Targeting ceramide synthases for the development of new antifungals

Deveney Dasilva; Nivea Pereira de Sa; Kathryn Takemura; Kalani Jayanetti; Jeehyun Karen You; Nathalia Vieira de Sa; Gabriel Soares Matos; Andy Zhong; Can E. Senkal; Yusuf Hannun; Iwao Ojima; John Mallamo; John B. McCarthy; Maurizio Del Poeta

doi:10.1016/j.str.2025.05.016

Targeting ceramide synthases for the development of new antifungals

Deveney Dasilva
, Nivea Pereira de Sa
, Kathryn Takemura
, Kalani Jayanetti
, Jeehyun Karen You
, Nathalia Vieira de Sa
, Gabriel Soares Matos
, Andy Zhong
, Can E. Senkal
, Yusuf Hannun
, Iwao Ojima
, John Mallamo
, John B. McCarthy
, Maurizio Del Poeta

Stony Brook University
Virginia Commonwealth University
MicroRid Technologies Inc.

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

3 Scopus citations

Abstract

Invasive fungal infections (IFIs) caused by pathogenic fungi are a major public health concern, particularly across various immunocompromised populations. Effective clinical management is currently hindered by limited treatment options. Fungal sphingolipids have emerged as potential antifungal targets based on cumulative evidence demonstrating that fungal sphingolipid metabolism is key to the virulence of pathogenic fungi. This study focuses on the sphingolipid metabolizing enzyme ceramide synthase. We developed an enzymatic assay to examine ceramide synthase activity and devised a high-throughput screening platform. Two synthetic compounds were identified that preferentially inhibit the fungal vs. the mammalian ceramide synthase activity. Further studies indicate that these compounds block fungal growth, with in silico and mutagenesis investigations revealing insights into the interactions between the inhibitors and the ceramide synthase active site. Together, our study establishes fungal ceramide synthase as a promising antifungal target and paves the way for new structure-activity relationship studies leveraging fungal sphingolipid metabolism.

Original language	English
Pages (from-to)	1565-1576.e4
Journal	Structure
Volume	33
Issue number	9
DOIs	https://doi.org/10.1016/j.str.2025.05.016
State	Published - Sep 4 2025

Keywords

Cryptococcus neoformans
antifungal
ceramide
ceramide synthase
docking
drug discovery
high-throughput screening
small molecule library
sphingolipid
sphingosine

Access to Document

10.1016/j.str.2025.05.016

Cite this

@article{14a700d93f254cf9bc5244ac4f441911,

title = "Targeting ceramide synthases for the development of new antifungals",

abstract = "Invasive fungal infections (IFIs) caused by pathogenic fungi are a major public health concern, particularly across various immunocompromised populations. Effective clinical management is currently hindered by limited treatment options. Fungal sphingolipids have emerged as potential antifungal targets based on cumulative evidence demonstrating that fungal sphingolipid metabolism is key to the virulence of pathogenic fungi. This study focuses on the sphingolipid metabolizing enzyme ceramide synthase. We developed an enzymatic assay to examine ceramide synthase activity and devised a high-throughput screening platform. Two synthetic compounds were identified that preferentially inhibit the fungal vs. the mammalian ceramide synthase activity. Further studies indicate that these compounds block fungal growth, with in silico and mutagenesis investigations revealing insights into the interactions between the inhibitors and the ceramide synthase active site. Together, our study establishes fungal ceramide synthase as a promising antifungal target and paves the way for new structure-activity relationship studies leveraging fungal sphingolipid metabolism.",

keywords = "Cryptococcus neoformans, antifungal, ceramide, ceramide synthase, docking, drug discovery, high-throughput screening, small molecule library, sphingolipid, sphingosine",

author = "Deveney Dasilva and \{Pereira de Sa\}, Nivea and Kathryn Takemura and Kalani Jayanetti and You, \{Jeehyun Karen\} and \{Vieira de Sa\}, Nathalia and Matos, \{Gabriel Soares\} and Andy Zhong and Senkal, \{Can E.\} and Yusuf Hannun and Iwao Ojima and John Mallamo and McCarthy, \{John B.\} and \{Del Poeta\}, Maurizio",

note = "Publisher Copyright: {\textcopyright} 2025 Elsevier Inc.",

year = "2025",

month = sep,

day = "4",

doi = "10.1016/j.str.2025.05.016",

language = "English",

volume = "33",

pages = "1565--1576.e4",

journal = "Structure",

issn = "0969-2126",

number = "9",

}

TY - JOUR

T1 - Targeting ceramide synthases for the development of new antifungals

AU - Dasilva, Deveney

AU - Pereira de Sa, Nivea

AU - Takemura, Kathryn

AU - Jayanetti, Kalani

AU - You, Jeehyun Karen

AU - Vieira de Sa, Nathalia

AU - Matos, Gabriel Soares

AU - Zhong, Andy

AU - Senkal, Can E.

AU - Hannun, Yusuf

AU - Ojima, Iwao

AU - Mallamo, John

AU - McCarthy, John B.

AU - Del Poeta, Maurizio

PY - 2025/9/4

Y1 - 2025/9/4

N2 - Invasive fungal infections (IFIs) caused by pathogenic fungi are a major public health concern, particularly across various immunocompromised populations. Effective clinical management is currently hindered by limited treatment options. Fungal sphingolipids have emerged as potential antifungal targets based on cumulative evidence demonstrating that fungal sphingolipid metabolism is key to the virulence of pathogenic fungi. This study focuses on the sphingolipid metabolizing enzyme ceramide synthase. We developed an enzymatic assay to examine ceramide synthase activity and devised a high-throughput screening platform. Two synthetic compounds were identified that preferentially inhibit the fungal vs. the mammalian ceramide synthase activity. Further studies indicate that these compounds block fungal growth, with in silico and mutagenesis investigations revealing insights into the interactions between the inhibitors and the ceramide synthase active site. Together, our study establishes fungal ceramide synthase as a promising antifungal target and paves the way for new structure-activity relationship studies leveraging fungal sphingolipid metabolism.

AB - Invasive fungal infections (IFIs) caused by pathogenic fungi are a major public health concern, particularly across various immunocompromised populations. Effective clinical management is currently hindered by limited treatment options. Fungal sphingolipids have emerged as potential antifungal targets based on cumulative evidence demonstrating that fungal sphingolipid metabolism is key to the virulence of pathogenic fungi. This study focuses on the sphingolipid metabolizing enzyme ceramide synthase. We developed an enzymatic assay to examine ceramide synthase activity and devised a high-throughput screening platform. Two synthetic compounds were identified that preferentially inhibit the fungal vs. the mammalian ceramide synthase activity. Further studies indicate that these compounds block fungal growth, with in silico and mutagenesis investigations revealing insights into the interactions between the inhibitors and the ceramide synthase active site. Together, our study establishes fungal ceramide synthase as a promising antifungal target and paves the way for new structure-activity relationship studies leveraging fungal sphingolipid metabolism.

KW - Cryptococcus neoformans

KW - antifungal

KW - ceramide

KW - ceramide synthase

KW - docking

KW - drug discovery

KW - high-throughput screening

KW - small molecule library

KW - sphingolipid

KW - sphingosine

UR - https://www.scopus.com/pages/publications/105008778075

U2 - 10.1016/j.str.2025.05.016

DO - 10.1016/j.str.2025.05.016

M3 - Article

C2 - 40555233

AN - SCOPUS:105008778075

SN - 0969-2126

VL - 33

SP - 1565-1576.e4

JO - Structure

JF - Structure

IS - 9

ER -

Targeting ceramide synthases for the development of new antifungals

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Cite this