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Poster session 10

573P - Multiparameter immunoprofiling reveals independent prognostic value of intraepithelial CD8 and intrastromal FoxP3 infiltrate in stage II/III colorectal cancer: Analysis of 3,409 cases from the SCOT and QUASAR2 trials

Date

21 Oct 2023

Session

Poster session 10

Topics

Tumour Immunology;  Translational Research

Tumour Site

Colon and Rectal Cancer

Presenters

David Church

Citation

Annals of Oncology (2023) 34 (suppl_2): S410-S457. 10.1016/S0923-7534(23)01935-X

Authors

A. Frei1, A. McGuigan2, R. Sinha2, A. Harkin3, T.J. Iveson4, M.P. Saunders5, J. Hay6, J. Edwards7, O.J. Sansom8, C. Kelly9, R. kerr10, D.J. Kerr10, E. Domingo11, V.H. Koelzer12

Author affiliations

  • 1 Pathology And Molecular Pathology, USZ - University Hospital Zurich - Institute of Pathology, 8091 - Zurich/CH
  • 2 Nuffield Department Of Medicine, University of Oxford - Nuffield Department of Medicine, OX3 7BN - Oxford/GB
  • 3 Cancer Research Uk Clinical Trials Unit, BWSCC - Beatson West of Scotland Cancer Centre - NHS Greater Glasgow and Clyde, G12 0YN - Glasgow/GB
  • 4 Medical Oncology, Southampton General Hospital, SO16 6YD - Southampton/GB
  • 5 Clinical Oncology Department, The Christie NHS Foundation Trust, M20 4BX - Manchester/GB
  • 6 Queen Elizabeth University Hospital, Govan Road, University of Glasgow, G12 8QQ - Glasgow/GB
  • 7 School Of Cancer Sciences, University of Glasgow, G12 8QQ - Glasgow/GB
  • 8 Institute Cancers Sciences, CRUK - Cancer Research UK Beatson Institute, G61 1BD - Glasgow/GB
  • 9 Clinical Trials, University of Glasgow, G12 8QQ - Glasgow/GB
  • 10 Medical Oncology, Churchill Hospital, OX3 7LE - Oxford/GB
  • 11 Department Of Oncology, University Of Oxford, University of Oxford, Oxford/GB
  • 12 Pathology, USZ - University Hospital Zurich - Institute of Pathology, 8091 - Zurich/CH

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Abstract 573P

Background

Tumour infiltrating CD8+ cytotoxic T cells confer favourable prognosis in colorectal cancer (CRC). The added prognostic value of other immune cells is unclear.

Methods

We used multiparameter co-immunofluorescence to determine the density of CD8+, CD20+, FoxP3+ and CD68+ cells in the intraepithelial (IE) and intrastromal (IS) compartments in stage II/III CRCs from the SCOT and QUASAR2 trials. We determined marker prognostic and predictive value by Cox regression of SCOT cases, with validation in the QUASAR2 cohort.

Results

Our study included 2,340 SCOT and 1,069 QUASAR2 cases. Univariable analysis of recurrence-free interval (RFI) in SCOT revealed expected prognostic value of intraepithelial CD8 (CD8IE) (continuous variable: HR for cases at 75th vs 25th percentile (HR75vs25)= 0.73, 95% CI=0.68-0.79, P=2.5e-16) and, less expectedly FoxP3 within tumour stroma (FoxP3IS) (HR75vs25)= 0.71, 95% CI=0.64-0.78, P=1.5e-13), but not epithelium. CD8IE and FoxP3IS were independently prognostic in multivariable analysis, and a composite marker including both (CD8IE-Foxp3IS) was superior to either alone as a continuous variable (adjHR75vs25= 0.70; 95%CI=0.63–0.78; P=5.1e-11), and when categorised into three groups (Low/Int/High) using sample medians (Int vs High HR = 1.60, 95%CI=1.24–2.05, P=2.5e-04; Low vs High HR = 2.30, 95%CI=1.80–2.95; P=3.6e-11). These results were validated in the QUASAR2 trial. Pooled analysis of both studies revealed interactions between CD8IE-FoxP3IS and tumour sidedness (adjP INT=0.010), stromal proportion (adjP INT=0.018), and MMR status (adjP INT=0.079). CD8IE-FoxP3IS refined stage III risk groups, with clinical low risk (T1-3, N1), CD8IE-FoxP3IS low cases demonstrating similar 3-year recurrence-free probability to clinical high risk (T4 and/or N2), CD8IE-FoxP3IS high cases (79.2 vs 76.4%, adj log-rank P=0.16).

Conclusions

Combined evaluation of CD8IE and FoxP3IS is superior to single markers and refines CRC risk stratification. FoxP3IS prognostic value is inconsistent with an immunosuppressive role; further investigation of these cells as an immunotherapy target is merited.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

D.N. Church.

Funding

Cancer Research UK, National Institutes for Health Research, Promedica Foundation.

Disclosure

All authors have declared no conflicts of interest.

Resources from the same session

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