Abstract
Background
The T cell cytokine profile is a key prognostic indicator of post-surgical outcome for colorectal cancer (CRC). Whilst TH1 (IFN-γ+) cell-mediated responses generated in CRC are well documented and are associated with improved survival, antigen-specific TH17 (IL-17A+) responses have not been similarly measured.
Methods
We sought to determine the cytokine profile of circulating tumour antigen-(5T4/CEA) specific T cells of 34 CRC patients to address whether antigen-specific IL-17A responses were detectable and whether these were distinct to IFN-γ responses.
Results
As with IFN-γ-producing T cells, anti-5T4/CEA TH17 responses were detectable predominantly in early stage (TNM I/II) CRC patients. Moreover, whilst IL-17A was always produced in association with IFN-γ, this release was mainly from two distinct T cell populations rather than by ‘dual producing’ T cells. Patients mounting both tumour-specific TH1+/TH17+ responses exhibited prolonged relapse-free survival.
Conclusions
Tumour antigen-specific TH17 responses play a beneficial role in preventing post-operative colorectal tumour recurrence.
Subject terms: Tumour immunology, Colorectal cancer
Background
The adaptive immune system plays a critical role in the control of colorectal cancer (CRC). Our previous work identified that the presence of pre-operative circulating TH1 responses specific for 5T4, an oncofoetal antigen not expressed in healthy adult tissue, has a positive association with post-operative relapse-free survival,1 in keeping with studies demonstrating that tumour infiltration of TH1-type (IFN-γ-producing) T cells associate with favourable outcome.2 Unexpectedly, the presence of TH1 responses directed towards carcinoembryonic antigen (CEA), an auto-antigen expressed at low levels in normal intestinal epithelium, associated with poor relapse-free survival in CRC patients.1 Whilst both CEA and 5T4 are upregulated in the majority of colorectal tumours, there is a potential that tumour-selective T cell responses impact clinical outcome differently to auto-antigen T cell responses.3
Since TH1 responses are usually associated with control of cancer progression, we postulated that CEA-specific IFN-γ-producing T cells were not the cause of the observed association with poor survival, but a surrogate marker for skewed tumour-specific T cell functionality. In particular, tumour-infiltrating TH17 cells have previously been associated with CRC progression.2 IL-17A itself has been implicated in tumour progression through STAT3 activation, promoting colonic epithelial cell transformation, tumour cell proliferation and invasion.4 Contrastingly, the presence of colorectal tumour-infiltrating TH17 cells was recently reported to correlate with improved survival,5 implying that IL-17A has important context and tissue-dependent roles in enacting pro- or anti-tumour immune mechanisms.6
This current study was designed to identify the presence of CEA-specific and 5T4-specific IL-17A- and IFN-γ-producing T cells within the blood of CRC patients and healthy controls and investigate their role on post-operative outcome and colonic epithelial barrier function.
Methods
Participants
Blood and colon samples were obtained from 34 patients undergoing colorectal cancer resection or investigative colonoscopy procedures at the University Hospital of Wales, Cardiff. Patient characteristics are summarised (Supplementary Table 1). Additional blood samples were obtained from age-matched healthy donors (age range 48–62; 5 male, 4 female). All participants gave written, informed consent personally prior to inclusion. The Wales Research Ethics Committee granted ethical approval for this study.
Antigens
The CEA protein was split into seventy 20mer peptides and 5T4 split into forty-one 20mers, each overlapping by 10 amino acids and synthesised to >90% purity (GLBiochem, Shanghai, China). Peptides were dissolved in minimal DMSO and incorporated into peptide pools, used at a final concentration of 1.45 μg/ml/peptide. Phytohaemagglutinin (PHA; Sigma Aldrich) was used as a positive control.
Peripheral blood mononuclear cell (PBMC) extraction and culture
PBMCs were extracted from whole blood as previously described.1 5 × 105 PBMCs were seeded per well in a 96-well plate in 100 μl R+ media supplemented with 5% human AB serum (Welsh Blood Service, Pontyclun, UK), 2 mM L-glutamine, 1 mM sodium pyruvate and 50 μg/ml penicillin/streptomycin (Gibco, Paisley, UK). PBMC lines were cultured for 14 days in the presence or absence of peptide pool, supplemented with 10 μl CellKine (purified T cell growth factors derived from pooled PHA-stimulated T cells; Helvetica Healthcare, Geneva, Switzerland), on day 3 and fresh media containing 40 IU/ml IL-2 on days 6 and 9.
FluoroSpot assays
The human IFN-γ/IL-17A FluoroSpot kit (MabTech, Sweden) was used and performed according to the manufacturer’s instructions. Duplicate lines of cultured PBMCs were pooled together, washed and plated at 5 × 105 cells/well with or without the corresponding peptide pool for direct comparison. FluoroSpot plates were incubated at 37 °C, 5% CO2 for 48 h. In some instances, blocking antibodies to MHC class-I (anti-HLA-A/B/B (W6/32); BioLegend, UK) and MHC class-II (anti-HLA-DR (L243); anti-HLA-DQ (1A3); BioLegend) were added at a final concentration of 10 μg/ml, incubated for 30 min before addition of antigen. Cytokine-producing PBMCs were enumerated using an automated FluoroSpot reader (CTL, Germany). Dual cytokine-secreting cells were visualised and enumerated by a computerised overlay. Positive IFN-γ and IL-17A responses were identified by a minimum of 10 and 5 spot-forming cells (SFC) per 1 × 105 cultured PBMC, respectively, and a minimum 2-fold increase above background.
Intestinal permeability measurements
Electrophysiological resistance and paracellular flux in human colonic biopsies was measured using an Ussing chamber, as previously described.7 Readouts of intestinal permeability were associated with the presence of IFN-γ and IL-17A CEA- and 5T4-specific T cell responses, with patients differentiated based on the median magnitude of response generated to each antigen.
Statistical analysis
GraphPad Prism (v.8) was used for all statistical analyses. Dataset normality was tested using the Shapiro-Wilk test. Significance was determined using one-way ANOVA with corrections for multiple comparisons made using the Tukey test; a P-value < 0.05 was considered significant. For survival analyses using Kaplan–Meier curves, relapse-free survival was calculated from the date of surgery to the date of relapse, as determined by follow-up CT scan and/or endoscopy. Non-relapsing patients were censored at the time of last follow-up assessment (September 2019). Survival curves were compared using the log-rank test.
Results
CEA-specific and 5T4-specific IFN-γ, IL-17A and IFN-γ/IL-17A dual-secreting T cell responses from pre-operative CRC patient and age-matched healthy donor PBMC were investigated. Culturing PBMC for 14 days in the presence of a particular cytokine cocktail was necessary to expand low frequency antigen-specific TH17 responses to detectable levels (Supplementary Fig. 1A). Whilst TH17 responses were identified, IFN-γ/IL-17A dual secretion from the same cell was rarely detected; example FluoroSpot well images and results are shown for CEA and 5T4 (Supplementary Fig. 1B). CEA- and 5T4-specific TH1 and TH17 cell responses were readily identifiable amongst healthy donors and cancer patients (Supplementary Fig. 1C); these responses were predominantly MHC class II-restricted (Supplementary Fig. 1D). The proportion of cancer patients mounting detectable CEA-specific IFN-γ T cell responses diminished in comparison to healthy age-matched controls (Fig. 1a) and further declined as the tumour became more advanced (Fig. 1b). No overall change in CEA-specific IL-17A production was noted between healthy donors and CRC patients (Fig. 1c).
Fig. 1. CEA- and 5T4-specific TH1/TH17 responses prevent colorectal tumour recurrence.
a The percentage of donors mounting a CEA-specific IFN-γ response (dark grey), a dual CEA-specific IFN-γ and IL-17A response (light grey), or no positive CEA-specific response (black), as indicated by results from the IFN-γ/IL-17A FluoroSpot assay. The magnitude of CEA-specific T cell response, normalised to spot-forming cells (SFC)/105 cultured PBMC, and associated with healthy donor (HD) or early-stage (TNM I/II) or late-stage (TNM III) CRC is shown for IFN-γ (b) and IL-17A (c). Error bars indicate median with interquartile range. d The percentage of donors mounting a 5T4-specific IFN-γ response (dark grey), a dual 5T4-specific IFN-γ and IL-17A response (light grey), or no positive 5T4-specific response (black), as indicated by results from the IFN-γ/IL-17A FluoroSpot assay. The magnitude of 5T4-specific T cell response, normalised to spot-forming cells (SFC)/105 cultured PBMC, and associated with healthy donor (HD) or early-stage (TNM I/II) or late-stage (TNM III) CRC is shown for IFN-γ (e) and IL-17A (f). Error bars indicate median with interquartile range. The CEA-specific (g) or 5T4-specific (h) TH1/TH17 response measured in all CRC patients (n = 34) was associated with relapse-free survival.
Similarly, 5T4-specific TH1 responses significantly declined as the colorectal tumour advanced (HD v III, P = 0.033; I/II v III, P = 0.031; Fig. 1d, e), validating previous findings with 5T41,8 and other widely-expressed upregulated tumour antigens.9 5T4-specific TH17 responses were rarely detectable in healthy donors, and only significantly increased in earlier stage CRC patients (P = 0.036, Fig. 1f).
The prognostic impact of pre-operative CEA and 5T4-specific TH1 and TH17 responses was determined by associating responses with 5-year relapse-free survival. Patients were separated based on whether they mounted both an IFN-γ and IL-17A response or not to CEA (Fig. 1g) and 5T4 (Fig. 1h); one patient that mounted an anti-5T4 IL-17A response only was included as a non-responder. Although the size of the groups did not allow statistical significance to be reached, it is clear that in both cases the most favourable immune profile pre-operatively for prolonged disease-free survival is the presence of both TH1 and TH17 responses (Fig. 1g, h).
From this data we conclude that release of IL-17A by CEA-specific T cells is not responsible for the poorer survival of patients with IFN-γ-producing CEA (but not 5T4)-specific T cells. Unlike 5T4, CEA is expressed at low levels in normal epithelium. A higher magnitude of IFN-γ+ CEA-specific T cell response, i.e. above the median of all anti-CEA responses tested in patients undergoing endoscopy (Supplementary Fig. 2A, B), was associated with decreased electrical resistance in ascending colonic epithelium (P = 0.037; Supplementary Fig. 2C) and increased paracellular passage (i.e. leak) of Lucifer yellow probe (P = 0.11; Supplementary Fig. 2D), implying that the integrity of the epithelial barrier is subtly compromised in patients with relatively high CEA TH1 response, a finding not replicated when separating responses based on IL-17A+ CEA responders, nor 5T4 responders from non-responders. This observation, specific to the right-sided ascending colonic epithelium, is worthy of further investigation.
Discussion
Mounting pre-operative tumour antigen-specific TH17 and TH1 combined responses appears to be associated with less post-operative CRC relapse. Despite the relatively small sample size, there is a clear indication that IL-17A production by tumour antigen-specific T cells has a positive influence on anti-tumour immunity, warranting further investigation. In particular, the emergence of 5T4-specific TH17 response is indicative of early stage CRC and may provide diagnostic/prognostic information. This study also highlights the possibility for detrimental clinical outcomes when using IL-17/TH17-targeted treatments; indeed it has been suggested that clinical response to anti-PD-1 may be reliant on TH17 responses and treatment success is compromised by IL-17A blockade.6,10,11
We have previously shown an adverse effects of ex vivo measured anti-CEA TH1 responses on post-operative CRC patient outcome.1 In this previous study, we did not measure IL-17A responses, which require a period of in vitro culture and expansion. This study, albeit on smaller patient numbers, strongly suggests that TH17 responses are beneficial when combined with TH1 responses. It is possible that an IFN-γ-driven chronic, sub-clinical enteropathy which facilitates tumorigenesis is reversed or alleviated by IL-17A production.
In conclusion, tumour antigen-specific TH17 responses play a beneficial role in preventing colorectal tumour recurrence after surgical resection.
Supplementary information
Acknowledgements
We thank Mr. Simon Phillips, Mr. Michael Davies, Ms. Rachel Hargest, Mr. Leigh Davies and Mr. James Horwood for provision of CRC patient bloods. We thank Dr. Tom Pembroke, Dr. Gautham Appanna, Dr. Lawrence Sunder Raj, Dr. Brijesh Srivastava and Dr. Dharmaraj Durai for provision of patient blood samples and colonic epithelial biopsies from endoscopy patients.
Author contributions
An.G. and Aw.G. conceived, designed and were the principal investigators of this study; A.T. and D.F.C.B. recruited the cohorts. A.T., D.F.C.B. and K.S. performed the immunological assays; A.T., K.S. and Mi.S. performed the Ussing chamber experiments; A.T. and D.F.C.B. performed data management, A.T., D.F.C.B. and M.J.S. interpreted the data and performed statistical analyses. A.T., M.J.S. and Aw.G. wrote the original draft of the paper. A.T., D.F.C.B., M.J.S., K.S., Mi.S., Aw.G. and An.G. reviewed and/or edited the paper.
Ethics approval and consent to participate
All patients and healthy donors gave their signed informed consent, and the protocol was approved by the Wales Research Ethics Committee (reference:15/WA/0291). The study was conducted in accordance with the Declaration of Helsinki.
Consent to publish
Not applicable.
Data availability
The datasets generated during this study are available from the corresponding author on reasonable request.
Competing interests
The authors declare no competing interests.
Funding information
This work was supported by Cancer Research Wales and a Cancer Research UK programme grant (C16731/A21200).
Footnotes
Publisher’s note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
These authors contributed equally: Amanda Thomson, Diana F. Costa Bento, Martin J. Scurr
These authors contributed equally: Awen Gallimore, Andrew Godkin
Supplementary information
The online version contains supplementary material available at 10.1038/s41416-021-01283-3.
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Associated Data
This section collects any data citations, data availability statements, or supplementary materials included in this article.
Supplementary Materials
Data Availability Statement
The datasets generated during this study are available from the corresponding author on reasonable request.