Dissecting intratumor heterogeneity of nodal B cell lymphomas on the transcriptional, genetic, and drug response level

Author:

Roider TobiasORCID,Seufert Julian,Uvarovskii Alexey,Frauhammer Felix,Bordas Marie,Abedpour Nima,Stolarczyk Marta,Mallm Jan-Philipp,Rabe Sophie,Bruch Peter-Martin,Balke-Want Hyatt,Hundemer Michael,Rippe Karsten,Goeppert Benjamin,Seiffert Martina,Brors Benedikt,Mechtersheimer Gunhild,Zenz Thorsten,Peifer Martin,Chapuy Björn,Schlesner MatthiasORCID,Müller-Tidow Carsten,Fröhling Stefan,Huber WolfgangORCID,Anders SimonORCID,Dietrich SaschaORCID

Abstract

AbstractTumor heterogeneity encompasses both the malignant cells and their microenvironment. While heterogeneity between individual patients is well-known to affect the efficacy of anti-cancer drugs, most personalized treatment approaches do not account for intratumor heterogeneity. We addressed this issue by studying the heterogeneity of lymph node-derived B cell non-Hodgkin lymphoma (B-NHL) by single cell RNA-sequencing (scRNA-seq) and transcriptome-informed flow cytometry. We identified transcriptionally distinct malignant subclones and compared their drug response and genomic profiles. Malignant subclones of the same patient responded strikingly different to anti-cancer drugs ex vivo, which recapitulated subclone-specific drug sensitivity during in vivo treatment. Tumor infiltrating T cells represented the majority of non-malignant cells, whose gene expression signatures were similar across all donors, whereas the frequencies of T cell subsets varied significantly between the donors. Our data provide new insights into the heterogeneity of B-NHL and highlight the relevance of intratumor heterogeneity for personalized cancer therapies.

Publisher

Cold Spring Harbor Laboratory

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