Reprogramming tumor-associated macrophages with lipid nanosystems reduces PDAC tumor burden and liver metastasis

Adrián Palencia-Campos; Laura Ruiz-Cañas; Marcelina Abal-Sanisidro; Juan Carlos López-Gil; Sandra Batres-Ramos; Sofia Mendes Saraiva; Balbino Yagüe; Diego Navarro; Sonia Alcalá; Juan A Rubiolo; Nadège Bidan; Laura Sánchez; Simona Mura; Patrick C Hermann; María de la Fuente; Bruno Sainz

doi:10.1186/s12951-024-03010-5

Reprogramming tumor-associated macrophages with lipid nanosystems reduces PDAC tumor burden and liver metastasis

J Nanobiotechnology. 2024 Dec 24;22(1):795. doi: 10.1186/s12951-024-03010-5.

Authors

Adrián Palencia-Campos^{1

2}, Laura Ruiz-Cañas^{1

2

3}, Marcelina Abal-Sanisidro^{4

5

6}, Juan Carlos López-Gil^{1

2

7}, Sandra Batres-Ramos^{1

2}, Sofia Mendes Saraiva^{4

6}, Balbino Yagüe^{1

2}, Diego Navarro^{1

2

7}, Sonia Alcalá^{1

2}, Juan A Rubiolo^{8

9}, Nadège Bidan¹⁰, Laura Sánchez⁸, Simona Mura¹⁰, Patrick C Hermann¹¹, María de la Fuente^{4

6

12}, Bruno Sainz^{13

14

15}

Affiliations

¹ Cancer Stem Cells and Fibroinflammatory Microenvironment Group, Instituto de Investigaciones Biomédicas (IIBm) Sols-Morreale CSIC-UAM, 28029, Madrid, Spain.
² Biomarkers and Personalized Approach to Cancer Group (BIOPAC), Instituto Ramón y Cajal de Investigación Sanitaria (IRYCIS), Area 3 Cancer, 28049, Madrid, Spain.
³ Biobanco Hospital Universitario Ramón y Cajal, IRYCIS, Madrid, Spain.
⁴ Nano-Oncology and Translational Therapeutics Group, IDIS, Complexo Hospitalario Universitario de Santiago de Compostela, 15706, Santiago de Compostela, Spain.
⁵ University of Santiago de Compostela (USC), 15782, Santiago de Compostela, Spain.
⁶ Centro de Investigación Biomédica en Red, CIBERONC, ISCIII, Área Cáncer, Madrid, Spain.
⁷ Department of Biochemistry, Autónoma University of Madrid (UAM), 28029, Madrid, Spain.
⁸ Department of Zoology, Genetics and Physical Anthropology, Faculty of Veterinary, University of Santiago de Compostela (USC), Lugo, Spain.
⁹ Laboratorio Mixto de Biotecnología Acuática, Facultad de Ciencias Bioquímicas y Farmacéuticas, UNR, 2000, Rosario, Argentina.
¹⁰ Université Paris-Saclay, CNRS, Institut Galien Paris-Saclay, 91400, Orsay, France.
¹¹ Department of Internal Medicine I, Ulm University, Ulm, Germany.
¹² DIVERSA Technologies S.L, Edificio Emprendia, Campus Sur, 15782, Santiago de Compostela, Spain.
¹³ Cancer Stem Cells and Fibroinflammatory Microenvironment Group, Instituto de Investigaciones Biomédicas (IIBm) Sols-Morreale CSIC-UAM, 28029, Madrid, Spain. [email protected].
¹⁴ Biomarkers and Personalized Approach to Cancer Group (BIOPAC), Instituto Ramón y Cajal de Investigación Sanitaria (IRYCIS), Area 3 Cancer, 28049, Madrid, Spain. [email protected].
¹⁵ Centro de Investigación Biomédica en Red, CIBERONC, ISCIII, Área Cáncer, Madrid, Spain. [email protected].

Abstract

Background: Pancreatic ductal adenocarcinoma (PDAC) requires innovative therapeutic strategies to counteract its progression and metastatic potential. Since the majority of patients are diagnosed with advanced metastatic disease, treatment strategies targeting not only the primary tumor but also metastatic lesions are needed. Tumor-Associated Macrophages (TAMs) have emerged as central players, significantly influencing PDAC progression and metastasis. Our objective was to validate an innovative therapeutic strategy involving the reprogramming of TAMs using lipid nanosystems to prevent the formation of a pro-metastatic microenvironment in the liver.

Results: In vitro results demonstrate that M2-polarized macrophages lose their M2-phenotype following treatment with lipid nanoemulsions composed of vitamin E and sphingomyelin (VitE:SM), transitioning to an M0/M1 state. Specifically, VitE:SM nanoemulsion treatment decreased the expression of macrophage M2 markers such as Arg1 and Egr2, while M1 markers such as Cd86, Il-1b and Il-12b increased. Additionally, the TGF-βR1 inhibitor Galunisertib (LY2157299) was loaded into VitE:SM nanoemulsions and delivered to C57BL/6 mice orthotopically injected with KPC PDAC tumor cells. Treated mice showed diminished primary tumor growth and reduced TAM infiltration in the liver. Moreover, we observed a decrease in liver metastasis with the nanoemulsion treatment in an intrasplenic model of PDAC liver metastasis. Finally, we validated the translatability of our VitE:SM nanosystem therapy in a human cell-based 3D co-culture model in vivo, underscoring the pivotal role of macrophages in the nanosystem's therapeutic effect in the context of human PDAC metastasis.

Conclusions: The demonstrated effectiveness and safety of our nanosystem therapy highlights a promising therapeutic approach for PDAC, showcasing its potential in reprogramming TAMs and mitigating the occurrence of liver metastasis.

Keywords: Galunisertib; Lipid nanoemulsions; Liver metastasis; Pancreatic ductal adenocarcinoma; Reprogramming; Tumor microenvironment; Tumor-associated macrophages.

MeSH terms

Animals
Carcinoma, Pancreatic Ductal* / drug therapy
Carcinoma, Pancreatic Ductal* / pathology
Cell Line, Tumor
Emulsions / chemistry
Humans
Lipids / chemistry
Liver Neoplasms* / drug therapy
Liver Neoplasms* / secondary
Mice
Mice, Inbred C57BL*
Nanoparticles / chemistry
Pancreatic Neoplasms* / drug therapy
Pancreatic Neoplasms* / pathology
Tumor Burden / drug effects
Tumor Microenvironment / drug effects
Tumor-Associated Macrophages* / drug effects
Vitamin E / chemistry
Vitamin E / pharmacology

Substances

Lipids
Vitamin E
Emulsions

Abstract

MeSH terms

Substances

Grants and funding