24 results on '"Cavey T"'
Search Results
2. Letter: wide variation in faecal calprotectin values according to the assay
- Author
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Sun, S., Cavey, T., Peltier, L., Bendavid, C., and Bouguen, G.
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- 2016
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3. Clinical management of hemochromatosis: current perspectives
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Brissot P, Cavey T, Ropert M, Guggenbuhl P, and Loréal O
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phlebotomy ,lcsh:R ,nutritional and metabolic diseases ,Iron overload ,lcsh:Medicine ,HFE ,hepcidin ,hemochromatosis ,ferroportin - Abstract
Pierre Brissot,1 Thibault Cavey,1,2 Martine Ropert,1,2 Pascal Guggenbuhl,1,3 Olivier Loréal1 1Inserm UMR991, 2Laboratory of Biochemistry, 3Department of Rheumatology, University Hospital, Rennes, France Abstract: Hemochromatosis (HC) corresponds to systemic iron overload of genetic origin. Its spectrum covers HFE-related HC, a frequent disease exclusively present in Caucasians; however, several entities of non-HFE-related HC, which correspond to very rare disorders, have been observed in both Caucasian and non-Caucasian populations. In most HC forms, iron overload is explained by hepcidin deficiency, which increases iron delivery into the plasma from both duodenal and splenic sources, with subsequent organ iron deposition. The diagnosis depends on a noninvasive approach combining clinical, biological, and imaging data. The treatment remains largely based on phlebotomy therapy, which is rarely replaced with erythrocytapheresis or chelation therapy. Hepcidin supplementation represents the logical therapeutics of the future for all HC forms related to hepcidin deficiency. Keywords: iron overload, HFE, ferroportin, hemojuvelin, transferrin receptor 2, hepcidin, phlebotomy
- Published
- 2017
4. L’analyse du sérum par spectroscopie moyen infrarouge permet d’obtenir une signature du statut métabolique du foie chez la souris
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Le Corvec, M., primary, Allain, C., additional, Lardjane, S., additional, Cavey, T., additional, Turlin, B., additional, Fautrel, A., additional, Begriche, K., additional, Monbet, V., additional, Fromenty, B., additional, Leroyer, P., additional, Guggenbuhl, P., additional, Ropert, M., additional, Sire, O., additional, and Loréal, O., additional
- Published
- 2016
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5. Letter: wide variation in faecal calprotectin values according to the assay
- Author
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Sun, S., primary, Cavey, T., additional, Peltier, L., additional, Bendavid, C., additional, and Bouguen, G., additional
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- 2015
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6. P006: Inter-relations entre le fer et des métaux non ferreux chez la souris : mise en évidence d’une incidence du contexte génétique
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Cavey, T., primary, Ropert, M., additional, De Tayrac, M., additional, Bardou-Jacquet, E., additional, Leroyer, P., additional, Bendavid, C., additional, Brissot, P., additional, and Loréal, O., additional
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- 2014
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7. Somatostatin and opioid receptors do not regulate proliferation or apoptosis of the human multiple myeloma U266 cells
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Allouche Stéphane, Jauzac Philippe, Sola Brigitte, Cavey Thibault, and Kerros Céline
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Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
Abstract Background opioid and somatostatin receptors (SSTRs) that can assemble as heterodimer were individually reported to modulate malignant cell proliferation and to favour apoptosis. Materials and methods: SSTRs and opioid receptors expression were examined by RT-PCR, western-blot and binding assays, cell proliferation was studied by XTT assay and propidium iodide (PI) staining and apoptosis by annexin V-PI labelling. Results almost all human malignant haematological cell lines studied here expressed the five SSTRs. Further experiments were conducted on the human U266 multiple myeloma cells, which express also μ-opioid receptors (MOP-R). XTT assays and cell cycle studies provide no evidence for a significant effect upon opioid or somatostatin receptors stimulation. Furthermore, neither direct effect nor potentiation of the Fas-receptor pathway was detected on apoptosis after these treatments. Conclusion these data suggest that SSTRs or opioid receptors expression is not a guaranty for an anti-tumoral action in U266 cell line.
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- 2009
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8. Differences in bone microarchitecture between genetic and secondary iron-overload mouse models suggest a role for hepcidin deficiency in iron-related osteoporosis.
- Author
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Robin F, Chappard D, Leroyer P, Latour C, Mabilleau G, Monbet V, Cavey T, Horeau M, Derbré F, Roth MP, Ropert M, Guggenbuhl P, and Loréal O
- Subjects
- Animals, Mice, Iron metabolism, Hepcidins genetics, Hepcidins metabolism, Alkaline Phosphatase metabolism, Hemochromatosis Protein genetics, Histocompatibility Antigens Class I genetics, Liver metabolism, Collagen metabolism, Mice, Knockout, Hemochromatosis genetics, Iron Overload complications, Iron Overload genetics, Iron Overload metabolism, Osteoporosis genetics
- Abstract
Iron overload is one of the secondary osteoporosis etiologies. Cellular and molecular mechanisms involved in iron-related osteoporosis are not fully understood., Aim: The aim of the study was to investigate the respective roles of iron excess and hepcidin, the systemic iron regulator, in the development of iron-related osteoporosis., Material and Methods: We used mice models with genetic iron overload (GIO) related to hepcidin deficiency (Hfe
-/- and Bmp6-/- ) and secondary iron overload (SIO) exhibiting a hepcidin increase secondary to iron excess. Iron concentration and transferrin saturation levels were evaluated in serum and hepatic, spleen, and bone iron concentrations were assessed by ICP-MS and Perl's staining. Gene expression was evaluated by quantitative RT-PCR. Bone micro-architecture was evaluated by micro-CT. The osteoblastic MC3T3 murine cells that are able to mineralize were exposed to iron and/or hepcidin., Results: Despite an increase of bone iron concentration in all overloaded mice models, bone volume/total volume (BV/TV) and trabecular thickness (Tb.Th) only decreased significantly in GIO, at 12 months for Hfe-/- and from 6 months for Bmp6-/- . Alterations in bone microarchitecture in the Bmp6-/- model were positively correlated with hepcidin levels (BV/TV (ρ = +.481, p < .05) and Tb.Th (ρ = +.690, p < .05). Iron deposits were detected in the bone trabeculae of Hfe-/- and Bmp6-/- mice, while iron deposits were mainly visible in bone marrow macrophages in secondary iron overload. In cell cultures, ferric ammonium citrate exposure abolished the mineralization process for concentrations above 5 μM, with a parallel decrease in osteocalcin, collagen 1, and alkaline phosphatase mRNA levels. Hepcidin supplementation of cells had a rescue effect on the collagen 1 and alkaline phosphatase expression level decrease., Conclusion: Together, these data suggest that iron in excess alone is not sufficient to induce osteoporosis and that low hepcidin levels also contribute to the development of osteoporosis., (© 2023 Federation of American Societies for Experimental Biology.)- Published
- 2023
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9. H fe Gene Knock-Out in a Mouse Model of Hereditary Hemochromatosis Affects Bodily Iron Isotope Compositions.
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Albalat E, Cavey T, Leroyer P, Ropert M, Balter V, and Loréal O
- Abstract
Hereditary hemochromatosis is a genetic iron overload disease related to a mutation within the HFE gene that controls the expression of hepcidin, the master regulator of systemic iron metabolism. The natural stable iron isotope composition in whole blood of control subjects is different from that of hemochromatosis patients and is sensitive to the amount of total iron removed by the phlebotomy treatment. The use of stable isotopes to unravel the pathological mechanisms of iron overload diseases is promising but hampered by the lack of data in organs involved in the iron metabolism. Here, we use H fe
-/- mice, a model of hereditary hemochromatosis, to study the impact of the knock-out on iron isotope compositions of erythrocytes, spleen and liver. Iron concentration increases in liver and red blood cells of H fe-/- mice compared to controls. The iron stable isotope composition also increases in liver and erythrocytes, consistent with a preferential accumulation of iron heavy isotopes in H fe-/- mice. In contrast, no difference in the iron concentration nor isotope composition is observed in spleen of H fe-/- and control mice. Our results in mice suggest that the observed increase of whole blood isotope composition in hemochromatosis human patients does not originate from, but is aggravated by, bloodletting. The subsequent rapid increase of whole blood iron isotope composition of treated hemochromatosis patients is rather due to the release of hepatic heavy isotope-enriched iron than augmented iron dietary absorption. Further research is required to uncover the iron light isotope component that needs to balance the accumulation of hepatic iron heavy isotope, and to better understand the iron isotope fractionation associated to metabolism dysregulation during hereditary hemochromatosis., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Albalat, Cavey, Leroyer, Ropert, Balter and Loréal.)- Published
- 2021
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10. Intermittent reloading does not prevent reduction in iron availability and hepcidin upregulation caused by hindlimb unloading.
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Nay K, Martin D, Orfila L, Saligaut D, Martin B, Horeau M, Cavey T, Kenawi M, Island ML, Ropert M, Loréal O, Koechlin-Ramonatxo C, and Derbré F
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- Animals, Male, Muscular Atrophy metabolism, Myosin Heavy Chains metabolism, Rats, Wistar, Up-Regulation, Rats, Hepcidins metabolism, Hindlimb metabolism, Hindlimb Suspension physiology, Iron metabolism, Muscle, Skeletal metabolism
- Abstract
New Findings: What is the central question of this study? Could skeletal muscle be involved in microgravity-induced iron misdistribution by modulating expression of hepcidin, the master regulator of iron metabolism? What is the main finding and its importance? We demonstrate, in rats, that hepcidin upregulation is not a transient adaptation associated with early exposure to microgravity and that intermittent reloading does not limit microgravity-induced iron misdistribution despite having a beneficial effect on soleus muscle wasting., Abstract: In humans, exposure to microgravity during spaceflight causes muscle atrophy, changes in iron storage and a reduction in iron availability. We previously observed that during 7 days of simulated microgravity in rats, hepcidin plays a key role in iron misdistribution, and we suggested that a crosstalk between skeletal muscle and liver could regulate hepcidin synthesis in this context. In the present study in rats, we investigated the medium-term effects of simulated microgravity on iron metabolism. We also tested whether intermittent reloading (IR) to target skeletal muscle atrophy limits iron misdistribution efficiently. For this purpose, Wistar rats underwent 14 days of hindlimb unloading (HU) combined or not combined with daily IR. At the end of this period, the serum iron concentration and transferrin saturation were significantly reduced, whereas hepatic hepcidin mRNA was upregulated. However, the main signalling pathways involved in hepcidin synthesis in the liver (BMP-small mothers against decapentaplegic (SMAD), interleukin-6-STAT3 and ERK1/2) were unaffected. Unlike what was observed after 7 days of HU, the iron concentration in the spleen, liver and skeletal muscle was comparable between control animals and those that underwent HU or HU plus IR for 14 days. Despite its beneficial effect on soleus muscle atrophy and slow-to-fast myosin heavy chain distribution, IR did not significantly prevent a reduction in iron availability and hepcidin upregulation. Altogether, these results highlight that iron availability is durably reduced during longer exposure to simulated microgravity and that the related hepcidin upregulation is not a transient adaptation to these conditions. The results also suggest that skeletal muscle does not necessarily play a key role in the iron misdistribution that occurs during simulated microgravity., (© 2020 The Authors. Experimental Physiology © 2020 The Physiological Society.)
- Published
- 2021
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11. Ceruloplasmin deficiency does not induce macrophagic iron overload: lessons from a new rat model of hereditary aceruloplasminemia.
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Kenawi M, Rouger E, Island ML, Leroyer P, Robin F, Rémy S, Tesson L, Anegon I, Nay K, Derbré F, Brissot P, Ropert M, Cavey T, and Loréal O
- Subjects
- Animals, Base Sequence, CRISPR-Cas Systems, Ceruloplasmin antagonists & inhibitors, Ceruloplasmin genetics, Female, Iron analysis, Iron Metabolism Disorders genetics, Iron Metabolism Disorders pathology, Iron Overload etiology, Liver metabolism, Liver pathology, Macrophages metabolism, Male, Mutation, Neurodegenerative Diseases genetics, Neurodegenerative Diseases pathology, Rats, Rats, Sprague-Dawley, Sequence Homology, Spleen metabolism, Spleen pathology, Ceruloplasmin deficiency, Disease Models, Animal, Iron metabolism, Iron Metabolism Disorders complications, Iron Overload pathology, Macrophages pathology, Neurodegenerative Diseases complications
- Abstract
Hereditary aceruloplasminemia (HA), related to mutations in the ceruloplasmin ( Cp ) gene, leads to iron accumulation. Ceruloplasmin ferroxidase activity being considered essential for macrophage iron release, macrophage iron overload is expected, but it is not found in hepatic and splenic macrophages in humans. Our objective was to get a better understanding of the mechanisms leading to iron excess in HA. A clustered regularly interspaced short palindromic repeats (CRISPR)/ CRISPR associated protein 9 (Cas9) knockout of the Cp gene was performed on Sprague-Dawley rats. We evaluated the iron status in plasma, the expression of iron metabolism genes, and the status of other metals whose interactions with iron are increasingly recognized. In Cp
-/- rats, plasma ceruloplasmin and ferroxidase activity were absent, together with decreased iron concentration and transferrin saturation. Similarly as in humans, the hepatocytes were iron overloaded conversely to hepatic and splenic macrophages. Despite a relative hepcidin deficiency in Cp-/- rats and the loss of ferroxidase activity, potentially expected to limit the interaction of iron with transferrin, no increase of plasma non-transferrin-bound iron level was found. Copper was decreased in the spleen, whereas manganese was increased in the plasma. These data suggest that the reported role of ceruloplasmin cannot fully explain the iron hepatosplenic phenotype in HA, encouraging the search for additional mechanisms.-Kenawi, M., Rouger, E., Island, M.-L., Leroyer, P., Robin, F., Remy, S., Tesson, L., Anegon, I., Nay, K., Derbré, F., Brissot, P., Ropert, M., Cavey, T., Loréal, O. Ceruloplasmin deficiency does not induce macrophagic iron overload: lessons from a new rat model of hereditary aceruloplasminemia.- Published
- 2019
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12. Skeletal muscle ceramides do not contribute to physical-inactivity-induced insulin resistance.
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Appriou Z, Nay K, Pierre N, Saligaut D, Lefeuvre-Orfila L, Martin B, Cavey T, Ropert M, Loréal O, Rannou-Bekono F, and Derbré F
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- Adenylate Kinase metabolism, Animals, Fatty Acids, Monounsaturated pharmacology, Glucose Tolerance Test, Glucose Transporter Type 4 metabolism, Male, Mice, Mice, Inbred C57BL, Phosphorylation, Physical Conditioning, Animal, Proto-Oncogene Proteins c-akt metabolism, Sphingolipids analysis, Triglycerides analysis, Ceramides analysis, Insulin Resistance, Muscle, Skeletal chemistry, Sedentary Behavior
- Abstract
Physical inactivity increases the risk to develop type 2 diabetes, a disease characterized by a state of insulin resistance. By promoting inflammatory state, ceramides are especially recognized to alter insulin sensitivity in skeletal muscle. The present study was designed to analyze, in mice, whether muscle ceramides contribute to physical-inactivity-induced insulin resistance. For this purpose, we used the wheel lock model to induce a sudden reduction of physical activity, in combination with myriocin treatment, an inhibitor of de novo ceramide synthesis. Mice were assigned to 3 experimental groups: voluntary wheel access group (Active), a wheel lock group (Inactive), and wheel lock group treated with myriocin (Inactive-Myr). We observed that 10 days of physical inactivity induces hyperinsulinemia and increases basal insulin resistance (HOMA-IR). The muscle ceramide content was not modified by physical inactivity and myriocin. Thus, muscle ceramides do not play a role in physical-inactivity-induced insulin resistance. In skeletal muscle, insulin-stimulated protein kinase B phosphorylation and inflammatory pathway were not affected by physical inactivity, whereas a reduction of glucose transporter type 4 content was observed. Based on these results, physical-inactivity-induced insulin resistance seems related to a reduction in glucose transporter type 4 content rather than defects in insulin signaling. We observed in inactive mice that myriocin treatment improves glucose tolerance, insulin-stimulated protein kinase B, adenosine-monophosphate-activated protein kinase activation, and glucose transporter type 4 content in skeletal muscle. Such effects occur regardless of changes in muscle ceramide content. These findings open promising research perspectives to identify new mechanisms of action for myriocin on insulin sensitivity and glucose metabolism.
- Published
- 2019
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13. Spleen iron, molybdenum, and manganese concentrations are coregulated in hepcidin-deficient and secondary iron overload models in mice.
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Cavey T, Latour C, Island ML, Leroyer P, Guggenbuhl P, Coppin H, Roth MP, Bendavid C, Brissot P, Ropert M, and Loréal O
- Subjects
- Animals, Hepcidins deficiency, Hepcidins metabolism, Iron Overload genetics, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Spleen metabolism, Hepcidins genetics, Iron metabolism, Iron Overload metabolism, Manganese metabolism, Molybdenum metabolism
- Abstract
Iron excess increases the hepatic expression of hepcidin, the systemic iron metabolism regulator that favors iron sequestration in the spleen. Genetic iron overload related to hepcidin insufficiency decreases the spleen iron concentration and increases hepatic iron concentration, whereas during secondary iron overload, the hepcidin expression increases together with spleen iron concentration in addition to hepatic iron concentrations increase. Links between iron metabolism and other metals being suggested, our aim was to investigate, during iron overload, the relationships between the hepatic hepcidin expression level and the hepatic and splenic concentrations of iron, manganese, copper, zinc, and molybdenum, determined using inductively coupled plasma mass spectrometry. Hepcidin-deficient mice, secondary iron overload mice models, and their respective controls were studied. Spleen molybdenum and manganese concentrations paralleled the modulation of both spleen iron concentrations, increasing in secondary iron overload and decreasing in hepcidin deficiency related iron overload, as well as hepatic hepcidin mRNA expression. Our data suggest that iron, manganese, and molybdenum metabolisms could share mechanisms controlling their distribution that are associated to hepcidin modulation. In diseases with abnormal hepcidin levels, including chronic inflammation, special attention should be paid to those metals that can participate with the phenotype.-Cavey, T., Latour, C., Island, M.-L., Leroyer, P., Guggenbuhl, P., Coppin, H., Roth, M.-P., Bendavid, C., Brissot, P., Ropert, M., Loréal, O. Spleen iron, molybdenum, and manganese concentrations are coregulated in hepcidin-deficient and secondary iron overload models in mice.
- Published
- 2019
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14. [Metals: common clinical applications in inductively coupled plasma mass spectrometry].
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Cavey T, Ropert M, Loréal O, Bendavid C, and Peoc'h K
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- Animals, Blood Chemical Analysis methods, Body Fluids chemistry, Humans, Mass Spectrometry methods, Metals blood, Pre-Analytical Phase methods, Pre-Analytical Phase standards, Metals analysis, Plasma Gases chemistry, Spectrometry, Mass, Electrospray Ionization methods
- Abstract
Inductively coupled plasma mass spectrometry (ICP-MS) is an analytical technique for inorganic, quantitative, and multi-elemental compounds commonly used in clinical biology. In recent years, it has gradually replaced atomic absorption techniques. It is based on the combination of an ion source formed of an inductively coupled plasma torch by a high-frequency electromagnetic generator, and a mass spectrometer, which allows the separation of ions generated according to their mass and energy. It allows the simultaneous detection of most metal and metalloid elements (about 80, 40 generally). It is extremely sensitive for determining analyte concentrations up to nanograms per liter. ICP-MS is fast and suitable for continued use on different types of biological samples. Its use requires, however, good knowledge of the different types of interferences, whether spectral or non-spectral. This method may require specific adaptations depending on the samples used due to the matrix effect. In this review, we will present the main principles of the realization of dosages, as well as the various devices currently commercialized. It is currently used for the determination of the most critical metals in clinical biochemistry, copper, zinc, and selenium, but also in clinical toxicology and pharmacology.
- Published
- 2019
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15. Iron as a Therapeutic Target in HFE -Related Hemochromatosis: Usual and Novel Aspects.
- Author
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Loréal O, Cavey T, Robin F, Kenawi M, Guggenbuhl P, and Brissot P
- Abstract
Genetic hemochromatosis is an iron overload disease that is mainly related to the C282Y mutation in the HFE gene. This gene controls the expression of hepcidin, a peptide secreted in plasma by the liver and regulates systemic iron distribution. Homozygous C282Y mutation induces hepcidin deficiency, leading to increased circulating transferrin saturation, and ultimately, iron accumulation in organs such as the liver, pancreas, heart, and bone. Iron in excess may induce or favor the development of complications such as cirrhosis, liver cancer, diabetes, heart failure, hypogonadism, but also complaints such as asthenia and disabling arthritis. Iron depletive treatment mainly consists of venesections that permit the removal of iron contained in red blood cells and the subsequent mobilization of stored iron in order to synthesize hemoglobin for new erythrocytes. It is highly efficient in removing excess iron and preventing most of the complications associated with excess iron in the body. However, this treatment does not target the biological mechanisms involved in the iron metabolism disturbance. New treatments based on the increase of hepcidin levels, by using hepcidin mimetics or inducers, or inhibitors of the iron export activity of ferroportin protein that is the target of hepcidin, if devoid of significant secondary effects, should be useful to better control iron parameters and symptoms, such as arthritis.
- Published
- 2018
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16. Hemochromatosis: a model of metal-related human toxicosis.
- Author
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Brissot P, Cavey T, Ropert M, Gaboriau F, and Loréal O
- Subjects
- Hemochromatosis metabolism, Humans, Iron metabolism, Iron Overload, Liver drug effects, Liver metabolism, Hemochromatosis chemically induced, Iron toxicity
- Abstract
Many environmental agents, such as excessive alcohol intake, xenobiotics, and virus, are able to damage the human body, targeting especially the liver. Metal excess may also assault the liver. Thus, chronic iron overload may cause, especially when associated with cofactors, diffuse organ damage that is a source of significant morbidity and mortality. Iron excess can be either of acquired (mostly transfusional) or of genetic origin. Hemochromatosis is the archetype of genetic iron overload diseases and represents a serious health problem. A better understanding of iron metabolism has deeply modified the hemochromatosis field which today benefits from much more efficient diagnostic and therapeutic approaches.
- Published
- 2018
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17. Genetic hemochromatosis: Pathophysiology, diagnostic and therapeutic management.
- Author
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Brissot P, Cavey T, Ropert M, Guggenbuhl P, and Loréal O
- Subjects
- Hemochromatosis diagnosis, Hemochromatosis physiopathology, Hemochromatosis therapy, Hepcidins physiology, Humans, Iron metabolism, Hemochromatosis genetics
- Abstract
The term hemochromatosis (HC) corresponds to several diseases characterized by systemic iron overload of genetic origin and affecting both the quality of life and life expectancy. Major improvement in the knowledge of iron metabolism permits to divide these diseases into two main pathophysiological categories. For most HC forms (types 1, 2, 3 and 4B HC) iron overload is related to cellular hepcidin deprivation which causes an increase of plasma iron concentration and the appearance of plasma non-transferrin bound iron. In contrast, iron excess in type 4A ferroportin disease is related to decreased cellular iron export. Whatever the HC type, the diagnosis rests on a non-invasive strategy, combining clinical, biological and imaging data. The mainstay of the treatment remains venesection therapy with the perspective of hepcidin supplementation for hepcidin deprivation-related HC. Prevention of HC is critical at the family level and, for type 1 HC, remains a major goal, although still debated, at the population level., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)
- Published
- 2017
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18. Simulated microgravity decreases circulating iron in rats: role of inflammation-induced hepcidin upregulation.
- Author
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Cavey T, Pierre N, Nay K, Allain C, Ropert M, Loréal O, and Derbré F
- Subjects
- Animals, Hindlimb Suspension physiology, Inflammation blood, Inflammation metabolism, Interleukin-6 metabolism, Liver metabolism, Liver physiopathology, Male, RNA, Messenger metabolism, Rats, Rats, Wistar, STAT3 Transcription Factor metabolism, Signal Transduction physiology, Space Flight methods, Transcriptional Activation physiology, Weightlessness, Hepcidins metabolism, Inflammation physiopathology, Iron blood, Up-Regulation physiology
- Abstract
New Findings: What is the central question of this study? Although microgravity is well known to reduce circulating iron in astronauts, the underlying mechanism is still unknown. We investigated whether hepcidin, a key hormone regulating iron metabolism, could be involved in this deleterious effect. What is the main finding and its importance? We show that hindlimb suspension, a model of microgravity, stimulates the production of hepcidin in liver of rats. In agreement with the biological role of hepcidin, we found a decrease of circulating iron and an increase of spleen iron content in hindlimb-unloaded rats. Consequently, our study supports the idea that hepcidin could play a role in the alteration of iron metabolism parameters observed during spaceflight. During spaceflight, humans exposed to microgravity exhibit an increase of iron storage and a reduction of circulating iron. Such perturbations could promote oxidative stress and anaemia in astronauts. The mechanism by which microgravity modulates iron metabolism is still unknown. Herein, we hypothesized that microgravity upregulates hepcidin, a hormone produced by the liver that is the main controller of iron homeostasis. To test this hypothesis, rats were submitted to hindlimb unloading (HU), the reference model to mimic the effects of microgravity in rodents. After 7 days, the mRNA level of hepcidin was increased in the liver of HU rats (+74%, P = 0.001). In agreement with the biological role of hepcidin, we found an increase of spleen iron content (+78%, P = 0.030) and a decrease of serum iron concentration (-35%, P = 0.002) and transferrin saturation (-25%, P = 0.011) in HU rats. These findings support a role of hepcidin in microgravity-induced iron metabolism alteration. Furthermore, among the signalling pathways inducing hepcidin mRNA expression, we found that only the interleukin-6/signal transducer and activator of transcription 3 (IL-6/STAT3) axis was activated by HU, as shown by the increase of phospho-STAT3 (+193%, P < 0.001) and of the hepatic mRNA level of haptoglobin (+167%, P < 0.001), a STAT3-inducible gene, in HU rats. Taken together, these data support the idea that microgravity may alter iron metabolism through an inflammatory process upregulating hepcidin., (© 2017 The Authors. Experimental Physiology © 2017 The Physiological Society.)
- Published
- 2017
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19. Evaluation of the Impact of Renal Failure on Correlation and Concordance Between 2 Free Light Chain Assays.
- Author
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Moreau C, Autier B, Cavey T, Rouger E, Norwood J, Bendavid C, Escoffre M, Sébillot M, and Decaux O
- Subjects
- Biomarkers, Follow-Up Studies, Humans, Immunoglobulin G blood, Immunoglobulin kappa-Chains blood, Immunoglobulin lambda-Chains blood, Kidney Function Tests, Paraproteinemias blood, Paraproteinemias diagnosis, Renal Insufficiency etiology, Renal Insufficiency urine, Renal Insufficiency, Chronic blood, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic urine, Reproducibility of Results, Immunoglobulin Light Chains blood, Renal Insufficiency blood
- Abstract
Background: Free light chain (FLC) assays are essential for diagnosis and follow-up of plasma cell dyscrasia. Two assays are available: Freelite (Binding Site) and N Latex FLC (Siemens). The aim of our study was to evaluate the impact of renal failure on concordance and correlation between the 2 FLC assays., Methods: FLC measurements using both assays were performed on 1215 fresh serum samples from patients with or without monoclonal gammopathy and renal failure. Concordance and correlation were evaluated using Passing-Bablock regression, Pearson correlation coefficient, and the Cohen kappa coefficient, taking into account the renal failure stage (evaluated with Chronic Kidney Disease-Epidemiology Collaboration formulae) and evaluation of treatment response in patients' follow-up., Results: A good correlation was demonstrated between both assays, irrespective of the renal failure stage (Pearson correlation coefficient > 0.90). For FLC ratio interpretation, there remained 7.6% to 20.8% discordances between the 2 methods throughout the whole range of renal impairment. To evaluate FLC evolution in patient follow-up, 41 patients were selected with at least 6 consecutive serum samples being collected during the study period: we observed a concordant evolution of FLC concentrations between both assays. However, few discrepancies were observed with 4 patients., Conclusions: Despite adjusted reference ranges for Freelite FLC ratio, there are approximately 12.5% discrepancies in interpretation of FLC ratio between the 2 available assays. They are not linked to renal failure stage and neither of the assays performed better than the other: results must be interpreted taking into account clinical data and the same assay must be used for patient follow-up., (Copyright © 2016 Elsevier Inc. All rights reserved.)
- Published
- 2016
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20. Mid-infrared fibre evanescent wave spectroscopy of serum allows fingerprinting of the hepatic metabolic status in mice.
- Author
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Le Corvec M, Allain C, Lardjane S, Cavey T, Turlin B, Fautrel A, Begriche K, Monbet V, Fromenty B, Leroyer P, Guggenbuhl P, Ropert M, Sire O, and Loréal O
- Subjects
- Animals, Male, Mice, Mice, Inbred C57BL, Non-alcoholic Fatty Liver Disease metabolism, Obesity, Liver metabolism, Non-alcoholic Fatty Liver Disease blood, Spectrophotometry, Infrared
- Abstract
Non-alcoholic fatty liver disease is associated with obesity, diabetes, and metabolic syndrome. The detection of systemic metabolic changes associated with alterations in the liver status during non-alcoholic fatty liver disease could improve patient follow-up. The aim of the present study was to evaluate the potential of mid-infrared fibre evanescent wave spectroscopy as a minimum-invasive method for evaluating the liver status during non-alcoholic fatty liver disease. Seventy-five mice were subjected to a control, high-fat or high-fat-high carbohydrate diets. We analysed the serum biochemical parameters and mRNA levels of hepatic genes by quantitative RT-PCR. Steatosis was quantified by image analysis. The mid-infrared spectra were acquired from serum, and then analysed to develop a predictive model of the steatosis level. Animals subjected to enriched diets were obese. Hepatic steatosis was found in all animals. The relationship between the spectroscopy-predicted and observed levels of steatosis, expressed as percentages of the liver biopsy area, was not linear. A transition around 10% steatosis was observed, leading us to consider two distinct predictive models (<10% and >10%) based on two different sets of discriminative spectral variables. The model performance was evaluated using random cross-validation (10%). The hypothesis that additional metabolic changes occur beyond this transition was supported by the fact that it was associated with increased serum ALT levels, and Col1α1 chain mRNA levels. Our data suggest that mid-infrared spectroscopy combined with statistical analysis allows identifying serum mid-infrared signatures that reflect the liver status during non-alcoholic fatty liver disease.
- Published
- 2016
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21. Myriocin prevents muscle ceramide accumulation but not muscle fiber atrophy during short-term mechanical unloading.
- Author
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Salaun E, Lefeuvre-Orfila L, Cavey T, Martin B, Turlin B, Ropert M, Loreal O, and Derbré F
- Subjects
- Animals, Apoptosis drug effects, Fatty Acids metabolism, Hepatocytes drug effects, Hepatocytes metabolism, Hindlimb Suspension methods, Male, Muscle Fibers, Skeletal metabolism, Muscular Atrophy blood, Muscular Atrophy metabolism, Rats, Rats, Wistar, Transaminases blood, Ceramides metabolism, Fatty Acids, Monounsaturated pharmacology, Muscle Fibers, Skeletal drug effects, Muscular Atrophy drug therapy
- Abstract
Bedridden patients in intensive care unit or after surgery intervention commonly develop skeletal muscle weakness. The latter is promoted by a variety of prolonged hospitalization-associated conditions. Muscle disuse is the most ubiquitous and contributes to rapid skeletal muscle atrophy and progressive functional strength reduction. Disuse causes a reduction in fatty acid oxidation, leading to its accumulation in skeletal muscle. We hypothesized that muscle fatty acid accumulation could stimulate ceramide synthesis and promote skeletal muscle weakness. Therefore, the present study was designed to determine the effects of sphingolipid metabolism on skeletal muscle atrophy induced by 7 days of disuse. For this purpose, male Wistar rats were treated with myriocin, an inhibitor of de novo synthesis of ceramides, and subjected to hindlimb unloading (HU) for 7 days. Soleus muscles were assayed for fiber diameter, ceramide levels, protein degradation, and apoptosis signaling. Serum and liver were removed to evaluate the potential hepatoxicity of myriocin treatment. We found that HU increases content of saturated C16:0 and C18:0 ceramides and decreases soleus muscle weight and fiber diameter. HU increased the level of polyubiquitinated proteins and induced apoptosis in skeletal muscle. Despite a prevention of C16:0 and C18:0 muscle accumulation, myriocin treatment did not prevent skeletal muscle atrophy and concomitant induction of apoptosis and proteolysis. Moreover, myriocin treatment increased serum transaminases and induced hepatocyte necrosis. These data highlight that inhibition of de novo synthesis of ceramides during immobilization is not an efficient strategy to prevent skeletal muscle atrophy and exerts adverse effects like hepatotoxicity., (Copyright © 2016 the American Physiological Society.)
- Published
- 2016
- Full Text
- View/download PDF
22. Mouse genetic background impacts both on iron and non-iron metals parameters and on their relationships.
- Author
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Cavey T, Ropert M, de Tayrac M, Bardou-Jacquet E, Island ML, Leroyer P, Bendavid C, Brissot P, and Loréal O
- Subjects
- Animals, Cobalt blood, Cobalt metabolism, Copper blood, Copper metabolism, Hepcidins blood, Hepcidins genetics, Hepcidins metabolism, Iron blood, Magnesium blood, Magnesium metabolism, Male, Manganese blood, Manganese metabolism, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Inbred DBA, Principal Component Analysis, RNA, Messenger blood, RNA, Messenger genetics, RNA, Messenger metabolism, Rubidium blood, Rubidium metabolism, Zinc blood, Zinc metabolism, Genetic Background, Iron metabolism
- Abstract
Iron is reported to interact with other metals. In addition, it has been shown that genetic background may impact iron metabolism. Our objective was to characterize, in mice of three genetic backgrounds, the links between iron and several non-iron metals. Thirty normal mice (C57BL/6, Balb/c and DBA/2; n = 10 for each group), fed with the same diet, were studied. Quantification of iron, zinc, cobalt, copper, manganese, magnesium and rubidium was performed by ICP/MS in plasma, erythrocytes, liver and spleen. Transferrin saturation was determined. Hepatic hepcidin1 mRNA level was evaluated by quantitative RT-PCR. As previously reported, iron parameters were modulated by genetic background with significantly higher values for plasma iron parameters and liver iron concentration in DBA/2 and Balb/c strains. Hepatic hepcidin1 mRNA level was lower in DBA/2 mice. No iron parameter was correlated with hepcidin1 mRNA levels. Principal component analysis of the data obtained for non-iron metals indicated that metals parameters stratified the mice according to their genetic background. Plasma and tissue metals parameters that are dependent or independent of genetic background were identified. Moreover, relationships were found between plasma and tissue content of iron and some other metals parameters. Our data: (i) confirms the impact of the genetic background on iron parameters, (ii) shows that genetic background may also play a role in the metabolism of non-iron metals, (iii) identifies links between iron and other metals parameters which may have implications in the understanding and, potentially, the modulation of iron metabolism.
- Published
- 2015
- Full Text
- View/download PDF
23. Iron, hepcidin, and the metal connection.
- Author
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Loréal O, Cavey T, Bardou-Jacquet E, Guggenbuhl P, Ropert M, and Brissot P
- Abstract
Identification of new players in iron metabolism, such as hepcidin, which regulates ferroportin and divalent metal transporter 1 expression, has improved our knowledge of iron metabolism and iron-related diseases. However, from both experimental data and clinical findings, "iron-related proteins" appear to also be involved in the metabolism of other metals, especially divalent cations. Reports have demonstrated that some metals may affect, directly or indirectly, the expression of proteins involved in iron metabolism. Throughout their lives, individuals are exposed to various metals during personal and/or occupational activities. Therefore, better knowledge of the connections between iron and other metals could improve our understanding of iron-related diseases, especially the variability in phenotypic expression, as well as a variety of diseases in which iron metabolism is secondarily affected. Controlling the metabolism of other metals could represent a promising innovative therapeutic approach.
- Published
- 2014
- Full Text
- View/download PDF
24. Somatostatin and opioid receptors do not regulate proliferation or apoptosis of the human multiple myeloma U266 cells.
- Author
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Kerros C, Cavey T, Sola B, Jauzac P, and Allouche S
- Subjects
- Blotting, Western, Cell Cycle, Humans, Multiple Myeloma genetics, Multiple Myeloma metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Opioid genetics, Receptors, Somatostatin genetics, Reverse Transcriptase Polymerase Chain Reaction, Somatostatin pharmacology, Tumor Cells, Cultured, Apoptosis, Cell Proliferation, Multiple Myeloma pathology, Receptors, Opioid metabolism, Receptors, Somatostatin metabolism
- Abstract
Background: opioid and somatostatin receptors (SSTRs) that can assemble as heterodimer were individually reported to modulate malignant cell proliferation and to favour apoptosis., Materials and Methods: SSTRs and opioid receptors expression were examined by RT-PCR, western-blot and binding assays, cell proliferation was studied by XTT assay and propidium iodide (PI) staining and apoptosis by annexin V-PI labelling., Results: almost all human malignant haematological cell lines studied here expressed the five SSTRs. Further experiments were conducted on the human U266 multiple myeloma cells, which express also micro-opioid receptors (MOP-R). XTT assays and cell cycle studies provide no evidence for a significant effect upon opioid or somatostatin receptors stimulation. Furthermore, neither direct effect nor potentiation of the Fas-receptor pathway was detected on apoptosis after these treatments., Conclusion: these data suggest that SSTRs or opioid receptors expression is not a guaranty for an anti-tumoral action in U266 cell line.
- Published
- 2009
- Full Text
- View/download PDF
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