8 results on '"Florentin, Jonathan"'
Search Results
2. A murine experimental model of the pulmonary thrombotic effect induced by the venom of the snake Bothrops lanceolatus.
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Rucavado, Alexandra, Camacho, Erika, Escalante, Teresa, Lomonte, Bruno, Fernández, Julián, Solano, Daniela, Quirós-Gutiérrez, Isabel, Ramírez-Vargas, Gabriel, Vargas, Karol, Argüello, Ivette, Navarro, Alejandro, Abarca, Carlos, Segura, Álvaro, Florentin, Jonathan, Kallel, Hatem, Resiere, Dabor, Neviere, Remi, and Gutiérrez, José María
- Subjects
SNAKE venom ,DISSEMINATED intravascular coagulation ,PARTIAL thromboplastin time ,ANTIVENINS ,VENOM ,SNAKEBITES - Abstract
Background: The venom of Bothrops lanceolatus, a viperid species endemic to the Lesser Antillean Island of Martinique, induces thrombosis in a number of patients. Previous clinical observations indicate that thrombotic events are more common in patients bitten by juvenile specimens. There is a need to develop an experimental model of this effect in order to study the mechanisms involved. Methodology/Principal findings: The venoms of juvenile and adult specimens of B. lanceolatus were compared by (a) describing their proteome, (b) assessing their ability to induce thrombosis in a mouse model, and (c) evaluating their in vitro procoagulant activity and in vivo hemostasis alterations. Venom proteomes of juvenile and adult specimens were highly similar, albeit showing some differences. When injected by the intraperitoneal (i.p.) route, the venom of juvenile specimens induced the formation of abundant thrombi in the pulmonary vasculature, whereas this effect was less frequent in the case of adult venom. Thrombosis was not abrogated by the metalloproteinase inhibitor Batimastat. Both venoms showed a weak in vitro procoagulant effect on citrated mouse plasma and bovine fibrinogen. When administered intravenously (i.v.) venoms did not affect classical clotting tests (prothrombin time and activated partial thromboplastin time) but caused a partial drop in fibrinogen concentration. The venom of juvenile specimens induced partial alterations in some rotational thromboelastometry parameters after i.v. injection. When venoms were administered i.p., only minor alterations in classical clotting tests were observed with juvenile venom, and no changes occurred for either venom in rotational thromboelastometry parameters. Both juvenile and adult venoms induced a marked thrombocytopenia after i.p. injection. Conclusions/Significance: An experimental model of the thrombotic effect induced by B. lanceolatus venom was developed. This effect is more pronounced in the case of venom of juvenile specimens, despite the observation that juvenile and adult venom proteomes are similar. Adult and juvenile venoms do not induce a consumption coagulopathy characteristic of other Bothrops sp venoms. Both venoms induce a conspicuous thrombocytopenia. This experimental model reproduces the main clinical findings described in these envenomings and should be useful to understand the mechanisms of the thrombotic effect. Author summary: Envenomings by the viperid species Bothrops lanceolatus, endemic of the Caribbean Island of Martinique, are characterized by a thrombotic effect responsible for infarcts in various organs. Until now, no experimental in vivo models of this effect have been described. In this study, we developed a mouse model of thrombosis by using the intraperitoneal route of venom injection. The venom of juvenile specimens of B. lanceolatus induced the formation of abundant thrombi in the lungs, whereas the effect was much less pronounced with the venom of adult specimens. This difference in the ability of juvenile and adult venoms occurs despite both venoms having highly similar proteomic profiles. Both adult and juvenile venoms showed a weak in vitro procoagulant effect on plasma and fibrinogen, underscoring a thrombin-like (pseudo-procoagulant) activity. In vivo, the venoms did not affect the classical clotting tests (prothrombin time and activated partial thromboplastin time) but induced a partial drop in fibrinogen concentration and limited alterations in rotational thromboelastometry parameters when injected by the i.v. route. In contrast, few alterations of these parameters were observed after i.p. injection of venoms, in conditions in which thrombosis occurred, hence evidencing the lack of a consumption coagulopathy. After i.p. injection both venoms induced a pronounced thrombocytopenia. This experimental model reproduces some of the main clinical manifestations of envenoming by this species. This model can be used to identify the toxins responsible for the thrombotic effect, to study the mechanism(s) of thrombosis and to assess the preclinical efficacy of antivenoms and novel therapies. [ABSTRACT FROM AUTHOR]
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- 2024
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3. The Contrasting Effects of Bothrops lanceolatus and Bothrops atrox Venom on Procoagulant Activity and Thrombus Stability under Blood Flow Conditions.
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Radouani, Fatima, Jalta, Prisca, Rapon, Caroline, Lezin, Chloe, Branford, Chelsea, Florentin, Jonathan, Gutierrez, Jose Maria, Resiere, Dabor, Neviere, Remi, and Pierre-Louis, Olivier
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FER-de-lance ,DISSEMINATED intravascular coagulation ,BLOOD coagulation factors ,BLOOD coagulation ,SHEARING force ,FIBRIN - Abstract
Background: Consumption coagulopathy and hemorrhagic syndrome are the typical features of Bothrops sp. snake envenoming. In contrast, B. lanceolatus envenoming can induce thrombotic complications. Our aim was to test whether crude B. lanceolatus and B. atrox venoms would display procoagulant activity and induce thrombus formation under flow conditions. Methods and Principal Findings: Fibrin formation in human plasma was observed for B. lanceolatus venom at 250–1000 ng/mL concentrations, which also induced clot formation in purified human fibrinogen, indicating thrombin-like activity. The degradation of fibrinogen confirmed the fibrinogenolytic activity of B. lanceolatus venom. B. lanceolatus venom displayed consistent thrombin-like and kallikrein-like activity increases in plasma conditions. The well-known procoagulant B. atrox venom activated plasmatic coagulation factors in vitro and induced firm thrombus formation under high shear rate conditions. In contrast, B. lanceolatus venom induced the formation of fragile thrombi that could not resist shear stress. Conclusions: Our results suggest that crude B. lanceolatus venom displays amidolytic activity and can activate the coagulation cascade, leading to prothrombin activation. B. lanceolatus venom induces the formation of an unstable thrombus under flow conditions, which can be prevented by the specific monovalent antivenom Bothrofav
® . [ABSTRACT FROM AUTHOR]- Published
- 2024
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4. Bothrops lanceolatus Envenoming in Martinique: A Historical Perspective of the Clinical Effectiveness of Bothrofav Antivenom Treatment
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Resiere, Dabor, primary, Florentin, Jonathan, additional, Mehdaoui, Hossein, additional, Kallel, Hatem, additional, Legris-Allusson, Veronique, additional, Gueye, Papa, additional, and Neviere, Remi, additional
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- 2024
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5. Aberrant mitochondrial DNA synthesis in macrophages exacerbates inflammation and atherosclerosis.
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Natarajan, Niranjana, Florentin, Jonathan, Johny, Ebin, Xiao, Hanxi, O'Neil, Scott Patrick, Lei, Liqun, Shen, Jixing, Ohayon, Lee, Johnson, Aaron R., Rao, Krithika, Li, Xiaoyun, Zhao, Yanwu, Zhang, Yingze, Tavakoli, Sina, Shiva, Sruti, Das, Jishnu, and Dutta, Partha
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CELL adhesion molecules ,DNA synthesis ,TRANSCRIPTION factors ,ATHEROSCLEROTIC plaque ,TRANSCRIPTOMES ,MITOCHONDRIAL DNA - Abstract
There is a large body of evidence that cellular metabolism governs inflammation, and that inflammation contributes to the progression of atherosclerosis. However, whether mitochondrial DNA synthesis affects macrophage function and atherosclerosis pathology is not fully understood. Here we show, by transcriptomic analyzes of plaque macrophages, spatial single cell transcriptomics of atherosclerotic plaques, and functional experiments, that mitochondrial DNA (mtDNA) synthesis in atherosclerotic plaque macrophages are triggered by vascular cell adhesion molecule 1 (VCAM-1) under inflammatory conditions in both humans and mice. Mechanistically, VCAM-1 activates C/EBPα, which binds to the promoters of key mitochondrial biogenesis genes - Cmpk2 and Pgc1a. Increased CMPK2 and PGC-1α expression triggers mtDNA synthesis, which activates STING-mediated inflammation. Consistently, atherosclerosis and inflammation are less severe in Apoe
−/− mice lacking Vcam1 in macrophages. Downregulation of macrophage-specific VCAM-1 in vivo leads to decreased expression of LYZ1 and FCOR, involved in STING signalling. Finally, VCAM-1 expression in human carotid plaque macrophages correlates with necrotic core area, mitochondrial volume, and oxidative damage to DNA. Collectively, our study highlights the importance of macrophage VCAM-1 in inflammation and atherogenesis pathology and proposes a self-acerbating pathway involving increased mtDNA synthesis. Macrophages and their metabolism are known to contribute to inflammation in the atherosclerotic plaques, but the underpinning molecular level regulatory processes are lesser known. Here authors show that under inflammatory conditions, macrophages express VCAM-1 within the atherosclerotic plaques, which leads to increased mitochondrial DNA synthesis via activation of the transcription factor C/EBPα, which in turn triggers inflammation by STING signalling. [ABSTRACT FROM AUTHOR]- Published
- 2024
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6. A health strategy for chlordecone (Kepone) exposure in the French Territories of America
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Resiere, Dabor, Lapostolle, Fréderic, Florentin, Jonathan, Banydeen, Rishika, Gueye, Papa, Pujo, Jean, Mégarbane, Bruno, Kallel, Hatem, and Névière, Rémi
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- 2024
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7. [Sargassum seaweed assaults the French West Indies].
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Resiere D, Florentin J, and Nevière R
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- Humans, Hydrogen Sulfide poisoning, Hydrogen Sulfide toxicity, Guadeloupe epidemiology, Martinique epidemiology, Ammonia toxicity, West Indies epidemiology, Environmental Exposure adverse effects, Sargassum, Seaweed
- Abstract
SARGASSUM SEAWEED AS SAULTS THE FRENCH WEST INDIES. Since 2011, Martinique and the islands of Guadeloupe have been affected by repeated groundings, culminating in an exceptional wave in 2018. While the sargassum ( Sargassum natans and S. fluitans ) involved in these phenomena are neither toxic nor urticating, indirect toxicity linked to the presence of microorganisms and heavy metals (arsenic, mercury, etc.) in sargassum clusters has been described. Similarly, after a 24 to 48 hours stay on the shore, sargassum algae enter a putrefaction cycle responsible to produce hydrogen sulfide (H2S) and ammonia (NH3). The acute toxicity of these gases is well known. However, very few data are available on the clinical effects of prolonged exposure to low doses of H2S and NH3. Our team has recently described the syndromic features of chronic exposure, supposing for deleterious effects on the cardiovascular, respiratory and neurological systems., Competing Interests: Les auteurs déclarent n’avoir aucun lien d’intérêts.
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- 2024
8. Addressing snakebite envenoming as a One Health issue in the Caribbean.
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Resiere D, Florentin J, Névière R, Gomez A, and Kallel H
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- 2024
- Full Text
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