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"Köpfe" der aktuellen Meldungen:

Theresa Helena Benezeder

Andrea Renate Teufelberger

Natascha Berger

Bettina Amtmann

Katharina Artinger

Martina Kollmann

Natalie Bordag

Ursula Hiden

Isabella Perchthaler

Regina Roller-Wirnsberger

Johannes Nikolaus Woltsche

Mahmoud Abdellatif

Christoph Suppan

Clemens Painsi

Alexander Mahnert

Amin El-Heliebi

Martin Hönigl

Robert Sucher

Harald Sourij

Simon Sedej

Michael Khalil

Christian Enzinger

Wolfgang Weger

Slave Trajanoski

Philipp Metnitz

Peter Wolf

Gewählte Publikation:

SHR Neuro Krebs Kardio Lipid Stoffw Microb

Rousseau, B; Patel, M; Artz, O; Vlachos, G; Patel, S; Hayatt, O; Argilés, G; Foote, MB; Luo, L; Shah, R; Mehta, S; Rangavajhula, K; Stewart, CM; Gerber, D; Bhattacharya, R; Stephens, D; Mieles, D; Randrian, V; Abdelfattah, S; Zhang, L; Membreno-Berganza, N; Lamendola-Essel, MF; Piastra-Facon, F; Vidal, J; Johannet, P; Lu, S; White, JR; Maron, SB; Barlas, A; Weipert, CM; Rosiek, E; Zhang, T; He, B; Monette, S; Qu, R; Fidele, D; Bowker, S; Kahn, A; Vitiello, PP; Germano, G; Bardelli, A; Mandal, R; Ma, X; Chan, TA; Lu, S; Cercek, A; Abdel-Wahab, O; de, Stanchina, E; Segal, NH; Diaz, LA.
Induction of a mismatch repair deficient genotype by tailored chemical mutagenesis in experimental models of cancer.
Cancer Cell. 2025; Doi: 10.1016/j.ccell.2025.05.010
PubMed FullText FullText_MUG

 

Co-Autor*innen der Med Uni Graz

Vlachos Georgios

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Abstract:

Mismatch repair deficient (MMRd) tumors harbor thousands of somatic mutations enriched for insertion-deletion (indels) conferring high sensitivity to immunotherapy. We sought to reproduce this phenotype using mutagenic agents to engineer an MMRd genotype in immunoresistant cells. The combination of temozolomide (TMZ) and cisplatin led to a rapid accumulation of a high mutational load enriched for indels in murine cell lines resulting from the epigenetic loss of Msh2. Pretreated cells showed sensitivity to PD-1 blockade. Systemic treatment with TMZ, cisplatin, and anti-PD-1 bearing immunoresistant tumor cells led to increased survival, intratumoral T cell infiltration, and downregulation of Msh2 expression without affecting healthy tissues. In a clinical trial with 18 patients with refractory mismatch repair proficient colorectal cancer, no responses were seen, but MMRd signatures emerged in cell-free DNA. These findings show that recapitulating an MMRd genotype through chemical mutagenesis can generate an immunogenic phenotype.

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