Comprehensive genomic and transcriptomic analysis enables molecularly guided therapy options in peritoneal and pleural mesothelioma

L. Möhrmann; M. Werner; M. Oleś; L. Knol; J. S. Arnold; T. Mundt; N. Paramasivam; D. Richter; M. Fröhlich; B. Hutter; J. Hüllein; A. Jahn; C. Scheffold; E. E. Möhrmann; D. Hanf; S. Kreutzfeldt; C. E. Heilig; M. V. Teleanu; D. B. Lipka; K. Beck; A. Baude-Müller; I. Jelas; D. T. Rieke; L. V. Klotz; R. Shah; T. Herold; M. Boerries; A. L. Illert; M. Allgäuer; A. Stenzinger; I. A. Kerle; P. Horak; C. Heining; E. Schröck; D. Hübschmann; S. Fröhling; H. Glimm

doi:10.1016/j.esmoop.2025.104532

Comprehensive genomic and transcriptomic analysis enables molecularly guided therapy options in peritoneal and pleural mesothelioma

Research output: Contribution to journal › Research article › Contributed › peer-review

Contributors

L. Möhrmann - , National Center for Tumor Diseases Dresden, German Cancer Research Center, partner site Dresden, University Hospital Carl Gustav Carus Dresden, Harvard University (Author)
M. Werner - , Department of Internal Medicine I, National Center for Tumor Diseases Dresden (NCT/UCC), University Hospital Carl Gustav Carus Dresden (Author)
M. Oleś - , German Cancer Research Center (DKFZ), Heidelberg University (Author)
L. Knol - , University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ) (Author)
J. S. Arnold - , Institute of Clinical Genetics, National Center for Tumor Diseases Dresden, University Hospital Carl Gustav Carus Dresden, Max Planck Institute of Molecular Cell Biology and Genetics (Author)
T. Mundt - , National Center for Tumor Diseases Dresden, University Cancer Centre Dresden, German Cancer Research Center, partner site Dresden (Author)
N. Paramasivam - , German Cancer Research Center (DKFZ), Heidelberg University (Author)
D. Richter - , National Center for Tumor Diseases (NCT) Dresden, University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ) (Author)
M. Fröhlich - , German Cancer Research Center (DKFZ), Heidelberg University (Author)
B. Hutter - , German Cancer Research Center (DKFZ), Heidelberg University (Author)
J. Hüllein - , German Cancer Research Center (DKFZ), Heidelberg University (Author)
A. Jahn - , Institute of Clinical Genetics, National Center for Tumor Diseases Dresden (NCT/UCC), University Hospital Carl Gustav Carus Dresden, Max Planck Institute of Molecular Cell Biology and Genetics (Author)
C. Scheffold - , University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ) (Author)
E. E. Möhrmann - , University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ) (Author)
D. Hanf - , National Center for Tumor Diseases Dresden (NCT/UCC), University Hospital Carl Gustav Carus Dresden (Author)
S. Kreutzfeldt - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
C. E. Heilig - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
M. V. Teleanu - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
D. B. Lipka - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
K. Beck - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
A. Baude-Müller - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
I. Jelas - , Charité – Universitätsmedizin Berlin (Author)
D. T. Rieke - , Charité – Universitätsmedizin Berlin (Author)
L. V. Klotz - , Heidelberg University (Author)
R. Shah - , Heidelberg University (Author)
T. Herold - , Ludwig Maximilian University of Munich (Author)
M. Boerries - , University Medical Center Freiburg (Author)
A. L. Illert - , University Medical Center Freiburg, Technical University of Munich (Author)
M. Allgäuer - , Heidelberg University (Author)
A. Stenzinger - , Heidelberg University (Author)
I. A. Kerle - , National Center for Tumor Diseases Dresden, University Hospital Carl Gustav Carus Dresden (Author)
P. Horak - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
C. Heining - , National Center for Tumor Diseases Dresden, University Hospital Carl Gustav Carus Dresden (Author)
E. Schröck - , Institute of Clinical Genetics, National Center for Tumor Diseases Dresden (NCT/UCC), University Hospital Carl Gustav Carus Dresden, Max Planck Institute of Molecular Cell Biology and Genetics (Author)
D. Hübschmann - , German Cancer Research Center (DKFZ), Heidelberg University , Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) (Author)
S. Fröhling - , Heidelberg University , German Cancer Research Center (DKFZ) (Author)
H. Glimm - , National Center for Tumor Diseases Dresden, University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ) (Author)

German Cancer Consortium (DKTK) Partner Site Dresden

Abstract

INTRODUCTION: Peritoneal, pericardial and pleural mesothelioma (PeM/PcM/PM) are rare and aggressive diseases with limited survival. Molecularly guided therapy is currently not part of standard care.

METHODS: This study integrates molecular and clinical data from 51 patients (among them 28 PM, one PcM, 21 PeM and one synchronous PeM/PM) enrolled in the National Center for Tumor Diseases and the German Cancer Consortium (NCT/DKTK) Molecularly Aided Stratification for Tumor Eradication Research (MASTER), a multicenter precision oncology registry trial addressing adults with rare advanced-stage cancers. Analysis comprised both somatic and germline whole exome sequencing/whole genome sequencing and transcriptome analysis leading to personalized treatment recommendations issued by a dedicated molecular tumor board. To assess clinical efficacy, progression-free survival (PFS) ratios comparing molecularly informed therapies (PFS2) to preceding systemic therapies (PFS1) were calculated. Efficacy of immune checkpoint inhibition applied during the observation period was assessed accordingly.

RESULTS: Cancer-related genes altered in more than 5 out of 44 assessable patients were BAP1, CDKN2A, NF2, SETD2 and TP53. Somatic (n = 23) or germline (n = 9) alterations in homologous recombination-related genes were detected in 27/44 patients. In 21/44 cases, they were supported by positive combined homologous recombination deficiency scores or BRCAness signature. Following American College of Medical Genetics and Genomics guidelines, (likely) pathogenic germline variants in autosomal dominant cancer predisposition genes were found in 8/51 patients. Molecular tumor board recommendations were issued in 46 cases and applied in 6 cases. Mean PFS ratio was 2.45 (n = 5). Median PFS2 was 6.5 months (n = 6), median PFS1 was 4.0 months (n = 5). A total of 27 patients received immune checkpoint inhibition during the observation period leading to a mean PFS ratio of 1.69 (n = 19).

CONCLUSIONS: In mesothelioma, comprehensive molecular analysis can provide valuable clinically actionable information. Molecularly informed therapy recommendations can lead to clinical benefit.

Details

Original language	English
Article number	104532
Number of pages	12
Journal	ESMO open
Volume	10 (2025)
Issue number	4
Publication status	Published - 1 Apr 2025
Peer-reviewed	Yes

External IDs

PubMedCentral	PMC11999262
Scopus	105001368505
ORCID	/0009-0003-2782-8190/work/198593805

Keywords

Sustainable Development Goals

SDG 3 - Good Health and Well-being

ASJC Scopus subject areas

Oncology
Cancer Research

Keywords

Key words: precision oncology, homologous repair deficiency, peritoneal mesothelioma, pleural mesothelioma, targeted therapy

Research Portal of the TU Dresden

Contributors

Abstract

Details

External IDs

Keywords

Sustainable Development Goals

ASJC Scopus subject areas

Keywords