Activated tissue resident memory T-cells (CD8+CD103+CD39+) uniquely predict survival in left sided “immune-hot” colorectal cancers

INTRODUCTION: Characterization of the tumour immune infiltrate (notably CD8+ T-cells) has strong predictive survival value for cancer patients. Quantification of CD8 T-cells alone cannot determine antigenic experience, as not all infiltrating T-cells recognize tumour antigens. Activated tumour-speci...

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Detalles Bibliográficos
Autores principales: Talhouni, Shahd, Fadhil, Wakkas, Mongan, Nigel P., Field, Lara, Hunter, Kelly, Makhsous, Sogand, Maciel-Guerra, Alexandre, Kaur, Nayandeep, Nestarenkaite, Ausrine, Laurinavicius, Arvydas, Willcox, Benjamin E., Dottorini, Tania, Spendlove, Ian, Jackson, Andrew M., Ilyas, Mohammad, Ramage, Judith M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10213916/
https://www.ncbi.nlm.nih.gov/pubmed/37251410
http://dx.doi.org/10.3389/fimmu.2023.1057292
Descripción
Sumario:INTRODUCTION: Characterization of the tumour immune infiltrate (notably CD8+ T-cells) has strong predictive survival value for cancer patients. Quantification of CD8 T-cells alone cannot determine antigenic experience, as not all infiltrating T-cells recognize tumour antigens. Activated tumour-specific tissue resident memory CD8 T-cells (T(RM)) can be defined by the co-express of CD103, CD39 and CD8. We investigated the hypothesis that the abundance and localization of T(RM) provides a higher-resolution route to patient stratification. METHODS: A comprehensive series of 1000 colorectal cancer (CRC) were arrayed on a tissue microarray, with representative cores from three tumour locations and the adjacent normal mucosa. Using multiplex immunohistochemistry we quantified and determined the localization of T(RM). RESULTS: Across all patients, activated T(RM) were an independent predictor of survival, and superior to CD8 alone. Patients with the best survival had immune-hot tumours heavily infiltrated throughout with activated T(RM). Interestingly, differences between right- and left-sided tumours were apparent. In left-sided CRC, only the presence of activated T(RM) (and not CD8 alone) was prognostically significant. Patients with low numbers of activated T(RM) cells had a poor prognosis even with high CD8 T-cell infiltration. In contrast, in right-sided CRC, high CD8 T-cell infiltration with low numbers of activated T(RM) was a good prognosis. CONCLUSION: The presence of high intra-tumoural CD8 T-cells alone is not a predictor of survival in left-sided CRC and potentially risks under treatment of patients. Measuring both high tumour-associated T(RM) and total CD8 T-cells in left-sided disease has the potential to minimize current under-treatment of patients. The challenge will be to design immunotherapies, for left-sided CRC patients with high CD8 T-cells and low activate T(RM,)that result in effective immune responses and thereby improve patient survival.

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