Pre-treatment inflamed tumor immune microenvironment is associated with FOLFIRINOX response in pancreatic cancer

Zachary Gao; Sung Wook Kang; Sung Wook Kang; Sung Wook Kang; Derek Erstad; Derek Erstad; Derek Erstad; Joseph Azar; George Van Buren; George Van Buren; William Fisher; William Fisher; Zequn Sun; Mark P. Rubinstein; Hyun-Sung Lee; Hyun-Sung Lee; Hyun-Sung Lee; E. Ramsay Camp; E. Ramsay Camp; E. Ramsay Camp

doi:10.3389/fonc.2023.1274783

Frontiers in Oncology (Nov 2023)

Pre-treatment inflamed tumor immune microenvironment is associated with FOLFIRINOX response in pancreatic cancer

Zachary Gao,
Sung Wook Kang,
Sung Wook Kang,
Sung Wook Kang,
Derek Erstad,
Derek Erstad,
Derek Erstad,
Joseph Azar,
George Van Buren,
George Van Buren,
William Fisher,
William Fisher,
Zequn Sun,
Mark P. Rubinstein,
Hyun-Sung Lee,
Hyun-Sung Lee,
Hyun-Sung Lee,
E. Ramsay Camp,
E. Ramsay Camp,
E. Ramsay Camp

Affiliations

Zachary Gao: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
Sung Wook Kang: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
Sung Wook Kang: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
Sung Wook Kang: Systems Onco-Immunology Laboratory, David J. Sugarbaker Division of Thoracic Surgery, Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
Derek Erstad: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
Derek Erstad: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
Derek Erstad: Department of Surgery, Michael E. DeBakey VA Medical Center, Houston, TX, United States
Joseph Azar: The Pelotonia Institute for Immuno-Oncology, Ohio State University Comprehensive Cancer Center, Columbus, OH, United States
George Van Buren: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
George Van Buren: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
William Fisher: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
William Fisher: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
Zequn Sun: Department of Preventative Medicine, Northwestern University Clinical and Translational Sciences Institute, Chicago, IL, United States
Mark P. Rubinstein: The Pelotonia Institute for Immuno-Oncology, Ohio State University Comprehensive Cancer Center, Columbus, OH, United States
Hyun-Sung Lee: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
Hyun-Sung Lee: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
Hyun-Sung Lee: Systems Onco-Immunology Laboratory, David J. Sugarbaker Division of Thoracic Surgery, Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
E. Ramsay Camp: Michael E. DeBakey Department of Surgery, Baylor College of Medicine, Houston, TX, United States
E. Ramsay Camp: Department of Surgery, Dan L. Duncan Comprehensive Cancer Center, Houston, TX, United States
E. Ramsay Camp: Department of Surgery, Michael E. DeBakey VA Medical Center, Houston, TX, United States

DOI: https://doi.org/10.3389/fonc.2023.1274783
Journal volume & issue: Vol. 13

Abstract

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IntroductionPancreatic adenocarcinoma (PDAC) is an aggressive tumor with limited response to both chemotherapy and immunotherapy. Pre-treatment tumor features within the tumor immune microenvironment (TiME) may influence treatment response. We hypothesized that the pre-treatment TiME composition differs between metastatic and primary lesions and would be associated with response to modified FOLFIRINOX (mFFX) or gemcitabine-based (Gem-based) therapy.MethodsUsing RNAseq data from a cohort of treatment-naïve, advanced PDAC patients in the COMPASS trial, differential gene expression analysis of key immunomodulatory genes in were analyzed based on multiple parameters including tumor site, response to mFFX, and response to Gem-based treatment. The relative proportions of immune cell infiltration were defined using CIBERSORTx and Dirichlet regression.Results145 samples were included in the analysis; 83 received mFFX, 62 received Gem-based therapy. Metastatic liver samples had both increased macrophage (1.2 times more, p < 0.05) and increased eosinophil infiltration (1.4 times more, p < 0.05) compared to primary lesion samples. Further analysis of the specific macrophage phenotypes revealed an increased M2 macrophage fraction in the liver samples. The pre-treatment CD8 T-cell, dendritic cell, and neutrophil infiltration of metastatic samples were associated with therapy response to mFFX (p < 0.05), while mast cell infiltration was associated with response to Gem-based therapy (p < 0.05). Multiple immunoinhibitory genes such as ADORA2A, CSF1R, KDR/VEGFR2, LAG3, PDCD1LG2, and TGFB1 and immunostimulatory genes including C10orf54, CXCL12, and TNFSF14/LIGHT were significantly associated with worse survival in patients who received mFFX (p = 0.01). There were no immunomodulatory genes associated with survival in the Gem-based cohort. DiscussionOur evidence implies that essential differences in the PDAC TiME exist between primary and metastatic tumors and an inflamed pretreatment TiME is associated with mFFX response. Defining components of the PDAC TiME that influence therapy response will provide opportunities for targeted therapeutic strategies that may need to be accounted for in designing personalized therapy to improve outcomes.

Published in Frontiers in Oncology

ISSN: 2234-943X (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.frontiersin.org/journals/oncology/

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