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Integrating Tumor Intraepithelial CD8+ and Stromal FOXP3+ T-Cell Densities as an Enhanced Immune Prognostic Index in Colorectal Cancer

Year of publication

2025

Authors

Tuomisto, Anne; Sirniö, Päivi; Elomaa, Hanna; Karjalainen, Henna; Äijälä, Ville K.; Kastinen, Meeri; Tapiainen, Vilja V.; Ahtiainen, Maarit; Helminen, Olli; Wirta, Erkki-Ville; Rintala, Jukka; Meriläinen, Sanna; Saarnio, Juha; Rautio, Tero; Seppälä, Toni T.; Böhm, Jan; Mecklin, Jukka-Pekka; Mäkinen, Markus J.; Väyrynen, Juha P.
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Abstract

High immune cell infiltration is generally associated with better survival in colorectal cancer (CRC). Recently, a prognostic score called CD8IE-FOXP3IS, which integrates the densities of tumor intraepithelial CD8+ and intrastromal FOXP3+ cells, was introduced using multiplex immunofluorescence. In this study, we developed a triple chromogenic immunohistochemistry assay to evaluate the CD8IE-FOXP3IS score and assessed its prognostic value in comparison with the CD3-CD8 T-cell density score (based on the principles of the Immunoscore) and conventional prognostic parameters. Multiplex immunohistochemistry combined with machine learning–assisted image analysis was used to quantify CD8IE and FOXP3IS densities in 2 independent cohorts comprising 1724 CRC patients. Multivariable Cox regression models were used to evaluate the prognostic value of the CD8IE-FOXP3IS score. We found that a low CD8IE-FOXP3IS score was associated with higher disease stage, more frequent lymphovascular invasion, and mismatch repair proficient status. In addition, a low CD8IE-FOXP3IS score was associated with higher CRC-specific mortality independent of the CD3-CD8 T-cell density score and other tumor and patient characteristics (cohort 1: hazard ratio [HR] for low vs high CD8IE-FOXP3IS score, 3.08; 95% CI, 1.54-6.15; Ptrend = 6.0E-4; cohort 2: HR, 4.30; 95% CI, 2.58-7.17; Ptrend = 3.2E-9). These findings indicate that triple chromogenic immunohistochemistry combined with digital pathology is an applicable method for quantifying tumor intraepithelial CD8+ and stromal FOXP3+ cell densities, allowing for the determination of the CD8IE-FOXP3IS score. The CD8IE-FOXP3IS score shows a strong prognostic value, which appears superior to overall CD3+ and CD8+ T-cell density measurement.
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Organizations and authors

University of Jyväskylä

Mecklin Jukka-Pekka

Tampere University

Wirta Erkki-Ville Orcid -palvelun logo

Seppälä Toni T Orcid -palvelun logo

University of Helsinki

Elomaa Hanna

Seppälä Toni T.

University of Oulu

Tuomisto Anne

Saarnio Juha Orcid -palvelun logo

Väyrynen Juha Orcid -palvelun logo

Mäkinen Markus

Kastinen Meeri

Helminen Olli

Sirniö Päivi

Meriläinen Sanna

Rautio Tero Orcid -palvelun logo

Tapiainen Vilja

Äijälä Ville Kusti Matias

Tampere University Hospital

Wirta Erkki-Ville Orcid -palvelun logo

Seppälä Toni T Orcid -palvelun logo

Helsinki University Hospital

Elomaa Hanna

Seppälä Toni T.

Publication type

Publication format

Article

Parent publication type

Journal

Article type

Original article

Audience

Scientific

Peer-reviewed

Peer-Reviewed

MINEDU's publication type classification code

A1 Journal article (refereed), original research

Publication channel information

Parent publication name

Laboratory Investigation

Volume

105

Issue

11

Article number

104213

​Publication forum

62387

​Publication forum level

1

Open access

Open access in the publisher’s service

Yes

Open access of publication channel

Partially open publication channel

License of the publisher’s version

CC BY

Self-archived

Yes

License of the self-archived publication

CC BY

Other information

Fields of science

Biomedicine; Cancers; Surgery, anesthesiology, intensive care, radiology

Keywords

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Publication country

United States

Internationality of the publisher

International

Language

English

International co-publication

No

Co-publication with a company

No

DOI

10.1016/j.labinv.2025.104213

The publication is included in the Ministry of Education and Culture’s Publication data collection

Yes