Association between local immune cell infiltration, mismatch repair status and systemic inflammatory response in colorectal cancer

Ulf Gunnarsson; Karin Strigård; Sofia Edin; Ioannis Gkekas; Harri Mustonen; Tuomas Kaprio; Camilla Böckelman; Jaana Hagström; Richard Palmqvist; Caj Haglund

doi:10.1186/s12967-020-02336-6

Association between local immune cell infiltration, mismatch repair status and systemic inflammatory response in colorectal cancer

J Transl Med. 2020 Apr 21;18(1):178. doi: 10.1186/s12967-020-02336-6.

Authors

Ulf Gunnarsson¹, Karin Strigård², Sofia Edin³, Ioannis Gkekas², Harri Mustonen^{4

5}, Tuomas Kaprio^{4

5}, Camilla Böckelman^{4

5}, Jaana Hagström^{5

6}, Richard Palmqvist³, Caj Haglund^{4

5}

Affiliations

¹ Department of Surgical and Perioperative Sciences, Umeå University, 901 87, Umeå, Sweden. ulf.gunnarsson@umu.se.
² Department of Surgical and Perioperative Sciences, Umeå University, 901 87, Umeå, Sweden.
³ Department of Medical Biosciences/Pathology, Umeå University, 901 87, Umeå, Sweden.
⁴ Department of Surgery, University of Helsinki and Helsinki University Hospital, 00114, Helsinki, Finland.
⁵ Translational Cancer Medicine Research Program, Faculty of Medicine, University of Helsinki, 00014, Helsinki, Finland.
⁶ Department of Pathology, University of Helsinki and Helsinki University Hospital, 00014, Helsinki, Finland.

Abstract

Background: Systemic inflammatory response in colorectal cancer (CRC) has been established as a prognostic factor for impaired cancer-specific survival, predominantly in patients with right-sided tumors. On the other hand, defective mismatch repair (dMMR) tumors, primarily located in the right colon, are known to have favorable survival and dense local immune infiltration. The aim of this study was to see if there is any form of relationship between these seemingly diverse entities.

Methods: Complete clinical and long-term survival data were retrieved for 316 CRC patients operated at Helsinki University Hospital between the years 1998 and 2003. Tissue microarrays were prepared from surgical specimens and further processed and analyzed for local immune cell infiltration using multispectral imaging with a Vectra quantitative pathology imaging system and Inform software. Multiplex immunohistochemistry was applied using antibodies against CD66b, CD8, CD20, FoxP3, CD68 and pan-Cytokeratin. After exclusions, data on immune infiltration were available for 275 patients. Mismatch repair status was determined by immunohistochemistry.

Results: CRP was seen to be an independent predictor of cancer-specific survival but not overall survival in uni- and multivariable (HR 1.01 (1.00-1.02); p = 0.028) analyses of non-irradiated patients. There was no significant difference in CRP according to mismatch repair status, but all cases (n = 10) with CRP ≥ 75 mg/l had proficient mismatch repair (pMMR). There was a significant negative correlation between intratumor stromal infiltration by T-regulatory FOXP3⁺ cells and CRP (p = 0.006). There was significantly lower intratumor stromal infiltration by FOXP3⁺ cells (p = 0.043) in the right colon compared to the rectum, but no significant difference in CRP (p = 0.44). CRP was not a predictor of overall survival (HR 0.99, 95% CI 0.98-1.01) nor cancer-specific survival in irradiated patients (HR 0.94, 95% CI 0.94-1.02).

Conclusions: There was a significant negative relationship between SIR, defined as an elevated CRP, and intratumor stromal infiltration by T-regulatory FOXP3⁺cells. This and the fact that all cases with a CRP > 75 mg/l had pMMR suggests that SIR and dMMR are independent entities in CRC. Indeed, the general lack of difference in CRP between cases with dMMR and pMMR may be evidence of overlap in cases with a less pronounced SIR.

Keywords: Colorectal cancer; Local immune response; Miscrosatellite instability; Mismatch repair; Systematic inflammatory response.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Colonic Neoplasms*
Colorectal Neoplasms*
DNA Mismatch Repair
Humans
Prognosis
Systemic Inflammatory Response Syndrome