Quantification and molecular correlates of tertiary lymphoid structures in primary prostate cancer

Author:

Shahait Mohammed1ORCID,Hakansson Alexander K.2,Daniel Reba E.3,Hosny Kareem3,Davicioni Elai2,Liu Seagle Yang2,Sandberg Alex4,Lee David I.5,Lal Priti3

Affiliation:

1. Department of Surgery Clemenceau Medical Center Dubai UAE

2. Veracyte Inc. South San Francisco California USA

3. Department of Pathology University of Pennsylvania Philadelphia Pennsylvania USA

4. Department of Surgery, Temple Medical School Temple University Philadelphia Pennsylvania USA

5. Department of Urology University of California Irvine Irvine California USA

Abstract

AbstractObjectiveTo morphologically describe tertiary lymphoid structures (TLS) in prostatectomy specimens and correlate them with clinical and transcriptomic features.MethodologyA total of 72 consecutive cases of entirely submitted radical prostatectomy (RP) patients tested with the Decipher Genomic Classifier were included in the study. Images were manually annotated using QuPath tools to denote tumor regions and each cluster of TLS. Clusters of lymphocytes that were surrounded on all four sides by tumor were defined as intra‐tumor TLS (IT‐TLS). Clusters of lymphocytes at the leading edge of carcinoma with either the prostatic pseudocapsule or benign parenchyma at one end were defined as peri‐tumor TLS (PT‐TLS). A classification algorithm to distinguish lymphocytes from non‐lymphocytic cells using a supervised machine learning model was used. The associations between TLS formation and 265 gene expression‐based signatures were examined.ResultsThe magnitude of total TLS correlations with primary tumor gene expression signatures was moderate (~0.35–0.5) with several HLA, T‐cell and B‐cell Cluster signatures, showing positive correlation with various metrics for quantification of TLS. On the other hand, immune suppressive signatures (Treg, MDSC) were negatively correlated. While signatures for macrophages, NK cells and other immune cell types were uncorrelated for the most part. PT‐TLS was associated with MHC signatures while IT TLS correlated with MHC and T‐cell signatures.ConclusionsClusters of inflammatory cells in the RP specimen can be divided spatially into PT TLS and IT‐TLS, each with its unique molecular correlates of tumor immune microenvironment. The presence of TLS is positively correlated with MHC signatures, T‐ cell and B‐cell cluster signatures but, negatively correlated with immune suppressive signatures. A subset of prostate cancer demonstrate a robust inflammatory response, and warrant further characterization in larger cohorts.

Publisher

Wiley

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