Your search keyword '"Morfoisse, Florent"' showing total 9 results

1. Coordinating Effect of VEGFC and Oleic Acid Participates to Tumor Lymphangiogenesis.

Author

Morfoisse, Florent, De Toni, Fabienne, Nigri, Jeremy, Hosseini, Mohsen, Zamora, Audrey, Tatin, Florence, Pujol, Françoise, Sarry, Jean-Emmanuel, Langin, Dominique, Lacazette, Eric, Prats, Anne-Catherine, Tomasini, Richard, Galitzky, Jean, Bouloumié, Anne, and Garmy-Susini, Barbara

Subjects

*UNSATURATED fatty acids, *ANIMAL experimentation, *FETAL development, *FAT cells, *VASCULAR endothelial growth factors, *TUMORS, *ADIPOSE tissues, *MICE

Abstract

Simple Summary: In cancer, the lymphatic system is hijacked by tumor cells that escape from primary tumor and metastasize to the sentinel lymph nodes. Tumor lymphangiogenesis is stimulated by the vascular endothelial growth factors-C (VEGFC) after binding to its receptor VEGFR-3. However, how VEGFC cooperates with other molecules to promote lymphatic neovessel growth has not been fully determined. Here, we showed that tumor lymphangiogenesis developed in tumoral lesions and in their surrounding adipose tissue (AT). Interestingly, lymphatic vessel density correlated with an increase in circulating free fatty acids (FFA) in the lymph from tumor-bearing mice. We showed that adipocyte-released FFA are uploaded by lymphatic endothelial cells (LEC) to stimulate their sprouting. Lipidomic analysis identified the monounsaturated oleic acid (OA) as the major circulating FFA in the lymph in a tumoral context. OA transporters FATP-3, -6 and CD36 were only upregulated on LEC in the presence of VEGFC showing a collaborative effect of these molecules. OA released from adipocytes is taken up by LECs to stimulate the fatty acid β-oxidation, leading to increased adipose tissue lymphangiogenesis. Our results provide new insights on the dialogue between tumors and adipocytes via the lymphatic system and identify a key role for adipocyte-derived FFA in the promotion of lymphangiogenesis, revealing novel therapeutic opportunities for inhibitors of lymphangiogenesis in cancer. In cancer, the lymphatic system is hijacked by tumor cells that escape from primary tumor and metastasize to the sentinel lymph nodes. Tumor lymphangiogenesis is stimulated by the vascular endothelial growth factors-C (VEGFC) after binding to its receptor VEGFR-3. However, how VEGFC cooperates with other molecules to promote lymphatics growth has not been fully determined. We showed that lymphangiogenesis developed in tumoral lesions and in surrounding adipose tissue (AT). Interestingly, lymphatic vessel density correlated with an increase in circulating free fatty acids (FFA) in the lymph from tumor-bearing mice. We showed that adipocyte-released FFA are uploaded by lymphatic endothelial cells (LEC) to stimulate their sprouting. Lipidomic analysis identified the monounsaturated oleic acid (OA) as the major circulating FFA in the lymph in a tumoral context. OA transporters FATP-3, -6 and CD36 were only upregulated on LEC in the presence of VEGFC showing a collaborative effect of these molecules. OA stimulates fatty acid β-oxidation in LECs, leading to increased AT lymphangiogenesis. Our results provide new insights on the dialogue between tumors and adipocytes via the lymphatic system and identify a key role for adipocyte-derived FFA in the promotion of lymphangiogenesis, revealing novel therapeutic opportunities for inhibitors of lymphangiogenesis in cancer. [ABSTRACT FROM AUTHOR]

Published

2021

2. Sex Hormones in Lymphedema.

Author

Morfoisse, Florent, Zamora, Audrey, Marchaud, Emmanuelle, Nougue, Manon, Diallo, Leila H., David, Florian, Roussel, Emilie, Lacazette, Eric, Prats, Anne-Catherine, Tatin, Florence, Garmy-Susini, Barbara, and Mehrara, Babak J.

Subjects

*LYMPHATIC physiology, *ESTROGEN, *HORMONES, *SEX hormones, *LYMPHEDEMA, *MOLECULAR structure, *THERAPEUTICS, *AROMATASE inhibitors

Abstract

Simple Summary: Lymphedema is a life-long disease that affects a large number of patients treated for breast-, gynecological-, and urologic cancers in Western countries. Given that hormone levels are strongly modified in these conditions, and that patients widely undergo through hormone therapy, it is tempting to speculate that hormones might be key regulators in the maintenance of lymphedema. Despite an obvious prevalence for women, the role of sex hormones and gender has been poorly investigated in this pathology. This review aims to decipher how sex hormones interact with lymphatic vessels and whether hormone therapy could participate in lymphedema development. Lymphedema is a disorder of the lymphatic vascular system characterized by impaired lymphatic return resulting in swelling of the extremities and accumulation of undrained interstitial fluid/lymph that results in fibrosis and adipose tissue deposition in the limb. Whereas it is clearly established that primary lymphedema is sex-linked with an average ratio of one male for three females, the role of female hormones, in particular estrogens, has been poorly explored. In addition, secondary lymphedema in Western countries affects mainly women who developed the pathology after breast cancer and undergo through hormone therapy up to five years after cancer surgery. Although lymphadenectomy is identified as a trigger factor, the effect of co-morbidities associated to lymphedema remains elusive, in particular, estrogen receptor antagonists or aromatase inhibitors. In addition, the role of sex hormones and gender has been poorly investigated in the etiology of the pathology. Therefore, this review aims to recapitulate the effect of sex hormones on the physiology of the lymphatic system and to investigate whetherhormone therapy could promote a lymphatic dysfunction leading to lymphedema. [ABSTRACT FROM AUTHOR]

Published

2021

3. The Impact of Estrogen Receptor in Arterial and Lymphatic Vascular Diseases.

Author

Fontaine, Coralie, Morfoisse, Florent, Tatin, Florence, Zamora, Audrey, Zahreddine, Rana, Henrion, Daniel, Arnal, Jean-François, Lenfant, Françoise, and Garmy-Susini, Barbara

Subjects

*LYMPHATIC diseases, *NUCLEAR membranes, *ESTROGEN receptors, *COLLATERAL circulation, *VASCULAR diseases, *SELECTIVE estrogen receptor modulators, *ARTERIAL diseases

Abstract

The lower incidence of cardiovascular diseases in pre-menopausal women compared to men is well-known documented. This protection has been largely attributed to the protective effect of estrogens, which exert many beneficial effects against arterial diseases, including vasodilatation, acceleration of healing in response to arterial injury, arterial collateral growth and atheroprotection. More recently, with the visualization of the lymphatic vessels, the impact of estrogens on lymphedema and lymphatic diseases started to be elucidated. These estrogenic effects are mediated not only by the classic nuclear/genomic actions via the specific estrogen receptor (ER) α and β, but also by rapid extra-nuclear membrane-initiated steroid signaling (MISS). The ERs are expressed by endothelial, lymphatic and smooth muscle cells in the different vessels. In this review, we will summarize the complex vascular effects of estrogens and selective estrogen receptor modulators (SERMs) that have been described using different transgenic mouse models with selective loss of ERα function and numerous animal models of vascular and lymphatic diseases. [ABSTRACT FROM AUTHOR]

Published

2020

4. Lymphatic and blood systems: Identical or fraternal twins?

Author

Morfoisse, Florent and Noel, Agnès

Subjects

*LYMPHATICS, *TWINS, *CARDIOVASCULAR system, *BLOOD vessels, *BIOLOGY

Abstract

Blood and lymphatic systems work in close collaboration to ensure their respective physiological functions. The lymphatic vessel network is being extensively studied, but has been overlooked as compared to the blood vasculature mainly due to the problematic discrimination of lymphatic vessels from the blood ones. This issue has been fortunately resolved in the past decade leading to the emergence of a huge amount of data in lymphatic biology revealing many shared features with the blood vasculature. However, this likeliness between the two vascular systems may lead to a simplistic view of lymphatics and a direct transcription of what is known for the blood system to the lymphatic one, thereby neglecting the lymphatic specificities. In this context, this review aims to clarify the main differences between the two vascular systems focusing on recently discovered lymphatic features. [ABSTRACT FROM AUTHOR]

Published

2019

5. Mitochondrial Ribosomal Protein MRPS15 Is a Component of Cytosolic Ribosomes and Regulates Translation in Stressed Cardiomyocytes.

Author

David, Florian, Roussel, Emilie, Froment, Carine, Draia-Nicolau, Tangra, Pujol, Françoise, Burlet-Schiltz, Odile, Henras, Anthony K., Lacazette, Eric, Morfoisse, Florent, Tatin, Florence, Diaz, Jean-Jacques, Catez, Frédéric, Garmy-Susini, Barbara, and Prats, Anne-Catherine

Subjects

*GENETIC translation, *MITOCHONDRIAL proteins, *RIBOSOMAL proteins, *UNFOLDED protein response, *RIBOSOMES, *RNA regulation, *ENDOPLASMIC reticulum

Abstract

Regulation of mRNA translation is a crucial step in controlling gene expression in stressed cells, impacting many pathologies, including heart ischemia. In recent years, ribosome heterogeneity has emerged as a key control mechanism driving the translation of subsets of mRNAs. In this study, we investigated variations in ribosome composition in human cardiomyocytes subjected to endoplasmic reticulum stress induced by tunicamycin treatment. Our findings demonstrate that this stress inhibits global translation in cardiomyocytes while activating internal ribosome entry site (IRES)-dependent translation. Analysis of translating ribosome composition in stressed and unstressed cardiomyocytes was conducted using mass spectrometry. We observed no significant changes in ribosomal protein composition, but several mitochondrial ribosomal proteins (MRPs) were identified in cytosolic polysomes, showing drastic variations between stressed and unstressed cells. The most notable increase in polysomes of stressed cells was observed in MRPS15. Its interaction with ribosomal proteins was confirmed by proximity ligation assay (PLA) and immunoprecipitation, suggesting its intrinsic role as a ribosomal component during stress. Knock-down or overexpression experiments of MRPS15 revealed its role as an activator of IRES-dependent translation. Furthermore, polysome profiling after immunoprecipitation with anti-MRPS15 antibody revealed that the "MRPS15 ribosome" is specialized in translating mRNAs involved in the unfolded protein response. [ABSTRACT FROM AUTHOR]

Published

2024

6. Translational control by long non-coding RNAs.

Author

Godet, Anne-Claire, Roussel, Emilie, Laugero, Nathalie, Morfoisse, Florent, Lacazette, Eric, Garmy-Susini, Barbara, and Prats, Anne-Catherine

Subjects

*LINCRNA, *GENETIC regulation, *SENSE of direction, *GENE expression, *NON-coding RNA

Abstract

Long non-coding (lnc) RNAs, once considered as junk and useless, are now broadly recognized to have major functions in the cell. LncRNAs are defined as non-coding RNAs of more than 200 nucleotides, regulate all steps of gene expression. Their origin is diverse, they can arise from intronic, intergenic or overlapping region, in sense or antisense direction. LncRNAs are mainly described for their action on transcription, while their action at the translational level is more rarely cited. However, the bibliography in the field is more and more abundant. The present synopsis of lncRNAs involved in the control of translation reveals a wide field of regulation of gene expression, with at least nine distinct molecular mechanisms. Furthermore, it appears that all these lncRNAs are involved in various pathologies including cancer, cardiovascular and neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2024

7. Specific Circular RNA Signature of Endothelial Cells: Potential Implications in Vascular Pathophysiology.

Author

Diallo, Leïla Halidou, Mariette, Jérôme, Laugero, Nathalie, Touriol, Christian, Morfoisse, Florent, Prats, Anne-Catherine, Garmy-Susini, Barbara, and Lacazette, Eric

Subjects

*CIRCULAR RNA, *ENDOTHELIAL cells, *GENE expression, *VASCULAR endothelial cells, *PHYSIOLOGY, *PATHOLOGICAL physiology

Abstract

Circular RNAs (circRNAs) are a recently characterized family of gene transcripts forming a covalently closed loop of single-stranded RNA. The extent of their potential for fine-tuning gene expression is still being discovered. Several studies have implicated certain circular RNAs in pathophysiological processes within vascular endothelial cells and cancer cells independently. However, to date, no comparative study of circular RNA expression in different types of endothelial cells has been performed and analysed through the lens of their central role in vascular physiology and pathology. In this work, we analysed publicly available and original RNA sequencing datasets from arterial, veinous, and lymphatic endothelial cells to identify common and distinct circRNA expression profiles. We identified 4713 distinct circRNAs in the compared endothelial cell types, 95% of which originated from exons. Interestingly, the results show that the expression profile of circular RNAs is much more specific to each cell type than linear RNAs, and therefore appears to be more suitable for distinguishing between them. As a result, we have discovered a specific circRNA signature for each given endothelial cell type. Furthermore, we identified a specific endothelial cell circRNA signature that is composed four circRNAs: circCARD6, circPLXNA2, circCASC15 and circEPHB4. These circular RNAs are produced by genes that are related to endothelial cell migration pathways and cancer progression. More detailed studies of their functions could lead to a better understanding of the mechanisms involved in physiological and pathological (lymph)angiogenesis and might open new ways to tackle tumour spread through the vascular system. [ABSTRACT FROM AUTHOR]

Published

2024

8. Long non-coding RNA Neat1 and paraspeckle components are translational regulators in hypoxia.

Author

Godet, Anne-Claire, Roussel, Emilie, David, Florian, Hantelys, Fransky, Morfoisse, Florent, Alves, Joffrey, Pujol, Françoise, Ader, Isabelle, Bertrand, Edouard, Burlet-Schiltz, Odile, Froment, Carine, Henras, Anthony K., Vitali, Patrice, Lacazette, Eric, Tatin, Florence, Garmy-Susini, Barbara, and Prats, Anne-Catherine

Subjects

*VASCULAR endothelial growth factors, *HYPOXEMIA, *LINCRNA, *NUCLEOLIN, *MASS spectrometry

Abstract

Internal ribosome entry sites (IRESs) drive translation initiation during stress. In response to hypoxia, (lymph)angiogenic factors responsible for tissue revascularization in ischemic diseases are induced by the IRES-dependent mechanism. Here, we searched for IRES trans-acting factors (ITAFs) active in early hypoxia in mouse cardiomyocytes. Using knock-down and proteomics approaches, we show a link between a stressed-induced nuclear body, the paraspeckle, and IRES-dependent translation. Furthermore, smiFISH experiments demonstrate the recruitment of IRES-containing mRNA into paraspeckle during hypoxia. Our data reveal that the long non-coding RNA Neat1, an essential paraspeckle component, is a key translational regulator, active on IRESs of (lymph)angiogenic and cardioprotective factor mRNAs. In addition, paraspeckle proteins p54nrb and PSPC1 as well as nucleolin and RPS2, two p54nrb-interacting proteins identified by mass spectrometry, are ITAFs for IRES subgroups. Paraspeckle thus appears as a platform to recruit IRES-containing mRNAs and possibly host IRESome assembly. Polysome PCR array shows that Neat1 isoforms regulate IRES-dependent translation and, more widely, translation of mRNAs involved in stress response. [ABSTRACT FROM AUTHOR]

Published

2022

9. High Level of Staufen1 Expression Confers Longer Recurrence Free Survival to Non-Small Cell Lung Cancer Patients by Promoting THBS1 mRNA Degradation.

Author

Bonnet-Magnaval, Florence, Diallo, Leïla Halidou, Brunchault, Valérie, Laugero, Nathalie, Morfoisse, Florent, David, Florian, Roussel, Emilie, Nougue, Manon, Zamora, Audrey, Marchaud, Emmanuelle, Tatin, Florence, Prats, Anne-Catherine, Garmy-Susini, Barbara, DesGroseillers, Luc, and Lacazette, Eric

Subjects

*NON-small-cell lung carcinoma, *CELL adhesion molecules, *CANCER patients, *NON-coding RNA, *CELL survival, *CELL migration, *MESSENGER RNA, *CELL adhesion

Abstract

Stau1 is a pluripotent RNA-binding protein that is responsible for the post-transcriptional regulation of a multitude of transcripts. Here, we observed that lung cancer patients with a high Stau1 expression have a longer recurrence free survival. Strikingly, Stau1 did not impair cell proliferation in vitro, but rather cell migration and cell adhesion. In vivo, Stau1 depletion favored tumor progression and metastases development. In addition, Stau1 depletion strongly impaired vessel maturation. Among a panel of candidate genes, we specifically identified the mRNA encoding the cell adhesion molecule Thrombospondin 1 (THBS1) as a new target for Staufen-mediated mRNA decay. Altogether, our results suggest that regulation of THBS1 expression by Stau1 may be a key process involved in lung cancer progression. [ABSTRACT FROM AUTHOR]

Published

2022