Profound cell wall remodeling in Candida parapsilosis during systemic infection confers simultaneous tolerance to echinocandins and host immunity

Farnaz Daneshnia; Liuyang Cai; Deepika Gunasekaran; Isha Gautam; Austin M Perry; Pegah Mosharaf Ghahfarokhy; Arefeh Ebadati; Julieta Munoz; Dorian Padilla; Süleyha Hilmioglu-Polat; Shenglin Mei; Daniel J Floyd; Miquel Àngel Schikora-Tamarit; Diego Fuentes; Maria Artigues-Lleixà; Louise A Walker; Samuel M Gonçalves; Mostafa Salehi; Agostinho Carvalho; Jigar V Desai; David S Perlin; Carol A Munro; Alex Hopke; Tuo Wang; Toni Gabaldón; Wenjie Fang; Clarissa J Nobile; Michael K Mansour; Amir Arastehfar

doi:10.1128/spectrum.03043-25

Profound cell wall remodeling in Candida parapsilosis during systemic infection confers simultaneous tolerance to echinocandins and host immunity

Microbiol Spectr. 2026 Apr 7;14(4):e0304325. doi: 10.1128/spectrum.03043-25. Epub 2026 Feb 13.

Authors

Farnaz Daneshnia^{1

2}, Liuyang Cai^{3

4}, Deepika Gunasekaran⁵, Isha Gautam⁶, Austin M Perry^{5

7}, Pegah Mosharaf Ghahfarokhy^{5

7

8}, Arefeh Ebadati^{5

7

8}, Julieta Munoz⁵, Dorian Padilla⁵, Süleyha Hilmioglu-Polat⁹, Shenglin Mei^{10

11}, Daniel J Floyd², Miquel Àngel Schikora-Tamarit^{12

13}, Diego Fuentes^{12

13}, Maria Artigues-Lleixà^{12

13}, Louise A Walker¹⁴, Samuel M Gonçalves^{15

16}, Mostafa Salehi¹⁷, Agostinho Carvalho^{15

16}, Jigar V Desai¹⁸, David S Perlin^{18

19

20}, Carol A Munro¹⁴, Alex Hopke²¹, Tuo Wang⁶, Toni Gabaldón^{12

13

22

23}, Wenjie Fang^{3

4}, Clarissa J Nobile^{5

8}, Michael K Mansour^{2

24}, Amir Arastehfar^{2

24

25}

Affiliations

¹ Institute of Biodiversity and Ecosystem Dynamics (IBED), University of Amsterdam, Amsterdam, Netherlands.
² Division of Infectious Diseases, Massachusetts General Hospital, Boston, Massachusetts, USA.
³ Department of Dermatology, Shanghai Key Laboratory of Molecular Medical Mycology, Shanghai Changzheng Hospital, Naval Medical University, Shanghai, China.
⁴ The Center for Fungal Infectious Diseases Basic Research and Innovation of Medicine and Pharmacy, Ministry of Education, Shanghai, China.
⁵ Department of Molecular and Cell Biology, School of Natural Sciences, University of California Merced, Merced, California, USA.
⁶ Department of Chemistry, Michigan State University, East Lansing, Michigan, USA.
⁷ Quantitative and Systems Biology Graduate Program, University of California, Merced, California, USA.
⁸ Health Sciences Research Institute, University of California, Merced, California, USA.
⁹ Department of Medical Microbiology, Ege University Faculty of Medicine, Izmir, Turkey.
¹⁰ Fralin Biomedical Research Institute, Virginia Tech FBRI21 Cancer Research Center, Washington, DC, USA.
¹¹ Department of Biomedical Sciences and Pathobiology, College of Veterinary Medicine, Virginia Tech, Blacksburg, Virginia, USA.
¹² Life Sciences Programme, Supercomputing Center (BSC-CNS), Barcelona, Spain.
¹³ Institute for Research in Biomedicine (IRB Barcelona), The Barcelona Institute of Science and Technology, Barcelona, Spain.
¹⁴ School of Medicine, Medical Sciences and Nutrition, Institute of Medical Sciences, University of Aberdeen, Aberdeen, United Kingdom.
¹⁵ School of Medicine, Life and Health Sciences Research Institute (ICVS), University of Minho, Braga, Portugal.
¹⁶ ICVS/3B's-PT Government Associate Laboratory, Guimarães, Braga, Portugal.
¹⁷ Department Industrial Engineering Faculty of K.N, KN Toosi University of Technology, Tehran, Iran.
¹⁸ Center for Discovery and Innovation, Hackensack Meridian Health, Nutley, New Jersey, USA.
¹⁹ Georgetown University Lombardi Comprehensive Cancer Center, Washington, DC, USA.
²⁰ Department of Medical Sciences, Hackensack Meridian School of Medicine, Nutley, New Jersey, USA.
²¹ Department of Biomedical Sciences, East Tennessee State University Quillen College of Medicine, Center of Excellence in Inflammation, Infectious Disease and Immunity, East Tennessee State University, Johnson City, Tennessee, USA.
²² Catalan Institution for Research and Advanced Studies, Barcelona, Spain.
²³ Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Barcelona, Spain.
²⁴ Department of Medicine, Harvard Medical School, Boston, Massachusetts, USA.
²⁵ University Hospital Wuerzburg, Medical Hospital II, Würzburg, Germany.

Abstract

Antifungal tolerance can promote the emergence of resistance yet often incurs fitness costs for fungal pathogens. How tolerant populations compensate for these deficits and how they may be therapeutically targeted remain poorly understood. Here, we investigate four sequential Candida parapsilosis isolates recovered from a patient with persistent candidemia and failure of micafungin therapy. The infection was ultimately cleared with liposomal amphotericin B (LAMB). Whole-genome sequencing (WGS) confirmed clonal relatedness and the absence of known resistance mutations. Later isolates displayed marked cell wall remodeling (CWR), characterized by increased mannan and reduced β-glucan content, as revealed by microscopy and solid-state nuclear magnetic resonance. These isolates formed thicker biofilms and displayed enhanced echinocandin tolerance but paradoxically showed increased susceptibility to amphotericin B (AMB) in vitro and during systemic infection in mice. Despite a complex mutational landscape, transcriptomic profiling across planktonic and biofilm growth showed minimal divergence from the earliest isolate. Functionally, evolved isolates suppressed M1 macrophage polarization, dampened proinflammatory cytokine production, survived better during neutrophil interactions, and transiently increased fungal burden in vivo. These findings show that host-driven CWR could promote echinocandin tolerance while simultaneously sensitizing C. parapsilosis to AMB. Our results suggest that alternating echinocandin and LAMB therapy may effectively eliminate echinocandin-tolerant fungal populations.IMPORTANCEAntifungal tolerance is increasingly recognized as a precursor to resistance, yet its clinical and biological consequences remain poorly defined. By analyzing sequential Candida parapsilosis isolates from a case of persistent candidemia, we show that cell wall remodeling is associated with echinocandin tolerance, alters host immune interactions, and increases susceptibility to amphotericin B (AMB). These findings reveal how tolerance-associated adaptations shape pathogen fitness during infection and highlight the therapeutic potential of alternating echinocandin and AMB therapy. This work advances our understanding of antifungal tolerance and suggests that exploiting opposing drug susceptibilities may improve treatment outcomes for challenging-to-treat Candida infections.

Keywords: biofilms; cell wall remodeling; echinocandins; immune evasion; macrophage polarization; polyenes; resistance; tolerance.

MeSH terms

Amphotericin B / pharmacology
Amphotericin B / therapeutic use
Animals
Antifungal Agents* / pharmacology
Antifungal Agents* / therapeutic use
Biofilms / drug effects
Biofilms / growth & development
Candida parapsilosis* / drug effects
Candida parapsilosis* / genetics
Candida parapsilosis* / immunology
Candida parapsilosis* / isolation & purification
Candidemia / drug therapy
Candidemia / immunology
Candidemia / microbiology
Candidiasis* / drug therapy
Candidiasis* / immunology
Candidiasis* / microbiology
Cell Wall* / drug effects
Cell Wall* / metabolism
Drug Resistance, Fungal
Echinocandins* / pharmacology
Echinocandins* / therapeutic use
Female
Humans
Micafungin / pharmacology
Micafungin / therapeutic use
Mice
Microbial Sensitivity Tests
Whole Genome Sequencing
beta-Glucans / metabolism

Substances

Antifungal Agents
Echinocandins
Amphotericin B
liposomal amphotericin B
Micafungin
beta-Glucans

Abstract

MeSH terms

Substances

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