Umeå University's logo

umu.sePublications
EnglishSvenskaNorsk
Change search
CiteExportLink to record
Permanent link

Direct link
Cite
Citation style
  • apa
  • ieee
  • vancouver
  • Other style
More styles
Language
  • de-DE
  • en-GB
  • en-US
  • fi-FI
  • nn-NO
  • nn-NB
  • sv-SE
  • Other locale
More languages
Output format
  • html
  • text
  • asciidoc
  • rtf
Photodynamic therapy using a heavy-atom-free g-quadruplex-targeted photosensitizer to efficiently regress rhabdomyosarcoma tumors in vivo
Umeå University, Faculty of Medicine, Department of Medical and Translational Biology.ORCID iD: 0000-0002-5631-2332
Umeå University, Faculty of Medicine, Department of Medical and Translational Biology.
University Angers, CNRS, MOLTECH-ANJOU, SFR MATRIX, Angers, France.
University Angers, CNRS, MOLTECH-ANJOU, SFR MATRIX, Angers, France.
Show others and affiliations
2025 (English)In: ACS Pharmacology & Translational Science, E-ISSN 2575-9108, Vol. 8, no 8, p. 2482-2492Article in journal (Refereed) Published
Abstract [en]

Rhabdomyosarcoma is a highly aggressive soft tissue cancer that predominantly affects children and adolescents. Current treatment outcomes are poor, highlighting the urgent need for potent therapeutic alternatives. Preclinical research on photodynamic therapy (PDT) continues to gain attention as a promising and minimally invasive treatment strategy. Recently, PDT using the heavy-atom-free photosensitizer dibenzothioxanthene imide (DBI), which targets cancer-associated G-quadruplex (G4) DNA, has demonstrated high efficacy at nanomolar concentrations. In here, transgenic zebrafish with rhabdomyosarcoma tumors were utilized to evaluate the therapeutic potential of DBI treatment. We demonstrate that photoactivated DBI efficiently induce localized tumor necrosis, resulting in significant rhabdomyosarcoma regression compared to untreated controls. In fact, in comparison to the healthy cells surrounding the tumor, a high level of G4s was detected, as visualized by a G4-specific antibody. Notably, muscle and nerve cells within the treated tumor area were particularly affected, further underscoring its potency. These findings position DBI as a promising candidate for PDT in the treatment of rhabdomyosarcoma, offering selective G4-targeting capabilities and delivering robust therapeutic outcomes in in vivo models.
Place, publisher, year, edition, pages
American Chemical Society (ACS), 2025. Vol. 8, no 8, p. 2482-2492
Keywords [en]
cancer, G-quadruplex, photodynamic therapy, photosensitizer, rhabdomyosarcoma, zebrafish
National Category
Cancer and Oncology
Identifiers
URN: urn:nbn:se:umu:diva-238234DOI: 10.1021/acsptsci.5c00061ISI: 001468563600001PubMedID: 40810172Scopus ID: 2-s2.0-105002836831OAI: oai:DiVA.org:umu-238234DiVA, id: diva2:1955354
Funder
Swedish Cancer Society, 23 2719 Pj 01 HSwedish Cancer Society, 22 2380 Pj 01 HKnut and Alice Wallenberg Foundation, KAW 2021.0173EU, Horizon 2020, 945339Available from: 2025-04-30 Created: 2025-04-30 Last updated: 2025-10-29Bibliographically approved
In thesis
1. Tumour progression and photodynamic therapy in a zebrafish model of rhabdomyosarcoma
Open this publication in new window or tab >>Tumour progression and photodynamic therapy in a zebrafish model of rhabdomyosarcoma
2025 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

Rhabdomyosarcoma (RMS) is the most common pediatric soft-tissue cancer, which primarily develops in muscle tissue during childhood. Despite advances in treatment, outcomes for many patients remain poor. This thesis aims to investigate RMS progression and regression in different genetic contexts, using zebrafish RMS models to evaluate a novel molecule as a potential RMS treatment.

Pax3 and Pax7 transcription factors play important roles in fusion-positive RMS. However, their role in fusion-negative RMS remains less clear. Therefore, we aimed to examine how the lack of Pax3 and Pax7 influences fusion-negative RMS formation and progression.

In the first study, we investigated the role of Pax3 in RAS-driven, fusion-negative RMS. Using pax3a-/-;pax3b-/- double mutant zebrafish, we found that the RAS/MAPK signalling pathway was downregulated in the mutants compared to controls, correlating with a delay in tumour progression. These findings suggest that, in fusion-negative RMS, Pax3 also contributes to tumour development by modulating oncogenic signalling. 

In the second study, we aimed to explore the role of Pax7 in fusion-negative RMS, using a pax7-deficient zebrafish model. Our RNA-seq and lipidomics analyses showed downregulation of mitochondrial-related genes, decreased cardiolipin levels, and altered microtubule dynamics in pax7a-/-;pax7b-/- mutants compared to healthy wild-type fish. We also showed lower mitochondria labelling in pax7a-/-;pax7b-/- tumours compared to wild-type tumours. These findings indicate that Pax7 plays an important role in maintaining mitochondrial membrane integrity and function in healthy and tumourigenic conditions.

In the last part of the thesis, we aimed to evaluate the feasibility of photodynamic therapy using a novel photosensitizer for cancer treatment.

In the third study we designed and synthesized a heavy-atom-free light-inducible compound called dibenzothioxanthene imide (DBI), which binds to G-quadruplex (G4) DNA. Upon targeted photoactivation of DBI, it produced reactive oxygen species and caused DNA damage in human cancer cells and healthy zebrafish embryos. 

Complementing this, the last study explored the potential of photodynamic therapy using the photosensitizer DBI for treating RMS in zebrafish models. Treatment with light-activated DBI resulted in targeted apoptosis and tumour regression, compared to control treatments. In addition, RMS tissue was more affected by photoactivated DBI than healthy tissue, likely due to the higher accumulation of G4 structures in tumours compared to healthy regions.

Together, these findings uncover new roles of Pax3 and Pax7 in RMS biology using zebrafish models and highlight the therapeutic potential of G4-targeted photodynamic therapy for RMS.
Place, publisher, year, edition, pages
Umeå: Umeå University, 2025. p. 60
Series
Umeå University medical dissertations, ISSN 0346-6612 ; 2384
Keywords
rhabdomyosarcoma, zebrafish, photodynamic therapy, G-quadruplex, cancer, Pax3, Pax7
National Category
Basic Cancer Research
Identifiers
urn:nbn:se:umu:diva-245793 (URN)978-91-8070-816-6 (ISBN)978-91-8070-815-9 (ISBN)
Public defence
2025-11-20, BIO.E.203 - Aula Biologica, Biologihuset, Umeå, 09:00 (English)
Opponent
Supervisors
Available from: 2025-10-30 Created: 2025-10-23 Last updated: 2025-10-29Bibliographically approved

Open Access in DiVA

fulltext(11948 kB)31 downloads
File information
File name FULLTEXT02.pdfFile size 11948 kBChecksum SHA-512
c74acd6d04e30e35da39623dc47a9a2d26660a86403b3ac679c811efcc888e2065fa23e59974b0293e21b1a26fd280f0afe92bc54187427d230f3525f564c2ce
Type fulltextMimetype application/pdf

Other links

Publisher's full textPubMedScopus

Authority records

Rodriguez-Marquez, EvaNord, HannaSabouri, Nasimvon Hofsten, Jonas

Search in DiVA

By author/editor
Rodriguez-Marquez, EvaNord, HannaSabouri, Nasimvon Hofsten, Jonas
By organisation
Department of Medical and Translational BiologyDepartment of Medical Biochemistry and Biophysics
In the same journal
ACS Pharmacology & Translational Science
Cancer and Oncology

Search outside of DiVA

GoogleGoogle Scholar
Total: 284 downloads
The number of downloads is the sum of all downloads of full texts. It may include eg previous versions that are now no longer available

doi
pubmed
urn-nbn

Altmetric score

doi
pubmed
urn-nbn
Total: 483 hits
CiteExportLink to record
Permanent link

Direct link
Cite
Citation style
  • apa
  • ieee
  • vancouver
  • Other style
More styles
Language
  • de-DE
  • en-GB
  • en-US
  • fi-FI
  • nn-NO
  • nn-NB
  • sv-SE
  • Other locale
More languages
Output format
  • html
  • text
  • asciidoc
  • rtf
v. 2.47.0
|
WCAG
|
Log in
|
Manuals
|
Contact the Library