Distinct Infiltration of T Cell Populations in Bladder Cancer Molecular Subtypes

Author:

Sincic Viktor12,Arlenhold Ken F.12,Richtmann Sarah12ORCID,Lilljebjörn Henrik3,Eriksson Pontus4,Sjödahl Gottfrid5ORCID,Wokander Mats6,Hägerbrand Karin7,Ellmark Peter17ORCID,Fioretos Thoas38,Borrebaeck Carl A. K.12,Liedberg Fredrik56,Lundberg Kristina12ORCID

Affiliation:

1. Department of Immunotechnology, Lund University, 223 81 Lund, Sweden

2. CREATE Health Cancer Center, Lund University, 223 81 Lund, Sweden

3. Division of Clinical Genetics, Department of Laboratory Medicine, Lund University, 221 84 Lund, Sweden

4. Division of Oncology, Department of Clinical Sciences Lund, Lund University, 221 84 Lund, Sweden

5. Department of Translational Medicine, Lund University, 205 02 Malmö, Sweden

6. Department of Urology, Skåne University Hospital, 205 02 Malmö, Sweden

7. Alligator Bioscience AB, Medicon Village, 223 63 Lund, Sweden

8. Department of Clinical Genetics, University and Regional Laboratories Region Skåne, 221 85 Lund, Sweden

Abstract

Bladder cancer is a heterogenous disease, and molecular subtyping is a promising method to capture this variability. Currently, the immune compartment in relation to subtypes is poorly characterized. Here, we analyzed the immune compartment in bladder tumors and normal bladder urothelium with a focus on T cell subpopulations using flow cytometry and RNA sequencing. The results were investigated in relation to tumor invasiveness (NMIBC/MIBC) and molecular subtypes according to the Lund Taxonomy system. Whereas the NMIBC/MIBC differed in the overall immune infiltration only, the molecular subtypes differed both in terms of immune infiltration and immune compartment compositions. The Basal/Squamous (Ba/Sq) and genomically unstable (GU) tumors displayed increased immune infiltration compared to urothelial-like (Uro) tumors. Additionally, the GU tumors had a higher proportion of regulatory T cells within the immune compartment compared to Uro tumors. Furthermore, sequencing showed higher levels of exhaustion in CD8+ T cells from GU tumors compared to both Uro tumors and the control. Although no such difference was detected at the transcriptomic level in Uro tumors compared to the controls, CD8+ T cells in Uro tumors showed higher expression of several exhaustion markers at the protein level. Taken together, our findings indicate that depending on the molecular subtype, different immunotherapeutic interventions might be warranted.

Funder

Cancera Foundation, Gunnar Nilssons Cancerstiftelse

Mats Paulsson Foundation

Stefan Paulsson Foundation

Per-Erik och Ulla Schybergs stiftelse/Royal Physiographic Society of Lund

ISREC Foundation

Faculty of Engineering at Lund University

Marie Skłodowska-Curie grant agreement

Swedish Cancer Society

Swedish Research Council

Lund Medical Faculty (ALF), Skåne University Hospital Research Funds

Cancer Research Fund at Malmö General Hospital

Hjelm Family Foundation for Medical Research

Gösta Jönsson Research Foundation

Foundation of Urological Research

Hillevi Fries Research Foundation

Publisher

MDPI AG

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