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Analysis of Circulating Immune Subsets in Primary Colorectal Cancer

by Jens Werner , Viktor von Ehrlich-Treuenstätt , Alexandr V. Bazhin , Can Lu , Ulrich Wirth , Josefine Schardey , Clemens Gießen-Jung , Jens Neumann , Florian Kühn

in Biomarkers / Cancer / CD69 antigen / Colorectal cancer / colorectal cancer; flow cytometry; immunophenotype; diagnostic model; differentially expressed genes / Cytotoxicity / Datasets / Dendritic cells / Development and progression / Diagnosis / Flow cytometry / Gene expression / Helper cells / Immune status / Immune system / Lymphocytes / Lymphocytes T / Medical prognosis / Metastasis / Monocytes / Neutrophils / Oncology, Experimental / Regression analysis / Software / Support vector machines / Suppressor cells / Tumor microenvironment / Tumor-infiltrating lymphocytes

2022

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Analysis of Circulating Immune Subsets in Primary Colorectal Cancer

by Jens Werner , Viktor von Ehrlich-Treuenstätt , Alexandr V. Bazhin , Can Lu , Ulrich Wirth , Josefine Schardey , Clemens Gießen-Jung , Jens Neumann , Florian Kühn

2022

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Analysis of Circulating Immune Subsets in Primary Colorectal Cancer

by Jens Werner , Viktor von Ehrlich-Treuenstätt , Alexandr V. Bazhin , Can Lu , Ulrich Wirth , Josefine Schardey , Clemens Gießen-Jung , Jens Neumann , Florian Kühn

2022

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Journal Article

Analysis of Circulating Immune Subsets in Primary Colorectal Cancer

Jens Werner,

Viktor von Ehrlich-Treuenstätt,

Alexandr V. Bazhin,

Can Lu,

Ulrich Wirth,

Josefine Schardey,

Clemens Gießen-Jung,

Jens Neumann,

Florian Kühn

2022

Overview

The development and progression of colorectal cancer (CRC) are known to be affected by the interplay between tumor and immune cells. However, the impact of CRC cells on the systemic immunity has yet to be elucidated. We aimed to comprehensively evaluate the circulating immune subsets and transcriptional profiles of CRC patients. In contrast to healthy controls (HCs), CRC patients had a lower percentage of B and T lymphocytes, T helper (Th) cells, non-classical monocytes, dendritic cells, and a higher proportion of polymorphonuclear myeloid-derived suppressor cells, as well as a reduced expression of CD69 on NK cells. Therefore, CRC patients exhibit a more evident systemic immune suppression than HCs. A diagnostic model integrating seven immune subsets was constructed to distinguish CRC patients from HCs with an AUC of 1.000. Moreover, NR3C2, CAMK4, and TRAT1 were identified as candidate genes regulating the number of Th cells in CRC patients. The altered composition of circulating immune cells in CRC could complement the regional immune status of the tumor microenvironment and contribute to the discovery of immune-related biomarkers for the diagnosis of CRC.

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Publisher

MDPI AG,MDPI

Subject

Biomarkers

/ Cancer

/ CD69 antigen

/ Colorectal cancer

/ colorectal cancer; flow cytometry; immunophenotype; diagnostic model; differentially expressed genes

/ Cytotoxicity

/ Datasets