Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway

Ruiman Geng; Huawei Cai; Xuxu Ji; Xiaoding Shen; Ziyao Wang; Zhao Li; Ruomeng Liu; Zhengkun Zhang; Dingxue Wang; Zhaoru Yin; Jiaqiong Zou; Rong Guo; Panpan Dai; Zhiyou Quan; Lihong Chen; Nengwen Ke; Ji Liu

doi:10.1038/s41416-026-03371-8

Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway

Ruiman Geng
, Huawei Cai^*
, Xuxu Ji
, Xiaoding Shen
, Ziyao Wang
, Zhao Li
, Ruomeng Liu
, Zhengkun Zhang
, Dingxue Wang
, Zhaoru Yin
, Jiaqiong Zou
, Rong Guo
, Panpan Dai
, Zhiyou Quan
, Lihong Chen^*
, Nengwen Ke^*
, Ji Liu^*

^*Corresponding author for this work

Sichuan University
Xi'an Medical University
Sichuan University

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

Abstract

Background: Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive cancer with a poor prognosis and is easy to developing drug resistance to conventional therapies due to its distinctive tumour microenvironment. Recent advancements have brought attention to the aberrant copper metabolism in this malignancy, but the influence of intracellular cuproplasia and balance on the tumoral immune microenvironment is still uncertain. Methods: We analysed copper concentrations and CTR1 expression in PDAC tissues and cell lines. Spatial transcriptomics was employed to delineate the relationship between CTR1 overexpression and tumour-associated neutrophils (TANs) infiltration. Chemokine arrays and molecular assays were used to identify key signalling pathways involved. Functional experiments, including CTR1 knockdown and TRAF6 overexpression, were conducted to assess its impact on neutrophil infiltration and therapeutic synergy with gemcitabine. Results: We identified that CTR1 overexpression drives intracellular copper overaccumulation, activating TRAF6-dependent phosphorylation of JAK/STAT3. Phosphorylated STAT3 transcriptionally upregulates the chemokine CCL2, fostering CCR2-mediated TANs infiltration, which correlates with poor prognosis. Crucially, single-cell RNA sequencing revealed CTR1 knockdown suppresses a pro-metastatic TAN subpopulation (TAN-2) and dramatically reduces TANs recruitment in orthotopic tumour models. This copper-targeted intervention concurrently enhances cytotoxic CD8⁺ effector T cells within the TME. The translational impact is underscored in gemcitabine-resistant PDAC, where hyperactive CTR1 and intensified TANs infiltration create a therapy-refractory condition. Combining CTR1 inhibition with gemcitabine synergistically overcomes this resistance by dual remodelling of the TME. Conclusions: Our findings shed light on how intracellular copper metabolism-regulating molecules modulate the neutrophil infiltration through the TRAF6/STAT3/CCL2 pathway, and particularly, targeting the copper regulator shows potential in optimising the tumour microenvironment in the treatment of pancreatic cancers. (Figure presented.)

Original language	English
Journal	British Journal of Cancer
DOIs	https://doi.org/10.1038/s41416-026-03371-8
State	Accepted/In press - 2026
Externally published	Yes

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SDG 3 Good Health and Well-being

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10.1038/s41416-026-03371-8

Cite this

Geng, R., Cai, H., Ji, X., Shen, X., Wang, Z., Li, Z., Liu, R., Zhang, Z., Wang, D., Yin, Z., Zou, J., Guo, R., Dai, P., Quan, Z., Chen, L., Ke, N., & Liu, J. (Accepted/In press). Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway. British Journal of Cancer. https://doi.org/10.1038/s41416-026-03371-8

@article{925b3fc0108d45e2be3ec888f01ad55b,

title = "Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway",

abstract = "Background: Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive cancer with a poor prognosis and is easy to developing drug resistance to conventional therapies due to its distinctive tumour microenvironment. Recent advancements have brought attention to the aberrant copper metabolism in this malignancy, but the influence of intracellular cuproplasia and balance on the tumoral immune microenvironment is still uncertain. Methods: We analysed copper concentrations and CTR1 expression in PDAC tissues and cell lines. Spatial transcriptomics was employed to delineate the relationship between CTR1 overexpression and tumour-associated neutrophils (TANs) infiltration. Chemokine arrays and molecular assays were used to identify key signalling pathways involved. Functional experiments, including CTR1 knockdown and TRAF6 overexpression, were conducted to assess its impact on neutrophil infiltration and therapeutic synergy with gemcitabine. Results: We identified that CTR1 overexpression drives intracellular copper overaccumulation, activating TRAF6-dependent phosphorylation of JAK/STAT3. Phosphorylated STAT3 transcriptionally upregulates the chemokine CCL2, fostering CCR2-mediated TANs infiltration, which correlates with poor prognosis. Crucially, single-cell RNA sequencing revealed CTR1 knockdown suppresses a pro-metastatic TAN subpopulation (TAN-2) and dramatically reduces TANs recruitment in orthotopic tumour models. This copper-targeted intervention concurrently enhances cytotoxic CD8+ effector T cells within the TME. The translational impact is underscored in gemcitabine-resistant PDAC, where hyperactive CTR1 and intensified TANs infiltration create a therapy-refractory condition. Combining CTR1 inhibition with gemcitabine synergistically overcomes this resistance by dual remodelling of the TME. Conclusions: Our findings shed light on how intracellular copper metabolism-regulating molecules modulate the neutrophil infiltration through the TRAF6/STAT3/CCL2 pathway, and particularly, targeting the copper regulator shows potential in optimising the tumour microenvironment in the treatment of pancreatic cancers. (Figure presented.)",

author = "Ruiman Geng and Huawei Cai and Xuxu Ji and Xiaoding Shen and Ziyao Wang and Zhao Li and Ruomeng Liu and Zhengkun Zhang and Dingxue Wang and Zhaoru Yin and Jiaqiong Zou and Rong Guo and Panpan Dai and Zhiyou Quan and Lihong Chen and Nengwen Ke and Ji Liu",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2026.",

year = "2026",

doi = "10.1038/s41416-026-03371-8",

language = "英语",

journal = "British Journal of Cancer",

issn = "0007-0920",

publisher = "Springer Nature",

}

TY - JOUR

T1 - Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway

AU - Geng, Ruiman

AU - Cai, Huawei

AU - Ji, Xuxu

AU - Shen, Xiaoding

AU - Wang, Ziyao

AU - Li, Zhao

AU - Liu, Ruomeng

AU - Zhang, Zhengkun

AU - Wang, Dingxue

AU - Yin, Zhaoru

AU - Zou, Jiaqiong

AU - Guo, Rong

AU - Dai, Panpan

AU - Quan, Zhiyou

AU - Chen, Lihong

AU - Ke, Nengwen

AU - Liu, Ji

PY - 2026

Y1 - 2026

N2 - Background: Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive cancer with a poor prognosis and is easy to developing drug resistance to conventional therapies due to its distinctive tumour microenvironment. Recent advancements have brought attention to the aberrant copper metabolism in this malignancy, but the influence of intracellular cuproplasia and balance on the tumoral immune microenvironment is still uncertain. Methods: We analysed copper concentrations and CTR1 expression in PDAC tissues and cell lines. Spatial transcriptomics was employed to delineate the relationship between CTR1 overexpression and tumour-associated neutrophils (TANs) infiltration. Chemokine arrays and molecular assays were used to identify key signalling pathways involved. Functional experiments, including CTR1 knockdown and TRAF6 overexpression, were conducted to assess its impact on neutrophil infiltration and therapeutic synergy with gemcitabine. Results: We identified that CTR1 overexpression drives intracellular copper overaccumulation, activating TRAF6-dependent phosphorylation of JAK/STAT3. Phosphorylated STAT3 transcriptionally upregulates the chemokine CCL2, fostering CCR2-mediated TANs infiltration, which correlates with poor prognosis. Crucially, single-cell RNA sequencing revealed CTR1 knockdown suppresses a pro-metastatic TAN subpopulation (TAN-2) and dramatically reduces TANs recruitment in orthotopic tumour models. This copper-targeted intervention concurrently enhances cytotoxic CD8+ effector T cells within the TME. The translational impact is underscored in gemcitabine-resistant PDAC, where hyperactive CTR1 and intensified TANs infiltration create a therapy-refractory condition. Combining CTR1 inhibition with gemcitabine synergistically overcomes this resistance by dual remodelling of the TME. Conclusions: Our findings shed light on how intracellular copper metabolism-regulating molecules modulate the neutrophil infiltration through the TRAF6/STAT3/CCL2 pathway, and particularly, targeting the copper regulator shows potential in optimising the tumour microenvironment in the treatment of pancreatic cancers. (Figure presented.)

AB - Background: Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive cancer with a poor prognosis and is easy to developing drug resistance to conventional therapies due to its distinctive tumour microenvironment. Recent advancements have brought attention to the aberrant copper metabolism in this malignancy, but the influence of intracellular cuproplasia and balance on the tumoral immune microenvironment is still uncertain. Methods: We analysed copper concentrations and CTR1 expression in PDAC tissues and cell lines. Spatial transcriptomics was employed to delineate the relationship between CTR1 overexpression and tumour-associated neutrophils (TANs) infiltration. Chemokine arrays and molecular assays were used to identify key signalling pathways involved. Functional experiments, including CTR1 knockdown and TRAF6 overexpression, were conducted to assess its impact on neutrophil infiltration and therapeutic synergy with gemcitabine. Results: We identified that CTR1 overexpression drives intracellular copper overaccumulation, activating TRAF6-dependent phosphorylation of JAK/STAT3. Phosphorylated STAT3 transcriptionally upregulates the chemokine CCL2, fostering CCR2-mediated TANs infiltration, which correlates with poor prognosis. Crucially, single-cell RNA sequencing revealed CTR1 knockdown suppresses a pro-metastatic TAN subpopulation (TAN-2) and dramatically reduces TANs recruitment in orthotopic tumour models. This copper-targeted intervention concurrently enhances cytotoxic CD8+ effector T cells within the TME. The translational impact is underscored in gemcitabine-resistant PDAC, where hyperactive CTR1 and intensified TANs infiltration create a therapy-refractory condition. Combining CTR1 inhibition with gemcitabine synergistically overcomes this resistance by dual remodelling of the TME. Conclusions: Our findings shed light on how intracellular copper metabolism-regulating molecules modulate the neutrophil infiltration through the TRAF6/STAT3/CCL2 pathway, and particularly, targeting the copper regulator shows potential in optimising the tumour microenvironment in the treatment of pancreatic cancers. (Figure presented.)

UR - https://www.scopus.com/pages/publications/105035716044

U2 - 10.1038/s41416-026-03371-8

DO - 10.1038/s41416-026-03371-8

M3 - 文章

AN - SCOPUS:105035716044

SN - 0007-0920

JO - British Journal of Cancer

JF - British Journal of Cancer

ER -

Blockage of cuproplasia inhibits pancreatic tumour-associated neutrophils infiltration through TRAF6/STAT3/CCL2 pathway

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