Your search keyword '"Jiri Keirsse"' showing total 11 results

1. Myeloid tumor necrosis factor and heme oxygenase-1 regulate the progression of colorectal liver metastases during hepatic ischemia-reperfusion

Author

Jean-François Hastir, Sophie Laurent, P. Demetter, Desislava Germanova, Lionel Larbanoix, Sergei A. Nedospasov, Laurine Verset, Nicolas Preyat, Jiri Keirsse, Sandrine Delbauve, Yvon Elkrim, Arnaud Köhler, Jo A. Van Ginderachter, Véronique Flamand, Vincent Donckier, Cellular and Molecular Immunology, and Department of Bio-engineering Sciences

Subjects

Male, Cancer Research, liver ischemia-reperfusion, Necrosis, Myeloid, Kupffer Cells, Inflammation, Monocytes, 03 medical and health sciences, colorectal metastasis, Mice, 0302 clinical medicine, Medicine, Animals, business.industry, Tumor Necrosis Factor-alpha, Monocyte, Liver Neoplasms, Interleukin, Sciences bio-médicales et agricoles, Heme oxygenase, Mice, Inbred C57BL, medicine.anatomical_structure, Oncology, Liver, Tumor progression, inflammation, 030220 oncology & carcinogenesis, Receptor-Interacting Protein Serine-Threonine Kinases, Reperfusion Injury, Cancer research, Disease Progression, Tumor necrosis factor alpha, medicine.symptom, Neoplasm Recurrence, Local, business, Colorectal Neoplasms, Heme Oxygenase-1

Abstract

The liver ischemia-reperfusion (IR) injury that occurs consequently to hepatic resection performed in patients with metastases can lead to tumor relapse for not fully understood reasons. We assessed the effects of liver IR on tumor growth and the innate immune response in a mouse model of colorectal (CR) liver metastasis. Mice subjected to liver ischemia 2 days after intrasplenic injection of CR carcinoma cells displayed a higher metastatic load in the liver, correlating with Kupffer cells (KC) death through the activation of receptor-interating protein 3 kinase (RIPK3) and caspase-1 and a recruitment of monocytes. Interestingly, the immunoregulatory mediators, tumor necrosis factor-α (TNF-α) and heme oxygenase-1 (HO-1) were strongly upregulated in recruited monocytes and were also expressed in the surviving KC following IR. Using TNFflox/flox LysMcre/wt mice, we showed that TNF deficiency in macrophages and monocytes favors tumor progression after IR. The antitumor effect of myeloid cell-derived TNF involved direct tumor cell apoptosis and a reduced expression of immunosuppressive molecules such as transforming growth factor-β, interleukin (IL)-10, inducible nitric oxyde synthase (iNOS), IL-33 and HO-1. Conversely, a monocyte/macrophage-specific deficiency in HO-1 (HO-1flox/flox LysMcre/wt ) or the blockade of HO-1 function led to the control of tumor progression post-liver IR. Importantly, host cell RIPK3 deficiency maintains the KC number upon IR, inhibits the IR-induced innate cell recruitment, increases the TNF level, decreases the HO-1 level and suppresses the tumor outgrowth. In conclusion, tumor recurrence in host undergoing liver IR is associated with the death of antitumoral KC and the recruitment of monocytes endowed with immunosuppressive properties. In both of which HO-1 inhibition would reinforce their antitumoral activity., info:eu-repo/semantics/published

Published

2021

2. Maintenance of B cells during chronic murine Trypanosoma brucei gambiense infection

Author

Jiri Keirsse, Magdalena Radwanska, F Kauffmann, Stefan Magez, Théo Baltz, C De Trez, Jennifer Cnops, Eric Muraille, Cellular and Molecular Immunology, Department of Bio-engineering Sciences, and Structural Biology Brussels

Subjects

0301 basic medicine, trypanosomiasis, Trypanosoma brucei gambiense, Trypanosoma spp, 030231 tropical medicine, Immunology, Virulence, Inflammation, Spleen, Apoptosis, Biology, 03 medical and health sciences, Interferon-gamma, Mice, 0302 clinical medicine, Immune system, parasitic diseases, medicine, Animals, Interferon gamma, B-Lymphocytes, Mice, Inbred BALB C, B lymphocyte, Tumor Necrosis Factor-alpha, medicine.disease, Virology, 030104 developmental biology, medicine.anatomical_structure, Trypanosomiasis, African, inflammation, Parasitic disease, Chronic Disease, Parasitology, Tumor necrosis factor alpha, Female, medicine.symptom, Trypanosomiasis, medicine.drug

Abstract

African trypanosomosis is a debilitating parasitic disease occurring in large parts of sub-Saharan Africa. Trypanosoma brucei gambiense accounts for 98% of the reported HAT infections and causes a chronic, gradually progressing disease. Multiple experimental murine models for trypanosomosis have demonstrated inflammation-dependent apoptosis of splenic follicular B (FoB) cells and the destruction of B-cell memory against previously encountered pathogens. Here, we report that during murine infection with a chronic T. b. gambiense field isolate, FoB cells are retained. This coincided with reduced levels of IFN-γ and TNF-α during the acute phase of the infection. This result suggests that in chronic infections with low virulent parasites, less inflammation is elicited and consequently no FoB cell destruction occurs.

Published

2016

3. The role of hepatic macrophages in liver metastasis

Author

Jo A. Van Ginderachter, Xenia Geeraerts, Jiri Keirsse, Helena Van Damme, Geert Raes, Alain Beschin, Faculty of Sciences and Bioengineering Sciences, Cellular and Molecular Immunology, and Department of Bio-engineering Sciences

Subjects

0301 basic medicine, Liver Neoplasms/immunology, Kupffer Cells, Immunology, Macrophages/immunology, Biology, Metastasis, 03 medical and health sciences, Immune system, Cytokines/immunology, Liver/immunology, medicine, Homeostasis, Macrophage, Animals, Humans, Neoplasm Metastasis, Liver immunology, Macrophages, Liver Neoplasms, Kupffer cell, Kupffer Cells/immunology, medicine.disease, Hepatic metastasis, 030104 developmental biology, medicine.anatomical_structure, Liver, Hepatocytes/immunology, Hepatocytes, Cancer research, Homeostasis/immunology, Cytokines, Hepatic macrophage, Target organ

Abstract

The liver is a major target organ for metastasis of both gastrointestinal and extra-gastrointestinal cancers. Due to its frequently inoperable nature, liver metastasis represents a leading cause of cancer-associated death worldwide. In the past years, the pivotal role of the immune system in this process is being increasingly recognised. In particular, the role of the hepatic macrophages, both recruited monocyte-derived macrophages (Mo-Mfs) and tissue-resident Kupffer cells (KCs), has been shown to be more versatile than initially imagined. However, the lack of tools to easily distinguish between these two macrophage populations has hampered the assignment of particular functionalities to specific hepatic macrophage subsets. In this Review, we highlight the most remarkable findings regarding the origin and functions of hepatic macrophage populations, and we provide a detailed description of their distinct roles in the different phases of the liver metastatic process.

Published

2018

4. STAT of the union: Dynamics of distinct tumor-associated macrophage subsets governed by STAT1

Author

Eva Van Overmeire, Damya Laoui, Jo A. Van Ginderachter, Jiri Keirsse, Qods Lahmar, and Stefano Bonelli

Subjects

Stromal cell, biology, Monocyte, Immunology, Context (language use), Tumor-associated macrophage, Gene signature, medicine.anatomical_structure, Tumor progression, Cancer research, medicine, biology.protein, Immunology and Allergy, STAT1, Macrophage proliferation

Abstract

The tumor stroma has long been ignored as therapeutic target, but it has become clear that several stromal cell types play a nonredundant role during tumor progression. In particular, macrophages possess the capacity to stimulate tumor growth and metastasis via multiple mechanisms. In this issue of the European Journal of Immunology, a study by Tymoszuk et al. Eur. J. Immunol. 2014. 44: 2247-2262 demonstrates that both monocyte recruitment and local macrophage proliferation determines the tumor-associated macrophage (TAM) pool size in HER2/Neu-driven mammary carcinomas. These tumors contain two main TAM subsets--MHC class II (MHC-II)(lo) F4/80(hi) and MHC-II(hi) F4/80(lo)--similar to what was observed in other tumor models. Interestingly, only the MHC-II(lo) F4/80(hi) subset is largely absent in a STAT1-deficient background. STAT1 induces the expression of CSF-1, which in turn drives TAM proliferation and possibly also the M2 gene signature of MHC-II(lo) F4/80(hi) TAM. Conversely, STAT1 deficiency upregulates M2 gene expression in MHC-II(hi) F4/80(lo) TAM, demonstrating that both TAM subsets are differentially regulated, probably as a consequence of their distinct intratumoral localization. In this Commentary, we place these findings in the context of current knowledge and propose new avenues for future research.

Published

2014

5. The tumour microenvironment harbours ontogenically distinct dendritic cell populations with opposing effects on tumour immunity

Author

Massimiliano Mazzone, Louis Boon, Charlotte L. Scott, Martin Guilliams, Jens Serneels, Xenia Geeraerts, Yannick Morias, Jiri Keirsse, Dorine Sichien, Jo A. Van Ginderachter, Damya Laoui, Patrick De Baetselier, Qods Lahmar, Eva Van Overmeire, Yvon Elkrim, Mate Kiss, Evangelia Bolli, Department of Bio-engineering Sciences, Cellular and Molecular Immunology, Faculty of Sciences and Bioengineering Sciences, and Vriendenkring VUB

Subjects

0301 basic medicine, SUBSETS, medicine.medical_treatment, General Physics and Astronomy, Inbred C57BL, Transgenic, Monocytes, Mice, Cancer immunotherapy, T-Lymphocyte Subsets, Neoplasms, Medicine and Health Sciences, Tumor Microenvironment, MACROPHAGES, Lymph node, IN-VIVO, Inbred BALB C, Cells, Cultured, Mice, Knockout, education.field_of_study, Mice, Inbred BALB C, Multidisciplinary, Tumor, Cultured, CYTOKINE GM-CSF, INTRATUMORAL DELIVERY, Multidisciplinary Sciences, medicine.anatomical_structure, DIFFERENTIATION, Science & Technology - Other Topics, CANCER-IMMUNOTHERAPY, Immunotherapy, Reprogramming, STEADY-STATE, Science, Cells, Knockout, Population, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, education, Tumor microenvironment, Science & Technology, Macrophages, Dendritic Cells, Mice, Inbred C57BL, Biology and Life Sciences, General Chemistry, Dendritic cell, 030104 developmental biology, Immunology, Cancer research, T-CELLS, CD8, RESPONSES

Abstract

Various steady state and inflamed tissues have been shown to contain a heterogeneous DC population consisting of developmentally distinct subsets, including cDC1s, cDC2s and monocyte-derived DCs, displaying differential functional specializations. The identification of functionally distinct tumour-associated DC (TADC) subpopulations could prove essential for the understanding of basic TADC biology and for envisaging targeted immunotherapies. We demonstrate that multiple mouse tumours as well as human tumours harbour ontogenically discrete TADC subsets. Monocyte-derived TADCs are prominent in tumour antigen uptake, but lack strong T-cell stimulatory capacity due to NO-mediated immunosuppression. Pre-cDC-derived TADCs have lymph node migratory potential, whereby cDC1s efficiently activate CD8+ T cells and cDC2s induce Th17 cells. Mice vaccinated with cDC2s displayed a reduced tumour growth accompanied by a reprogramming of pro-tumoural TAMs and a reduction of MDSCs, while cDC1 vaccination strongly induces anti-tumour CTLs. Our data might prove important for therapeutic interventions targeted at specific TADC subsets or their precursors., Dendritic cells are antigen-presenting cells consisting of distinct subsets originating from different lineages. Here, the authors identify the subsets of dendritic cells populating the tumour tissue in both mice and humans and find they have opposing functions in regulating the anti-tumour immune response.

Published

2016

6. Ischemia-induced tumor progression after portal triad clamping in a murine model of colorectal liver metastases: Roles of TNF-a and HO-1

Author

Véronique Flamand, Desislava Germanova, Oberdan Leo, Arnaud Köhler, Pieter Demetter, Laurine Verset, Jo A. Van Ginderachter, Nicolas Preyat, Sandrine Delbauve, Vincent Donckier, and Jiri Keirsse

Subjects

Cancer Research, Portal triad, Innate immune system, business.industry, Inflammatory response, Ischemia, food and beverages, medicine.disease, Liver ischemia, medicine.anatomical_structure, Oncology, Murine model, Tumor progression, medicine, Cancer research, Tumor necrosis factor alpha, business

Abstract

e15539Background: Liver ischemia and reperfusion (I/R) was shown to cause an inflammatory response that can result in metastatic progression. A better understanding of this innate immune cell-depen...

Published

2018

7. Tissue-resident versus monocyte-derived macrophages in the tumor microenvironment

Author

Kiavash Movahedi, Eva Van Overmeire, Jo A. Van Ginderachter, Damya Laoui, Jiri Keirsse, Qods Lahmar, Department of Bio-engineering Sciences, and Cellular and Molecular Immunology

Subjects

0301 basic medicine, Cancer Research, Tumor microenvironment, Microglia, Monocyte, Macrophages, Kupffer cell, Context (language use), Biology, Monocytes, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Oncology, Neoplasms, Immunology, Genetics, medicine, Tumor Microenvironment, Macrophage, Animals, Humans, Progenitor cell, Yolk sac

Abstract

The tumor-promoting role of macrophages has been firmly established in most cancer types. However, macrophage identity has been a matter of debate, since several levels of complexity result in considerable macrophage heterogeneity. Ontogenically, tissue-resident macrophages derive from yolk sac progenitors which either directly or via a fetal liver monocyte intermediate differentiate into distinct macrophage types during embryogenesis and are maintained throughout life, while a disruption of the steady state mobilizes monocytes and instructs the formation of monocyte-derived macrophages. Histologically, the macrophage phenotype is heavily influenced by the tissue microenvironment resulting in molecularly and functionally distinct macrophages in distinct organs. Finally, a change in the tissue microenvironment as a result of infectious or sterile inflammation instructs different modes of macrophage activation. These considerations are relevant in the context of tumors, which can be considered as sites of chronic sterile inflammation encompassing subregions with distinct environmental conditions (for example, hypoxic versus normoxic). Here, we discuss existing evidence on the role of macrophage subpopulations in steady state tissue and primary tumors of the breast, lung, pancreas, brain and liver.

Published

2015

8. Targeting Cell-Intrinsic and Cell-Extrinsic Mechanisms of Intravasation in Invasive Breast Cancer

Author

Eva Van Overmeire, Jiri Keirsse, Jo A. Van Ginderachter, Damya Laoui, Department of Bio-engineering Sciences, and Cellular and Molecular Immunology

Subjects

Cell, Breast Neoplasms, Biology, Biochemistry, Article, Paracrine signalling, Breast cancer, CSF-1, Biomarkers, Tumor, medicine, Carcinoma, Animals, Humans, Neoplasm Invasiveness, skin and connective tissue diseases, Receptor, Autocrine signalling, Molecular Biology, Mena protein, Macrophages, Carcinoma, Ductal, Breast, Microfilament Proteins, Transendothelial and Transepithelial Migration, Intravasation, Cell Biology, medicine.disease, Neoplasm Proteins, medicine.anatomical_structure, Cancer cell, Immunology, Cancer research, Female, Invasive breast cancer, CSF-1R

Abstract

Metastasis is a complex, multistep process of cancer progression that has few treatment options. A critical event is the invasion of cancer cells into blood vessels (intravasation), through which cancer cells disseminate to distant organs. Breast cancer cells with increased abundance of Mena [an epidermal growth factor (EGF)–responsive cell migration protein] are present with macrophages at sites of intravasation, called TMEM sites (for tumor microenvironment of metastasis), in patient tumor samples. Furthermore, the density of these intravasation sites correlates with metastatic risk in patients. We found that intravasation of breast cancer cells may be prevented by blocking the signaling between cancer cells and macrophages. We obtained invasive breast ductal carcinoma cells of various subtypes by fine-needle aspiration (FNA) biopsies from patients and found that, in an in vitro transendothelial migration assay, cells that migrated through a layer of human endothelial cells were enriched for the transcript encoding MenaINV, an invasive isoform of Mena. This enhanced transendothelial migration required macrophages and occurred with all of the breast cancer subtypes. Using mouse macrophages and the human cancer cells from the FNAs, we identified paracrine and autocrine activation of colony-stimulating factor-1 receptor (CSF-1R). The paracrine or autocrine nature of the signal depended on the breast cancer cell subtype. Knocking down MenaINV or adding an antibody that blocks CSF-1R function prevented transendothelial migration. Our findings indicate that MenaINV and TMEM frequency are correlated prognostic markers and CSF-1 and MenaINV may be therapeutic targets to prevent metastasis of multiple breast cancer subtypes.

Published

2014

9. NK-, NKT- and CD8-Derived IFNγ Drives Myeloid Cell Activation and Erythrophagocytosis, Resulting in Trypanosomosis-Associated Acute Anemia

Author

Carl De Trez, Florence Kauffmann, Mark Barkhuizen, Stefan Magez, Jiri Keirsse, Jennifer Cnops, Louis Boon, Roanne Keeton, Benoit Stijlemans, Frank Brombacher, Division of Immunology, Faculty of Health Sciences, Department of Bio-engineering Sciences, and Cellular and Molecular Immunology

Subjects

Erythrocytes, Myeloid, Cell Separation, Parasitemia, CD8-Positive T-Lymphocytes, Mice, Myeloid Cells, lcsh:QH301-705.5, Mice, Knockout, Anemia, Flow Cytometry, Natural killer T cell, Adoptive Transfer, Erythrophagocytosis, Killer Cells, Natural, medicine.anatomical_structure, Female, medicine.symptom, Research Article, lcsh:Immunologic diseases. Allergy, Bone marrow cells, Immunology, T cells, Cytotoxic T cells, Inflammation, Spleen, Biology, Microbiology, Interferon-gamma, Immune system, Phagocytosis, Virology, Genetics, medicine, Animals, Molecular Biology, Macrophages, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Trypanosomiasis, African, lcsh:Biology (General), Natural Killer T-Cells, Parasitology, lcsh:RC581-607, CD8, Cloning

Abstract

African trypanosomes are the causative agents of Human African Trypanosomosis (HAT/Sleeping Sickness) and Animal African Trypanosomosis (AAT/Nagana). A common hallmark of African trypanosome infections is inflammation. In murine trypanosomosis, the onset of inflammation occurs rapidly after infection and is manifested by an influx of myeloid cells in both liver and spleen, accompanied by a burst of serum pro-inflammatory cytokines. Within 48 hours after reaching peak parasitemia, acute anemia develops and the percentage of red blood cells drops by 50%. Using a newly developed in vivo erythrophagocytosis assay, we recently demonstrated that activated cells of the myeloid phagocytic system display enhanced erythrophagocytosis causing acute anemia. Here, we aimed to elucidate the mechanism and immune pathway behind this phenomenon in a murine model for trypanosomosis. Results indicate that IFNγ plays a crucial role in the recruitment and activation of erythrophagocytic myeloid cells, as mice lacking the IFNγ receptor were partially protected against trypanosomosis-associated inflammation and acute anemia. NK and NKT cells were the earliest source of IFNγ during T. b. brucei infection. Later in infection, CD8+ and to a lesser extent CD4+ T cells become the main IFNγ producers. Cell depletion and transfer experiments indicated that during infection the absence of NK, NKT and CD8+ T cells, but not CD4+ T cells, resulted in a reduced anemic phenotype similar to trypanosome infected IFNγR-/- mice. Collectively, this study shows that NK, NKT and CD8+ T cell-derived IFNγ is a critical mediator in trypanosomosis-associated pathology, driving enhanced erythrophagocytosis by myeloid phagocytic cells and the induction of acute inflammation-associated anemia., Author Summary African trypanosomes are the causative agents of Human and Animal African Trypanosomosis, impairing economic development and causing death throughout the African continent. Anemia and inflammation are hallmark features of virtually every type of trypanosome infection. During experimental murine trypanosomosis, early inflammation causes enhanced red blood cell phagocytosis by cells of the myeloid phagocytic system, leading to severe anemia within 48 hours past peak parasitemia. Here, we identify the pro-inflammatory cytokine IFNγ as the main driver of the early inflammatory reaction and enhanced red blood cell phagocytosis. This IFNγ is derived consecutively by NK, NKT and CD8+ T cells, hence these cells all play a crucial role in the induction of inflammation and anemia.

Published

2015

10. Murine Liver Myeloid Cell Isolation Protocol

Author

Alain Beschin, Benoit Stijlemans, Chloé Abels, Lea Brys, Jiri Keirsse, Amanda Sparkes, Yvon Elkrim, Jo A. Van Ginderachter, Patrick De Baetselier, Department of Bio-engineering Sciences, Cellular and Molecular Immunology, and Faculty of Sciences and Bioengineering Sciences

Subjects

Liver injury, Myeloid, business.industry, Strategy and Management, Mechanical Engineering, Metals and Alloys, medicine.disease, Industrial and Manufacturing Engineering, medicine.anatomical_structure, Monocyte-Derived Macrophages, medicine, Cancer research, Cell isolation, Murine liver, business

Abstract

In homeostasis, the liver is critical for the metabolism of nutrients including sugars, lipids, proteins and iron, for the clearance of toxins, and to induce immune tolerance to gut-derived antigens. These functions predispose the liver to infection by blood-borne pathogens, and to a variety of diseases ranging from toxin and medication-induced disorders (CCl4, acetaminophen) to metabolic disorders (steatohepatitis, alcoholic liver disease, biliary obstruction, cholestasis) or autoimmunity. Chronic liver injury often progresses to life threatening fibrosis and can end in liver cirrhosis and hepatocellular carcinoma (Pellicoro et al., 2014). The liver contains parenchymal cells or hepatocytes that make up the majority of hepatic cells. It also contains non-parenchymal structural cells such as sinusoidal endothelial cells and a large number of non-parenchymal innate immune cells, mainly monocytes, neutrophils, macrophages, DCs, NK and NKT cells that can trigger an adaptive immune response in the case of infections or other pathogenic insults (Jenne and Kubes, 2013). How this immune response is regulated determines the extent of acute and chronic liver injury (Stijlemans et al., 2014). In this context, liver macrophages have been demonstrated to play central but divergent (from initiating to resolving) functions in liver injury (Sica et al., 2014). It has become clear in the last years that hepatic macrophages consist of two classes, tissue-resident macrophages, the Kupffer cells (KCs) originating from yolk sac/fetal liver progenitors and tissue-infiltrating macrophages originating from bone marrow-derived Ly6CHi monocytes (Jinhoux and Jung, 2014; Tacke and Zimmerman, 2014). Distinguishing the activities of KCs from those of monocyte-derived macrophages during liver injury or repair is currently a frontline research topic in the macrophage field. Indeed, considering that clinical management of liver failure remains problematic, a better understanding of the immune mechanisms regulating liver injury is expected to allow the development of new therapeutic modalities. Here, we describe an isolation technique for liver non-parenchymal polymorphonuclear (PMN) and mononuclear myeloid cells permitting their molecular and functional characterization.

11. Tumor hypoxia does not drive differentiation of tumor-associated macrophages but rather fine-tunes the M2-like macrophage population

Author

Giusy Di Conza, Damya Laoui, Kiavash Movahedi, Isabelle Houbracken, Oussama Karroum, Yannick Morias, Patrick De Baetselier, Peter Carmeliet, Eva Van Overmeire, Massimiliano Mazzone, Elio Schouppe, Bénédicte F. Jordan, Jo A. Van Ginderachter, Jiri Keirsse, Chiara Aldeni, Conny Gysemans, Yvon Elkrim, Department of Bio-engineering Sciences, Cellular and Molecular Immunology, Pathological Anatomy, Basic (bio-) Medical Sciences, Cell Differentiation, and UCL - SSS/LDRI - Louvain Drug Research Institute

Subjects

Cancer Research, Myeloid, Animals, Cell Differentiation, Cell Hypoxia, Disease Models, Animal, Female, Macrophages, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neoplasms, Transcriptome, hypoxia-sensitive genes, Biology, Inbred C57BL, Transgenic, stomatognathic system, In vivo, Gene expression, medicine, skin and connective tissue diseases, Tumor hypoxia, Animal, Hypoxia (medical), Phenotype, PHD2+/+ → PHD2+/−, medicine.anatomical_structure, Oncology, Integrin alpha M, Disease Models, Cancer cell, Immunology, Cancer research, biology.protein, prolyl hydroxylase domain 2 (PHD2), medicine.symptom, MHC-IIlo MHC-IIhi, hormones, hormone substitutes, and hormone antagonists

Abstract

Tumor-associated macrophages (TAM) are exposed to multiple microenvironmental cues in tumors, which collaborate to endow these cells with protumoral activities. Hypoxia, caused by an imbalance in oxygen supply and demand because of a poorly organized vasculature, is often a prominent feature in solid tumors. However, to what extent tumor hypoxia regulates the TAM phenotype in vivo is unknown. Here, we show that the myeloid infiltrate in mouse lung carcinoma tumors encompasses two morphologically distinct CD11bhiF4/80hiLy6Clo TAM subsets, designated as MHC-IIlo and MHC-IIhi TAM, both of which were derived from tumor-infiltrating Ly6Chi monocytes. MHC-IIlo TAM express higher levels of prototypical M2 markers and reside in more hypoxic regions. Consequently, MHC-IIlo TAM contain higher mRNA levels for hypoxia-regulated genes than their MHC-IIhi counterparts. To assess the in vivo role of hypoxia on these TAM features, cancer cells were inoculated in prolyl hydroxylase domain 2 (PHD2)-haplodeficient mice, resulting in better-oxygenated tumors. Interestingly, reduced tumor hypoxia did not alter the relative abundance of TAM subsets nor their M2 marker expression, but specifically lowered hypoxia-sensitive gene expression and angiogenic activity in the MHC-IIlo TAM subset. The same observation in PHD2+/+→ PHD2+/− bone marrow chimeras also suggests organization of a better-oxygenized microenvironment. Together, our results show that hypoxia is not a major driver of TAM subset differentiation, but rather specifically fine-tunes the phenotype of M2-like MHC-IIlo TAM. Cancer Res; 74(1); 24–30. ©2013 AACR.