Mutational Analysis of Gene Fusions Predicts Novel MHC Class I–Restricted T-Cell Epitopes and Immune Signatures in a Subset of Prostate Cancer

Kalina, Jennifer L.; Neilson, David S.; Lin, Yen-Yi; Hamilton, Phineas T.; Comber, Alexandra P.; Loy, Emma M.H.; Şahinalp, S. Cenk; Hach, Faraz; Lum, Julian J.

doi:10.1158/1078-0432.ccr-17-0618

Cited by 16 publications

(12 citation statements)

References 43 publications

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“…4 At fusion level, it has been postulated that TMPRSS2:ERG fusions generate chimeric amino acid sequences that are targetable by T cells. 10 Prediction algorithms have been used to identify potentially antigenic epitopes from TMPRSS2:ERG fusions. 11 Herein, we studied the relationship between immune cell infiltration and mutations in prostate cancer by using an integrative approach combining image analysis and DNA and RNA sequencing.…”

mentioning

confidence: 99%

Detailed Molecular and Immune Marker Profiling of Archival Prostate Cancer Samples Reveals an Inverse Association between TMPRSS2:ERG Fusion Status and Immune Cell Infiltration

Rao

Alham

Upton

et al. 2020

The Journal of Molecular Diagnostics

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Prostate cancer is a major global health issue and the second most common cause of cancer death in males in the developing world. 1 Better methods for patient stratification are urgently needed.Our understanding of the molecular pathology of prostate cancer is evolving fast, with advances in sequencing methods and bioinformatics. The Cancer Genome Atlas performed detailed molecular analysis on 333 primary prostate J.R. and C.V. contributed equally to this work.

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mentioning

confidence: 99%

Detailed Molecular and Immune Marker Profiling of Archival Prostate Cancer Samples Reveals an Inverse Association between TMPRSS2:ERG Fusion Status and Immune Cell Infiltration

Rao

Alham

Upton

et al. 2020

The Journal of Molecular Diagnostics

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“…Finally, gene fusions in prostate cancer can result in the formation of unique chimeric amino acid sequences that span the breakpoint of the two fused gene products and potentially generating fusion proteins with neoepitopes. In a recent computational study, type VI TMPRSS2-ERG gene fusions contained high-affinity HLA-restricted epitopes and were recognized by CD8+ T-cells in vitro ( 54 ). Though these mechanistic possibilities are intriguing, it is also possible that the association of higher lymphocyte densities with ERG rearrangement is due to a confounding additional molecular alteration, which is itself associated with ERG fusion.…”

Section: Discussionmentioning

confidence: 99%

Association of tumor-infiltrating T-cell density with molecular subtype, racial ancestry and clinical outcomes in prostate cancer

Kaur

Guedes

et al. 2018

Modern Pathology

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The inflammatory microenvironment plays an important role in the pathogenesis and progression of tumors and may be associated with somatic genomic alterations. We examined the association of tumor infiltrating T-cell density with clinical-pathologic variables, tumor molecular subtype and oncologic outcomes in surgically-treated primary prostate cancer occurring in patients of European-American or African-American ancestry. We evaluated 312 primary prostate tumors, enriched for patients with African-American ancestry and high grade disease. Tissue microarrays were immunostained for CD3, CD8 and FOXP3 and were previously immunostained for ERG and PTEN using genetically validated protocols. Image analysis for quantification of T-cell density in tissue microarray tumor spots was performed. Automated quantification of T-cell densities in tumor-containing regions of tissue microarray spots and standard histologic sections were correlated (r=0.73, p<0.00001) and there was good agreement between visual and automated T-cell density counts on tissue microarray spots (r=0.93, p<0.00001). There was a significant correlation between CD3+, CD8+ and FOXP3+ T-cell densities (p<0.00001), but these were not associated with most clinical or pathologic variables. Increased T-cell density was significantly associated with ERG positivity (median 309 vs 188 CD3+ T-cells/mm2; p=0.0004) and also with PTEN loss (median 317 vs 192 CD3+ T-cells/mm2; p=0.001) in the combined cohort of matched European-American and African-American ancestry patients. The same association or a similar trend was present in patients of both ancestries when analyzed separately. When the African-American patients from the matched race set were combined with a separate high grade set of African-American cases, there was a weak association of increased FOXP3+ T-cell densities with increased risk of metastasis in multivariable analysis. Though high T-cell density is associated with specific molecular subclasses of prostate cancer, we did not find an association of T-cell density with racial ancestry.

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“…This finding suggests that the Tmprss2-Erg fusion promotes recruitment of regulatory T cells to the tumor site [50]. Recent studies have shown an association between low levels of TILs comparing TMPRSS2-ERG fusions producing chimeric transcripts in the coding in the fusion-positive cases results in suppression of immune response by alteration of cytokine production [51,52].…”

Section: Phosphatase and Tensin Homologue (Pten)mentioning

confidence: 94%

The Role of Somatic Mutations on the Immune Response of the Tumor Microenvironment in Prostate Cancer

Melo

Vidotto

Chaves

et al. 2021

IJMS

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Immunotherapy has improved patient survival in many types of cancer, but for prostate cancer, initial results with immunotherapy have been disappointing. Prostate cancer is considered an immunologically excluded or cold tumor, unable to generate an effective T-cell response against cancer cells. However, a small but significant percentage of patients do respond to immunotherapy, suggesting that some specific molecular subtypes of this tumor may have a better response to checkpoint inhibitors. Recent findings suggest that, in addition to their function as cancer genes, somatic mutations of PTEN, TP53, RB1, CDK12, and DNA repair, or specific activation of regulatory pathways, such as ETS or MYC, may also facilitate immune evasion of the host response against cancer. This review presents an update of recent discoveries about the role that the common somatic mutations can play in changing the tumor microenvironment and immune response against prostate cancer. We describe how detailed molecular genetic analyses of the tumor microenvironment of prostate cancer using mouse models and human tumors are providing new insights into the cell types and pathways mediating immune responses. These analyses are helping researchers to design drug combinations that are more likely to target the molecular and immunological pathways that underlie treatment failure.

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Mutational Analysis of Gene Fusions Predicts Novel MHC Class I–Restricted T-Cell Epitopes and Immune Signatures in a Subset of Prostate Cancer

Cited by 16 publications

References 43 publications

Detailed Molecular and Immune Marker Profiling of Archival Prostate Cancer Samples Reveals an Inverse Association between TMPRSS2:ERG Fusion Status and Immune Cell Infiltration

Detailed Molecular and Immune Marker Profiling of Archival Prostate Cancer Samples Reveals an Inverse Association between TMPRSS2:ERG Fusion Status and Immune Cell Infiltration

Association of tumor-infiltrating T-cell density with molecular subtype, racial ancestry and clinical outcomes in prostate cancer

The Role of Somatic Mutations on the Immune Response of the Tumor Microenvironment in Prostate Cancer

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