High dose-rate brachytherapy of localized prostate cancer converts tumors from cold to hot
Preprint 2020 en
Authors
SK
Simon P. Keam
HH
Heloise M. Halse
TN
Thu Quynh Nguyen
Abstract
1 min read
Abstract Prostate cancer (PCa) has a profoundly immunosuppressive microenvironment, we hypothesized that radiation therapy would break this immune suppression. To investigate this, we performed high-throughput immune cell subset analysis, and gene expression profiling of pre-versus post-radiation tissue in a cohort of patients with localized disease that received high dose-rate brachytherapy (HDRBT). We resolved tumor and non-tumor zones in our spatial analysis to explore what drives the immunological response. Nanostring immune profiling revealed numerous immune checkpoint molecules were stimulated in response to HDRBT (e.g. B7-H3, CTLA4, PDL1 and PDL2). A published 16-gene tumor inflammation signature (TIS) gene profiling of immune activation states (high: hot , intermediate and low: cold ) showed that most tissues possessed a low TIS pre-HDRBT. Crucially, HDRBT converted 80% of these ‘cold’-phenotype tumors into an ‘intermediate’ or ‘hot’ class. We used digital spatial profiling to show these HDRBT-induced changes in prostate TIS scores were derived from the non-tumor regions. Furthermore, these changes in TIS were also associated with pervasive changes in immune cell density and spatial relationships – in particularly between T cell subsets and antigen presenting cells. We identified increased density of CD4 + FOXP3 + T cells, CD68 + macrophages and CD68 + CD11c + dendritic cells in response to HDRBT. The only subset change in tumor zones was PDL1 + macrophages. While these immune responses were heterogeneous, HDRBT induced significant changes in immune cell associations, including a gained T cell and HMWCK + PDL1 + interaction in tumor zones. In conclusion, we showed HDRBT has a clear impact in converting “cold” prostate tumors into more immunologically activated “hot” tissues, with accompanying spatially-organized immune infiltrates and signaling changes. Understanding and potentially harnessing these changes will have widespread implications for the future treatment of localized PCa and the possible use of combination immunotherapies.
Simon P. Keam, Heloise M. Halse, Thu Quynh Nguyen, Minyu Wang, Nicolas Van Kooten Losio, Catherine Mitchell, Franco Caramia, David J. Byrne, Sue Haupt, Georgina L. Ryland, Phillip K. Darcy, Shahneen Sandhu, Piers Blombery, Ygal Haupt, Scott Williams, Paul J. Neeson
Simon P. Keam, Heloise M. Halse, ThuNgoc Nguyen, Minyu Wang, Nicolas Van Kooten Losio, Catherine Mitchell, Franco Caramia, David J. Byrne, Sue Haupt, Georgina L. Ryland, Phillip K. Darcy, Shahneen Sandhu, Piers Blombery, Ygal Haupt, Scott Williams, Paul J. Neeson
Scott Williams, Simon P. Keam, Heloise M. Halse, Catherine Mitchell, Franco Caramia, David J. Byrne, Sue Haupt, Georgina L. Ryland, Phillip K. Darcy, Shahneen Sandhu, Piers Blombery, Ygal Haupt, Paul J. Neeson
Anna Trigos, Anupama Pasam, Patricia Banks, Roslyn Wallace, Christina Guo, Simon P. Keam, Heather Thorne, Catherine Mitchell, Stephen Lade, David Clouston, Alexander Hakansson, Yang Liu, Benjamin J. Blyth, Declan G. Murphy, Nathan Lawrentschuk, Damien Bolton, Daniel Moon, Phillip K. Darcy, Ygal Haupt, Scott Williams, Elena Castro, David Olmos, David L. Goode, ,
Simon P. Keam, Heloise M. Halse, ThuNgoc Nguyen, Catherine Mitchell, Franco Caramia, David J. Byrne, Sue Haupt, Georgina L. Ryland, Phillip K. Darcy, Shahneen Sandhu, Piers Blombery, Ygal Haupt, Scott Williams, Paul J. Neeson
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