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Multi-omics analysis reveals key immunogenic signatures induced by oncolytic Zika virus infection of paediatric brain tumour cells

Multi-omics analysis reveals key immunogenic signatures induced by oncolytic Zika virus infection of paediatric brain tumour cells
Multi-omics analysis reveals key immunogenic signatures induced by oncolytic Zika virus infection of paediatric brain tumour cells

Brain tumours disproportionately affect children and are the largest cause of paediatric cancer-related death. Novel therapies that engage the immune system, such as oncolytic viruses (OVs), hold great promise and are desperately needed. Zika virus (ZIKV) infects and destroys aggressive cells from multiple paediatric central nervous system (CNS) tumours. Despite this, the molecular mechanisms underpinning this response are largely unknown. We comprehensively investigate the transcriptomic response of paediatric medulloblastoma and atypical teratoid rhabdoid tumour (ATRT) cells to ZIKV infection. We observe conserved TNF signalling and cytokine signalling-related signatures and show that the TNF-alpha signalling pathway is implicated in oncolysis by reducing the viability of ZIKV-infected brain tumour cells. Our findings highlight TNF-alpha as a potential prognostic marker for oncolytic ZIKV (oZIKV) therapy. Complementing our analysis with a 49-plex ELISA, we demonstrate that ZIKV infection induces a clinically relevant and diverse pro-inflammatory brain tumour cell secretome, including TNF-alpha. We assess publicly available scRNA-Seq data to model how ZIKV-induced secretome paracrine and endocrine signalling may orchestrate the anti-tumoural immune response during oZIKV infection of brain tumours. Our findings significantly contribute to understanding the molecular mechanisms governing oZIKV infection and will help pave the way towards oZIKV therapy.

Brain Neoplasms/immunology, Cell Line, Tumor, Child, Humans, Medulloblastoma/immunology, Multiomics, Oncolytic Virotherapy/methods, Oncolytic Viruses/immunology, Rhabdoid Tumor/immunology, Signal Transduction, Transcriptome, Tumor Necrosis Factor-alpha/metabolism, Zika Virus Infection/immunology, Zika Virus/immunology, Multiplex ELISA, Cytokine, Zika virus, Paediatric brain tumours, TNF signalling, RNA-sequencing, Oncolytic virotherapy
2045-2322
Sherwood, Matthew
a7cf817d-8d5e-44f9-af50-516741c8c91c
Mitsugi, Thiago G.
bbb4290c-980a-459f-94d8-5021b4c42abe
Kaid, Carolini
290160fb-4f2e-4326-9a07-3a05db3dff35
Coke, Brandon
9e52fdaf-3c8c-4c2b-b2a9-21486dcfd0a5
Zatz, Mayana
2ef35681-e705-48c9-85d5-fe8b4cd579c2
Maringer, Kevin
180b08d1-26f4-4346-b218-887732d18d79
Okamoto, Oswaldo K.
ddfc4523-4997-4a91-99fe-a998210efa21
Ewing, Rob M.
022c5b04-da20-4e55-8088-44d0dc9935ae
Sherwood, Matthew
a7cf817d-8d5e-44f9-af50-516741c8c91c
Mitsugi, Thiago G.
bbb4290c-980a-459f-94d8-5021b4c42abe
Kaid, Carolini
290160fb-4f2e-4326-9a07-3a05db3dff35
Coke, Brandon
9e52fdaf-3c8c-4c2b-b2a9-21486dcfd0a5
Zatz, Mayana
2ef35681-e705-48c9-85d5-fe8b4cd579c2
Maringer, Kevin
180b08d1-26f4-4346-b218-887732d18d79
Okamoto, Oswaldo K.
ddfc4523-4997-4a91-99fe-a998210efa21
Ewing, Rob M.
022c5b04-da20-4e55-8088-44d0dc9935ae

Sherwood, Matthew, Mitsugi, Thiago G., Kaid, Carolini, Coke, Brandon, Zatz, Mayana, Maringer, Kevin, Okamoto, Oswaldo K. and Ewing, Rob M. (2025) Multi-omics analysis reveals key immunogenic signatures induced by oncolytic Zika virus infection of paediatric brain tumour cells. Scientific Reports, 15 (1), [13090]. (doi:10.1038/s41598-025-97804-8).

Record type: Article

Abstract

Brain tumours disproportionately affect children and are the largest cause of paediatric cancer-related death. Novel therapies that engage the immune system, such as oncolytic viruses (OVs), hold great promise and are desperately needed. Zika virus (ZIKV) infects and destroys aggressive cells from multiple paediatric central nervous system (CNS) tumours. Despite this, the molecular mechanisms underpinning this response are largely unknown. We comprehensively investigate the transcriptomic response of paediatric medulloblastoma and atypical teratoid rhabdoid tumour (ATRT) cells to ZIKV infection. We observe conserved TNF signalling and cytokine signalling-related signatures and show that the TNF-alpha signalling pathway is implicated in oncolysis by reducing the viability of ZIKV-infected brain tumour cells. Our findings highlight TNF-alpha as a potential prognostic marker for oncolytic ZIKV (oZIKV) therapy. Complementing our analysis with a 49-plex ELISA, we demonstrate that ZIKV infection induces a clinically relevant and diverse pro-inflammatory brain tumour cell secretome, including TNF-alpha. We assess publicly available scRNA-Seq data to model how ZIKV-induced secretome paracrine and endocrine signalling may orchestrate the anti-tumoural immune response during oZIKV infection of brain tumours. Our findings significantly contribute to understanding the molecular mechanisms governing oZIKV infection and will help pave the way towards oZIKV therapy.

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s41598-025-97804-8 - Version of Record
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Accepted/In Press date: 7 April 2025
Published date: 16 April 2025
Keywords: Brain Neoplasms/immunology, Cell Line, Tumor, Child, Humans, Medulloblastoma/immunology, Multiomics, Oncolytic Virotherapy/methods, Oncolytic Viruses/immunology, Rhabdoid Tumor/immunology, Signal Transduction, Transcriptome, Tumor Necrosis Factor-alpha/metabolism, Zika Virus Infection/immunology, Zika Virus/immunology, Multiplex ELISA, Cytokine, Zika virus, Paediatric brain tumours, TNF signalling, RNA-sequencing, Oncolytic virotherapy

Identifiers

Local EPrints ID: 503019
URI: http://eprints.soton.ac.uk/id/eprint/503019
ISSN: 2045-2322
PURE UUID: c8723ea4-132e-4683-8173-f48c4f1c4660
ORCID for Brandon Coke: ORCID iD orcid.org/0000-0002-0847-6885
ORCID for Rob M. Ewing: ORCID iD orcid.org/0000-0001-6510-4001

Catalogue record

Date deposited: 16 Jul 2025 16:31
Last modified: 22 Aug 2025 02:30

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Contributors

Author: Matthew Sherwood
Author: Thiago G. Mitsugi
Author: Carolini Kaid
Author: Brandon Coke ORCID iD
Author: Mayana Zatz
Author: Kevin Maringer
Author: Oswaldo K. Okamoto
Author: Rob M. Ewing ORCID iD

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