Clinical and Hospital Environmental Fusarium in Taiwan: Molecular Identification, Antifungal Susceptibilities, and Phylogenetic Analyses

Yi Chun Chen; Jie Hao Ou; Chi Jung Wu; Shu Fang Kuo; Susan Shin Jung Lee; Ming I. Hsieh; Yin Shiou Lin; Pei Lun Sun; Chen Hsiang Lee

doi:10.1111/myc.70056

Clinical and Hospital Environmental Fusarium in Taiwan: Molecular Identification, Antifungal Susceptibilities, and Phylogenetic Analyses

Yi Chun Chen, Jie Hao Ou, Chi Jung Wu, Shu Fang Kuo, Susan Shin Jung Lee, Ming I. Hsieh, Yin Shiou Lin, Pei Lun Sun^*, Chen Hsiang Lee^*

^*Corresponding author for this work

School of Medicine

Research output: Contribution to journal › Journal Article › peer-review

Abstract

Background: Fusarium species are emerging pathogens known to cause both superficial and disseminated human infections. Aerosolized Fusarium species in healthcare settings have been associated with nosocomial fusariosis, particularly in patients with severe immunosuppression. Objectives: To analyse the phylogenetic relationships of clinical and hospital environmental Fusarium isolates and assess their susceptibility to available antifungal agents. Methods: Clinical Fusarium isolates were procured from four hospitals in Taiwan, with environmental air and water sampling collected at Kaohsiung Chang Gung Memorial Hospital (KCGMH). All clinical and hospital environmental Fusarium isolates were identified through gene sequencing of translation elongation factor 1-α and internal transcribed spacer regions of ribosomal DNA. Antifungal susceptibility testing followed the CLSI M38-A3 broth microdilution method. Results: A total of 41 clinical and 4 hospital environmental Fusarium isolates were identified, belonging to five species complexes (SC): F. solani SC (FSSC) (62.8%), F. fujikuroi SC (FFSC) (14.0%), F. incarnatum-equiseti SC (11.6%), F. dimerum SC (7.0%), and F. oxysporum SC (4.7%). Phylogenetic analysis revealed that clinical Fusarium isolates from KCGMH were closely related to environmental Fusarium isolates from air samples at the same hospital. Amphotericin B exhibited high activity against most Fusarium species. With the exception of FFSC, other Fusarium SC demonstrated significantly elevated MIC values to itraconazole, voriconazole, posaconazole, and isavuconazole. Conclusions: FSSC was the most prevalent SC in Taiwan, exhibiting higher MIC values for azoles than FFSC isolates. The clinical Fusarium isolates were observed to form clusters with the corresponding environmental isolates. The potential of airborne nosocomial infections in the healthcare environment cannot be overlooked.

Original language	English
Article number	e70056
Pages (from-to)	e70056
Journal	Mycoses
Volume	68
Issue number	4
DOIs	https://doi.org/10.1111/myc.70056
State	Published - 04 2025

Bibliographical note

Publisher Copyright:
© 2025 Wiley-VCH GmbH. Published by John Wiley & Sons Ltd.

Keywords

MALDI-TOF
air sampling
filamentous fungi
fusarium
molecular identification

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10.1111/myc.70056

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@article{f4f4607c387b4cf4abe180f0568f35e8,

title = "Clinical and Hospital Environmental Fusarium in Taiwan: Molecular Identification, Antifungal Susceptibilities, and Phylogenetic Analyses",

abstract = "Background: Fusarium species are emerging pathogens known to cause both superficial and disseminated human infections. Aerosolized Fusarium species in healthcare settings have been associated with nosocomial fusariosis, particularly in patients with severe immunosuppression. Objectives: To analyse the phylogenetic relationships of clinical and hospital environmental Fusarium isolates and assess their susceptibility to available antifungal agents. Methods: Clinical Fusarium isolates were procured from four hospitals in Taiwan, with environmental air and water sampling collected at Kaohsiung Chang Gung Memorial Hospital (KCGMH). All clinical and hospital environmental Fusarium isolates were identified through gene sequencing of translation elongation factor 1-α and internal transcribed spacer regions of ribosomal DNA. Antifungal susceptibility testing followed the CLSI M38-A3 broth microdilution method. Results: A total of 41 clinical and 4 hospital environmental Fusarium isolates were identified, belonging to five species complexes (SC): F. solani SC (FSSC) (62.8\%), F. fujikuroi SC (FFSC) (14.0\%), F. incarnatum-equiseti SC (11.6\%), F. dimerum SC (7.0\%), and F. oxysporum SC (4.7\%). Phylogenetic analysis revealed that clinical Fusarium isolates from KCGMH were closely related to environmental Fusarium isolates from air samples at the same hospital. Amphotericin B exhibited high activity against most Fusarium species. With the exception of FFSC, other Fusarium SC demonstrated significantly elevated MIC values to itraconazole, voriconazole, posaconazole, and isavuconazole. Conclusions: FSSC was the most prevalent SC in Taiwan, exhibiting higher MIC values for azoles than FFSC isolates. The clinical Fusarium isolates were observed to form clusters with the corresponding environmental isolates. The potential of airborne nosocomial infections in the healthcare environment cannot be overlooked.",

keywords = "MALDI-TOF, air sampling, filamentous fungi, fusarium, molecular identification",

author = "Chen, \{Yi Chun\} and Ou, \{Jie Hao\} and Wu, \{Chi Jung\} and Kuo, \{Shu Fang\} and Lee, \{Susan Shin Jung\} and Hsieh, \{Ming I.\} and Lin, \{Yin Shiou\} and Sun, \{Pei Lun\} and Lee, \{Chen Hsiang\}",

note = "Publisher Copyright: {\textcopyright} 2025 Wiley-VCH GmbH. Published by John Wiley \& Sons Ltd.",

year = "2025",

month = apr,

doi = "10.1111/myc.70056",

language = "英语",

volume = "68",

pages = "e70056",

journal = "Mycoses",

issn = "0933-7407",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "4",

}

TY - JOUR

T1 - Clinical and Hospital Environmental Fusarium in Taiwan

T2 - Molecular Identification, Antifungal Susceptibilities, and Phylogenetic Analyses

AU - Chen, Yi Chun

AU - Ou, Jie Hao

AU - Wu, Chi Jung

AU - Kuo, Shu Fang

AU - Lee, Susan Shin Jung

AU - Hsieh, Ming I.

AU - Lin, Yin Shiou

AU - Sun, Pei Lun

AU - Lee, Chen Hsiang

PY - 2025/4

Y1 - 2025/4

N2 - Background: Fusarium species are emerging pathogens known to cause both superficial and disseminated human infections. Aerosolized Fusarium species in healthcare settings have been associated with nosocomial fusariosis, particularly in patients with severe immunosuppression. Objectives: To analyse the phylogenetic relationships of clinical and hospital environmental Fusarium isolates and assess their susceptibility to available antifungal agents. Methods: Clinical Fusarium isolates were procured from four hospitals in Taiwan, with environmental air and water sampling collected at Kaohsiung Chang Gung Memorial Hospital (KCGMH). All clinical and hospital environmental Fusarium isolates were identified through gene sequencing of translation elongation factor 1-α and internal transcribed spacer regions of ribosomal DNA. Antifungal susceptibility testing followed the CLSI M38-A3 broth microdilution method. Results: A total of 41 clinical and 4 hospital environmental Fusarium isolates were identified, belonging to five species complexes (SC): F. solani SC (FSSC) (62.8%), F. fujikuroi SC (FFSC) (14.0%), F. incarnatum-equiseti SC (11.6%), F. dimerum SC (7.0%), and F. oxysporum SC (4.7%). Phylogenetic analysis revealed that clinical Fusarium isolates from KCGMH were closely related to environmental Fusarium isolates from air samples at the same hospital. Amphotericin B exhibited high activity against most Fusarium species. With the exception of FFSC, other Fusarium SC demonstrated significantly elevated MIC values to itraconazole, voriconazole, posaconazole, and isavuconazole. Conclusions: FSSC was the most prevalent SC in Taiwan, exhibiting higher MIC values for azoles than FFSC isolates. The clinical Fusarium isolates were observed to form clusters with the corresponding environmental isolates. The potential of airborne nosocomial infections in the healthcare environment cannot be overlooked.

AB - Background: Fusarium species are emerging pathogens known to cause both superficial and disseminated human infections. Aerosolized Fusarium species in healthcare settings have been associated with nosocomial fusariosis, particularly in patients with severe immunosuppression. Objectives: To analyse the phylogenetic relationships of clinical and hospital environmental Fusarium isolates and assess their susceptibility to available antifungal agents. Methods: Clinical Fusarium isolates were procured from four hospitals in Taiwan, with environmental air and water sampling collected at Kaohsiung Chang Gung Memorial Hospital (KCGMH). All clinical and hospital environmental Fusarium isolates were identified through gene sequencing of translation elongation factor 1-α and internal transcribed spacer regions of ribosomal DNA. Antifungal susceptibility testing followed the CLSI M38-A3 broth microdilution method. Results: A total of 41 clinical and 4 hospital environmental Fusarium isolates were identified, belonging to five species complexes (SC): F. solani SC (FSSC) (62.8%), F. fujikuroi SC (FFSC) (14.0%), F. incarnatum-equiseti SC (11.6%), F. dimerum SC (7.0%), and F. oxysporum SC (4.7%). Phylogenetic analysis revealed that clinical Fusarium isolates from KCGMH were closely related to environmental Fusarium isolates from air samples at the same hospital. Amphotericin B exhibited high activity against most Fusarium species. With the exception of FFSC, other Fusarium SC demonstrated significantly elevated MIC values to itraconazole, voriconazole, posaconazole, and isavuconazole. Conclusions: FSSC was the most prevalent SC in Taiwan, exhibiting higher MIC values for azoles than FFSC isolates. The clinical Fusarium isolates were observed to form clusters with the corresponding environmental isolates. The potential of airborne nosocomial infections in the healthcare environment cannot be overlooked.

KW - MALDI-TOF

KW - air sampling

KW - filamentous fungi

KW - fusarium

KW - molecular identification

UR - https://www.scopus.com/pages/publications/105003802215

U2 - 10.1111/myc.70056

DO - 10.1111/myc.70056

M3 - 文章

C2 - 40275734

AN - SCOPUS:105003802215

SN - 0933-7407

VL - 68

SP - e70056

JO - Mycoses

JF - Mycoses

IS - 4

M1 - e70056

ER -

Clinical and Hospital Environmental Fusarium in Taiwan: Molecular Identification, Antifungal Susceptibilities, and Phylogenetic Analyses

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Keywords

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