Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms

Shivan Sivakumar; Ashwin Jainarayanan; Edward Arbe-Barnes; Piyush Kumar Sharma; Maire Ni Leathlobhair; Sakina Amin; David J Reiss; Lara Heij; Samarth Hegde; Assaf Magen; Felicia Tucci; Bo Sun; Shihong Wu; Nithishwer Mouroug Anand; Hubert Slawinski; Santiago Revale; Isar Nassiri; Jonathon Webber; Gerard D Hoeltzel; Adam E Frampton; Georg Wiltberger; Ulf Neumann; Philip Charlton; Laura Spiers; Tim Elliott; Maria Wang; Suzana Couto; Thomas Lila; Pallavur V Sivakumar; Alexander V Ratushny; Mark R Middleton; Dimitra Peppa; Benjamin Fairfax; Miriam Merad; Michael L Dustin; Enas Abu-Shah; Rachael Bashford-Rogers

doi:10.1038/s41467-024-55424-2

Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms

Shivan Sivakumar^*
, Ashwin Jainarayanan
, Edward Arbe-Barnes
, Piyush Kumar Sharma
, Maire Ni Leathlobhair
, Sakina Amin
, David J Reiss
, Lara Heij
, Samarth Hegde
, Assaf Magen
, Felicia Tucci
, Bo Sun
, Shihong Wu
, Nithishwer Mouroug Anand
, Hubert Slawinski
, Santiago Revale
, Isar Nassiri
, Jonathon Webber
, Gerard D Hoeltzel
, Adam E Frampton

Georg Wiltberger, Ulf Neumann, Philip Charlton, Laura Spiers, Tim Elliott, Maria Wang, Suzana Couto, Thomas Lila, Pallavur V Sivakumar, Alexander V Ratushny, Mark R Middleton, Dimitra Peppa, Benjamin Fairfax, Miriam Merad, Michael L Dustin, Enas Abu-Shah^*, Rachael Bashford-Rogers^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Pancreatic ductal adenocarcinoma has a dismal prognosis. A comprehensive analysis of single-cell multi-omic data from matched tumour-infiltrated CD45+ cells and peripheral blood in 12 patients, and two published datasets, reveals a complex immune infiltrate. Patients have either a myeloid-enriched or adaptive-enriched tumour microenvironment. Adaptive immune cell-enriched is intrinsically linked with highly distinct B and T cell clonal selection, diversification, and differentiation. Using TCR data, we see the largest clonal expansions in CD8 effector memory, senescent cells, and highly activated regulatory T cells which are induced within the tumour from naïve cells. We identify pathways that potentially lead to a suppressive microenvironment, including investigational targets TIGIT/PVR and SIRPA/CD47. Analysis of patients from the APACT clinical trial shows that myeloid enrichment had a shorter overall survival compared to those with adaptive cell enrichment. Strategies for rationale therapeutic development in this disease include boosting of B cell responses, targeting immunosuppressive macrophages, and specific Treg cell depletion approaches.

Original language	English
Article number	1397
Number of pages	20
Journal	Nature Communications
Volume	16
Issue number	1
DOIs	https://doi.org/10.1038/s41467-024-55424-2
Publication status	Published - 6 Feb 2025

Keywords

Humans
Carcinoma, Pancreatic Ductal/immunology pathology mortality
Tumor Microenvironment/immunology
Pancreatic Neoplasms/immunology pathology mortality
T-Lymphocytes, Regulatory/immunology
Lymphocytes, Tumor-Infiltrating/immunology
Female
CD8-Positive T-Lymphocytes/immunology
Male
Myeloid Cells/immunology
B-Lymphocytes/immunology
Single-Cell Analysis
Macrophages/immunology
Middle Aged
Aged
Prognosis

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Sivakumar, S., Jainarayanan, A., Arbe-Barnes, E., Sharma, P. K., Leathlobhair, M. N., Amin, S., Reiss, D. J., Heij, L., Hegde, S., Magen, A., Tucci, F., Sun, B., Wu, S., Anand, N. M., Slawinski, H., Revale, S., Nassiri, I., Webber, J., Hoeltzel, G. D., ... Bashford-Rogers, R. (2025). Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms. Nature Communications, 16(1), Article 1397. https://doi.org/10.1038/s41467-024-55424-2

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abstract = "Pancreatic ductal adenocarcinoma has a dismal prognosis. A comprehensive analysis of single-cell multi-omic data from matched tumour-infiltrated CD45+ cells and peripheral blood in 12 patients, and two published datasets, reveals a complex immune infiltrate. Patients have either a myeloid-enriched or adaptive-enriched tumour microenvironment. Adaptive immune cell-enriched is intrinsically linked with highly distinct B and T cell clonal selection, diversification, and differentiation. Using TCR data, we see the largest clonal expansions in CD8 effector memory, senescent cells, and highly activated regulatory T cells which are induced within the tumour from na{\"i}ve cells. We identify pathways that potentially lead to a suppressive microenvironment, including investigational targets TIGIT/PVR and SIRPA/CD47. Analysis of patients from the APACT clinical trial shows that myeloid enrichment had a shorter overall survival compared to those with adaptive cell enrichment. Strategies for rationale therapeutic development in this disease include boosting of B cell responses, targeting immunosuppressive macrophages, and specific Treg cell depletion approaches.",

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author = "Shivan Sivakumar and Ashwin Jainarayanan and Edward Arbe-Barnes and Sharma, \{Piyush Kumar\} and Leathlobhair, \{Maire Ni\} and Sakina Amin and Reiss, \{David J\} and Lara Heij and Samarth Hegde and Assaf Magen and Felicia Tucci and Bo Sun and Shihong Wu and Anand, \{Nithishwer Mouroug\} and Hubert Slawinski and Santiago Revale and Isar Nassiri and Jonathon Webber and Hoeltzel, \{Gerard D\} and Frampton, \{Adam E\} and Georg Wiltberger and Ulf Neumann and Philip Charlton and Laura Spiers and Tim Elliott and Maria Wang and Suzana Couto and Thomas Lila and Sivakumar, \{Pallavur V\} and Ratushny, \{Alexander V\} and Middleton, \{Mark R\} and Dimitra Peppa and Benjamin Fairfax and Miriam Merad and Dustin, \{Michael L\} and Enas Abu-Shah and Rachael Bashford-Rogers",

year = "2025",

month = feb,

day = "6",

doi = "10.1038/s41467-024-55424-2",

language = "English",

volume = "16",

journal = "Nature Communications",

issn = "2041-1723",

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Sivakumar, S, Jainarayanan, A, Arbe-Barnes, E, Sharma, PK, Leathlobhair, MN, Amin, S, Reiss, DJ, Heij, L, Hegde, S, Magen, A, Tucci, F, Sun, B, Wu, S, Anand, NM, Slawinski, H, Revale, S, Nassiri, I, Webber, J, Hoeltzel, GD, Frampton, AE, Wiltberger, G, Neumann, U, Charlton, P, Spiers, L, Elliott, T, Wang, M, Couto, S, Lila, T, Sivakumar, PV, Ratushny, AV, Middleton, MR, Peppa, D, Fairfax, B, Merad, M, Dustin, ML, Abu-Shah, E & Bashford-Rogers, R 2025, 'Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms', Nature Communications, vol. 16, no. 1, 1397. https://doi.org/10.1038/s41467-024-55424-2

Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms. / Sivakumar, Shivan; Jainarayanan, Ashwin; Arbe-Barnes, Edward et al.
In: Nature Communications, Vol. 16, No. 1, 1397, 06.02.2025.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms

AU - Sivakumar, Shivan

AU - Jainarayanan, Ashwin

AU - Arbe-Barnes, Edward

AU - Sharma, Piyush Kumar

AU - Leathlobhair, Maire Ni

AU - Amin, Sakina

AU - Reiss, David J

AU - Heij, Lara

AU - Hegde, Samarth

AU - Magen, Assaf

AU - Tucci, Felicia

AU - Sun, Bo

AU - Wu, Shihong

AU - Anand, Nithishwer Mouroug

AU - Slawinski, Hubert

AU - Revale, Santiago

AU - Nassiri, Isar

AU - Webber, Jonathon

AU - Hoeltzel, Gerard D

AU - Frampton, Adam E

AU - Wiltberger, Georg

AU - Neumann, Ulf

AU - Charlton, Philip

AU - Spiers, Laura

AU - Elliott, Tim

AU - Wang, Maria

AU - Couto, Suzana

AU - Lila, Thomas

AU - Sivakumar, Pallavur V

AU - Ratushny, Alexander V

AU - Middleton, Mark R

AU - Peppa, Dimitra

AU - Fairfax, Benjamin

AU - Merad, Miriam

AU - Dustin, Michael L

AU - Abu-Shah, Enas

AU - Bashford-Rogers, Rachael

PY - 2025/2/6

Y1 - 2025/2/6

N2 - Pancreatic ductal adenocarcinoma has a dismal prognosis. A comprehensive analysis of single-cell multi-omic data from matched tumour-infiltrated CD45+ cells and peripheral blood in 12 patients, and two published datasets, reveals a complex immune infiltrate. Patients have either a myeloid-enriched or adaptive-enriched tumour microenvironment. Adaptive immune cell-enriched is intrinsically linked with highly distinct B and T cell clonal selection, diversification, and differentiation. Using TCR data, we see the largest clonal expansions in CD8 effector memory, senescent cells, and highly activated regulatory T cells which are induced within the tumour from naïve cells. We identify pathways that potentially lead to a suppressive microenvironment, including investigational targets TIGIT/PVR and SIRPA/CD47. Analysis of patients from the APACT clinical trial shows that myeloid enrichment had a shorter overall survival compared to those with adaptive cell enrichment. Strategies for rationale therapeutic development in this disease include boosting of B cell responses, targeting immunosuppressive macrophages, and specific Treg cell depletion approaches.

AB - Pancreatic ductal adenocarcinoma has a dismal prognosis. A comprehensive analysis of single-cell multi-omic data from matched tumour-infiltrated CD45+ cells and peripheral blood in 12 patients, and two published datasets, reveals a complex immune infiltrate. Patients have either a myeloid-enriched or adaptive-enriched tumour microenvironment. Adaptive immune cell-enriched is intrinsically linked with highly distinct B and T cell clonal selection, diversification, and differentiation. Using TCR data, we see the largest clonal expansions in CD8 effector memory, senescent cells, and highly activated regulatory T cells which are induced within the tumour from naïve cells. We identify pathways that potentially lead to a suppressive microenvironment, including investigational targets TIGIT/PVR and SIRPA/CD47. Analysis of patients from the APACT clinical trial shows that myeloid enrichment had a shorter overall survival compared to those with adaptive cell enrichment. Strategies for rationale therapeutic development in this disease include boosting of B cell responses, targeting immunosuppressive macrophages, and specific Treg cell depletion approaches.

KW - Humans

KW - Carcinoma, Pancreatic Ductal/immunology pathology mortality

KW - Tumor Microenvironment/immunology

KW - Pancreatic Neoplasms/immunology pathology mortality

KW - T-Lymphocytes, Regulatory/immunology

KW - Lymphocytes, Tumor-Infiltrating/immunology

KW - Female

KW - CD8-Positive T-Lymphocytes/immunology

KW - Male

KW - Myeloid Cells/immunology

KW - B-Lymphocytes/immunology

KW - Single-Cell Analysis

KW - Macrophages/immunology

KW - Middle Aged

KW - Aged

KW - Prognosis

U2 - 10.1038/s41467-024-55424-2

DO - 10.1038/s41467-024-55424-2

M3 - Article

SN - 2041-1723

VL - 16

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 1397

ER -

Distinct immune cell infiltration patterns in pancreatic ductal adenocarcinoma (PDAC) exhibit divergent immune cell selection and immunosuppressive mechanisms

Abstract

Keywords

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