Your search keyword '"M Spella"' showing total 47 results

1. Role of angiopoietins in mesothelioma progression

Author

Maria-Eleni Vazakidou, Androniki Kollintza, Sophia Magkouta, Ioannis Kalomenidis, Ioannis Skianis, M Spella, Georgios T. Stathopoulos, Charalampos Moschos, and Apostolos Pappas

Subjects

Male, Mesothelioma, Vascular Endothelial Growth Factor A, 0301 basic medicine, Tumor angiogenesis, Angiogenesis, Immunology, Biochemistry, Angiopoietin-2, Mice, 03 medical and health sciences, 0302 clinical medicine, Vascularity, In vivo, Angiopoietin-1, Animals, Humans, Immunology and Allergy, Medicine, Clinical significance, RNA, Messenger, Molecular Biology, Mice, Inbred BALB C, Neovascularization, Pathologic, business.industry, Angiopoietins, Hematology, medicine.disease, Pathophysiology, Mice, Inbred C57BL, Platelet Endothelial Cell Adhesion Molecule-1, 030104 developmental biology, 030220 oncology & carcinogenesis, Disease Progression, cardiovascular system, Cancer research, Female, medicine.symptom, business, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Background and objective Anti-angiogenic treatment has been recently shown to be clinically beneficial for mesothelioma patients. Angiopoietins-1 and -2 are key regulators of tumor angiogenesis. Ang-1 is mainly known to promote angiogenesis and vessel stability, while Ang-2 could serve as an antagonist of Ang-1 causing vessel regression and destabilization or enhance angiogenesis in a context-dependent manner. We hypothesized that Ang-1 would promote and Ang2 would halt experimental mesothelioma by affecting tumor angiogenesis. Methods To examine the effects of angiopoietins in mesothelioma angiogenesis and in vivo growth we constructed Ang-1 or Ang-2 overexpressing AE17 and AB1 mesothelioma cells and implanted them in the respective syngeneic animals. We also explored the clinical relevance of our observations using the human tumoral mRNAseq data available in the TCGA database. Results and conclusions Ang-1 promotes mesothelioma angiogenesis and growth while the effect of Ang-2 is context-dependent. Low Ang-1 levels in human mesotheliomas are associated with the epitheloid subtype. Tumors of high Ang-1, or concurrent high Ang-2 and VEGF expression present high PECAM-1 and CDH5 expression, markers of vascularity and vascular stability, respectively. Our results highlight the importance of angiopoietins in mesothelioma pathophysiology and pave the way for the clinical development of novel anti-angiogenic strategies.

Published

2019

2. Immune-evasion of KRAS-mutant lung adenocarcinoma mediated by cAMP response element-binding protein

Author

Evanthia Tourkochristou, Marianthi Iliopoulou, Nikolitsa Spiropoulou, Torsten Goldmann, Ioanna Giopanou, Theo Mantamadiotis, Ioannis Lilis, M Spella, Aigli Korfiati, Georgia A. Giotopoulou, Antonia Marazioti, Sebastian Marwitz, Rosero C, Giannoula Ntaliarda, F Kalogianni, and Georgios T. Stathopoulos

Subjects

Stromal cell, biology, Neurodegeneration, Cancer, medicine.disease, medicine.disease_cause, CREB, Immune system, medicine, biology.protein, Cancer research, Adenocarcinoma, KRAS, CREB1

Abstract

cAMP response element-binding protein (CREB) mediates proliferative and inflammatory gene transcription in neurodegeneration and cancer, but its role in malignant immune-evasion of lung adenocarcinoma (LUAD) is unknown. We show that human LUAD of smokers are frequently altered along the CREB pathway and we employ mouse models to discover that KRAS-mutant LUAD co- opt CREB to evade immune rejection by tumoricidal neutrophils. For this, KRAS- driven CREB activation suppresses CXC-chemokine expression and prevents recruitment of CXCR1+ neutrophils. CREB1 is shown to be pro-tumorigenic in five different LUAD models, a function that is dependent on host CXCR1. Pharmacologic CREB blockade prevents tumor growth and restores neutrophil recruitment only when initiated before immune-evasion of KRAS-mutant LUAD. CREB and CXCR1 expression in human LUAD are compartmentalized to tumor and stromal cells, respectively, while CREB-regulated genes and neutrophils impact survival. In summary, CREB-mediated immune evasion of KRAS-mutant LUAD relies on signaling to neutrophil CXCR1 and is actionable.

Published

2021

3. Tumor-secreted versican co-opts myeloid IKKβ during metastasis

Author

Fiona E. Yull, G Skiadas, David Brunn, Michael Lindner, M Spella, Giannoula Ntaliarda, Rajkumar Savai, Weiss Sa, Mario A.A. Pepe, Rudolf Hatz, Georgios T. Stathopoulos, Ioanna Giopanou, Petrera A, Ina Koch, Bouloukou E, Timothy S. Blackwell, Antonia Marazioti, Malamati Vreka, Georgia A. Giotopoulou, Ioannis Lilis, Dieter E. Jenne, K. Arendt, Juergen Behr, Stefanie M. Hauck, and Anne-Sophie Lamort

Subjects

Tumor microenvironment, Myeloid, biology, Chemistry, Interleukin, IκB kinase, medicine.disease, Metastasis, medicine.anatomical_structure, Cancer cell, biology.protein, medicine, Cancer research, Versican, Gene silencing

Abstract

The mechanisms tumor cells use to hijack the immune system are largely uncharted. Here we used bioluminescent nuclear factor (NF)-κB reporter mice and macrophages to discover that metastatic tumors trigger NF-κB activation in host macrophages, dependent on mutant KRAS signaling and delivered via secretory versican. Versican activates NF-κB in tumor-associated macrophages via inhibitor of NF-κB kinase (IKK) β, resulting in release of interleukin (IL)-1β into the tumor microenvironment. Versican silencing in cancer cells or conditional IKKβ deletion in macrophages prevents myeloid NF-κB activation and metastasis. Versican is overexpressed and/or mutated in human cancers and metastatic effusions with KRAS mutations, predicts poor survival, can aid in the development of diagnostic platforms for pleural metastasis, and is druggable via toll-like receptor (TLR) 1/2 inhibition. The data indicate a cardinal role for tumor-derived versican in establishing cross-talk with macrophage IKKβ during metastasis and may foster the development of new therapies and diagnostic tools.

Published

2021

4. Airway cells in adult lung homeostasis and carcinogenesis

Author

M Spella, Ioannis Lilis, Georgios T. Stathopoulos, and Bouloukou E

Subjects

Lung, business.industry, Cell, respiratory system, Cell fate determination, Bleomycin, medicine.disease_cause, medicine.disease, respiratory tract diseases, Green fluorescent protein, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Cancer research, Medicine, Respiratory system, business, Carcinogenesis, Lung cancer

Abstract

Background: Respiratory epithelial dynamics and molecular signatures participating in adult lung maintenance and chemical carcinogenesis need to be clearly identified. Aims: We used mouse models of lung epithelial fate to chart the contribution of the respective cell lineages in the mouse lung during aging and after challenge with noxious and carcinogenic insults. Methods: We generated lung cell fate reporter mice by crossing Scgb1a1.Cre, Sftpc.Cre and Lyz2.Cre mice with the mT/mG Cre-reporter mice, resulting in expression of GFP in all Cre-recombined cells. These reporter mice were then subjected to various noxious (bleomycin and naphthalene administration at 0.08 units and 250 mg/kg, respectively; n≥10 mice/group) and carcinogenic insults (urethane administration at 1 g/Kg; n≥10 mice/group). The GFP-labelled cells were then monitored in the injured lungs and the developed adenocarcinomas. Results: We observed that lung adenocarcinomas were spatially linked to neighboring airways. The cells of all tumors of GFP;Sftpc.Cre mice and all cells of ~50% of GFP;Lyz2.Cre tumors were GFP+. Interestingly, a significant cell proportion of all tumors of GFP;Scgb1a1.Cre mice were GFP+, indicating a bronchial origin. Furthermore, the airway-specific signature was redistributed to the alveoli after toxic insults and resulted in marked contributions of airway-labeled cells to injury-recovered alveoli. Our results also indicate that airway cells maintain Kras mutations, possibly contributing to lung cancer initiation. Conclusions: Our findings identify an involvement of airway molecular programs in alveolar maintenance and carcinogen-induced lung adenocarcinomas. Funding General Secretariat for Research and Technology (GSRT) and Hellenic Foundation for Research and Innovation (HFRI) grant #1853.

Published

2021

5. Macrophages in lung adenocarcinoma

Author

M Spella, Ioannis Lilis, Georgios T. Stathopoulos, and Giannoula Ntaliarda

Subjects

business.industry, Cancer cell, medicine, Cancer research, Cancer, Adenocarcinoma, Macrophage, Tumor initiation, Genetically modified animal, medicine.disease, Lung cancer, business, Metastasis

Abstract

Lung cancer is the most lethal cancer worldwide, and its epidemic appears to be on a continuous rise despite smoking prevention and cessation programs. It is generally believed that inflammation alters the microenvironment of tobacco carcinogen-mutated respiratory epithelial cells, fostering their survival and sustained growth instead of their eradication. Macrophages are inflammatory leukocytes that play key and contradicting roles in tumor initiation and progression, but the reason for their divergent functions in cancer remain elusive. This study is designed in order to clarify macrophages’ role during the development of lung adenocarcinoma. To investigate this, we employed mouse models of early adenocarcinoma induction, in parallel with in vivo models of adenocarcinoma growth and metastasis. The aforementioned models have been combined with genetically modified animal models of macrophage localization and ablation to study the recruitment of these cells to tumors as well as their interaction with cancer cells at different stages of the disease. Moreover, we developed in vitro and utilized in vivo different macrophage types to clarify their distinctive roles in lung adenocarcinoma progression. Our results indicate that macrophages are actively recruited to lung tumors and may play contradicting roles in lung adenocarcinoma development. Although, GM-CSF macrophages function as innocent bystanders, M-CSF macrophages induce both tumor initiation in the respiratory epithelium and the progression of the disease. M-CSF macrophages were found here to fuel KRAS-mutant lung adenocarcinoma formation and growth in mice by secreting IL-1β setting a rational framework for further study of macrophage functions in lung tumors.

Published

2021

6. Preclinical evaluation of IL-1ß inhibition against KRAS-mutant lung adenocarcinoma

Author

M Spella, Giannoula Ntaliarda, Georgios T. Stathopoulos, M De Chateau, and G Skiadas

Subjects

Lung, business.industry, medicine.disease_cause, medicine.disease, Primary tumor, respiratory tract diseases, medicine.anatomical_structure, In vivo, Cancer cell, Cancer research, medicine, Adenocarcinoma, Malignant pleural effusion, KRAS, Mesothelioma, business

Abstract

Malignant pleural effusion (MPE) constitutes a negative prognostic factor in patients suffering from lung adenocarcinoma and mesothelioma. Our lab has previously highlighted a role for NF-κΒ activation in promoting tumor growth and MPE development in Kras-mutant tumors, a phenomenon driven by host IL-1β. Thus, blocking IL-1β-induced NF-κB signaling may represent an attractive route for inhibiting tumor development and pleural fluid accumulation in preclinical models of Kras-mutant lung adenocarcinoma and mesothelioma. To test this, we used a novel, specific inhibitor of IL-1β signaling called isunakinra and cancer cell lines stably expressing a NF-κB reporter bioluminescent plasmid, in both in vitro and in vivo assays. Isunakinra was successful in reducing IL-1β-elicited tumor NF-κB signaling, specifically in Kras-mutant and not in Kras-wild type cancer cell lines, as assessed by the bioluminescence readout of these cells corresponding to NF-κB activation. When these Kras-mutant cancer cells were delivered to the pleural space of syngeneic mice followed by administration of isunakinra, a marked reduction in NF-κB activation and pleural fluid formation was observed compared to the saline-treated control mice. Similar results were also obtained using the flank tumor model, in which the drug was effective in reducing primary tumor volume and occurrence of pulmonary metastases. Collectively, our results show that IL-1β inhibition may constitute a novel therapeutic strategy to target KRAS-mutant tumors.

Published

2021

7. KRASsignalling in malignant pleural mesothelioma

Author

Michael Lindner, Marianthi Iliopoulou, Mario A.A. Pepe, Ina Koch, Sophia G. Antimisiaris, Marc Grégoire, I Psallidas, Rudolf Hatz, Ioannis Lilis, Anthi C. Krontira, M Spella, Darcy E. Wagner, Georgios T. Stathopoulos, C. M. Hackl, A. Marazioti, Ioanna Giopanou, Helen Papadaki, S. Deshayes, Malamati Vreka, Christophe Blanquart, Juergen Behr, and Anne-Sophie Lamort

Subjects

BAP1, Pleural effusion, Point mutation, Pleural cavity, Biology, medicine.disease_cause, medicine.disease, respiratory tract diseases, medicine.anatomical_structure, CDKN2A, medicine, Cancer research, Ectopic expression, KRAS, Gene

Abstract

Malignant pleural mesothelioma (MPM) arises from mesothelial cells lining the pleural cavity of asbestos-exposed individuals and rapidly leads to the development of pleural effusion and death. MPM harbours loss-of-function mutations in genes likeBAP1, NF2, CDKN2A, andTP53, but isolated deletion of these genes alone in mice does not cause MPM and mouse models of the disease are sparse. Here we show that a significant proportion of human MPM harbour point mutations and copy number alterations in theKRASproto-oncogene. These mutations are likely pathogenic, since ectopic expression of mutantKRASG12Din the pleural mesothelium of conditional mice causes MPM. Murine MPM cell lines derived from these tumours carry the initiatingKRASG12Dlesions, secondaryBap1alterations, and human MPM-like gene expression profiles. Moreover, they are transplantable and actionable by KRAS inhibition. Our results indicate thatKRASmutations likely play an important and underestimated role in MPM, which warrants further exploration.

Published

2020

8. Histologic hallmarks of smoking in the Gauting lung adenocarcinoma donors cohort

Author

A Lamort, Giannoula Ntaliarda, G. Stathopoulos, M Spella, W Kujawa, M Pepe, and Ioannis Lilis

Subjects

Oncology, medicine.medical_specialty, Lung, Angiogenesis, business.industry, Histology, medicine.disease_cause, medicine.disease, medicine.anatomical_structure, Internal medicine, Cohort, medicine, Adenocarcinoma, KRAS, business, Carcinogenesis, Body mass index

Abstract

The Gauting lung adenocarcinoma donors cohort already established that the age and lung functions influence patients´ survival (1). Here, we conducted a retrospective, exploratory combination of clinical information with tumor tissue profiles in 200 patients of this cohort. Relevant tumor mutations (KRAS, EGFR, p53, and NF1), tissue profiling (angiogenesis, inflammation, apoptosis and proliferation rates) were quantified for all patients. Then, 100 patients were randomly selected for a training sub-cohort. Mutation status, tissue profiling and clinical variables (age, sex, body mass index, lung functions, TNM descriptors, tumor location, and histology) were analyzed for correlation with the smoking status. The tumors from smokers positively correlate with KRAS mutation, high body mass index, and proliferation. They also negatively correlate with EGFR and p53 mutations, high lung functions, and angiogenesis. In the training sub-cohort, these variables can discriminate the smoking status of 88% tumors. Those variables were used to analyze a second sub-cohort of 100 other patients and were able to identify the smoking status in 86 percent of the cases. In conclusion, we identified an association of molecular biomarkers and clinical variables that highlight novel tumor genome‐phenome links. This association also discriminates the smoking status of tumors indicating two distinct pathways of carcinogenesis evolution in the lungs. (1) Klotz LV, et al. Comprehensive clinical profiling of the Gauting locoregional lung adenocarcinoma donors. Cancer Med. 2019 Apr;8(4):1486-1499.

Published

2020

9. S7 Mouse lung adenocarcinoma cell lines reveal PRL2C2 as a novel lung tumour promoter

Author

M Spella, Nikolaos I. Kanellakis, Ian D. Pavord, Georgios T. Stathopoulos, Ioannis Psallidas, Dimitra E. Zazara, Malamati Vreka, Ioanna Giopanou, Antonia Marazioti, Theodora Agalioti, Anastassios D. Giannou, NM Rahman, Ioannis Lilis, and Mario A.A. Pepe

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Genetically modified mouse, Pathology, medicine.medical_specialty, education, Cell, Cancer, Biology, medicine.disease, medicine.disease_cause, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, medicine, Cancer research, Gene silencing, Adenocarcinoma, KRAS, Lung cancer

Abstract

Background Carcinogen-inflicted human cancers, including lung tumours harbour thousands of mutations per genome, most of which are unknown (Garraway, LA et al, Cell 2013;153:17–37). Aim To develop a faithful mouse model of human tobacco carcinogen-induced lung adenocarcinoma suitable for the identification of novel oncogenic genes and pathways. Methods We repeatedly managed to obtain several murine lung adenocarcinoma cell lines (MLA) by chronically exposing various mouse strains to different tobacco carcinogens. MLA were characterised for cancer stemness and oncogenes, as well as global gene expression. Results To date, 12 MLA cell lines have been derived from Wt and transgenic mice on the FVB, Balb/c, and C57BL/6 strains by means of urethane or diethylnitrosamine exposure. All MLA were immortal, phenotypically stable, and indefinitely passaged in vitro over a period of over 18 months and/or 60 passages. In addition, all cell lines were oncogenic, transplantable, metastatic, and uniformly lethal in vivo. Interestingly, MLA displayed Kras mutations in codon 61, mono- or bi-allelic Trp53 loss, and expression of lung cancer stemness factors Itgb3 and Lgr6, in amazing similarity to human lung cancers. Microarray revealed that all MLA cell lines heavily overexpressed Prl2c2, encoding proliferin, in comparison to the native lungs. Prl2c2 silencing diminished MLA proliferation and stemness, to a degree comparable with Itgb3 interference. Conclusions MLA are faithful models of human lung adenocarcinoma that led to the discovery of Prl2c2 as a candidate lung tumour promoter. Funding European Research Council Starting Independent Investigator Grant #260524. Respire 2 European Respiratory Society Fellowship, European Respiratory Society Short Term Research Fellowship.

Published

2019

10. A requirement for mast cells in lung adenocarcinoma

Author

Sebastian Marwitz, Georgios T. Stathopoulos, A Marazioti, M Spella, Ioanna Giopanou, Giannoula Ntaliarda, Torsten Goldmann, Ioannis Lilis, Georgia A. Giotopoulou, Maria Oplopoiou, Marina Lianou, Vassilios Papaleonidopoulos, and Vasiliki Bravou

Subjects

Mast (sailing), Lung, medicine.anatomical_structure, business.industry, Cancer research, Medicine, Adenocarcinoma, business, medicine.disease

Published

2018

11. Tumor-derived granulocyte chemotactic protein 2 cooperates with neutrophil proteinase 3 to drive lung adenocarcinoma

Author

Dieter E. Jenne, M Spella, S.A. Weiß, L Klotz, Giannoula Ntaliarda, Marina Lianou, K. Arendt, Anne-Sophie Lamort, Georgios T. Stathopoulos, Mario A.A. Pepe, V. Armenis, Maria Oplopoiou, A Marazioti, I Lillis, K Kauka, Georgia A. Giotopoulou, and Ioanna Giopanou

Subjects

Lung, medicine.anatomical_structure, business.industry, Proteinase 3, Chemokine CXCL6, Cancer research, Medicine, Adenocarcinoma, Tumor-Derived, business, medicine.disease

Published

2018

12. P2.03-48 Tumor-Derived Granulocyte Chemotactic Protein 2 Cooperates with Proteases to Drive Lung Adenocarcinoma

Author

S.A. Weiß, G. Stathopoulos, K. Arendt, M. Spella, A.S. Lamort, Giannoula Ntaliarda, Dieter E. Jenne, Ioannis Lilis, and M Pepe

Subjects

Pulmonary and Respiratory Medicine, Proteases, Lung, medicine.anatomical_structure, Oncology, business.industry, Chemokine CXCL6, medicine, Cancer research, Adenocarcinoma, Tumor-Derived, medicine.disease, business

Published

2019

13. P1.03-30 Transcriptome Signatures of Tobacco Carcinogens on Lung Adenocarcinoma Cell Lines

Author

Nikolaos I. Kanellakis, M Pepe, F Pelizza, A.S. Lamort, M. Spella, and G. Stathopoulos

Subjects

Pulmonary and Respiratory Medicine, Transcriptome, Lung, medicine.anatomical_structure, Oncology, business.industry, Adenocarcinoma cell, medicine, Cancer research, business, Carcinogen

Published

2019

14. Isoform RANK-c affects stem cell properties of breast cancer cells

Author

A.D. Papanastasiou, M. Schizas, M. Spella, H.P. Kalofonos, C. Sirinian, and G. Stathopoulos

Subjects

Gene isoform, business.industry, Cancer research, Rank (graph theory), Medicine, Surgery, General Medicine, Breast cancer cells, Stem cell, business

Published

2019

15. LATE-BREAKING ABSTRACT: Host-environmental IL-1β drives mutant KRAS-IKKα addiction in malignant pleural effusion

Author

Theodora Agalioti, M Spella, Antonia Marazioti, Nikolaos I. Kanellakis, Malamati Vreka, Ioanna Giopanou, Georgios T. Stathopoulos, and Anastasios D. Giannou

Subjects

Kinase, Biology, medicine.disease_cause, Phenotype, digestive system diseases, respiratory tract diseases, Small hairpin RNA, Immune system, Cell culture, medicine, Cancer research, Gene silencing, Tumor necrosis factor alpha, KRAS

Abstract

Introduction: Malignant pleural effusion (MPE) is primarily an immune-mediated manifestation of pleural-metastasized cancers, particularly adenocarcinomas that harbour KRAS mutations ( Δ KRAS ).We have previously determined that NF-κΒ activation in pleural tumor cells drives MPE formation, but the NF-κΒ pathways involved are obscure. Aims and objectives: To investigate the mechanisms of NF-κB activation in pleural tumor cells that leads to MPE development. Methods: We profiled baseline and host-induced NF-κB activity of mouse and human tumor cells, and examined its relationship with KRAS status. We further silenced NF-κB activating kinases aiming to eliminate endogenous and inducible NF-κB activity of mouse and human tumors. Results: Tumor cells bearing KRAS mutations, competent of causing MPE, displayed IL-1β-induced IKKα translocation to the nucleus that was lost when KRAS knockdown was performed. In contrast, cell lines with wt KRAS that do not cause MPE did not respond to IL-1β with nuclear IKKα shuttling. shRNA IKKα, but not IKKβ, silencing of ΔKRAS tumors severely hampered their ability for MPE formation. IKKαoverexpression in wt KRAS tumors failed to restore the MPE-competent phenotype of ΔKRAS tumors, suggesting an addiction of IKKα with Δ KRAS in the tumor cell during MPE development. Furthermore, IL-1β, but not TNFα, originated from host immune cells was required to sustain the MPE-competent phenotype of IKKα-addicted KRAS-mutant tumors. Conclusions: We demonstrate that KRAS- mutant tumor cells require host-IL-1β signaling for MPE precipitation. This phenotype is mediated by IKKα and not IKKβ. This study was supported by a European Research Council Starting Independent Investigator Grant (#260524).

Published

2015

16. Mono and Dually Decorated Nanoliposomes for Brain Targeting, In Vitro and In Vivo Studies

Author

Konstantina Papadia, Georgios T. Stathopoulos, Sophia G. Antimisiaris, Anastassios D. Giannou, Eleni Markoutsa, Alfredo Cagnotto, Mario Salmona, and M Spella

Subjects

Apolipoprotein E, Pharmaceutical Science, Peptide, In Vitro Techniques, Microscopy, Electron, Transmission, In vivo, Humans, Pharmacology (medical), Receptor, Cell Line, Transformed, Pharmacology, chemistry.chemical_classification, Liposome, Chemistry, Organic Chemistry, Brain, Ligand (biochemistry), In vitro, 3. Good health, Nanostructures, Biochemistry, Transferrin, Blood-Brain Barrier, Liposomes, Molecular Medicine, Endothelium, Vascular, Biotechnology

Abstract

Mono- and dual-decorated (DUAL) liposomes (LIP) were prepared, by immobilization of MAb against transferrin (TfR[OX26 or RI7217]) and/or a peptide analogue of ApoΕ3 (APOe) -to target low-density lipoprotein receptor(LPR)-, characterized physicochemically and investigated for BBB-targeting, in-vitro and in-vivo.Human microvascular endothelial cells (hCMEC/D3) were used as BBB model, and brain targeting was studied by in-vivo imaging of DiR-labelled formulations (at two doses and surface ligand densities), followed by ex-vivo organ imaging.LIP diameter was between 100 nm and 150 nm, their stability was good and they were non-cytotoxic. LIP uptake and transport across the hCMEC/D3 cell monolayer was significantly affected by decoration with APOe or MAb, the DUAL exerting an additive effect. Intact vesicle-transcytosis was confirmed by equal transport of hydrophilic and lipophilic labels. In-vivo and ex-vivo results confirmed MAb and DUAL-LIP increased brain targeting compared to non-targeted PEG-LIPs, but not for APOe (also targeting ability of DUAL-LIP was not higher than MAb-LIP). The contradiction between in-vitro and in-vivo results was overruled when in-vitro studies (uptake and monolayer transport) were carried out in presence of serum proteins, revealing their important role in targeted-nanoformulation performance.A peptide analogue of ApoΕ3 was found to target BBB and increase the targeting potential of TfR-MAb decorated LIP, in-vitro, but not in-vivo, indicating that different types of ligands (small peptides and antibodies) are affected differently by in-vivo applying conditions. In-vitro tests, carried out in presence of serum proteins, may be a helpful predictive "targetability" tool.

Published

2013

17. "Crosstalk between non-coding RNAs and transcription factor LRF in non-small cell lung cancer".

Author

Spella M, Bochalis E, Athanasopoulou K, Chroni A, Dereki I, Ntaliarda G, Makariti I, Psarias G, Constantinou C, Chondrou V, and Sgourou A

Abstract

Epigenetic approaches in direct correlation with assessment of critical genetic mutations in non-small cell lung cancer (NSCLC) are currently very intensive, as the epigenetic components underlying NSCLC development and progression have attained high recognition. In this level of research, established human NSCLC cell lines as well as experimental animals are widely used to detect novel biomarkers and pharmacological targets to treat NSCLC. The epigenetic background holds a great potential for the identification of epi-biomarkers for treatment response however, it is highly complex and requires precise definition as these phenomena are variable between NSCLC subtypes and systems origin. We engaged an in-depth characterization of non-coding (nc)RNAs prevalent in human KRAS -mutant NSCLC cell lines A549 and H460 and mouse KRAS -mutant NSCLC tissue by Next Generation Sequencing (NGS) and quantitative Real Time PCRs (qPCRs). Also, the transcription factor (TF) LRF, a known epigenetic silencer, was examined as a modulator of non-coding RNAs expression. Finally, interacting networks underlying epigenetic variations in NSCLC subtypes were created. Data derived from our study highlights the divergent epigenetic profiles of NSCLC of human and mouse origin, as well as the significant contribution of 12qf1: 109,709,060-109,747,960 mouse chromosomal region to micro-RNA upregulated species. Furthermore, the novel epigenetic miR-148b-3p/lnc PVT1/ZBTB7A axis was identified, which differentiates human cell line of lung adenocarcinoma from large cell lung carcinoma, two characteristic NSCLC subtypes. The detailed recording of epigenetic events in NSCLC and combinational studies including networking between ncRNAs and TFs validate the identification of significant epigenetic features, prevailing in NSCLC subtypes and among experimental models. Our results enrich knowledge in the field and empower research on the epigenetic prognostic biomarkers of the disease progression, NSCLC subtypes discrimination and advancement to patient-tailored treatments., Competing Interests: Ifigeneia Makariti is financially supported by BioAnalytica SA, Biotechnology supplier company and also a member of the research team of biology HOU lab. The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2024 The Authors.)

Published

2024

18. Non-Oncogene Addiction of KRAS -Mutant Cancers to IL-1β via Versican and Mononuclear IKKβ.

Author

Spella M, Ntaliarda G, Skiadas G, Lamort AS, Vreka M, Marazioti A, Lilis I, Bouloukou E, Giotopoulou GA, Pepe MAA, Weiss SAI, Petrera A, Hauck SM, Koch I, Lindner M, Hatz RA, Behr J, Arendt KAM, Giopanou I, Brunn D, Savai R, Jenne DE, de Château M, Yull FE, Blackwell TS, and Stathopoulos GT

Abstract

Kirsten rat sarcoma virus (KRAS) -mutant cancers are frequent, metastatic, lethal, and largely undruggable. While interleukin (IL)-1β and nuclear factor (NF)-κB inhibition hold promise against cancer, untargeted treatments are not effective. Here, we show that human KRAS -mutant cancers are addicted to IL-1β via inflammatory versican signaling to macrophage inhibitor of NF-κB kinase (IKK) β. Human pan-cancer and experimental NF-κB reporter, transcriptome, and proteome screens reveal that KRAS -mutant tumors trigger macrophage IKKβ activation and IL-1β release via secretory versican. Tumor-specific versican silencing and macrophage-restricted IKKβ deletion prevents myeloid NF-κB activation and metastasis. Versican and IKKβ are mutually addicted and/or overexpressed in human cancers and possess diagnostic and prognostic power. Non-oncogene KRAS /IL-1β addiction is abolished by IL-1β and TLR1/2 inhibition, indicating cardinal and actionable roles for versican and IKKβ in metastasis.

Published

2023

19. Prognostic phenotypes of early-stage lung adenocarcinoma.

Author

Lamort AS, Kaiser JC, Pepe MAA, Lilis I, Ntaliarda G, Somogyi K, Spella M, Behrend SJ, Giotopoulou GA, Kujawa W, Lindner M, Koch I, Hatz RA, Behr J, Sotillo R, Schamberger AC, and Stathopoulos GT

Subjects

Humans, Phenotype, Prognosis, Proliferating Cell Nuclear Antigen genetics, Prospective Studies, Adenocarcinoma of Lung genetics, Adenocarcinoma of Lung pathology, Lung Neoplasms pathology

Abstract

Background: Survival after curative resection of early-stage lung adenocarcinoma (LUAD) varies and prognostic biomarkers are urgently needed., Methods: Large-format tissue samples from a prospective cohort of 200 patients with resected LUAD were immunophenotyped for cancer hallmarks TP53, NF1, CD45, PD-1, PCNA, TUNEL and FVIII, and were followed for a median of 2.34 (95% CI 1.71-3.49) years., Results: Unsupervised hierarchical clustering revealed two patient subgroups with similar clinicopathological features and genotype, but with markedly different survival: "proliferative" patients (60%) with elevated TP53, NF1, CD45 and PCNA expression had 50% 5-year overall survival, while "apoptotic" patients (40%) with high TUNEL had 70% 5-year survival (hazard ratio 2.23, 95% CI 1.33-3.80; p=0.0069). Cox regression and machine learning algorithms including random forests built clinically useful models: a score to predict overall survival and a formula and nomogram to predict tumour phenotype. The distinct LUAD phenotypes were validated in The Cancer Genome Atlas and KMplotter data, and showed prognostic power supplementary to International Association for the Study of Lung Cancer tumour-node-metastasis stage and World Health Organization histologic classification., Conclusions: Two molecular subtypes of LUAD exist and their identification provides important prognostic information., Competing Interests: Conflict of interest: The authors declare no potential conflicts of interest., (Copyright ©The authors 2022. For reproduction rights and permissions contact permissions@ersnet.org.)

Published

2022

20. KRAS signaling in malignant pleural mesothelioma.

Author

Marazioti A, Krontira AC, Behrend SJ, Giotopoulou GA, Ntaliarda G, Blanquart C, Bayram H, Iliopoulou M, Vreka M, Trassl L, Pepe MAA, Hackl CM, Klotz LV, Weiss SAI, Koch I, Lindner M, Hatz RA, Behr J, Wagner DE, Papadaki H, Antimisiaris SG, Jean D, Deshayes S, Grégoire M, Kayalar Ö, Mortazavi D, Dilege Ş, Tanju S, Erus S, Yavuz Ö, Bulutay P, Fırat P, Psallidas I, Spella M, Giopanou I, Lilis I, Lamort AS, and Stathopoulos GT

Subjects

Animals, Humans, Mice, Signal Transduction, Tumor Suppressor Proteins genetics, Tumor Suppressor Proteins metabolism, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism, Lung Neoplasms genetics, Lung Neoplasms pathology, Mesothelioma genetics, Mesothelioma pathology, Mesothelioma, Malignant genetics, Mesothelioma, Malignant pathology, Pleural Neoplasms genetics, Pleural Neoplasms pathology, Proto-Oncogene Proteins p21(ras) genetics, Proto-Oncogene Proteins p21(ras) metabolism

Abstract

Malignant pleural mesothelioma (MPM) arises from mesothelial cells lining the pleural cavity of asbestos-exposed individuals and rapidly leads to death. MPM harbors loss-of-function mutations in BAP1, NF2, CDKN2A, and TP53, but isolated deletion of these genes alone in mice does not cause MPM and mouse models of the disease are sparse. Here, we show that a proportion of human MPM harbor point mutations, copy number alterations, and overexpression of KRAS with or without TP53 changes. These are likely pathogenic, since ectopic expression of mutant KRAS G12D in the pleural mesothelium of conditional mice causes epithelioid MPM and cooperates with TP53 deletion to drive a more aggressive disease form with biphasic features and pleural effusions. Murine MPM cell lines derived from these tumors carry the initiating KRAS G12D lesions, secondary Bap1 alterations, and human MPM-like gene expression profiles. Moreover, they are transplantable and actionable by KRAS inhibition. Our results indicate that KRAS alterations alone or in accomplice with TP53 alterations likely play an important and underestimated role in a proportion of patients with MPM, which warrants further exploration., (© 2021 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2022

21. A role for club cells in smoking-associated lung adenocarcinoma.

Author

Behrend SJ, Giotopoulou GA, Spella M, and Stathopoulos GT

Subjects

Animals, Epithelial Cells, Humans, Mice, Smoking adverse effects, Adenocarcinoma, Adenocarcinoma of Lung, Lung Neoplasms

Abstract

The cellular origin of lung adenocarcinoma remains a focus of intense research efforts. The marked cellular heterogeneity and plasticity of the lungs, as well as the vast variety of molecular subtypes of lung adenocarcinomas perplex the field and account for the extensive variability of experimental results. While most experts would agree on the cellular origins of other types of thoracic tumours, great controversy exists on the tumour-initiating cells of lung adenocarcinoma, since this histologic subtype of lung cancer arises in the distal pulmonary regions where airways and alveoli converge, occurs in smokers as well as nonsmokers, is likely caused by various environmental agents, and is marked by vast molecular and pathologic heterogeneity. Alveolar type II, club, and their variant cells have all been implicated in lung adenocarcinoma progeny and the lineage hierarchies in the distal lung remain disputed. Here we review the relevant literature in this rapidly expanding field, including results from mouse models and human studies. In addition, we present a case for club cells as cells of origin of lung adenocarcinomas that arise in smokers., Competing Interests: Conflict of interest: S.J. Behrend has nothing to disclose. Conflict of interest: G.A. Giotopoulou has nothing to disclose. Conflict of interest: M. Spella has nothing to disclose. Conflict of interest: G.T. Stathopoulos has nothing to disclose., (Copyright ©The authors 2021.)

Published

2021

22. Immune Resistance in Lung Adenocarcinoma.

Author

Spella M and Stathopoulos GT

Abstract

Lung cancer is the leading cancer killer worldwide, imposing grievous challenges for patients and clinicians. The incidence of lung adenocarcinoma (LUAD), the main histologic subtype of lung cancer, is still increasing in current-, ex-, and even non-smokers, whereas its five-year survival rate is approximately 15% as the vast majority of patients usually present with advanced disease at the time of diagnosis. The generation of novel drugs targeting key disease driver mutations has created optimism for the treatment of LUAD, but, as these mutations are not universal, this therapeutic line benefits only a subset of patients. More recently, the advent of targeted immunotherapies and their documented clinical efficacy in many different cancers, including LUAD, have started to change cancer management. Immunotherapies have been developed in order to overcome the cancer's ability to develop mechanisms of immune resistance, i.e., to adapt to and evade the host inflammatory and immune responses. Identifying a cancer's immune resistance mechanisms will likely advance the development of personalized immunotherapies. This review examines the key pathways of immune resistance at play in LUAD and explores therapeutic strategies which can unleash potent antitumor immune responses and significantly improve therapeutic efficacy, quality of life, and survival in LUAD.

Published

2021

23. A Method for the Establishment and Characterization of Mouse Lung Adenocarcinoma Cell Lines that Mimic Traits of Human Adenocarcinomas.

Author

Spella M, Lilis I, and Stathopoulos GT

Subjects

Animals, Cell Line, Tumor, Humans, Mice, Smoking adverse effects, Smoking metabolism, Smoking pathology, Adenocarcinoma of Lung metabolism, Adenocarcinoma of Lung pathology, Lung Neoplasms metabolism, Lung Neoplasms pathology

Abstract

Lung adenocarcinoma (LADC) is the leading cause of cancer death worldwide and is largely inflicted by carcinogens contained in tobacco smoke. The generation of cell lines mimicking traits of human LADC will profoundly advance our understanding of the pathobiology of the disease, as they offer an easy and valuable tool to study the cellular and molecular aspects of carcinogenesis. Here we describe a detailed protocol for the generation of such cell lines, following the exposure of experimental mouse strains to different tobacco carcinogens and isolation of the resulting lung tumors.

Published

2021

24. MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically.

Author

Munkhbaatar E, Dietzen M, Agrawal D, Anton M, Jesinghaus M, Boxberg M, Pfarr N, Bidola P, Uhrig S, Höckendorf U, Meinhardt AL, Wahida A, Heid I, Braren R, Mishra R, Warth A, Muley T, Poh PSP, Wang X, Fröhling S, Steiger K, Slotta-Huspenina J, van Griensven M, Pfeiffer F, Lange S, Rad R, Spella M, Stathopoulos GT, Ruland J, Bassermann F, Weichert W, Strasser A, Branca C, Heikenwalder M, Swanton C, McGranahan N, and Jost PJ

Subjects

Animals, Antineoplastic Agents therapeutic use, Apoptosis drug effects, Apoptosis genetics, Carcinoma, Non-Small-Cell Lung diagnostic imaging, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung pathology, Cell Line, Tumor, Cell Survival drug effects, Cell Survival genetics, Clonal Evolution, DNA Copy Number Variations, Datasets as Topic, Disease Models, Animal, Disease Progression, Humans, Lung diagnostic imaging, Lung pathology, Lung Neoplasms diagnostic imaging, Lung Neoplasms drug therapy, Lung Neoplasms pathology, Mice, Mice, Transgenic, Mutation, Myeloid Cell Leukemia Sequence 1 Protein antagonists & inhibitors, Primary Cell Culture, Prospective Studies, Proto-Oncogene Proteins p21(ras) genetics, Pyrimidines pharmacology, Pyrimidines therapeutic use, RNA-Seq, Retrospective Studies, Spheroids, Cellular, Thiophenes pharmacology, Thiophenes therapeutic use, Tumor Burden drug effects, Tumor Burden genetics, Tumor Suppressor Protein p53 genetics, X-Ray Microtomography, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung genetics, Lung Neoplasms genetics, Myeloid Cell Leukemia Sequence 1 Protein genetics

Abstract

Evasion of programmed cell death represents a critical form of oncogene addiction in cancer cells. Understanding the molecular mechanisms underpinning cancer cell survival despite the oncogenic stress could provide a molecular basis for potential therapeutic interventions. Here we explore the role of pro-survival genes in cancer cell integrity during clonal evolution in non-small cell lung cancer (NSCLC). We identify gains of MCL-1 at high frequency in multiple independent NSCLC cohorts, occurring both clonally and subclonally. Clonal loss of functional TP53 is significantly associated with subclonal gains of MCL-1. In mice, tumour progression is delayed upon pharmacologic or genetic inhibition of MCL-1. These findings reveal that MCL-1 gains occur with high frequency in lung adenocarcinoma and can be targeted therapeutically.

Published

2020

25. Osteopontin drives KRAS-mutant lung adenocarcinoma.

Author

Giopanou I, Kanellakis NI, Giannou AD, Lilis I, Marazioti A, Spella M, Papaleonidopoulos V, Simoes DCM, Zazara DE, Agalioti T, Moschos C, Magkouta S, Kalomenidis I, Panoutsakopoulou V, Lamort AS, Stathopoulos GT, and Psallidas I

Subjects

Adenocarcinoma of Lung chemically induced, Adenocarcinoma of Lung genetics, Animals, HEK293 Cells, Humans, Lung Neoplasms chemically induced, Mice, Mice, Inbred C57BL, Mutation, Neoplasms, Experimental chemically induced, Neoplasms, Experimental genetics, Neoplasms, Experimental pathology, Osteopontin genetics, Adenocarcinoma of Lung pathology, Carcinogenesis genetics, Lung Neoplasms genetics, Lung Neoplasms pathology, Osteopontin metabolism, Proto-Oncogene Proteins p21(ras) genetics, Smoking adverse effects

Abstract

Increased expression of osteopontin (secreted phosphoprotein 1, SPP1) is associated with aggressive human lung adenocarcinoma (LADC), but its function remains unknown. Our aim was to determine the role of SPP1 in smoking-induced LADC. We combined mouse models of tobacco carcinogen-induced LADC, of deficiency of endogenous Spp1 alleles, and of adoptive pulmonary macrophage reconstitution to map the expression of SPP1 and its receptors and determine its impact during carcinogenesis. Co-expression of Spp1 and mutant KrasG12C in benign cells was employed to investigate SPP1/KRAS interactions in oncogenesis. Finally, intratracheal adenovirus encoding Cre recombinase was delivered to LSL.KRASG12D mice lacking endogenous or overexpressing transgenic Spp1 alleles. SPP1 was overexpressed in experimental and human LADC and portended poor survival. In response to two different smoke carcinogens, Spp1-deficient mice developed fewer and smaller LADC with decreased cellular survival and angiogenesis. Both lung epithelial- and macrophage-secreted SPP1 drove tumor-associated inflammation, while epithelial SPP1 promoted early tumorigenesis by fostering the survival of KRAS-mutated cells. Finally, loss and overexpression of Spp1 was, respectively, protective and deleterious for mice harboring KRASG12D-driven LADC. Our data support that SPP1 is functionally involved in early stages of airway epithelial carcinogenesis driven by smoking and mutant KRAS and may present an important therapeutic target., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2020

26. The multi-faceted functioning portrait of LRF/ZBTB7A.

Author

Constantinou C, Spella M, Chondrou V, Patrinos GP, Papachatzopoulou A, and Sgourou A

Subjects

Adipogenesis genetics, Animals, Erythroid Cells metabolism, Humans, Neoplasms metabolism, Oncogenes, Transcription Factors genetics, Tumor Suppressor Proteins metabolism, Transcription Factors metabolism

Abstract

Transcription factors (TFs) consisting of zinc fingers combined with BTB (for broad-complex, tram-track, and bric-a-brac) domain (ZBTB) are a highly conserved protein family that comprises a multifunctional and heterogeneous group of TFs, mainly modulating cell developmental events and cell fate. LRF/ZBTB7A, in particular, is reported to be implicated in a wide variety of physiological and cancer-related cell events. These physiological processes include regulation of erythrocyte maturation, B/T cell differentiation, adipogenesis, and thymic insulin expression affecting consequently insulin self-tolerance. In cancer, LRF/ZBTB7A has been reported to act either as oncogenic or as oncosuppressive factor by affecting specific cell processes (proliferation, apoptosis, invasion, migration, metastasis, etc) in opposed ways, depending on cancer type and molecular interactions. The molecular mechanisms via which LRF/ZBTB7A is known to exert either physiological or cancer-related cellular effects include chromatin organization and remodeling, regulation of the Notch signaling axis, cellular response to DNA damage stimulus, epigenetic-dependent regulation of transcription, regulation of the expression and activity of NF-κB and p53, and regulation of aerobic glycolysis and oxidative phosphorylation (Warburg effect). It is a pleiotropic TF, and thus, alterations to its expression status become detrimental for cell survival. This review summarizes its implication in different cellular activities and the commonly invoked molecular mechanisms triggered by LRF/ZBTB7A's orchestrated action.

Published

2019

27. Tobacco chemical-induced mouse lung adenocarcinoma cell lines pin the prolactin orthologue proliferin as a lung tumour promoter.

Author

Kanellakis NI, Giannou AD, Pepe MAA, Agalioti T, Zazara DE, Giopanou I, Psallidas I, Spella M, Marazioti A, Arendt KAM, Lamort AS, Champeris Tsaniras S, Taraviras S, Papadaki H, Lilis I, and Stathopoulos GT

Subjects

Adenocarcinoma of Lung chemically induced, Adenocarcinoma of Lung genetics, Animals, Carcinogenesis, Carcinogens, Diethylnitrosamine toxicity, Disease Models, Animal, Genes, ras genetics, Lung Neoplasms chemically induced, Lung Neoplasms genetics, Mice, Thyroid Nuclear Factor 1 genetics, Tumor Suppressor Protein p53 genetics, Urethane toxicity, Adenocarcinoma of Lung metabolism, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Lung Neoplasms metabolism, Mutation, Prolactin genetics

Abstract

Lung adenocarcinoma (LADC) is the leading cause of cancer death worldwide. Nevertheless, syngeneic mouse models of the disease are sparse, and cell lines suitable for transplantable and immunocompetent mouse models of LADC remain unmet needs. We established multiple mouse LADC cell lines by repeatedly exposing two mouse strains (FVB, Balb/c) to the tobacco carcinogens urethane or diethylnitrosamine and by culturing out the resulting lung tumours for prolonged periods of time. Characterization of the resulting cell lines (n = 7) showed that they were immortal and phenotypically stable in vitro, and oncogenic, metastatic and lethal in vivo. The primary tumours that gave rise to the cell lines, as well as secondary tumours generated by transplantation of the cell lines, displayed typical LADC features, such as glandular architecture and mucin and thyroid transcription factor 1 expression. Moreover, these cells exhibited marked molecular similarity with human smokers' LADC, including carcinogen-specific Kras point mutations (KrasQ61R in urethane- and KrasQ61H in diethylnitrosamine-triggered cell lines) and Trp53 deletions and displayed stemness features. Interestingly, all cell lines overexpressed proliferin, a murine prolactin orthologue, which functioned as a lung tumour promoter. Furthermore, prolactin was overexpressed and portended poor prognosis in human LADC. In conclusion, we report the first LADC cell lines derived from mice exposed to tobacco carcinogens. These cells closely resemble human LADC and provide a valuable tool for the functional investigation of the pathobiology of the disease., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2019

28. Elimination of KLK5 inhibits early skin tumorigenesis by reducing epidermal proteolysis and reinforcing epidermal microstructure.

Author

Pampalakis G, Zingkou E, Kaklamanis L, Spella M, Stathopoulos GT, and Sotiropoulou G

Subjects

Animals, Carcinogenesis pathology, Desmosomes genetics, Desmosomes pathology, Gene Deletion, Humans, Male, Mice, Mice, Inbred C57BL, Proteolysis, Skin metabolism, Skin pathology, Skin Neoplasms pathology, Carcinogenesis genetics, Gene Expression Regulation, Neoplastic, Kallikreins genetics, Skin Neoplasms genetics

Abstract

Epidermal desquamation involves a finely-tuned proteolytic cascade ensuring the regulated cleavage of desmosomes that releases old stratum corneum outermost layers. Although the roles of desmosomes in normal physiology are well-established, their putative involvement in cancer remains unexplored. The KLK5 protease is thought of having fundamental roles in epidermal proteolysis and homeostasis, and its aberrant activity has been linked to skin pathologies. We found that deletion of Klk5 results in significantly higher numbers of lengthier desmosomes and enhanced skin strength. Klk5 -/- mice retained normal skin barrier function and are resistant to chemically-induced skin tumorigenesis. The resistance to tumorigenesis was not due to inhibition of inflammation, and on the contrary, absence of Klk5 increased the TPA-induced inflammatory skin response. We found that increased desmosomes and reduced proteolysis prevent oncogenic signaling by capturing β-catenin into the cytoplasm and facilitate epidermal keratinocyte apoptosis, thus, inhibiting tumor initiation. We highlight that the skin ultrastructure affects early neoplastic transformation by modulating intracellular signaling and suggest that tissue reinforcement provides a novel mode of tumor suppression., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

29. Cellular Vesicles: New Insights in Engineering Methods, Interaction with Cells and Potential for Brain Targeting.

Author

Marazioti A, Papadia K, Kannavou M, Spella M, Basta A, de Lastic AL, Rodi M, Mouzaki A, Samiotaki M, Panayotou G, Stathopoulos GT, and Antimisiaris SG

Subjects

Animals, Blood-Brain Barrier cytology, Brain Diseases therapy, Drug Delivery Systems, Fluoresceins chemistry, HEK293 Cells transplantation, Humans, Liposomes chemistry, Melanoma, Experimental, Mice, Mice, Inbred C57BL, Particle Size, Proteomics, Brain, Cell Engineering methods, Cytoplasmic Vesicles transplantation

Abstract

Cellular vesicles (CVs) have been proposed as alternatives to exosomes for targeted drug delivery. CVs, prepared from human embryonic kidney 293 cells (HEK-293), C57BL/6 mouse B16F10 skin melanoma cells (B16F10), and immortalized human cerebral microvascular endothelial cells (hCMEC/D3) by liposome technology methods, were characterized for morphology, cytotoxicity, and cell uptake properties. CV brain-targeting potential was evaluated in vitro on the hCMEC/D3 blood-brain barrier (BBB) model, and in vivo/ex vivo. CV sizes were between 135 and 285 nm, and the ζ -potential was negative. The dehydration-rehydration method conferred highest calcein loading and latency to CVs compared with other methods. The increased calcein leakage from CVs when compared with liposomes indicated their poor integrity, which was increased by pegylation. The in vivo results confirmed lower liver uptake by PEG-CVs (compared with nonpegylated) proving that the calcein integrity test is useful for prediction of CV biodistribution, as used for liposomes. The cell uptake of homologous origin CVs was not always higher compared with that of non-homologous. Nevertheless, CVs from hCMEC/D3 demonstrated the highest BBB permeability (in vitro) compared with OX-26 targeted liposomes, and brain localization (in vivo). CVs from hCMEC/D3 cells grown in different media demonstrated decreased interaction with brain cells and brain localization. Significant differences in proteome of the two latter CV types were identified by proteomics, suggesting a potential methodology for identification of organotropism-determining CV components., (Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2019

30. Club cells form lung adenocarcinomas and maintain the alveoli of adult mice.

Author

Spella M, Lilis I, Pepe MA, Chen Y, Armaka M, Lamort AS, Zazara DE, Roumelioti F, Vreka M, Kanellakis NI, Wagner DE, Giannou AD, Armenis V, Arendt KA, Klotz LV, Toumpanakis D, Karavana V, Zakynthinos SG, Giopanou I, Marazioti A, Aidinis V, Sotillo R, and Stathopoulos GT

Subjects

Animals, Cell Proliferation, Cell Survival, Disease Models, Animal, Epithelial Cells drug effects, Mice, Pulmonary Alveoli cytology, Respiratory Mucosa cytology, Tobacco Smoking adverse effects, Adenocarcinoma of Lung pathology, Carcinogens metabolism, Environmental Exposure, Epithelial Cells pathology, Epithelial Cells physiology

Abstract

Lung cancer and chronic lung diseases impose major disease burdens worldwide and are caused by inhaled noxious agents including tobacco smoke. The cellular origins of environmental-induced lung tumors and of the dysfunctional airway and alveolar epithelial turnover observed with chronic lung diseases are unknown. To address this, we combined mouse models of genetic labeling and ablation of airway (club) and alveolar cells with exposure to environmental noxious and carcinogenic agents. Club cells are shown to survive KRAS mutations and to form lung tumors after tobacco carcinogen exposure. Increasing numbers of club cells are found in the alveoli with aging and after lung injury, but go undetected since they express alveolar proteins. Ablation of club cells prevents chemical lung tumors and causes alveolar destruction in adult mice. Hence club cells are important in alveolar maintenance and carcinogenesis and may be a therapeutic target against premalignancy and chronic lung disease., Competing Interests: MS, IL, MP, YC, MA, AL, DZ, FR, MV, NK, DW, AG, VA, KA, LK, DT, VK, SZ, IG, AM, VA, RS, GS No competing interests declared, (© 2019, Spella et al.)

Published

2019

31. Interleukin-1β provided by KIT-competent mast cells is required for KRAS -mutant lung adenocarcinoma.

Author

Lilis I, Ntaliarda G, Papaleonidopoulos V, Giotopoulou GA, Oplopoiou M, Marazioti A, Spella M, Marwitz S, Goldmann T, Bravou V, Giopanou I, and Stathopoulos GT

Abstract

Mast cells (MC) have been identified in human lung adenocarcinoma (LADC) tissues, but their functional role has not been investigated in vivo . For this, we applied three mouse models of KRAS- mutant LADC to two different MC-deficient mouse strains ( cKit Wsh and Cpa3.Cre ). Moreover, we derived MC gene signatures from murine bone marrow-derived MC and used them to interrogate five human cohorts of LADC patients. Tumor-free cKit Wsh and Cpa3.Cre mice were deficient in alveolar and skin KIT-dependent (KIT+) MC, but cKit Wsh mice retained normal KIT-independent (KIT-) MC in the airways. Both KIT+ and KIT- MC infiltrated murine LADC to varying degrees, but KIT+ MC were more abundant and promoted LADC initiation and progression through interleukin-1β secretion. KIT+ MC and their transcriptional signature were significantly enriched in human LADC compared to adjacent normal tissue, especially in the subset of patients with KRAS mutations. Importantly, MC density increased with tumor stage and high overall expression of the KIT+ MC signature portended poor survival. Collectively, our results indicate that KIT+ MC foster LADC development and represent marked therapeutic targets.

Published

2019

32. RANK-c attenuates aggressive properties of ER-negative breast cancer by inhibiting NF-κB activation and EGFR signaling.

Author

Sirinian C, Papanastasiou AD, Schizas M, Spella M, Stathopoulos GT, Repanti M, Zarkadis IK, King TA, and Kalofonos HP

Subjects

Animals, Cell Line, Tumor, Female, Gene Expression Regulation, Neoplastic physiology, Humans, Mice, Mice, Inbred NOD, Mice, SCID, RANK Ligand metabolism, Breast Neoplasms metabolism, ErbB Receptors metabolism, NF-kappa B metabolism, Receptor Activator of Nuclear Factor-kappa B metabolism, Receptors, Estrogen metabolism, Signal Transduction physiology

Abstract

The RANK/RANKL axis emerges as a key regulator of breast cancer initiation, progression, and metastasis. RANK-c is a RANK receptor isoform produced through alternative splicing of the TNFRSF11A (RANK) gene and a dominant-negative regulator of RANK-induced nuclear factor-κB (NF-κB) activation. Here we report that RANK-c transcript is expressed in 3.2% of cases in The Cancer Genome Atlas breast cancer cohort evenly between ER-positive and ER-negative cases. Nevertheless, the ratio of RANK to RANK-c (RANK/RANK-c) is increased in ER-negative breast cancer cell lines compared to ER-positive breast cancer cell lines. In addition, forced expression of RANK-c in ER-negative breast cancer cell lines inhibited stimuli-induced NF-κB activation and attenuated migration, invasion, colony formation, and adhesion of cancer cells. Further, RANK-c expression in MDA-MB-231 cells inhibited lung metastasis and colonization in vivo. The RANK-c-mediated inhibition of cancer cell aggressiveness and nuclear factor-κB (NF-κB) activation in breast cancer cells seems to rely on a RANK-c/TNF receptor-associated factor-2 (TRAF2) protein interaction. This was further confirmed by a mutated RANK-c that is unable to interact with TRAF2 and abolishes the ability to attenuate NF-κB activation, migration, and invasion. Additional protein interaction characterization revealed epidermal growth factor receptor (EGFR) as a novel interacting partner for RANK-c in breast cancer cells with a negative effect on EGFR phosphorylation and EGF-dependent downstream signaling pathway activation. Our findings further elucidate the complex molecular biology of the RANKL/RANK system in breast cancer and provide preliminary data for RANK-c as a possible marker for disease progression and aggressiveness.

Published

2018

33. IκB Kinase α Is Required for Development and Progression of KRAS -Mutant Lung Adenocarcinoma.

Author

Vreka M, Lilis I, Papageorgopoulou M, Giotopoulou GA, Lianou M, Giopanou I, Kanellakis NI, Spella M, Agalioti T, Armenis V, Goldmann T, Marwitz S, Yull FE, Blackwell TS, Pasparakis M, Marazioti A, and Stathopoulos GT

Subjects

A549 Cells, Animals, Cell Line, Cell Line, Tumor, Disease Progression, HEK293 Cells, Humans, Lung Neoplasms genetics, Mice, Mice, Inbred C57BL, NF-kappa B genetics, Protein Serine-Threonine Kinases genetics, Signal Transduction genetics, NF-kappaB-Inducing Kinase, Adenocarcinoma of Lung genetics, Adenocarcinoma of Lung pathology, I-kappa B Kinase genetics, Lung Neoplasms pathology, Proto-Oncogene Proteins p21(ras) genetics

Abstract

Although oncogenic activation of NFκB has been identified in various tumors, the NFκB-activating kinases (inhibitor of NFκB kinases, IKK) responsible for this are elusive. In this study, we determined the role of IKKα and IKKβ in KRAS -mutant lung adenocarcinomas induced by the carcinogen urethane and by respiratory epithelial expression of oncogenic KRAS G12D Using NFκB reporter mice and conditional deletions of IKKα and IKKβ, we identified two distinct early and late activation phases of NFκB during chemical and genetic lung adenocarcinoma development, which were characterized by nuclear translocation of Rel B, IκBβ, and IKKα in tumor-initiated cells. IKKα was a cardinal tumor promoter in chemical and genetic KRAS -mutant lung adenocarcinoma, and respiratory epithelial IKKα-deficient mice were markedly protected from the disease. IKKα specifically cooperated with mutant KRAS for tumor induction in a cell-autonomous fashion, providing mutant cells with a survival advantage in vitro and in vivo IKKα was highly expressed in human lung adenocarcinoma, and a heat shock protein 90 inhibitor that blocks IKK function delivered superior effects against KRAS -mutant lung adenocarcinoma compared with a specific IKKβ inhibitor. These results demonstrate an actionable requirement for IKKα in KRAS -mutant lung adenocarcinoma, marking the kinase as a therapeutic target against this disease. Significance: These findings report a novel requirement for IKKα in mutant KRAS lung tumor formation, with potential therapeutic applications. Cancer Res; 78(11); 2939-51. ©2018 AACR ., (©2018 American Association for Cancer Research.)

Published

2018

34. Myeloid-derived interleukin-1β drives oncogenic KRAS-NF-κΒ addiction in malignant pleural effusion.

Author

Marazioti A, Lilis I, Vreka M, Apostolopoulou H, Kalogeropoulou A, Giopanou I, Giotopoulou GA, Krontira AC, Iliopoulou M, Kanellakis NI, Agalioti T, Giannou AD, Jones-Paris C, Iwakura Y, Kardamakis D, Blackwell TS, Taraviras S, Spella M, and Stathopoulos GT

Subjects

Animals, Cell Line, Tumor, Chemokine CXCL1 metabolism, Female, Humans, I-kappa B Kinase metabolism, Male, Mice, Mice, Inbred C57BL, Mutation, Receptors, Interleukin-1 metabolism, Genes, ras, Interleukin-1beta metabolism, Myeloid Cells metabolism, NF-kappa B metabolism, Pleural Effusion, Malignant metabolism

Abstract

Malignant pleural effusion (MPE) is a frequent metastatic manifestation of human cancers. While we previously identified KRAS mutations as molecular culprits of MPE formation, the underlying mechanism remained unknown. Here, we determine that non-canonical IKKα-RelB pathway activation of KRAS-mutant tumor cells mediates MPE development and this is fueled by host-provided interleukin IL-1β. Indeed, IKKα is required for the MPE-competence of KRAS-mutant tumor cells by activating non-canonical NF-κB signaling. IL-1β fuels addiction of mutant KRAS to IKKα resulting in increased CXCL1 secretion that fosters MPE-associated inflammation. Importantly, IL-1β-mediated NF-κB induction in KRAS-mutant tumor cells, as well as their resulting MPE-competence, can only be blocked by co-inhibition of both KRAS and IKKα, a strategy that overcomes drug resistance to individual treatments. Hence we show that mutant KRAS facilitates IKKα-mediated responsiveness of tumor cells to host IL-1β, thereby establishing a host-to-tumor signaling circuit that culminates in inflammatory MPE development and drug resistance.

Published

2018

35. RAS oncogenes direct metastasis.

Author

Spella M, Marazioti A, Arendt KAM, and Stathopoulos GT

Abstract

RAS genes are cardinal driver oncogenes frequently and differentially mutated across bodily tumors. Their tumorigenic potential has been mainly ascribed to autonomous promotion of tumor cell proliferation and survival. However, recent evidence shows that RAS oncogenes also function to define metastatic tropism. Interestingly, RAS -driven metastasis is mediated by distinct chemokine sets that signal to endothelial and myeloid cells.

Published

2017

36. Shared epithelial pathways to lung repair and disease.

Author

Spella M, Lilis I, and Stathopoulos GT

Subjects

Animals, Cell Differentiation, Cell Proliferation, Epithelial Cells pathology, Gene Expression Regulation, Humans, Lung pathology, Lung physiopathology, Lung Diseases genetics, Lung Diseases pathology, Lung Diseases physiopathology, Phenotype, Recovery of Function, Epithelial Cells metabolism, Lung metabolism, Lung Diseases metabolism, Re-Epithelialization, Regeneration, Signal Transduction

Abstract

Chronic lung diseases present tremendous health burdens and share a common pathobiology of dysfunctional epithelial repair. Lung adenocarcinoma, the leading cancer killer worldwide, is caused mainly by chemical carcinogens of tobacco smoke that induce mutations in pulmonary epithelial cells leading to uncontrolled epithelial proliferation. Lung epithelial cells that possess the capacity for self-renewal and regeneration of other lung cell types are believed to underlie the pathobiology of chronic obstructive, fibrotic and neoplastic lung disorders. However, the understanding of lung epithelial progenitor cell hierarchy and turnover is incomplete and a comprehensive model of the cellular and transcriptional events that underlie lung regeneration and carcinogenesis is missing. The mapping of these processes is extremely important, since their modulation would potentially allow effective cure and/or prevention of chronic lung diseases. In this review we describe current knowledge on cellular and molecular pathways at play during lung repair and carcinogenesis and summarise the critical lung cell populations with regenerative and cancerous potential., Competing Interests: Conflict of interest: None declared., (Copyright ©ERS 2017.)

Published

2017

37. Mutant KRAS promotes malignant pleural effusion formation.

Author

Agalioti T, Giannou AD, Krontira AC, Kanellakis NI, Kati D, Vreka M, Pepe M, Spella M, Lilis I, Zazara DE, Nikolouli E, Spiropoulou N, Papadakis A, Papadia K, Voulgaridis A, Harokopos V, Stamou P, Meiners S, Eickelberg O, Snyder LA, Antimisiaris SG, Kardamakis D, Psallidas I, Marazioti A, and Stathopoulos GT

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma pathology, Adenocarcinoma of Lung, Animals, Antineoplastic Agents therapeutic use, Benzimidazoles pharmacology, Benzimidazoles therapeutic use, Cell Line, Tumor, Chemokine CCL2 antagonists & inhibitors, Chemokine CCL2 metabolism, Chickens, Chorioallantoic Membrane, Female, HEK293 Cells, Humans, Lung Neoplasms drug therapy, Lung Neoplasms pathology, Male, Mice, Mice, Inbred C57BL, Mice, Inbred NOD, Pleural Cavity cytology, Pleural Cavity pathology, Pleural Effusion, Malignant drug therapy, Pleural Effusion, Malignant pathology, Proto-Oncogene Proteins p21(ras) antagonists & inhibitors, Proto-Oncogene Proteins p21(ras) metabolism, RNA, Small Interfering metabolism, Spleen cytology, Spleen pathology, Up-Regulation, Xenograft Model Antitumor Assays, Adenocarcinoma genetics, Antineoplastic Agents pharmacology, Lung Neoplasms genetics, Myeloid Cells pathology, Pleural Effusion, Malignant genetics, Proto-Oncogene Proteins p21(ras) genetics

Abstract

Malignant pleural effusion (MPE) is the lethal consequence of various human cancers metastatic to the pleural cavity. However, the mechanisms responsible for the development of MPE are still obscure. Here we show that mutant KRAS is important for MPE induction in mice. Pleural disseminated, mutant KRAS bearing tumour cells upregulate and systemically release chemokine ligand 2 (CCL2) into the bloodstream to mobilize myeloid cells from the host bone marrow to the pleural space via the spleen. These cells promote MPE formation, as indicated by splenectomy and splenocyte restoration experiments. In addition, KRAS mutations are frequently detected in human MPE and cell lines isolated thereof, but are often lost during automated analyses, as indicated by manual versus automated examination of Sanger sequencing traces. Finally, the novel KRAS inhibitor deltarasin and a monoclonal antibody directed against CCL2 are equally effective against an experimental mouse model of MPE, a result that holds promise for future efficient therapies against the human condition.

Published

2017

38. NRAS destines tumor cells to the lungs.

Author

Giannou AD, Marazioti A, Kanellakis NI, Giopanou I, Lilis I, Zazara DE, Ntaliarda G, Kati D, Armenis V, Giotopoulou GA, Krontira AC, Lianou M, Agalioti T, Vreka M, Papageorgopoulou M, Fouzas S, Kardamakis D, Psallidas I, Spella M, and Stathopoulos GT

Subjects

Animals, Cell Line, Tumor, GTP Phosphohydrolases immunology, Gene Expression Regulation, Neoplastic, Humans, Inflammation genetics, Inflammation immunology, Inflammation pathology, Interleukin-8 immunology, Lung immunology, Lung metabolism, Lung Neoplasms genetics, Lung Neoplasms immunology, Membrane Proteins immunology, Mice, Inbred BALB C, Mice, Inbred C57BL, Monomeric GTP-Binding Proteins, Mutation, Signal Transduction, GTP Phosphohydrolases genetics, Lung blood supply, Lung Neoplasms blood supply, Lung Neoplasms secondary, Membrane Proteins genetics, Up-Regulation

Abstract

The lungs are frequently affected by cancer metastasis. Although NRAS mutations have been associated with metastatic potential, their exact role in lung homing is incompletely understood. We cross-examined the genotype of various tumor cells with their ability for automatic pulmonary dissemination, modulated NRAS expression using RNA interference and NRAS overexpression, identified NRAS signaling partners by microarray, and validated them using Cxcr1 - and Cxcr2 -deficient mice. Mouse models of spontaneous lung metastasis revealed that mutant or overexpressed NRAS promotes lung colonization by regulating interleukin-8-related chemokine expression, thereby initiating interactions between tumor cells, the pulmonary vasculature, and myeloid cells. Our results support a model where NRAS -mutant, chemokine-expressing circulating tumor cells target the CXCR1-expressing lung vasculature and recruit CXCR2-expressing myeloid cells to initiate metastasis. We further describe a clinically relevant approach to prevent NRAS-driven pulmonary metastasis by inhibiting chemokine signaling. In conclusion, NRAS promotes the colonization of the lungs by various tumor types in mouse models. IL-8-related chemokines, NRAS signaling partners in this process, may constitute an important therapeutic target against pulmonary involvement by cancers of other organs., (© 2017 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2017

39. Tumor-derived osteopontin isoforms cooperate with TRP53 and CCL2 to promote lung metastasis.

Author

Giopanou I, Lilis I, Papaleonidopoulos V, Agalioti T, Kanellakis NI, Spiropoulou N, Spella M, and Stathopoulos GT

Abstract

The lungs are ubiquitous receptacles of metastases originating from various bodily tumors. Although osteopontin (SPP1) has been associated with tumor dissemination, the role of its isoforms in lung-directed metastasis is incompletely understood. We employed syngeneic mouse models of spontaneous and induced lung-targeted metastasis in C57BL/6 mice competent and deficient in both Spp1 alleles. Tumor-derived osteopontin expression was modulated using either stable anti- Spp1 RNA interference, or forced overexpression of intracellular and secreted Spp1 isoforms. Identified osteopontin's downstream partners were validated using lung adenocarcinoma cells conditionally lacking the Trp53 gene and Ccr2 -deficient mice. We determined that host-derived osteopontin was dispensable for pulmonary colonization by different tumor types. Oppositely, tumor-originated intracellular osteopontin promoted tumor cell survival by preventing tumor-related protein 53-mediated apoptosis, while the secretory osteopontin functioned in a paracrine mode to accelerate lung metastasis by enhancing tumor-derived C-C-motif chemokine ligand 2 signaling to cognate host receptors. As new ways to target osteopontin signaling are becoming available, the cytokine may constitute an important therapeutic target against pulmonary involvement by cancers of other organs.

Published

2016

40. Comprehensive Evaluation of Nuclear Factor-κΒ Expression Patterns in Non-Small Cell Lung Cancer.

Author

Giopanou I, Lilis I, Papaleonidopoulos V, Marazioti A, Spella M, Vreka M, Papadaki H, and Stathopoulos GT

Subjects

Adenocarcinoma pathology, Aged, Aged, 80 and over, Animals, Carcinoma, Large Cell pathology, Carcinoma, Squamous Cell pathology, Cell Nucleus metabolism, Disease Models, Animal, Female, Humans, Lung pathology, Lung Neoplasms pathology, Male, Mice, Middle Aged, NF-kappa B p50 Subunit metabolism, NF-kappa B p52 Subunit metabolism, Transcription Factor RelA metabolism, Transcription Factor RelB metabolism, Adenocarcinoma metabolism, Carcinoma, Large Cell metabolism, Carcinoma, Squamous Cell metabolism, Lung metabolism, Lung Neoplasms metabolism, NF-kappa B metabolism

Abstract

Nuclear factor (NF)-κB signalling is required for lung adenocarcinoma development in mice, and both of its subunits RelA and RelB were independently reported to be highly expressed in human non-small cell lung cancer (NSCLC). To comprehensively examine NF-κB expression in NSCLC, we analyzed serial sections of primary tumor samples from 77 well-documented patients (36 adenocarcinomas, 40 squamous cell carcinomas and 3 large cell carcinomas) for immunoreactivity of RelA, RelB, P50, and P52/P100. Tumor and intratumoral stroma areas were discriminated based on proliferating cell nuclear antigen immunoreactivity and inflammatory infiltration was assessed in intratumoral stroma areas. NF-κB immunoreactivity was quantified by intensity, extent, and nuclear localization and was cross-examined with tumor cell proliferation, inflammatory infiltration, and clinical-pathologic data. We found that the expression of the different NF-κB subunits was not concordant, warranting our integral approach. Overall, RelA, RelB, and P50 were expressed at higher levels compared with P52/P100. However, RelA and P50 were predominantly expressed in intratumoral stroma, but RelB in tumor cells. Importantly, tumor area RelA expression was correlated with the intensity of inflammatory infiltration, whereas RelB expression was identified in proliferating tumor cells. Using multiple logistic regression, we identified that tumor RelB expression was an independent predictor of lymph node metastasis, and tumor P50 was an independent predictor of TNM6 stage IIB or higher, whereas tumor RelA was an independent predictor of inflammatory infiltration. We conclude that pathologic studies of NF-κB expression in cancer should include multiple pathway components. Utilizing such an approach, we identified intriguing associations between distinct NF-κB subunits and clinical and pathologic features of NSCLC.

Published

2015

41. Switching off malignant pleural effusion formation-fantasy or future?

Author

Spella M, Giannou AD, and Stathopoulos GT

Abstract

Malignant pleural effusion (MPE) is common and difficult to treat. In the vast majority of patients the presence of MPE heralds incurable disease, associated with poor quality of life, morbidity and mortality. Current therapeutic approaches are inefficient and merely offer palliation of associated symptoms. Recent scientific progress has shed light in the biologic processes governing the mechanisms behind the pathobiology of MPE. Pleural based tumors interfere with pleural fluid drainage, as well as the host vasculature and immune system, resulting in decreased fluid absorption and increased pleural fluid production via enhanced plasma extravasation into the pleural space. In order to achieve this feat, pleural based tumors must elicit critical vasoactive events in the pleura, thus forming a favorable microenvironment for tumor dissemination and MPE development. Such properties involve specific transcriptional signaling cascades in addition to secretion of important mediators which attract and activate host cell populations which, in turn, impact tumor cell functions. The dissection of the biologic steps leading to MPE formation provides novel therapeutic targets and recent research findings provide encouraging results towards future therapeutic innovations in MPE management.

Published

2015

42. Mast cells mediate malignant pleural effusion formation.

Author

Giannou AD, Marazioti A, Spella M, Kanellakis NI, Apostolopoulou H, Psallidas I, Prijovich ZM, Vreka M, Zazara DE, Lilis I, Papaleonidopoulos V, Kairi CA, Patmanidi AL, Giopanou I, Spiropoulou N, Harokopos V, Aidinis V, Spyratos D, Teliousi S, Papadaki H, Taraviras S, Snyder LA, Eickelberg O, Kardamakis D, Iwakura Y, Feyerabend TB, Rodewald HR, Kalomenidis I, Blackwell TS, Agalioti T, and Stathopoulos GT

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma genetics, Adenocarcinoma metabolism, Adenocarcinoma pathology, Animals, Benzamides pharmacology, Cell Line, Tumor, Colonic Neoplasms drug therapy, Colonic Neoplasms genetics, Colonic Neoplasms metabolism, Colonic Neoplasms pathology, Humans, Imatinib Mesylate, Interleukin-1beta genetics, Interleukin-1beta metabolism, Lung Neoplasms diet therapy, Lung Neoplasms genetics, Lung Neoplasms metabolism, Lung Neoplasms pathology, Male, Mast Cells pathology, Mice, Mice, Inbred NOD, Mice, SCID, Mice, Transgenic, Piperazines pharmacology, Pleural Cavity metabolism, Pleural Cavity pathology, Pleural Effusion, Malignant drug therapy, Pleural Effusion, Malignant genetics, Pleural Effusion, Malignant pathology, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-kit antagonists & inhibitors, Proto-Oncogene Proteins c-kit genetics, Proto-Oncogene Proteins c-kit metabolism, Pyrimidines pharmacology, Tryptases genetics, Tryptases metabolism, Mast Cells metabolism, Pleural Effusion, Malignant metabolism

Abstract

Mast cells (MCs) have been identified in various tumors; however, the role of these cells in tumorigenesis remains controversial. Here, we quantified MCs in human and murine malignant pleural effusions (MPEs) and evaluated the fate and function of these cells in MPE development. Evaluation of murine MPE-competent lung and colon adenocarcinomas revealed that these tumors actively attract and subsequently degranulate MCs in the pleural space by elaborating CCL2 and osteopontin. MCs were required for effusion development, as MPEs did not form in mice lacking MCs, and pleural infusion of MCs with MPE-incompetent cells promoted MPE formation. Once homed to the pleural space, MCs released tryptase AB1 and IL-1β, which in turn induced pleural vasculature leakiness and triggered NF-κB activation in pleural tumor cells, thereby fostering pleural fluid accumulation and tumor growth. Evaluation of human effusions revealed that MCs are elevated in MPEs compared with benign effusions. Moreover, MC abundance correlated with MPE formation in a human cancer cell-induced effusion model. Treatment of mice with the c-KIT inhibitor imatinib mesylate limited effusion precipitation by mouse and human adenocarcinoma cells. Together, the results of this study indicate that MCs are required for MPE formation and suggest that MC-dependent effusion formation is therapeutically addressable.

Published

2015

43. Beneficial impact of CCL2 and CCL12 neutralization on experimental malignant pleural effusion.

Author

Marazioti A, Kairi CA, Spella M, Giannou AD, Magkouta S, Giopanou I, Papaleonidopoulos V, Kalomenidis I, Snyder LA, Kardamakis D, and Stathopoulos GT

Subjects

Adenocarcinoma complications, Adenocarcinoma pathology, Adenocarcinoma of Lung, Animals, Cell Line, Tumor, Cell Proliferation, Colonic Neoplasms complications, Colonic Neoplasms pathology, Humans, Lung Neoplasms complications, Lung Neoplasms pathology, Mice, Mice, Inbred C57BL, Pleural Effusion, Malignant etiology, Pleural Effusion, Malignant metabolism, Antibodies, Neutralizing immunology, Antibodies, Neutralizing therapeutic use, Chemokine CCL2 immunology, Monocyte Chemoattractant Proteins immunology, Pleural Effusion, Malignant therapy

Abstract

Using genetic interventions, we previously determined that C-C motif chemokine ligand 2 (CCL2) promotes malignant pleural effusion (MPE) formation in mice. Here we conducted preclinical studies aimed at assessing the specific therapeutic potential of antibody-mediated CCL2 blockade against MPE. For this, murine MPEs or skin tumors were generated in C57BL/6 mice by intrapleural or subcutaneous delivery of lung (LLC) or colon (MC38) adenocarcinoma cells. Human lung adenocarcinoma cells (A549) were used to induce MPEs in severe combined immunodeficient mice. Intraperitoneal antibodies neutralizing mouse CCL2 and/or CCL12, a murine CCL2 ortholog, were administered at 10 or 50 mg/kg every three days. We found that high doses of CCL2/12 neutralizing antibody treatment (50 mg/kg) were required to limit MPE formation by LLC cells. CCL2 and CCL12 blockade were equally potent inhibitors of MPE development by LLC cells. Combined CCL2 and CCL12 neutralization was also effective against MC38-induced MPE and prolonged the survival of mice in both syngeneic models. Mouse-specific CCL2-blockade limited A549-caused xenogeneic MPE, indicating that host-derived CCL2 also contributes to MPE precipitation in mice. The impact of CCL2/12 antagonism was associated with inhibition of immune and vascular MPE-related phenomena, such as inflammation, new blood vessel assembly and plasma extravasation into the pleural space. We conclude that CCL2 and CCL12 blockade are effective against experimental MPE induced by murine and human adenocarcinoma in mice. These results suggest that CCL2-targeted therapies may hold promise for future use against human MPE.

Published

2013

44. Reduced Geminin levels promote cellular senescence.

Author

Iliou MS, Kotantaki P, Karamitros D, Spella M, Taraviras S, and Lygerou Z

Subjects

Animals, Cell Cycle Proteins biosynthesis, Cell Cycle Proteins genetics, DNA-Binding Proteins biosynthesis, DNA-Binding Proteins genetics, Embryo, Mammalian cytology, Embryo, Mammalian metabolism, Fibroblasts cytology, HeLa Cells, Humans, Mice, SMN Complex Proteins genetics, Cellular Senescence physiology, Fibroblasts metabolism, G1 Phase physiology, Gene Expression Regulation physiology, S Phase physiology, SMN Complex Proteins biosynthesis

Abstract

Cellular senescence is a permanent out-of-cycle state regulated by molecular circuits acting during the G1 phase of the cell cycle. Cdt1 is a central regulator of DNA replication licensing acting during the G1 phase and it is negatively controlled by Geminin. Here, we characterize the cell cycle expression pattern of Cdt1 and Geminin during successive passages of primary fibroblasts and compare it to tumour-derived cell lines. Cdt1 and Geminin are strictly expressed in distinct subpopulations of young fibroblasts, similarly to cancer cells, with Geminin accumulating shortly after the onset of S phase. Cdt1 and Geminin are down-regulated when primary human and mouse fibroblasts undergo replicative or stress-induced senescence. RNAi-mediated Geminin knock-down in human cells enhances the appearance of phenotypic and molecular features of senescence. Mouse embryonic fibroblasts heterozygous for Geminin exhibit accelerated senescence compared to control fibroblasts. In contrast, ectopic expression of Geminin in mouse embryonic fibroblasts delays the appearance of the senescent phenotype. Taken together, our data suggest that changes in Geminin expression levels affect the establishment of senescence pathways., (Copyright © 2012 Elsevier Ireland Ltd. All rights reserved.)

Published

2013

45. Geminin regulates cortical progenitor proliferation and differentiation.

Author

Spella M, Kyrousi C, Kritikou E, Stathopoulou A, Guillemot F, Kioussis D, Pachnis V, Lygerou Z, and Taraviras S

Subjects

Animals, Cell Cycle Proteins metabolism, Cells, Cultured, Cerebral Cortex embryology, Cerebral Cortex metabolism, Eye Proteins metabolism, Female, Geminin, Gene Knockout Techniques, Homeodomain Proteins metabolism, Mice, Mice, Knockout, Neural Stem Cells physiology, Nissl Bodies metabolism, Nuclear Proteins metabolism, PAX6 Transcription Factor, Paired Box Transcription Factors metabolism, Pregnancy, Repressor Proteins metabolism, T-Box Domain Proteins metabolism, Cell Cycle Proteins genetics, Cell Differentiation, Cell Proliferation, Cerebral Cortex cytology, Neural Stem Cells cytology, Nuclear Proteins genetics

Abstract

During cortical development, coordination of proliferation and differentiation ensures the timely generation of different neural progenitor lineages that will give rise to mature neurons and glia. Geminin is an inhibitor of DNA replication and it has been proposed to regulate cell proliferation and fate determination during neurogenesis via interactions with transcription factors and chromatin remodeling complexes. To investigate the in vivo role of Geminin in the maintenance and differentiation of cortical neural progenitors, we have generated mice that lack Geminin expression in the developing cortex. Our results show that loss of Geminin leads to the expansion of neural progenitor cells located at the ventricular and subventricular zones of the developing cortex. Early cortical progenitors lacking Geminin exhibit a longer S-phase and a reduced ability to generate early born neurons, consistent with a preference on self-renewing divisions. Overexpression of Geminin in progenitor cells of the cortex reduces the number of neural progenitor cells, promotes cell cycle exit and subsequent neuronal differentiation. Our study suggests that Geminin has an important role during cortical development in regulating progenitor number and ultimately neuron generation., (Copyright © 2011 AlphaMed Press.)

Published

2011

46. Idas, a novel phylogenetically conserved geminin-related protein, binds to geminin and is required for cell cycle progression.

Author

Pefani DE, Dimaki M, Spella M, Karantzelis N, Mitsiki E, Kyrousi C, Symeonidou IE, Perrakis A, Taraviras S, and Lygerou Z

Subjects

Amino Acid Sequence, Anaphase physiology, Animals, Cell Cycle Proteins genetics, Cell Differentiation physiology, Cell Nucleus genetics, Choroid Plexus cytology, Choroid Plexus embryology, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Geminin, Gene Expression Regulation, Developmental physiology, HeLa Cells, Humans, Mice, Molecular Sequence Data, Multiprotein Complexes genetics, Nuclear Proteins genetics, Phylogeny, S Phase physiology, Telencephalon cytology, Telencephalon embryology, Transcription Factors, Cell Cycle Proteins metabolism, Cell Nucleus metabolism, Multiprotein Complexes metabolism, Nuclear Proteins metabolism

Abstract

Development and homeostasis of multicellular organisms relies on an intricate balance between cell proliferation and differentiation. Geminin regulates the cell cycle by directly binding and inhibiting the DNA replication licensing factor Cdt1. Geminin also interacts with transcriptional regulators of differentiation and chromatin remodelling factors, and its balanced interactions are implicated in proliferation-differentiation decisions during development. Here, we describe Idas (Idas being a cousin of the Gemini in Ancient Greek Mythology), a previously uncharacterised coiled-coil protein related to Geminin. We show that human Idas localizes to the nucleus, forms a complex with Geminin both in cells and in vitro through coiled-coil mediated interactions, and can change Geminin subcellular localization. Idas does not associate with Cdt1 and prevents Geminin from binding to Cdt1 in vitro. Idas depletion from cells affects cell cycle progression; cells accumulate in S phase and are unable to efficiently progress to mitosis. Idas protein levels decrease in anaphase, whereas its overexpression causes mitotic defects. During development, we show that Idas exhibits high level expression in the choroid plexus and the cortical hem of the mouse telencephalon. Our data highlight Idas as a novel Geminin binding partner, implicated in cell cycle progression, and a putative regulator of proliferation-differentiation decisions during development.

Published

2011

47. Licensing regulators Geminin and Cdt1 identify progenitor cells of the mouse CNS in a specific phase of the cell cycle.

Author

Spella M, Britz O, Kotantaki P, Lygerou Z, Nishitani H, Ramsay RG, Flordellis C, Guillemot F, Mantamadiotis T, and Taraviras S

Subjects

Animals, Antimetabolites, Bromodeoxyuridine, Cell Cycle Proteins genetics, Cell Differentiation physiology, Central Nervous System cytology, Central Nervous System embryology, DNA-Binding Proteins genetics, Down-Regulation physiology, Female, Fluorescent Antibody Technique, Geminin, In Situ Hybridization, Mice, Mice, Inbred C57BL, Nerve Tissue Proteins biosynthesis, Nerve Tissue Proteins genetics, Nuclear Proteins genetics, Plasmids genetics, Pregnancy, RNA, Messenger biosynthesis, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Cell Cycle physiology, Cell Cycle Proteins physiology, Central Nervous System physiology, DNA-Binding Proteins physiology, Nuclear Proteins physiology, Stem Cells physiology

Abstract

Nervous system formation integrates control of cellular proliferation and differentiation and is mediated by multipotent neural progenitor cells that become progressively restricted in their developmental potential before they give rise to differentiated neurons and glial cells. Evidence from different experimental systems suggests that Geminin is a candidate molecule linking proliferation and differentiation during nervous system development. We show here that Geminin and its binding partner Cdt1 are expressed abundantly by neural progenitor cells during early mouse neurogenesis. Their expression levels decline at late developmental stages and become undetectable upon differentiation. Geminin and Cdt1 expressing cells also express Sox2 while no overlap is detected with cells expressing markers of a differentiated neuronal phenotype. A fraction of radial glial cells expressing RC2 and Pax6 are also immunoreactive for Geminin and Cdt1. The majority of the Geminin and Cdt1 expressing cell populations appears to be distinct from fate-restricted precursor cells expressing Mash1 or Neurogenin2. Bromo-deoxy-uridine (BrdU) incorporation experiments reveal a cell cycle specific expression in neural progenitor cells, with Geminin being present from S to M phase, while Cdt1 expression characterizes progenitor cells in G1 phase. Furthermore, in vitro differentiation of adult neurosphere cultures shows downregulation of Geminin/Cdt1 in the differentiated state, in line with our data showing that Geminin is present in neural progenitor cells of the CNS during mouse embryogenesis and adulthood and becomes downregulated upon cell fate specification and differentiation. This suggests a role for Geminin in the formation and maintenance of the neural progenitor cells.

Published

2007