FOLFIRINOX chemotherapy modulates the peripheral immune landscape in pancreatic cancer: Implications for combination therapies and early response prediction

Casper W F van Eijck; Gaby Strijk; Eveline E Vietsch; Fleur van der Sijde; Maaike Verheij; Dana A M Mustafa; Madelief Vink; Joachim G J V Aerts; Casper H J van Eijck; Marcella Willemsen

doi:10.1016/j.ejca.2023.113440

FOLFIRINOX chemotherapy modulates the peripheral immune landscape in pancreatic cancer: Implications for combination therapies and early response prediction

Eur J Cancer. 2024 Jan:196:113440. doi: 10.1016/j.ejca.2023.113440. Epub 2023 Nov 17.

Affiliations

¹ Department of Surgery, Erasmus University Medical Centre, Rotterdam, the Netherlands; Genetic and Molecular Epidemiology Group, Spanish National Cancer Research Centre, Madrid, Spain.
² Department of Surgery, Erasmus University Medical Centre, Rotterdam, the Netherlands.
³ Department of Surgery, Erasmus University Medical Centre, Rotterdam, the Netherlands; Erasmus MC Cancer Institute, Erasmus University Medical Centre, Rotterdam, the Netherlands.
⁴ Department of Pathology, Erasmus University Medical Centre, Rotterdam, the Netherlands.
⁵ Erasmus MC Cancer Institute, Erasmus University Medical Centre, Rotterdam, the Netherlands; Department of Pulmonary Medicine, Erasmus University Medical Centre, Rotterdam, the Netherlands.
⁶ Erasmus MC Cancer Institute, Erasmus University Medical Centre, Rotterdam, the Netherlands; Department of Pulmonary Medicine, Erasmus University Medical Centre, Rotterdam, the Netherlands. Electronic address: m.willemsen@erasmusmc.nl.

PMID: 37988843
DOI: 10.1016/j.ejca.2023.113440

Abstract

Background: FOLFIRINOX chemotherapy has improved outcomes for pancreatic cancer patients, but poor long-term survival outcomes and high toxicity remain challenges. This study investigates the impact of FOLFIRINOX on plasma proteins and peripheral immune cells to guide immune-based combination therapies and, ideally, to identify a potential biomarker to predict early disease progression during FOLFIRINOX.

Methods: Blood samples were collected from 86 pancreatic cancer patients before and two weeks after the first FOLFIRINOX cycle and subjected to comprehensive immune cell and proteome profiling. Principal Component Analysis and Linear Mixed Effect Regression models were used for data analysis. FOLFIRINOX efficacy was radiologically evaluated after the fourth cycle.

Results: One cycle of FOLFIRINOX diminished tumour-cell-related pathways and enhanced pathways related to immune activation, illustrated by an increase in pro-inflammatory IL-18, IL-15, and TNFRSF4. Similarly, FOLFIRINOX promoted the activation of CD4 + and CD8 + T cells, the proliferation of NK(T), and the activation of antigen-presenting cells. Furthermore, high pre-treatment levels of VEGFA and PRDX3 and an elevation in FCRL3 levels after one cycle predicted early progression under FOLFIRINOX. Finally, patients with progressive disease exhibited high levels of inhibitory markers on B cells and CD8 + T cells, while responding patients exhibited high levels of activation markers on CD4 + and CD8 + T cell subsets.

Conclusion: FOLFIRINOX has immunomodulatory effects, providing a foundation for clinical trials exploring immune-based combination therapies that harness the immune system to treat pancreatic cancer. In addition, several plasma proteins hold potential as circulating predictive biomarkers for early prediction of FOLFIRINOX response in patients with pancreatic cancer.

Keywords: Biomarkers; Blood proteins; Combined modality therapy; FOLFIRINOX; Immunomodulation; Pancreatic neoplasms.

MeSH terms

Antineoplastic Combined Chemotherapy Protocols / therapeutic use
Blood Proteins
Fluorouracil / therapeutic use
Humans
Irinotecan / therapeutic use
Leucovorin / therapeutic use
Pancreatic Neoplasms*

Substances

folfirinox
Irinotecan
Fluorouracil
Leucovorin
Blood Proteins