Lipid metabolism reprograming by SREBP1‐PCSK9 targeting sensitizes pancreatic cancer to immunochemotherapy

Lipid metabolism reprograming by SREBP1‐PCSK9 targeting sensitizes pancreatic cancer to immunochemotherapy

Abstract Background Pancreatic cancer's aberrant lipid metabolism fuels cell growth, invasion, and metastasis, yet its impact on immune surveillance and immunotherapy is unclear. This study investigated how sterol regulatory element‐binding transcription factor 1 (SREBP1)‐driven lipid metabolis...

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Main Authors: Mengyi Lao, Xiaozhen Zhang, Zejun Li, Kang Sun, Hanshen Yang, Sicheng Wang, Lihong He, Yan Chen, Hanjia Zhang, Jiatao Shi, Daqian Xu, Tingbo Liang, Xueli Bai
Format: Article
Language:English
Published: Wiley 2025-08-01
Series:Cancer Communications
Subjects:
Pancreatic ductal adenocarcinoma
lipid metabolism
immunochemotherapy
SREBP1
PCSK9
immunosuppressive tumor microenvironment
Online Access:https://doi.org/10.1002/cac2.70038
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Summary:Abstract Background Pancreatic cancer's aberrant lipid metabolism fuels cell growth, invasion, and metastasis, yet its impact on immune surveillance and immunotherapy is unclear. This study investigated how sterol regulatory element‐binding transcription factor 1 (SREBP1)‐driven lipid metabolism affects the tumor microenvironment (TME) in pancreatic ductal adenocarcinoma (PDAC). Methods Clinical significance of SREBP1 was assessed in a PDAC cohort from China and The Cancer Genome Atlas (TCGA) cohorts. The in vitro mechanisms that SREBP1 regulated programmed cell death‐ligand 1 (PD‐L1) and proprotein convertase subtilisin/kexin type 9 (PCSK9) were investigated using immunofluorescence, flow cytometry, Western blotting, luciferase assays and chromatin immunoprecipitation. In vivo studies using PDAC‐bearing mice, humanized patient‐derived tumor xenograft (PDX) models, and autochthonous model of mutation (GEMM‐KTC) evaluated the efficacy and mechanisms of programmed death receptor 1 (PD‐1) antibodies and lipid inhibitors. Results Patients responding to anti‐PD‐1 therapy exhibited lower serum lipid levels than non‐responders. Targeting SREBP1 disrupted lipid metabolism, decelerated tumor growth, and boosted the efficacy of immunotherapy for PDAC. Mechanistically, SREBP1 directly bound the PD‐L1 promoter, suppressing its transcription. Meanwhile, PCSK9, a direct transcriptional target of SREBP1, modulated PD‐L1 levels via lysosomal degradation. Consequently, the combination of PCSK9‐neutralizing antibodies with PD‐1 monotherapy showed a robust antitumor effect in both humanized PDX and GEMM‐KTC models. Conclusions The SREBP1‐PCSK9 axis‐mediated lipid metabolism is crucial for triggering immune evasion and resistance to anti‐PD‐1. Targeting the SREBP1‐PCSK9 axis could potentially reverse PDAC's resistance to anti‐PD‐1 therapy.
ISSN:2523-3548

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