Drug screening on tumor organoids exposes therapeutic vulnerabilities of meningiomas to HDAC1/2i panobinostat.

Jungwirth, Gerhard; Moustafa, Mahmoud; Trong, Philip Dao; Cao, Junguo; von Deimling, Andreas; Braun, Viktor; Krieg, Sandro M; Warta, Rolf; Abdollahi, Amir; Knoll, Maximilian; Sahm, Felix; Yu, Tao; Younsi, Alexander; Jassowicz, Lena; Bendszus, Martin; Pan, Yimin; Herold-Mende, Christel; Wang, Zhenlin; Scherer, Moritz; Debus, Juergen; Unterberg, Andreas; Lotsch, Catharina

doi:10.1126/scitranslmed.aea3115

Journal Article

DKFZ-2026-00519

Drug screening on tumor organoids exposes therapeutic vulnerabilities of meningiomas to HDAC1/2i panobinostat.

Jungwirth, G.DKFZ* ; Cao, J. ; Pan, Y. ; Warta, R. ; Lotsch, C. ; Moustafa, M.DKFZ* ; Knoll, M.DKFZ* ; Yu, T. ; Braun, V. ; Jassowicz, L. ; Trong, P. D. ; Wang, Z. ; Younsi, A. ; Scherer, M. ; Bendszus, M. ; Krieg, S. M. ; von Deimling, A.DKFZ* ; Debus, J.DKFZ* ; Abdollahi, A.DKFZ* ; Unterberg, A. ; Sahm, F.DKFZ* ; Herold-Mende, C.

2026
AAAS Washington, DC

Science translational medicine 18(839), eaea3115 (2026) [10.1126/scitranslmed.aea3115]

Abstract: Managing aggressive meningiomas remains challenging because of limited treatment options besides surgical tumor removal and radiotherapy. To increase the repertoire of promising therapies for aggressive meningiomas, we established a multistep drug screening workflow, focusing on targetable genes obtained from transcriptome data of highly aggressive grade 3 meningiomas. In vitro screening of 107 targeted drugs identified nine effective inhibitors. To study these drugs in a more natural environment, we established a standardized patient-derived tumor organoid (TO) model preserving accurately the original tissue's genotype and phenotype. Individual drug responses were assessed in TOs from 60 meningioma cases characterized at the molecular level. In particular, the US Food and Drug Administration-approved epigenetic drug panobinostat demonstrated high antimeningioma efficacy in 70% of TOs, mediated through histone deacetylase 1 and 2 (HDAC1/2) inhibition. In addition, treatment in an orthotopic in vivo model revealed improved survival. In search of the molecular mechanism underlying a potentially intrinsic panobinostat resistance, we identified up-regulation of the HDAC8-transforming growth factor-β (TGFβ)-epithelial-to-mesenchymal transition (EMT) axis in the TO model, whereas subsequent HDAC8 depletion increased the sensitivity to panobinostat. These data highlight the utility of personalized drug screenings on TOs to identify suitable drug targets and inhibitors for more effective treatment of clinically aggressive meningiomas and to help advance our understanding of counteracting resistance mechanisms.

Classification:

ddc:500

Contributing Institute(s):

Research Program(s):

319H - Addenda (POF4-319H) (POF4-319H)

Appears in the scientific report 2026

Database coverage:
Medline

; BIOSIS Previews ; Biological Abstracts ; Clarivate Analytics Master Journal List ; Essential Science Indicators ; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection

Click to display QR Code for this record

The record appears in these collections:
Document types > Articles > Journal Article
Public records
Publications database

Record created 2026-03-05, last modified 2026-03-05

Similar records

Rate this document:

(Not yet reviewed)

Add to personal basket
Export as Author List with IDs BibTeX (UTF-8), EndNote XML, EndNote Text, RIS, MARC, Print MARC, MARCXML, DC,
Request correction
Submit fulltext

guest :: login DKFZ
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help