FPR2 Shapes an Immune-Excluded Pancreatic Tumor Microenvironment and Drives T-cell Exhaustion in a Sex-Dependent Manner

Fei He; Apple H M Tay; Ahmed Calandigary; Enana Malki; Sayaka Suzuki; Tianjie Liu; Qi Wang; Carlos Fernández-Moro; Marina Kaisso; Peter Olofsson-Sahl; Marit Melssen; Siu Kwan Sze; Mikael Björnstedt; Matthias J Löhr; Mikael C I Karlsson; Rainer Heuchel; Dhifaf Sarhan

doi:10.1158/0008-5472.CAN-22-2932

FPR2 Shapes an Immune-Excluded Pancreatic Tumor Microenvironment and Drives T-cell Exhaustion in a Sex-Dependent Manner

Cancer Res. 2023 May 15;83(10):1628-1645. doi: 10.1158/0008-5472.CAN-22-2932.

Authors

Fei He^{1

2}, Apple H M Tay^#^{3

4}, Ahmed Calandigary^#⁵, Enana Malki¹, Sayaka Suzuki¹, Tianjie Liu⁶, Qi Wang⁶, Carlos Fernández-Moro¹, Marina Kaisso¹, Peter Olofsson-Sahl⁷, Marit Melssen⁸, Siu Kwan Sze^{3

9}, Mikael Björnstedt¹, Matthias J Löhr¹⁰, Mikael C I Karlsson¹¹, Rainer Heuchel¹⁰, Dhifaf Sarhan¹

Affiliations

¹ Division of Pathology, Department of Laboratory Medicine, Karolinska Institutet, Stockholm, Sweden.
² Department of Urology, Second Affiliated Hospital, Zhejiang University School of Medicine, Zhejiang University, Hangzhou, China.
³ Department of Biological Science, Nanyang Technological University, Singapore, Singapore.
⁴ Department of Oncology-Pathology, Karolinska Institute, Stockholm, Sweden.
⁵ Department of Immunology, Genetics, and Pathology, Clinical Immunology, Uppsala, Sweden.
⁶ Department of Urology, First affiliated hospital of Xi'an Jiaotong university, Xi'an, Shaanxi, China.
⁷ Pronoxis AB, Medicon Village, Lund, Sweden.
⁸ Department of Immunology, Genetics and Pathology, Vascular Biology, Uppsala, Sweden.
⁹ Department of Health Sciences, Faculty of Applied Health Sciences, Brock University, Ontario, Canada.
¹⁰ Department of Clinical Science, Intervention and Technology, Pancreatic Cancer Research Laboratory, Karolinska Institutet, Stockholm, Sweden.
¹¹ Department of Microbiology, Tumor and Cell Biology, Karolinska Insitutet, Stockholm, Sweden.

^# Contributed equally.

PMID: 36919330
DOI: 10.1158/0008-5472.CAN-22-2932

Abstract

Sex-driven immune differences can affect tumor progression and the landscape of the tumor microenvironment. Deeper understanding of these differences in males and females can inform patient selection to improve sex-optimized immunotherapy treatments. In this study, single-cell RNA sequencing and protein analyses uncovered a subpopulation of myeloid cells in pancreatic lesions associated with an immune-excluded tumor phenotype and effector T-cell exhaustion exclusively in females. This myeloid subpopulation was positively correlated with poor survival and genetic signatures of M2-like macrophages and T-cell exhaustion in females. The G-protein coupled receptor formyl peptide receptor 2 (FPR2) mediated these immunosuppressive effects. In vitro, treatment of myeloid cells with a specific FPR2 antagonist prevented exhaustion and enhanced cytotoxicity of effector cells. Proteomic analysis revealed high expression of immunosuppressive secretory proteins PGE2 and galectin-9, enriched integrin pathway, and reduced proinflammatory signals like TNFα and IFNγ in female M2-like macrophages upon FPR2 agonist treatment. In addition, myeloid cells treated with FPR2 agonists induced TIM3 and PD-1 expression only in female T cells. Treatment with anti-TIM3 antibodies reversed T-cell exhaustion and stimulated their ability to infiltrate and kill pancreatic spheroids. In vivo, progression of syngeneic pancreatic tumors was significantly suppressed in FPR2 knockout (KO) female mice compared with wild-type (WT) female mice and to WT and FPR2 KO male mice. In female mice, inoculation of tumors with FPR2 KO macrophages significantly reduced tumor growth compared with WT macrophages. Overall, this study identified an immunosuppressive function of FPR2 in females, highlighting a potential sex-specific precision immunotherapy strategy.

Significance: FPR2 is a sex-dependent mediator of macrophage function in pancreatic cancer and can be targeted to reprogram macrophages and stimulate antitumor immunity in females.

Publication types

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

MeSH terms

Animals
Female
Male
Mice
Mice, Knockout
Myeloid Cells
Pancreatic Neoplasms* / genetics
Proteomics
T-Cell Exhaustion
Tumor Microenvironment*