Assessment of compartment-specific CD103-positive cells for prognosis prediction of colorectal cancer.

BACKGROUND

CD103 tissue-resident memory T cells was detected in various solid malignancies, like colorectal cancer (CRC), and associated with improved survival. However, clinical significance of CD103 cells in specific intratumor compartment remains unclear.

METHODS

The abundance and distribution of CD103 cells were assessed using immunohistochemistry and quantified separately for 3 compartments, including intraepithelial compartments at center of tumor (CT-IEL), stromal compartments at center of tumor (CT-ST) and invasive margin (IM) in a cohort of 224 CRC patients under radical surgery and correlated with outcome. Findings in each compartment were then validated in an external validation cohort comprising 294 CRC patients.

RESULTS

Elevated density of CD103 cells infiltration in the CT-IEL, CT-ST or IM compartment was correlated with favorable survival in both the initial discovery cohort and subsequent validation cohort. Notably, abundant CD103 cells located in the CT-IEL compartment was remained an independent prognostic indicator for CRC patients by multivariant analysis. Characterization study showed that intraepithelial CD103 cells were predominantly single positive CD8 T cells. Conversely, CD103 cells exhibited a heterogeneous population comprising CD103CD8 cells, CD103CD4 cells, and nonconventional CD103CD4CD8 cells in the CT-ST and IM compartments. Finally, a CD103 score was generated comprising abundance of CD103 cells in the 3 compartments. This score had the highest relative contribution to the risk of all clinical parameters for prognosis in both cohorts.

CONCLUSION

This study supported a phenotypic heterogeneity of CD103 cells in CRC, and provided a reliable estimate of the risk of death and recurrence in CRC patients based on combined analysis of CD103 cells within 3 intratumor compartments.