and Mucorales-PCR (70%) were similar and microscopy was superior to that of culture (53%; p = 0.039). Initial systemic AFT was liposomal amphotericin B (n = 12) or posaconazole (n = 1) given as monotherapy (n = 4) or in combination with isavuconazole/posaconazole (n = 3/6) and terbinafine (n = 3). Nine patients received topical amphotericin B. All received isavuconazole or posaconazole consolidation therapy (n = 13). Mucormycosis related six month mortality was 3/5 in 2012-2015 and 0/7 patients in 2016-2019 (one patient was lost for follow-up). Implementation of combination therapy (systemic+topical AFT/combination systemic AFT) and aggressive surgical debridement guided by optimised diagnostic tests may improve the outcome of mucormycosis in haematologic patients.

Published
2020
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164. Invasive pulmonary aspergillosis treatment duration in haematology patients in Europe: An EFISG, IDWP-EBMT, EORTC-IDG and SEIFEM survey

Author

Lanternier, Fanny, Seidel, Danila, Pagano, Livio, Styczynski, Jan, Mikulska, Malgorzata, Pulcini, Celine, Maertens, Johan, Munoz, Patricia, Garcia-Vidal, Carol, Rijnders, Bart, Arendrup, Maiken Cavling, Sabino, Raquel, Verissimo, Cristina, Gaustad, Peter, Klimko, Nikolay, Arikan-Akdagli, Sevtap, Arsic, Valentina, Barac, Aleksandra, Skiada, Anna, Klingspor, Lena, Herbrecht, Raoul, Donnelly, Peter, Cornely, Oliver A., Lass-Floerl, Cornelia, Lortholary, Olivier, Lanternier, Fanny, Seidel, Danila, Pagano, Livio, Styczynski, Jan, Mikulska, Malgorzata, Pulcini, Celine, Maertens, Johan, Munoz, Patricia, Garcia-Vidal, Carol, Rijnders, Bart, Arendrup, Maiken Cavling, Sabino, Raquel, Verissimo, Cristina, Gaustad, Peter, Klimko, Nikolay, Arikan-Akdagli, Sevtap, Arsic, Valentina, Barac, Aleksandra, Skiada, Anna, Klingspor, Lena, Herbrecht, Raoul, Donnelly, Peter, Cornely, Oliver A., Lass-Floerl, Cornelia, and Lortholary, Olivier

Abstract

Invasive pulmonary aspergillosis (IPA) optimal duration of antifungal treatment is not known. In a joint effort, four international scientific societies/groups performed a survey to capture current practices in European haematology centres regarding management of IPA. We conducted a cross-sectional internet-based questionnaire survey in 2017 to assess practices in sixteen European countries concerning IPA management in haematology patients including tools to evaluate treatment response, duration and discontinuation. The following four groups/societies were involved in the project: European Society of Clinical Microbiology and Infectious Diseases (ESCMID) Fungal Infection Study Group (EFISG), Infectious Diseases Working Party-European Society for Blood and Bone Marrow Transplantation (IDWP-EBMT), European Organisation for Research and Treatment-Infectious Disease group (EORTC-IDG) and Sorveglianza Epidemiologica Infezioni nelle Emopatie (SEIFEM). A total of 112 physicians from 14/16 countries answered the survey. Galactomannan antigen was available in serum and bronchoalveolar lavage in most centres (106/112 [95%] and 97/112 [87%], respectively), quantitative Aspergillus PCR in 27/112 (24%) centres, beta-D-glucan in 24/112 (21%) and positron emission tomography in 50/112 (45%). Treatment duration differed between haematological malignancies, with a median duration of 6 weeks [IQR 3-12] for patients with AML, 11 [4-12] for patients with allogenic stem cell transplantation and GvHD and 6 [3-12] for patients with lymphoproliferative disease. Treatment duration significantly differed according to country. Essential IPA biomarkers are not available in all European countries, and treatment duration is highly variable according to country. It will be important to provide guidelines to help with IPA treatment cessation with algorithms according to biomarker availability.

Published
2020

165. Tinea capitis in children is an overlooked disease

Author

Andersen, Pernille Lindsø, Jemec, Gregor B., Arendrup, Maiken Cavling, Saunte, Ditte Marie, Andersen, Pernille Lindsø, Jemec, Gregor B., Arendrup, Maiken Cavling, and Saunte, Ditte Marie

Abstract

In this review, we discuss tinea capitis, which is a disease most prevalent in children and caused by dermatophytes infecting the hair and scalp. The clinical presentation varies from scaling and alopecia to inflammatory lesions with pain and pruritus. Treatment includes systemic and topical antifungal agents. Due to the aetiological shift in pathogens from zoophilic dermatophytes to anthropophilic dermatophytes, spread of the infection may occur more easily. Therefore, early disease detection and treatment of asymptomatic carriers is important to avoid epidemics.

Published
2020

166. Tinea capitis er en overset sygdom hos børn

Author

Andersen, Pernille Lindsø, Jemec, Gregor B., Arendrup, Maiken Cavling, Saunte, Ditte Marie, Andersen, Pernille Lindsø, Jemec, Gregor B., Arendrup, Maiken Cavling, and Saunte, Ditte Marie

Abstract

Pernille Lindsø Andersen, Gregor B. Jemec, Maiken Cavling Arendrup & Ditte Marie Saunte: Tinea capitis in children is an overlooked disease Ugeskr Læger 2020;182:V10190560 In this review, we discuss tinea capitis, which is a disease most prevalent in children and caused by dermatophytes infecting the hair and scalp. The clinical presentation varies from scaling and alopecia to inflammatory lesions with pain and pruritus. Treatment includes systemic and topical antifungal agents. Due to the aetiological shift in pathogens from zoophilic dermatophytes to anthropophilic dermatophytes, spread of the infection may occur more easily. Therefore, early disease detection and treatment of asymptomatic carriers is important to avoid epidemics.

Published
2020

167. The one health problem of azole resistance in Aspergillus fumigatus:current insights and future research agenda

Author

Verweij, Paul E., Lucas, John A., Arendrup, Maiken C., Bowyer, Paul, Brinkmann, Arjen J.F., Denning, David W., Dyer, Paul S., Fisher, Matthew C., Geenen, Petra L., Gisi, Ulrich, Hermann, Dietrich, Hoogendijk, Andre, Kiers, Eric, Lagrou, Katrien, Melchers, Willem J.G., Rhodes, Johanna, Rietveld, Anton G., Schoustra, Sijmen E., Stenzel, Klaus, Zwaan, Bas J., Fraaije, Bart A., Verweij, Paul E., Lucas, John A., Arendrup, Maiken C., Bowyer, Paul, Brinkmann, Arjen J.F., Denning, David W., Dyer, Paul S., Fisher, Matthew C., Geenen, Petra L., Gisi, Ulrich, Hermann, Dietrich, Hoogendijk, Andre, Kiers, Eric, Lagrou, Katrien, Melchers, Willem J.G., Rhodes, Johanna, Rietveld, Anton G., Schoustra, Sijmen E., Stenzel, Klaus, Zwaan, Bas J., and Fraaije, Bart A.

Abstract

Azole resistance is a concern for the management of diseases caused by Aspergillus fumigatus in humans. Azole fungicide use in the environment has been identified as a possible cause for development of resistance, which increases the complexity and number of stakeholders involved in this emerging problem. A workshop was held in Amsterdam early 2019 in which stakeholders, including medical and agricultural researchers, representatives from the government, public health, fungicide producers and end-users, reviewed the current evidence supporting environmental selection for resistance and to discuss which research and measures are needed to retain the effectiveness of the azole class for environmental and medical applications. This paper provides an overview of the latest insights and understanding of azole resistance development in the clinical setting and the wider environment. A One Health problem approach was undertaken to list and prioritize which research will be needed to provide missing evidence and to enable preventive interventions.

Published
2020

168. Introduction of a comprehensive diagnostic and interdisciplinary management approach in haematological patients with mucormycosis:A pre and post-intervention analysis

Author

Risum, Malene, Helweg-Larsen, Jannik, Petersen, Søren Lykke, Kampmann, Peter, Overgaard, Ulrik Malthe, Fassi, Daniel El, Nielsen, Ove Juul, Brabrand, Mette, Rubek, Niclas, Munksgaard, Lars, Severinsen, Marianne Tang, Nielsen, Bendt, Gertsen, Jan Berg, Gylfe, Åsa, Hjort, Ulla, Vourtsi, Angeliki, Hare, Rasmus Krøger, Arendrup, Maiken Cavling, Risum, Malene, Helweg-Larsen, Jannik, Petersen, Søren Lykke, Kampmann, Peter, Overgaard, Ulrik Malthe, Fassi, Daniel El, Nielsen, Ove Juul, Brabrand, Mette, Rubek, Niclas, Munksgaard, Lars, Severinsen, Marianne Tang, Nielsen, Bendt, Gertsen, Jan Berg, Gylfe, Åsa, Hjort, Ulla, Vourtsi, Angeliki, Hare, Rasmus Krøger, and Arendrup, Maiken Cavling

Abstract

Mucormycosis is a life threatening infection in patients with haematological disease. We introduced a Mucorales-PCR and an aggressive, multidisciplinary management approach for mucormycosis during 2016–2017 and evaluated patient outcomes in 13 patients diagnosed and treated in 2012–2019. Management principle: repeated surgical debridement until biopsies from the resection margins were clean as defined by negative Blankophor microscopy, Mucorales-PCR (both reported within 24 h), and cultures. Cultured isolates underwent EUCAST E.Def 9.3.1 susceptibility testing. Antifungal therapy (AFT) (mono/combination) combined with topical AFT (when possible) was given according to the minimal inhibitory concentration (MIC), severity of the infection, and for azoles, specifically, it was guided by therapeutic drug monitoring. The outcome was evaluated by case record review. All patients underwent surgery guided by diagnostic biopsies from tissue and resection margins (195 samples in total). Comparing 2012–2015 and 2016–2019, the median number of patients of surgical debridements was 3 and 2.5 and of diagnostic samples: microscopy/culture/PCR was 3/3/6 and 10.5/10/10.5, respectively. The sensitivity of microscopy (76%) and Mucorales-PCR (70%) were similar and microscopy was superior to that of culture (53%; p = 0.039). Initial systemic AFT was liposomal amphotericin B (n = 12) or posaconazole (n = 1) given as monotherapy (n = 4) or in combination with isavuconazole/posaconazole (n = 3/6) and terbinafine (n = 3). Nine patients received topical amphotericin B. All received isavuconazole or posaconazole consolidation therapy (n = 13). Mucormycosis related six month mortality was 3/5 in 2012–2015 and 0/7 patients in 2016–2019 (one patient was lost for follow-up). Implementation of combination therapy (systemic+topical AFT/combination systemic AFT) and aggressive surgical debridement guided by optimised diagnostic tests may improve the outcome of mucormycosis in haematologic patient

Published
2020

169. Etiology and Outcome of Candidemia in Neonates and Children in Europe:An 11-year Multinational Retrospective Study

Author

Warris, Adilia, Pana, Zoi Dorothea, Oletto, Andrea, Lundin, Rebecca, Castagnola, Elio, Lehrnbecher, Thomas, Groll, Andreas H., Roilides, Emmanuel, Andersen, Cecilie T., Arendrup, Maiken C., Arsenijevic, Valentina Arsic, Bianchini, Sonia, Von Both, Ulrich, Chmelnik, Martin, Controzzi, Tiziana, Emonts, Marieke, Esposito, Susanna, Ferreras-Antolin, Laura, Henriet, Stefanie, Iosifidis, Elias, Irwin, Adam, Kopsidas, John, Lagrou, Katrien, Lyall, Hermione, Casteleiro, Angela Manzanares, Mesini, Alessio, Olbrich, Peter, Paulus, Stephane, Lausch, Karen Rokkedal, Soler-Palacin, Pere, Spyridis, Nikos, Strenger, Volker, Theodoraki, Martha, Wolfs, Tom, Warris, Adilia, Pana, Zoi Dorothea, Oletto, Andrea, Lundin, Rebecca, Castagnola, Elio, Lehrnbecher, Thomas, Groll, Andreas H., Roilides, Emmanuel, Andersen, Cecilie T., Arendrup, Maiken C., Arsenijevic, Valentina Arsic, Bianchini, Sonia, Von Both, Ulrich, Chmelnik, Martin, Controzzi, Tiziana, Emonts, Marieke, Esposito, Susanna, Ferreras-Antolin, Laura, Henriet, Stefanie, Iosifidis, Elias, Irwin, Adam, Kopsidas, John, Lagrou, Katrien, Lyall, Hermione, Casteleiro, Angela Manzanares, Mesini, Alessio, Olbrich, Peter, Paulus, Stephane, Lausch, Karen Rokkedal, Soler-Palacin, Pere, Spyridis, Nikos, Strenger, Volker, Theodoraki, Martha, and Wolfs, Tom

Abstract

Background: Data on Candida bloodstream infections in pediatric patients in Europe are limited. We performed a retrospective multicenter European study of the epidemiology and outcome of neonatal and pediatric candidemia. Material and Methods: All first positive blood cultures from patients ≤ 18 years of age with candidemia were registered. Patients' demographic and clinical characteristics and causative Candida species were collected and analyzed. Regression analysis was used to identify factors independently associated with mortality. Results: One thousand three hundred ninety-five episodes of candidemia (57.8% male) were reported from 23 hospitals in 10 European countries. Of the 1395 episodes, 36.4% occurred in neonates (≤ 44 weeks postmenstrual age), 13.8% in infants (> 44 weeks postmenstrual age to 1 year) and 49.8% in children and adolescents. Candida albicans (52.5%) and Candida parapsilosis (28%) were the predominant species. A higher proportion of candidemia caused by C. albicans was observed among neonatal patients (60.2%) with highest rates of C. parapsilosis seen among infants (42%). Children admitted to hematology-oncology wards presented the highest rates of non-albicans Candida species. Candidemia because of C. albicans was more frequent than non-albicans Candida in Northern versus Southern Europe (odds ratio, 2.3; 95% confidence interval, 1.8-2.9; P < 0.001). The all-cause mortality at 30 days was 14.4%. All-cause mortality was higher among patients admitted to the neonatal or pediatric intensive care units than other wards. Over time, no significant changes in species distribution were observed. Conclusions: This first multicenter European study shows unique characteristics of the epidemiology of pediatric candidemia. The insights obtained from this study will be useful to guide clinical management and antifungal stewardship.

Published
2020

170. Genotyping Reveals High Clonal Diversity and Widespread Genotypes of Candida Causing Candidemia at Distant Geographical Areas

Author

Guinea, Jesús, Arendrup, Maiken C., Cantón, Rafael, Cantón, Emilia, García-Rodríguez, Julio, Gómez, Ana, de la Pedrosa, Elia Gómez G., Hare, Rasmus K., Orden, Beatriz, Sanguinetti, Maurizio, Pemán, Javier, Posteraro, Brunella, Ruiz-Gaitán, Alba, Parisi, Gabriella, Da Matta, Daniel Archimedes, Colombo, Arnaldo L., Sánchez-Carrillo, Carlos, Reigadas, Elena, Muñoz, Patricia, Escribano, Pilar, Guinea, Jesús, Arendrup, Maiken C., Cantón, Rafael, Cantón, Emilia, García-Rodríguez, Julio, Gómez, Ana, de la Pedrosa, Elia Gómez G., Hare, Rasmus K., Orden, Beatriz, Sanguinetti, Maurizio, Pemán, Javier, Posteraro, Brunella, Ruiz-Gaitán, Alba, Parisi, Gabriella, Da Matta, Daniel Archimedes, Colombo, Arnaldo L., Sánchez-Carrillo, Carlos, Reigadas, Elena, Muñoz, Patricia, and Escribano, Pilar

Abstract

The objectives of this study were to gain further insight on Candida genotype distribution and percentage of clustered isolates between hospitals and to identify potential clusters involving different hospitals and cities. We aim to genotype Candida spp. isolates causing candidemia in patients admitted to 16 hospitals in Spain, Italy, Denmark, and Brazil. Eight hundred and eighty-four isolates (Candida albicans, n = 534; C. parapsilosis, n = 282; and C. tropicalis, n = 68) were genotyped using species-specific microsatellite markers. CDC3, EF3, HIS3, CAI, CAIII, and CAVI were used for C. albicans, Ctrm1, Ctrm10, Ctrm12, Ctrm21, Ctrm24, and Ctrm28 for C. tropicalis, and CP1, CP4a, CP6, and B for C. parapsilosis. Genotypes were classified as singletons (genotype only found once) or clusters (same genotype infecting two or more patients). Clusters were defined as intra-hospital (involving patients admitted to a single hospital), intra-ward (involving patients admitted to the same hospital ward) or widespread (involving patients admitted to different hospitals). The percentage of clusters and the proportion of patients involved in clusters among species, genotypic diversity and distribution of genetic diversity were assessed. Seven hundred and twenty-three genotypes were detected, 78 (11%) being clusters, most of which (57.7%; n = 45/78) were intra-hospital clusters including intra-ward ones (42.2%; n = 19/45). The proportion of clusters was not statistically different between species, but the percentage of patients in clusters varied among hospitals. A number of genotypes (7.2%; 52/723) were widespread (found at different hospitals), comprising 66.7% (52/78) of clusters, and involved patients at hospitals in the same city (n = 21) or in different cities (n = 31). Only one C. parapsilosis cluster was a widespread genotype found in all four countries. Around 11% of C. albicans and C. parapsilosis isolates causing candidemia are clusters that may result from patient-to

Published
2020

171. Toward Harmonization of Voriconazole CLSI and EUCAST Breakpoints for Candida albicans Using a Validated in Vitro Pharmacokinetic/Pharmacodynamic Model

Author

Beredaki, Maria Ioanna, Georgiou, Panagiota Christina, Siopi, Maria, Kanioura, Lamprini, Andes, David, Arendrup, Maiken Cavling, Mouton, Johan W., Meletiadis, Joseph, Beredaki, Maria Ioanna, Georgiou, Panagiota Christina, Siopi, Maria, Kanioura, Lamprini, Andes, David, Arendrup, Maiken Cavling, Mouton, Johan W., and Meletiadis, Joseph

Abstract

CLSI and EUCAST susceptibility breakpoints for voriconazole and Candida albicans differ by one dilution (0.125 and 0.06 mg/liter, respectively) whereas the epidemiological cutoff values for EUCAST (ECOFF) and CLSI (ECV) are the same (0.03 mg/liter). We therefore determined the pharmacokinetic/pharmacodynamic (PK/PD) breakpoints of voriconazole against C. albicans for both methodologies with an in vitro PK/PD model, which was validated using existing animal PK/PD data. Four clinical wild-type and non-wild-type C. albicans isolates (voriconazole MICs, 0.008 to 0.125 mg/liter) were tested in an in vitro PK/PD model. For validation purposes, mouse PK were simulated and in vitro PD were compared with in vivo outcomes. Human PK were simulated, and the exposure-effect relationship area under the concentration-time curve for the free, unbound fraction of a drug from 0 to 24 h (fAUC0-24)/MIC was described for EUCAST and CLSI 24/48-h methods. PK/PD breakpoints were determined using the fAUC0-24/MIC associated with half-maximal activity (EI50) and Monte Carlo simulation analysis. The in vitro 24-h PD EI50 values of voriconazole against C. albicans were 2.5 to 5 (1.5 to 17) fAUC/MIC. However, the 72-h PD were higher at 133 (51 to 347) fAUC/MIC for EUCAST and 94 (35 to 252) fAUC/MIC for CLSI. The mean (95% confidence interval) probability of target attainment (PTA) was 100% (95 to 100%), 97% (72 to 100%), 83% (35 to 99%), and 49% (8 to 91%) for EUCAST and 100% (97 to 100%), 99% (85 to 100%), 91% (52 to 100%), and 68% (17 to 96%) for CLSI for MICs of 0.03, 0.06, 0.125, and 0.25 mg/liter, respectively. Significantly,95% PTA values were found for EUCAST/CLSI MICs of0.03 mg/liter. For MICs of 0.06 to 0.125 mg/liter, trough levels 1 to 4 mg/liter would be required to attain the PK/PD target. A PK/PD breakpoint of C. albicans voriconazole at the ECOFF/ECV of 0.03 mg/liter was determined for both the EUCAST and CLSI methods, indicating the need for breakpoint harmonization for the r

Published
2020

172. In vitro activity of manogepix (APX001A) and comparators against contemporary molds:MEC comparison and preliminary experience with colorimetric MIC determination

Author

Jørgensen, Karin Meinike, Astvad, Karen M.T., Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Astvad, Karen M.T., and Arendrup, Maiken Cavling

Abstract

Manogepix (APX001A) is the active moiety of the drug candidate fosmanogepix (APX001), currently in clinical development for the treatment of invasive fungal infections. We compared manogepix EUCAST minimum effective concentrations (MECs) to MICs of five comparators and CLSI MECs and MICs by a colorimetric method against contemporary molds. EUCAST susceptibility testing was performed for 161 isolates. Interlaboratory and intermethod reproducibility were determined by comparison with published manogepix MECs. Colorimetric MICs (measuring metabolic activity) were evaluated using three Aspergillus fumigatus isolates and one Aspergillus flavus isolate with four inocula at 24 to 48 h of incubation and 1 to 3 h 2,3-bis-(2-methoxy-4-nitro-5-sulfophenyl)- 2H-tetrazolium-5-carboxanilide salt (XTT)/menadione (MEN) exposure. Manogepix modal MECs (range in mg/liter) against Aspergillus species were 0.03 to 0.06 (0.008 to 0.125) and unaffected by itraconazole resistance. Manogepix was as active against two Fusarium isolates but inactive against Trichophyton interdigitale, Lichtheimia ramosa, and Rhizomucor pusillus isolates (MECs > 0.5). Modal MEC/MICs were ≥3 2-fold dilutions apart without overlapping ranges comparing manogepix with amphotericin B, isavuconazole, and voriconazole against Aspergillus isolates. Manogepix and posaconazole MECs/MICs correlated for Aspergillus niger (Pearson's r = 0.711; P = 0.0044). The MEC at which 50% of the isolates tested are inhibited (MEC50), mode, and MEC90values were within ±1 dilution in all cases compared with published EUCAST and CLSI data. The colorimetric method showed excellent agreement with the MECs when plates were inoculated with the lowest inoculum (1×102CFU/ml to 2.5×102CFU/ml), incubated for 24 h, and exposed for 1 to 3 h to XTT/MEN. Broad-spectrum in vitro activity of manogepix against clinically relevant molds was confirmed with excellent agreement across EUCAST and CLSI method

Published
2020

173. Multicentre validation of a EUCAST method for the antifungal susceptibility testing of microconidia-forming dermatophytes

Author

Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Guinea, Jesus, Lagrou, Katrien, Chryssanthou, Erja, Hayette, Marie Pierre, Barchiesi, Francesco, Lass-Flörl, Cornelia, Hamal, Petr, Dannaoui, Eric, Chowdhary, Anuradha, Meletiadis, Joseph, Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Guinea, Jesus, Lagrou, Katrien, Chryssanthou, Erja, Hayette, Marie Pierre, Barchiesi, Francesco, Lass-Flörl, Cornelia, Hamal, Petr, Dannaoui, Eric, Chowdhary, Anuradha, and Meletiadis, Joseph

Abstract

Terbinafine resistance is increasingly reported in Trichophyton, rendering susceptibility testing particularly important in non-responding cases. We performed a multicentre evaluation of six EUCAST-based methods. Methods: Ten laboratories susceptibility tested terbinafine, itraconazole, voriconazole and amorolfine against a blinded panel of 38 terbinafine WT and target gene mutant isolates. E.Def 9.3.1 modifications included: medium with/without addition of chloramphenicol and cycloheximide (CC), incubation at 25°C to 28°C for 5-7 days and three MIC endpoints [visually and spectrophotometrically (90%/50% inhibition)], generating 7829 MICs. Quality control (QC) strains were Aspergillus flavus ATCC 204304 and CNM-CM1813. Eyeball, ECOFFinder (where ECOFF stands for epidemiological cut-off) and derivatization WT upper limits (WT-ULs), very major errors (VMEs; mutants with MICs ≤WT-ULs) and major errors (MEs; WT isolates with MICs >WT-ULs) were determined. Results: MICs fell within the QC ranges for ATCC 204304/CNM-CM1813 for 100%/96% (voriconazole) and 84%/84% (itraconazole), respectively. Terbinafine MICs fell within 0.25-1 mg/L for 96%/92%, suggesting high reproducibility. Across the six methods, the number of terbinafine MEs varied from 2 to 4 (2.6%-5.2%) for Trichophyton rubrum and from 0 to 2 (0%-2.0%) for Trichophyton interdigitale. Modes for WT and mutant populations were at least seven 2-fold dilutions apart in all cases. Excluding one I121M/V237I T. rubrum mutant and two mixed WT/mutant T. interdigitale specimens, the numbers of VMEs were as follows: T. rubrum: CC visual, 1/67 (1.5%); CC spectrophotometric 90% inhibition, 3/59 (5.1%); and CC spectrophotometric 50% inhibition, 1/67 (1.5%); and T. interdigitale: none. Voriconazole and amorolfine MICs were quite uniform, but trailing growth complicated determination of itraconazole visual and spectrophotometric 90% inhibition MIC. Conclusions: Although none of the laboratories was experienced in dermatophyte

Published
2020

174. Manogepix (APX001A) displays potent in vitro activity against human pathogenic yeast, but with an unexpected correlation to fluconazole MICs

Author

Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Arendrup, Maiken Cavling, and Jørgensen, Karin Meinike

Abstract

Manogepix (APX001A) is the active moiety of the novel drug candidate fosmanogepix (APX001). We previously reported the broad-spectrum activity of manogepix but also observed a correlation between increased manogepix and fluconazole MICs. Here, we extended this study and included isolates with acquired fluconazole resistance. Isolates (n=835) were identified using CHROMagar, matrixassisted laser desorption ionization-time of flight mass spectrometry (MALDI-TOF MS), and, when needed, internal transcribed spacer (ITS) sequencing. EUCAST E.Def 7.3.1 susceptibility testing included manogepix, amphotericin B, anidulafungin, micafungin, fluconazole, and voriconazole. Manogepix wild-type-upper-limit (WT-UL) values were established following EUCAST principles for the epidemiological cutoff value (ECOFF) setting allowing wild-type/non-wild-type classification. Drug-specific MIC correlations were investigated using Pearson's correlation. Manogepix modal MICs were low (range, 0.004 to 0.06 mg/liter against 16/20 included species). Exceptions were Candida krusei and Candida inconspicua and, to a lesser extent, Candida kefyr and Pichia kluyveri. The activity was independent of Fks echinocandin hot spot alterations (n=17). Adopting the WT-UL established for Candida albicans, Candida dubliniensis, Candida glabrata, Candida parapsilosis, and Candida tropicalis, 14/724 (1.9%) isolates were non-wild type for manogepix. Twelve of these (85.7%) were also non-wild type for fluconazole. A statistically significant correlation was observed between manogepix and fluconazole MICs for C. albicans, C. dubliniensis, C. glabrata, C. parapsilosis, and C. tropicalis (Pearson's r=0.401 to 0.575) but not between manogepix and micafungin or amphotericin B MICs for any species except C. tropicalis (r=0.519 for manogepix versus micafungin). Broad-spectrum activity was confirmed for manogepix against contemporary yeast. However, a 1 to 4 2-fold dilutions increase in manogepix MICs is observed in a su

Published
2020

175. Revision of EUCAST breakpoints:consequences for susceptibility of contemporary Danish mould isolates to isavuconazole and comparators

Author

Jørgensen, Karin Meinike, Guinea, Jesus, Meletiadis, Joseph, Hare, Rasmus Krøger, Arendrup, Maiken Cavling, Jørgensen, Karin Meinike, Guinea, Jesus, Meletiadis, Joseph, Hare, Rasmus Krøger, and Arendrup, Maiken Cavling

Abstract

BACKGROUND: EUCAST recently revised the definition of the 'I' category from 'intermediate' to 'susceptible, increased exposure'. Consequently, all current antifungal breakpoints have been reviewed and revised breakpoints (v 10.0) have been released. OBJECTIVES: We investigated isavuconazole and comparator MICs (mg/L) against contemporary moulds and the consequences of the breakpoint revision for susceptibility classification. METHODS: Six hundred and ninety-six Aspergillus and 46 other moulds were included. EUCAST E.Def 10.1 azole resistance screening was performed for Aspergillus fumigatus and E.Def 9.3.1 testing of non-susceptible A. fumigatus and other moulds. Most non-wildtype/resistant isolates underwent cyp51A sequencing. RESULTS: Isavuconazole MIC50/MIC90s were ≤1/≤2 mg/L for Aspergillus flavus, A. fumigatus and Aspergillus nidulans versus 2/4 mg/L for Aspergillus niger and 2/16 mg/L for Aspergillus terreus. For the remaining moulds, MICs were highest for Fusarium (16 to >16 mg/L), lowest for dermatophytes (0.06-0.5 mg/L) and in between for Mucorales and others (1 to >16 mg/L). A very strong isavuconazole-voriconazole MIC correlation was found for A. fumigatus (Pearson r = 0.888) and itraconazole-posaconazole correlation for A. fumigatus (r = 0.905) and A. terreus (r = 0.848). For A. fumigatus, the revised breakpoints lowered isavuconazole resistance (22.6% to 7.7%, P < 0.0001) and increased voriconazole resistance (3.8% to 6.7%, P = 0.025), resulting in similar resistance rates across the four azoles (range: 6.7%-7.7%). For A. terreus, isavuconazole resistance remained unchanged (81.3%) and higher than itraconazole (43.8%, P = 0.004) and posaconazole (53.1%, P = 0.03) resistance. Azole cross-resistance was found in 24/24, 13/20 and 4/90 isolates, and Cyp51A alterations in 16/18, 1/7 and 2/4 sequenced isolates with isavuconazole MICs of >4, 4 and 2 mg/L, respectively. CONCLUSIONS: Isavuconazole displays broad anti-mould activity. The revised br

Published
2020

176. Manogepix (APX001A) in Vitro Activity against Candida auris:Head-to-Head Comparison of EUCAST and CLSI MICs

Author

Arendrup, Maiken Cavling, Chowdhary, Anuradha, Jørgensen, Karin Meinike, Meletiadis, Joseph, Arendrup, Maiken Cavling, Chowdhary, Anuradha, Jørgensen, Karin Meinike, and Meletiadis, Joseph

Abstract

Fosmanogepix is a novel prodrug in a new class of antifungal agents. Manogepix is the active moiety. We evaluated the CLSI and EUCAST MICs of manogepix and eight comparators against Candida auris. CLSI M27-A3 susceptibility testing of manogepix was performed for 122 C. auris isolates and compared to CLSI and EUCAST MICs for manogepix and eight comparators. Differences and agreement were calculated for each compound. Wild-type upper limits (WT-ULs; the upper MIC where the wild-type distribution ends) for manogepix and correlations with other drugs’ MICs were determined. Manogepix MICs (CLSI/EUCAST [mg/liter]) and WT-ULs were as follows: MIC50s, 0.008/0.016; MIC90s, 0.03/0.03; ranges, 0.001 to 0.25/0.001 to 0.125; 97.5% and 99% WT-ULs, 0.03/0.125 and 0.06/0.125, respectively. The manogepix CLSI/EUCAST MIC distributions spanned 9/8 dilutions, respectively. Significant correlation was found for all azoles, particularly fluconazole (r = 0.22 to 0.74, P < 0.05). Isolates with EUCAST manogepix MICs of ≤0.004 had 7.6-/10.2-fold-lower fluconazole CLSI/EUCAST MICs than the remaining isolates that had higher manogepix MICs. The highest essential agreement between CLSI and EUCAST results was observed for manogepix and fluconazole, with a median difference of -1 to 0 2-fold dilutions, 90th percentile absolute difference of 1, and 90 to 92% and 98 to 100% agreement within ±1 and ±2 dilutions. The lowest agreements within ±1 and ±2 dilutions were found for isavuconazole and anidulafungin (44 to 50% and 69 to 76%). The correlation between CLSI and EUCAST manogepix MICs against C. auris was excellent. Differential MICs were found, and these correlated with fluconazole MICs, suggesting that the C. auris population is a mix of wild-type isolates and non-wild-type isolates with low-grade manogepix MIC elevation, probably involving efflux pump expression. However, manogepix was the most potent agent against C. auris in this in vitro study.

Published
2020

177. Photodynamic therapy treatment of superficial fungal infections:A systematic review

Author

Shen, Julia J., Jemec, Gregor B.E., Arendrup, Maiken C., Saunte, Ditte Marie L., Shen, Julia J., Jemec, Gregor B.E., Arendrup, Maiken C., and Saunte, Ditte Marie L.

Abstract

Background: Fungal infections in skin, hair and nails affect up to 25 % of the global population. Conventional antifungal treatment is effective but due to resistance, treatment failure, drug interactions, and treatment related toxicity, there is a need for alternative treatments. Photodynamic therapy (PDT) has shown antimicrobial properties and is used increasingly for fungal infections. This review investigates the reported efficacy and side effects of PDT of superficial mycoses. Methods: Pubmed and Embase were searched 26-01-2020 for “superficial fungal infections” and “photodynamic therapy” in “Human subjects” using a predefined search string. Criteria for inclusion were: clinical trials and cases involving PDT-treated patients with primary fungal infections in skin, hair and nails. Criteria for exclusion were: languages other than English, animal models, in vitro trials, secondary fungal infections, reviews and guidelines. Results: 541 records were identified and 34 papers fulfilled the criteria. PDT of onychomycosis (n = 380 patients) found treatment with methylene blue (MB) photosensitizer (PS) more efficacious with complete cure rates of 70 %–80 % than 5-aminolevulinic acid (ALA)-PDT (mycological cure rates of 17 %–57 %) and methyl aminolevulinate (MAL)-PDT (mycological cure rate of 32 %). Other PDT-treated fungal diseases included (n = 55): foot infections (n = 19), tinea cruris (n = 10), scalp infections (n = 2), Malassezia infections (n = 9) and subcutaneous fungal infections (n = 15) achieved promising effect. Conclusion: PDT-treatment of superficial mycoses can be efficacious as salvage therapy. In the light of increasing resistance and few licensed treatment alternatives, larger randomized controlled trials investigations and optimization of the PDT-treatment protocol are warranted to evaluate PDT's potential as a future antifungal treatment.

Published
2020

178. Candidemia Candida albicans clusters have higher tendency to form biofilms than singleton genotypes†

Author

Díaz-García, Judith, Arendrup, Maiken C., Cantón, Rafael, García-Rodríguez, Julio, Gómez, Ana, Gómez, Elia, Orden, Beatriz, Parisi, Gabriella, Pemán, Javier, Posteraro, Brunella, Sanguinetti, Maurizio, Da Matta, Daniel Archimedes, Colombo, Arnaldo L., Muñoz, Patricia, Sánchez-Carrillo, Carlos, Guinea, Jesús, Escribano, Pilar, Díaz-García, Judith, Arendrup, Maiken C., Cantón, Rafael, García-Rodríguez, Julio, Gómez, Ana, Gómez, Elia, Orden, Beatriz, Parisi, Gabriella, Pemán, Javier, Posteraro, Brunella, Sanguinetti, Maurizio, Da Matta, Daniel Archimedes, Colombo, Arnaldo L., Muñoz, Patricia, Sánchez-Carrillo, Carlos, Guinea, Jesús, and Escribano, Pilar

Abstract

The capacity of Candida spp. to form biofilms allows them to attach either to living or inert surfaces, promoting their persistence in hospital environments. In a previous study, we reported strain-to-strain variations in Candida spp. biofilm development, suggesting that some genotypes may be greater biofilm formers than others. In this study, we hypothesize that isolates pertaining to clusters may be found more frequently in the environment due to their ability to form biofilms compared to singleton genotypes. Two hundred and thirty-nine Candida spp. isolates (78 clusters) from candidemia patients admitted to 16 hospitals located in different cities and countries-and the same number of singleton genotypes used as controls-were tested in terms of biofilm formation using the crystal violet and the XTT reduction assays. Candida albicans clusters showed higher biofilm formation in comparison to singleton genotypes (P < .01). The biofilms formed by intra-hospital C. albicans clusters showed higher metabolic activity (P < .05). Furthermore, marked variability was found among species and type of cluster. We observed that the higher the number of isolates, the higher the variability of biofilm production by isolates within the cluster, suggesting that the production of biofilm by isolates of the same genotype is quite diverse and does not depend on the type of cluster studied. In conclusion, candidemia Candida spp. clusters-particularly in the case of C. albicans-show significantly more biomass production and metabolic activity than singleton genotypes.

Published
2020

179. Voriconazole efficacy against Candida glabrata and Candida krusei:preclinical data using a validated in vitro pharmacokinetic/pharmacodynamic model

Author

Beredaki, Maria Ioanna, Georgiou, Panagiota Christina, Siopi, Maria, Kanioura, Lamprini, Arendrup, Maiken Cavling, Mouton, Johan W., Meletiadis, Joseph, Beredaki, Maria Ioanna, Georgiou, Panagiota Christina, Siopi, Maria, Kanioura, Lamprini, Arendrup, Maiken Cavling, Mouton, Johan W., and Meletiadis, Joseph

Abstract

Background: Voriconazole exhibits in vitro activity against Candida glabrata and Candida krusei (EUCAST/CLSI epidemiological cut-off values 1/0.25 and 1/0.5 mg/L, respectively). Yet, EUCAST found insufficient evidence to set breakpoints for these species. We explored voriconazole pharmacodynamics (PD) in an in vitro dynamic model simulating human pharmacokinetics (PK). Methods: Four C. glabrata and three C. krusei isolates (voriconazole EUCAST and CLSI MICs of 0.03-2 mg/L) were tested in the PK/PD model simulating voriconazole exposures (t½ ∼6 h q12h dosing for 3 days). PK/PD breakpoints were determined calculating the PTA for exposure indices fAUC0-24/MIC associated with half-maximal activity (EI50) using Monte Carlo simulation analysis. Results: Fungal load increased from 3.60±0.35 to 8.41±0.24 log10 cfu/mL in the drug-free control, with a maximum effect of ∼1 log10 kill of C. glabrata and C. krusei isolates with MICs of 0.06 and 0.25 mg/L, respectively, at high drug exposures. The 72 h log10 cfu/mL change versus fAUC0-24/MIC relationship followed a sigmoid curve for C. glabrata (R2=0.85-0.87) and C. krusei (R2=0.56-0.76) with EI50 of 49 (32-76) and 52 (33-78) fAUC/MIC for EUCAST and 55 (31-96) and 80 (42-152) fAUC/MIC for CLSI, respectively. The PTAs for C. glabrata and C. krusei isolates with EUCAST/CLSI MICs ≤0.125/≤0.06 mg/L were >95%. Isolates with EUCAST/CLSI MICs of 0.25-1/0.125-0.5 would require trough levels 1-4 mg/L; isolates with higher MICs would not attain the corresponding PK/PD targets without reaching toxicity. Conclusions: The in vitro PK/PD breakpoints for C. glabrata and C. krusei for EUCAST (0.125 mg/L) and CLSI (0.06 mg/L) bisected the WT populations. Trough levels of >4 mg/L, which are not clinically feasible, are necessary for efficacy against WT isolates.

Published
2020

180. Rezafungin In Vitro Activity against Contemporary Nordic Clinical Candida Isolates and Candida auris Determined by the EUCAST Reference Method

Author

Helleberg, Marie, Jørgensen, Karin Meinike, Hare, Rasmus Krøger, Datcu, Raluca, Chowdhary, Anuradha, Arendrup, Maiken Cavling, Helleberg, Marie, Jørgensen, Karin Meinike, Hare, Rasmus Krøger, Datcu, Raluca, Chowdhary, Anuradha, and Arendrup, Maiken Cavling

Abstract

Rezafungin (formerly CD101) is a novel echinocandin in clinical development. EUCAST epidemiological cutoff values (ECOFFs) have not yet been established. We determined the in vitro activity of rezafungin and comparators against 1,293 Nordic yeast isolates and 122 Indian Candida auris isolates and established single-center wild-type upper limits (WT-UL). The isolates (19 Candida spp. and 13 other yeast species) were identified using Chromagar; matrix-assisted laser desorption ionization–time of flight (MALDI-TOF); and, when needed, internal transcribed spacer sequencing. EUCAST E.Def 7.3.1 susceptibility testing included rezafungin, anidulafungin, micafungin, amphotericin B, and fluconazole. WT-UL were established following EUCAST principles for visual and statistical ECOFF setting. fks target genes were sequenced for rezafungin non-wild-type isolates. EUCAST clinical breakpoints for fungi version 9.0 were adopted for susceptibility classification. Rezafungin had species-specific activity similar to that of anidulafungin and micafungin. On a milligram-per-liter basis, rezafungin was overall less active than anidulafungin and micafungin but equally or more active than fluconazole and amphotericin B against the most common Candida species, except C. parapsilosis. We identified 37 (3.1%) rezafungin non-wild-type isolates of C. albicans (1.9%), C. glabrata (3.0%), C. tropicalis (2.7%), C. dubliniensis (2.9%), C. krusei (1.2%), and C. auris (14.8%). Alterations in Fks hot spots were found in 26/26 Nordic and 8/18 non-wild-type C. auris isolates. Rezafungin displayed broad in vitro activity against Candida spp., including C. auris. Adopting WT-UL established here, few Nordic strains, but a significant proportion of C. auris isolates, had elevated MICs with mutations in fks target genes that conferred echinocandin cross-resistance. fks1 mutations raised rezafungin MICs notably less than anidulafungin and micafungin MICs in C. auris.

Published
2020

181. Species distribution and antifungal susceptibility profile of Candida isolates from blood and other normally sterile foci from pediatric ICU patients in Tehran, Iran

Author

Mirhendi, Hossein, Charsizadeh, Arezoo, Eshaghi, Hamid, Nikmanesh, Bahram, Arendrup, Maiken Cavling, Mirhendi, Hossein, Charsizadeh, Arezoo, Eshaghi, Hamid, Nikmanesh, Bahram, and Arendrup, Maiken Cavling

Abstract

As data on pediatric invasive candidiasis (IC) and the antifungal susceptibility pattern of associated isolates are scarce in Iran, this study aimed to determine species distribution and antifungal susceptibility profile of Candida species isolated from pediatric patients with suspected or documented IC. A total of 235 yeast strains recovered from normally sterile body fluids of patients admitted at the intensive care units of Children's Medical Centre, Tehran, Iran, were identified using CHROMagar Candida, molecular methods (ITS PCR-RFLP and sequencing), and MALDI-TOF. Susceptibility to amphotericin B, fluconazole, voriconazole, micafungin, and anidulafungin was determined according to the European on Antimicrobial Susceptibility testing reference microdilution method (EUCAST E.Def 7.3.1). Candida albicans (53.6%), C. parapsilosis (24.7%), and C. tropicalis (8.5%) were the most common species, followed by C. lusitaniae (4.3%), C. glabrata (3.0%), C. guilliermondii and C. orthopsilosis (each 1.7%), C. kefyr (1.3%), C. dubliniensis (0.8%), and C. intermedia (0.4%). Amphotericin B MICs were ≤1 mg/l for all Candida isolates. C. albicans isolates were susceptible to all five antifungal agents. All C. parapsilosis isolates categorised as intermediate to micafungin and anidulafungin, except two isolates that had the MICs >2 mg/l for micafungin. MIC50, MIC90, and MIC range for fluconazole were 0.25 mg/l, 1 mg/l, and 0.125 - ≥32 mg/l, respectively. Fluconazole and voriconazole showed 100% activity against the most prevalent Candida species. The low resistance rate, favorable safety profile and low cost of fluconazole make it a reasonable choice for treatment of candidemia/invasive candidemia in Iran.

Published
2020

182. The Emerging Terbinafine-Resistant Trichophyton Epidemic: What Is the Role of Antifungal Susceptibility Testing?

Author

Shen, Julia J., Arendrup, Maiken C., Verma, Shyam, and Saunte, Ditte Marie L.

Subjects
TRICHOPHYTON, TERBINAFINE, GENETIC mutation, ANTIFUNGAL agents, EPIDEMICS
Abstract

Background: Dermatophytosis is commonly encountered in the dermatological clinics. The main aetiological agents in dermatophytosis of skin and nails in humans are Trichophyton (T.) rubrum, T. mentagrophytes and T. interdigitale (former T. mentagrophytes-complex). Terbinafine therapy is usually effective in eradicating infections due to these species by inhibiting their squalene epoxidase (SQLE) enzyme, but increasing numbers of clinically resistant cases and mutations in the SQLE gene have been documented recently. Resistance to antimycotics is phenotypically determined by antifungal susceptibility testing (AFST). However, AFST is not routinely performed for dermatophytes and no breakpoints classifying isolates as susceptible or resistant are available, making it difficult to interpret the clinical impact of a minimal inhibitory concentration (MIC). Summary: PubMed was systematically searched for terbinafine susceptibility testing of dermatophytes on October 20, 2020, by two individual researchers. The inclusion criteria were in vitro terbinafine susceptibility testing of Trichophyton (T.) rubrum, T. mentagrophytes and T. interdigitale with the broth microdilution technique. The exclusion criteria were non-English written papers. Outcomes were reported as MIC range, geometric mean, modal MIC and MIC50 and MIC90 in which 50 or 90% of isolates were inhibited, respectively. The reported MICs ranged from <0.001 to >64 mg/L. The huge variation in MIC is partly explained by the heterogeneity of the Trichophyton isolates, where some originated from routine specimens (wild types) whereas others came from non-responding patients with a known SQLE gene mutation. Another reason for the great variation in MIC is the use of different AFST methods where MIC values are not directly comparable. High MICs were reported particularly in isolates with SQLE gene mutation. The following SQLE alterations were reported: F397L, L393F, L393S, H440Y, F393I, F393V, F415I, F415S, F415V, S443P, A448T, L335F/A448T, S395P/A448T, L393S/A448T, Q408L/A448T, F397L/A448T, I121M/V237I and H440Y/F484Y in terbinafine-resistant isolates. [ABSTRACT FROM AUTHOR]

Published
2022
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187. Azole-Resistance in Aspergillus terreus and Related Species: An Emerging Problem or a Rare Phenomenon? (vol 9, 516, 2018)

Author

Zoran, Tamara, Sartori, Bettina, Sappl, Laura, Aigner, Maria, Sanchez-Reus, Ferran, Rezusta, Antonio, Chowdhary, Anuradha, Taj-Aldeen, Saad J., Arendrup, Maiken C., Oliveri, Salvatore, Kontoyiannis, Dimitrios P., Alastruey-Izquierdo, Ana, Lagrou, Katrien, Lo Cascio, Giuliana, Meis, Jacques F., Buzina, Walter, Farina, Claudio, Drogari-Apiranthitou, Miranda, Grancini, Anna, Tortorano, Anna M., Willinger, Birgit, Hamprecht, Axel, Johnson, Elizabeth, Klingspor, Lena, Arsic-Arsenijevic, Valentina, Cornely, Oliver A., Meletiadis, Joseph, Prammer, Wolfgang, Tullio, Vivian, Vehreschild, Joerg-Janne, Trovato, Laura, Lewis, Russell E., Segal, Esther, Rath, Peter-Michael, Hamal, Petr, Rodriguez-Iglesias, Manuel, Roilides, Emmanuel, Arikan-Akdagli, Sevtap, Chakrabarti, Arunaloke, Colombo, Arnaldo L., Fernandez, Mariana S., Teresa Martin-Gomez, M., Badali, Hamid, Petrikkos, Georgios, Klimko, Nikolai, Heimann, Sebastian M., Uzun, Omrum, Roudbary, Maryam, de la Fuente, Sonia, Houbraken, Jos, Risslegger, Brigitte, Sabino, Raquel, Lass-Florl, Cornelia, Lackner, Michaela, Westerdijk Fungal Biodiversity Institute - Food and Indoor Mycology, and Westerdijk Fungal Biodiversity Institute

Subjects
cryptic species, Cyp51A alterations, azoles, susceptibility profiles, Aspergillus section Terrei
Published
2019

189. Candidemia Candida albicans clusters have higher tendency to form biofilms than singleton genotypes†

Author

Díaz-García, Judith, primary, Arendrup, Maiken C, additional, Cantón, Rafael, additional, García-Rodríguez, Julio, additional, Gómez, Ana, additional, Gómez, Elia, additional, Orden, Beatriz, additional, Parisi, Gabriella, additional, Pemán, Javier, additional, Posteraro, Brunella, additional, Sanguinetti, Maurizio, additional, Da Matta, Daniel Archimedes, additional, Colombo, Arnaldo L, additional, Muñoz, Patricia, additional, Sánchez-Carrillo, Carlos, additional, Guinea, Jesús, additional, and Escribano, Pilar, additional

Published
2020
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191. Emerging Terbinafine Resistance in Trichophyton : Clinical Characteristics, Squalene Epoxidase Gene Mutations, and a Reliable EUCAST Method for Detection

Author

Saunte, Ditte M. L., primary, Hare, Rasmus K., additional, Jørgensen, Karin M., additional, Jørgensen, René, additional, Deleuran, Mette, additional, Zachariae, Claus O., additional, Thomsen, Simon F., additional, Bjørnskov-Halkier, Lars, additional, Kofoed, Kristian, additional, and Arendrup, Maiken C., additional

Published
2019
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198. Pediatric Candidemia Epidemiology and Morbidities

Author

Lausch, Karen Rokkedal, primary, Schultz Dungu, Kia Hee, additional, Callesen, Michael Thude, additional, Schrøder, Henrik, additional, Rosthøj, Steen, additional, Poulsen, Anja, additional, Østergaard, Lars, additional, Mortensen, Klaus Leth, additional, Storgaard, Merete, additional, Schønheyder, Henrik Carl, additional, Søgaard, Mette, additional, and Arendrup, Maiken Cavling, additional

Published
2019
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