Your search keyword '"Ribeil, Jean‐Antoine"' showing total 35 results

1. An integrated therapeutic approach to sickle cell disease management beyond infancy.

Author

Ribeil, Jean‐Antoine, Pollock, Galia, Frangoul, Haydar, and Steinberg, Martin H.

Published

2023

2. Lovo‐cel gene therapy for sickle cell disease: Treatment process evolution and outcomes in the initial groups of the HGB‐206 study.

Author

Kanter, Julie, Thompson, Alexis A., Pierciey, Francis J., Hsieh, Matthew, Uchida, Naoya, Leboulch, Philippe, Schmidt, Manfred, Bonner, Melissa, Guo, Ruiting, Miller, Alex, Ribeil, Jean‐Antoine, Davidson, David, Asmal, Mohammed, Walters, Mark C., and Tisdale, John F.

Published

2023

3. Pregnancy outcome in women with transfused beta-thalassemia in France.

Author

Virot, Emilie, Thuret, Isabelle, Jardel, Sabine, Herbrecht, Raoul, Lachenal, Florence, Lionnet, François, Lucchini, Marie-José, Machin, Julie, Nimubona, Stanislas, Ribeil, Jean-Antoine, Galacteros, Frederic, Cannas, Giovanna, and Hot, Arnaud

Subjects

PREGNANCY outcomes, BETA-Thalassemia, PREGNANCY complications, FETAL growth retardation, MULTIPLE pregnancy, AMENORRHEA, KALLMANN syndrome

Abstract

Because of chronic anemia, hypogonadotropic hypogonadism, and iron chelation, pregnancy in homozygous and heterozygous compound beta-thalassemia patients stays a challenge. Pregnancies of transfused beta-thalassemia women registered in the French National Registry, conducted between 1995 and 2015, are described. These pregnancies were compared with pregnancies in healthy women and to data previously published in the literature. Fifty-six pregnancies of 37 women were studied. There were 5 twin pregnancies. Assisted reproductive technologies (ART) were used in 9 pregnancies. Median term at delivery was 39 amenorrhea weeks, and median weight at birth was 2780 g. Cesarean section was performed in 53.6% of the pregnancies. There were 6 thromboembolic events, 6 serious infections, 6 pregnancy-induced hypertensions (PIH), 6 intrauterine growth retardations (IUGR), 5 severe hemorrhages, 4 gestational diabetes, 3 alloimmunizations, 2 heart diseases, and 1 pre-eclampsia. There were 5 infections and 4 osteoporosis in the first year of post-partum. ART and cesarean sections were more often used in the beta-thalassemia group, compared to control subjects. Thromboembolic events, PIH, hemorrhage at delivery, and IUGR were more frequent in the beta-thalassemia group. Time to delivery was not different, but infant weight at birth was significantly smaller in the beta-thalassemia group. In the post-partum period, global maternal complications were more frequent in the beta-thalassemia group. Pregnancy in transfused beta-thalassemia women is safe with rare obstetrical and fetal complications. Cesarean section remains often chosen, and infant weight at birth remains smaller than that in the general population, despite delivery at full term. [ABSTRACT FROM AUTHOR]

Published

2022

4. Sickle Cell Trait Modulates the Proteome and Phosphoproteome of Plasmodium falciparum -Infected Erythrocytes.

Author

Chauvet, Margaux, Chhuon, Cerina, Lipecka, Joanna, Dechavanne, Sébastien, Dechavanne, Célia, Lohezic, Murielle, Ortalli, Margherita, Pineau, Damien, Ribeil, Jean-Antoine, Manceau, Sandra, Le Van Kim, Caroline, Luty, Adrian J. F., Migot-Nabias, Florence, Azouzi, Slim, Guerrera, Ida Chiara, and Merckx, Anaïs

Subjects

SICKLE cell trait, PLASMODIUM falciparum, CARRIER proteins, ERYTHROCYTES, SICKLE cell anemia, MALARIA, ERYTHROCYTE membranes

Abstract

The high prevalence of sickle cell disease in some human populations likely results from the protection afforded against severe Plasmodium falciparum malaria and death by heterozygous carriage of HbS. P. falciparum remodels the erythrocyte membrane and skeleton, displaying parasite proteins at the erythrocyte surface that interact with key human proteins in the Ankyrin R and 4.1R complexes. Oxidative stress generated by HbS, as well as by parasite invasion, disrupts the kinase/phosphatase balance, potentially interfering with the molecular interactions between human and parasite proteins. HbS is known to be associated with abnormal membrane display of parasite antigens. Studying the proteome and the phosphoproteome of red cell membrane extracts from P. falciparum infected and non-infected erythrocytes, we show here that HbS heterozygous carriage, combined with infection, modulates the phosphorylation of erythrocyte membrane transporters and skeletal proteins as well as of parasite proteins. Our results highlight modifications of Ser-/Thr- and/or Tyr- phosphorylation in key human proteins, such as ankyrin, β-adducin, β-spectrin and Band 3, and key parasite proteins, such as RESA or MESA. Altered phosphorylation patterns could disturb the interactions within membrane protein complexes, affect nutrient uptake and the infected erythrocyte cytoadherence phenomenon, thus lessening the severity of malaria symptoms. [ABSTRACT FROM AUTHOR]

Published

2021

5. Safety and feasibility of hematopoietic progenitor stem cell collection by mobilization with plerixafor followed by apheresis vs bone marrow harvest in patients with sickle cell disease in the multi‐center HGB‐206 trial.

Author

Tisdale, John F., Pierciey, Francis J., Bonner, Melissa, Thompson, Alexis A., Krishnamurti, Lakshmanan, Mapara, Markus Y., Kwiatkowski, Janet L., Shestopalov, Ilya, Ribeil, Jean‐Antoine, Huang, Wenmei, Asmal, Mohammed, Kanter, Julie, and Walters, Mark C.

Published

2020

6. S274: A NEW, EFFECTIVE, SAFE, NON‐MYELOABLATIVE CONDITIONING REGIMEN WITH A HLA‐MATCHED SIBLING DONOR FOR THE SEVERE SICKLE CELL PHENOTYPE IN ADULTS.

Author

Ihlem, Rahal, Marçais, Ambroise, Cazelles, Clarisse, Manceau, Sandra, Ribeil, Jean‐Antoine, Arlet, Jean‐Benoît, Meunier, Benoit, Corsia, Alice, Cavazzana, Marina, Suarez, Felipe, and Joseph, Laure

Published

2023

7. Innovative Curative Treatment of Beta Thalassemia: Cost-Efficacy Analysis of Gene Therapy Versus Allogenic Hematopoietic Stem-Cell Transplantation.

Author

Coquerelle, Séverine, Ghardallou, Mariem, Rais, Setti, Taupin, Pierre, Touzot, Fabien, Boquet, Laure, Blanche, Stéphane, Benaouadi, Semir, Brice, Thomas, Tuchmann-Durand, Caroline, Ribeil, Jean Antoine, Magrin, Elisa, Lissillour, Etienne, Rochaix, Lise, Cavazzana, Marina, and Durand-Zaleski, Isabelle

Published

2019

8. Sickle SCAN™ (BioMedomics) fulfills analytical conditions for neonatal screening of sickle cell disease.

Author

Nguyen-Khoa, Thao, Mine, Louis, Allaf, Bichr, Ribeil, Jean-Antoine, Remus, Christelle, Stanislas, Aurélie, Gauthereau, Valérie, Enouz, Sarah, Kim, Jason S., Yang, Xiaoxi, Gluckman, Eliane, Beaudeux, Jean-Louis, Munnich, Arnold, Girot, Robert, and Cavazzana, Marina

Published

2018

9. Transfusion‐related adverse events are decreased in pregnant women with sickle cell disease by a change in policy from systematic transfusion to prophylactic oxygen therapy at home: A retrospective survey by the international sickle cell disease observatory

Author

Ribeil, Jean‐Antoine, Labopin, Myriam, Stanislas, Aurélie, Deloison, Benjamin, Lemercier, Delphine, Habibi, Anoosha, Albinni, Souha, Charlier, Caroline, Lortholary, Olivier, Lefrere, François, De Montalembert, Mariane, Blanche, Stéphane, Galactéros, Frédéric, Tréluyer, Jean‐Marc, Gluckman, Eliane, Ville, Yves, Joseph, Laure, Delville, Marianne, Benachi, Alexandra, and Cavazzana, Marina

Published

2018

10. Roles of APOL1 G1 and G2 variants in sickle cell disease patients: kidney is the main target.

Author

Kormann, Raphaël, Jannot, Anne‐Sophie, Narjoz, Céline, Ribeil, Jean‐Antoine, Manceau, Sandra, Delville, Marianne, Joste, Valentin, Prié, Dominique, Pouchot, Jacques, Thervet, Eric, Courbebaisse, Marie, and Arlet, Jean‐Benoît

Subjects

SICKLE cell anemia, KIDNEY disease risk factors, BLOOD diseases, DISEASES in African Americans, CHRONIC kidney failure

Abstract

In African-American patients with sickle cell disease (SCD), APOL1 G1 and G2 variants are associated with increased risk of sickle cell nephropathy (SCN). To determine the role of APOL1 variants in SCD patients living in Europe, we genotyped 152 SCD patients [aged 30·4 (24·3-36·4) years], mainly of Sub-Saharan African ancestry, for APOL1 G1 and G2 and for variants of four genes with kidney tropism ( GSTM1, GSTT1, GSTP1, and HMOX1). Homozygous or double-heterozygous APOL G1 and G2 genotypes were strongly associated with end stage renal disease ( P = 0·003) and worse Kidney Disease: Improving Global Outcomes stages ( P = 0·001). Further, these genotypes were associated in an age-dependent manner with lower estimated glomerular filtration rate (eGFR, P = 0·008), proteinuria ( P = 0·009) and albuminuria ( P < 0·001) but not with other SCD complications. Compared to APOL1 G1/wild type (WT), the APOL1 G2/WT genotype was associated with a lower eGFR ( P = 0·04) in an age-dependent manner, suggesting that the G2/WT patients are likely to have worse kidney prognosis. Other genes variants analysed were not associated with SCN or other SCD complications. Our data indicate that APOL1 screening should be considered for the management of SCD patients, including those of non-African-American origin, as those with homozygous or double heterozygous variants are clearly at higher risk of SCN . [ABSTRACT FROM AUTHOR]

Published

2017

11. Cardiac iron overload in chronically transfused patients with thalassemia, sickle cell anemia, or myelodysplastic syndrome.

Author

de Montalembert, Mariane, Ribeil, Jean-Antoine, Brousse, Valentine, Guerci-Bresler, Agnes, Stamatoullas, Aspasia, Vannier, Jean-Pierre, Dumesnil, Cécile, Lahary, Agnès, Touati, Mohamed, Bouabdallah, Krimo, Cavazzana, Marina, Chauzit, Emmanuelle, Baptiste, Amandine, Lefebvre, Thibaud, Puy, Hervé, Elie, Caroline, Karim, Zoubida, Ernst, Olivier, and Rose, Christian

Subjects

BLOOD transfusion, IRON in the blood, CHRONICALLY ill, THALASSEMIA, SICKLE cell anemia, MYELODYSPLASTIC syndromes

Abstract

The risk and clinical significance of cardiac iron overload due to chronic transfusion varies with the underlying disease. Cardiac iron overload shortens the life expectancy of patients with thalassemia, whereas its effect is unclear in those with myelodysplastic syndromes (MDS). In patients with sickle cell anemia (SCA), iron does not seem to deposit quickly in the heart. Our primary objective was to assess through a multicentric study the prevalence of cardiac iron overload, defined as a cardiovascular magnetic resonance T2*<20 ms, in patients with thalassemia, SCA, or MDS. Patient inclusion criteria were an accurate record of erythrocyte concentrates (ECs) received, a transfusion history >8 ECs in the past year, and age older than 6 years. We included from 9 centers 20 patients with thalassemia, 41 with SCA, and 25 with MDS in 2012-2014. Erythrocytapharesis did not consistently prevent iron overload in patients with SCA. Cardiac iron overload was found in 3 (15%) patients with thalassemia, none with SCA, and 4 (16%) with MDS. The liver iron content (LIC) ranged from 10.4 to 15.2 mg/g dry weight, with no significant differences across groups (P = 0.29). Abnormal T2* was not significantly associated with any of the measures of transfusion or chelation. Ferritin levels showed a strong association with LIC. Non-transferrin-bound iron was high in the thalassemia and MDS groups but low in the SCA group (P<0.001). Hepcidin was low in thalassemia, normal in SCA, and markedly elevated in MDS (P<0.001). Two mechanisms may explain that iron deposition largely spares the heart in SCA: the high level of erythropoiesis recycles the iron and the chronic inflammation retains iron within the macrophages. Thalassemia, in contrast, is characterized by inefficient erythropoiesis, unable to handle free iron. Iron accumulation varies widely in MDS syndromes due to the competing influences of abnormal erythropoiesis, excess iron supply, and inflammation. [ABSTRACT FROM AUTHOR]

Published

2017

12. Arterio-venous fistula for automated red blood cells exchange in patients with sickle cell disease: Complications and outcomes.

Author

Delville, Marianne, Manceau, Sandra, Ait Abdallah, Nassim, Stolba, Jan, Awad, Sameh, Damy, Thibaud, Gellen, Barnabas, Sabbah, Laurent, Debbache, Karima, Audard, Vincent, Beaumont, Jean-Louis, Arnaud, Cécile, Chantalat-Auger, Christelle, Driss, Françoise, Lefrère, François, Cavazzana, Marina, Franco, Gilbert, Galacteros, Frederic, Ribeil, Jean-Antoine, and Gellen-Dautremer, Justine

Published

2017

13. Gene Therapy with Hematopoietic Stem Cells: The Diseased Bone Marrow's Point of View.

Author

Cavazzana, Marina, Ribeil, Jean-Antoine, Lagresle-Peyrou, Chantal, and André-Schmutz, Isabelle

Published

2017

14. Gene Therapy of the β-Hemoglobinopathies by Lentiviral Transfer of the βA(T87Q)- Globin Gene.

Author

Negre, Olivier, Eggimann, Anne-Virginie, Beuzard, Yves, Ribeil, Jean-Antoine, Bourget, Philippe, Borwornpinyo, Suparerk, Hongeng, Suradej, Hacein-Bey, Salima, Cavazzana, Marina, Leboulch, Philippe, and Payen, Emmanuel

Published

2016

15. A biomimetic microfluidic chip to study the circulation and mechanical retention of red blood cells in the spleen.

Author

Picot, Julien, Ndour, Papa Alioune, Lefevre, Sophie D., El Nemer, Wassim, Tawfik, Harvey, Galimand, Julie, Da Costa, Lydie, Ribeil, Jean-Antoine, de Montalembert, Mariane, Brousse, Valentine, Le Pioufle, Bruno, Buffet, Pierre, Le Van Kim, Caroline, and Français, Olivier

Published

2015

16. Thérapie génique dans la drépanocytose.

Author

Ribeil, Jean-Antoine, Blanche, Stéphane, and Cavazzana, Marina

Published

2017

17. HSP70 sequestration by free α-globin promotes ineffective erythropoiesis in β-thalassaemia.

Author

Arlet, Jean-Benoît, Leboulch, Philippe, Baudin-Creuza, Véronique, Seigneuric, Renaud, Fontenay, Michaela, Garrido, Carmen, Hermine, Olivier, Courtois, Geneviève, Ribeil, Jean-Antoine, Guillem, Flavia, Belaid-Choucair, Zakia, Negre, Olivier, Beuzard, Yves, Chretien, Stany, Hazoume, Adonis, Marcion, Guillaume, Sevin, Margaux, Dussiot, Michaël, Moura, Ivan Cruz, and Maciel, Thiago Trovati

Subjects

HSP70 heat-shock proteins, ERYTHROPOIESIS, GLOBIN, MOLECULAR chaperones, APOPTOSIS, GATA proteins

Abstract

β-Thalassaemia major (β-TM) is an inherited haemoglobinopathy caused by a quantitative defect in the synthesis of β-globin chains of haemoglobin, leading to the accumulation of free α-globin chains that form toxic aggregates. Despite extensive knowledge of the molecular defects causing β-TM, little is known of the mechanisms responsible for the ineffective erythropoiesis observed in the condition, which is characterized by accelerated erythroid differentiation, maturation arrest and apoptosis at the polychromatophilic stage. We have previously demonstrated that normal human erythroid maturation requires a transient activation of caspase-3 at the later stages of maturation. Although erythroid transcription factor GATA-1, the master transcriptional factor of erythropoiesis, is a caspase-3 target, it is not cleaved during erythroid differentiation. We have shown that, in human erythroblasts, the chaperone heat shock protein70 (HSP70) is constitutively expressed and, at later stages of maturation, translocates into the nucleus and protects GATA-1 from caspase-3 cleavage. The primary role of this ubiquitous chaperone is to participate in the refolding of proteins denatured by cytoplasmic stress, thus preventing their aggregation. Here we show in vitro that during the maturation of human β-TM erythroblasts, HSP70 interacts directly with free α-globin chains. As a consequence, HSP70 is sequestrated in the cytoplasm and GATA-1 is no longer protected, resulting in end-stage maturation arrest and apoptosis. Transduction of a nuclear-targeted HSP70 mutant or a caspase-3-uncleavable GATA-1 mutant restores terminal maturation of β-TM erythroblasts, which may provide a rationale for new targeted therapies of β-TM. [ABSTRACT FROM AUTHOR]

Published

2014

18. An activin receptor IIA ligand trap corrects ineffective erythropoiesis in β-thalassemia.

Author

Dussiot, Michael, Maciel, Thiago T, Fricot, Aurélie, Chartier, Céline, Negre, Olivier, Veiga, Joel, Grapton, Damien, Paubelle, Etienne, Payen, Emmanuel, Beuzard, Yves, Leboulch, Philippe, Ribeil, Jean-Antoine, Arlet, Jean-Benoit, Coté, Francine, Courtois, Geneviève, Ginzburg, Yelena Z, Daniel, Thomas O, Chopra, Rajesh, Sung, Victoria, and Hermine, Olivier

Subjects

ACTIVIN receptors, ERYTHROPOIESIS, THALASSEMIA, PATHOLOGICAL physiology, ERYTHROCYTE membranes, CYTOKINES, GLOBIN

Abstract

The pathophysiology of ineffective erythropoiesis in β-thalassemia is poorly understood. We report that RAP-011, an activin receptor IIA (ActRIIA) ligand trap, improved ineffective erythropoiesis, corrected anemia and limited iron overload in a mouse model of β-thalassemia intermedia. Expression of growth differentiation factor 11 (GDF11), an ActRIIA ligand, was increased in splenic erythroblasts from thalassemic mice and in erythroblasts and sera from subjects with β-thalassemia. Inactivation of GDF11 decreased oxidative stress and the amount of α-globin membrane precipitates, resulting in increased terminal erythroid differentiation. Abnormal GDF11 expression was dependent on reactive oxygen species, suggesting the existence of an autocrine amplification loop in β-thalassemia. GDF11 inactivation also corrected the abnormal ratio of immature/mature erythroblasts by inducing apoptosis of immature erythroblasts through the Fas-Fas ligand pathway. Taken together, these observations suggest that ActRIIA ligand traps may have therapeutic relevance in β-thalassemia by suppressing the deleterious effects of GDF11, a cytokine which blocks terminal erythroid maturation through an autocrine amplification loop involving oxidative stress and α-globin precipitation. [ABSTRACT FROM AUTHOR]

Published

2014

19. Sickle-cell disease stroke throughout life: A retrospective study in an adult referral center.

Author

Gueguen, Antoine, Mahevas, Matthieu, Nzouakou, Ruben, Hosseini, Hassan, Habibi, Anoosha, Bachir, Dora, Brugière, Pierre, Lionnet, François, Ribeil, Jean-Antoine, Godeau, Bertrand, Girot, Robert, Ibrahima, Vahid, Calvet, David, Galactéros, Frédéric, and Bartolucci, Pablo

Published

2014

20. A specific time course for mobilization of peripheral blood CD34+ cells after plerixafor injection in very poor mobilizer patients: impact on the timing of the apheresis procedure.

Author

Lefrère, François, Mauge, Laeticia, Réa, Delphine, Ribeil, Jean‐Antoine, Dal Cortivo, Liliane, Brignier, Anne C., Aoun, Charbel, Larghéro, Jérôme, Cavazzana‐Calvo, Marina, and Micléa, Jean‐Michel

Subjects

BLOOD cells, HEMAPHERESIS, INJECTIONS, STEM cells, GRANULOCYTE-colony stimulating factor, DRUG dosage

Abstract

BACKGROUND: This report describes the specific kinetics of the peripheral blood (PB) CD34+ cell concentration in a selected group of very poor stem cell mobilizer patients treated with granulocyte-colony-stimulating factor (G-CSF) and plerixafor and determines the kinetics' impact on apheresis. STUDY DESIGN AND METHODS: All patients had previously experienced at least two failures of mobilization (without use of plerixafor). The present salvage therapy consisted in the administration of 10 µg/kg/day G-CSF for 5 days added to a dose of plerixafor administered at between 5 a.m. and 6 a.m. on Day 5. The PB CD34+ cell counts were tested every 3 hours thereafter. Apheresis was initiated as soon as the PB CD34+ cell count reached 10 × 106/L. RESULTS: A PB CD34+ cell count higher than 10 × 106/L was observed as soon as 3 hours after plerixafor administration in 10 of the 11 patients who reached this threshold at some point in the monitoring process. Interestingly, all patients presented an early decrease in the PB CD34+ cell count 8 to 12 hours after plerixafor administration (below 10 × 106/L for seven patients). CONCLUSION: Had such patients been tested for PB CD34+ cell mobilization according to conventional criteria (i.e., 11 hr after plerixafor administration), apheresis would not have been performed at the optimal timing. For very poor stem cell mobilizer patients, early monitoring of PB CD34+ cell count may be required for the optimal initiation of apheresis. [ABSTRACT FROM AUTHOR]

Published

2013

21. Ineffective Erythropoiesis in β-Thalassemia.

Author

Ribeil, Jean-Antoine, Arlet, Jean-Benoit, Dussiot, Michael, Moura, Ivan Cruz, Courtois, Geneviève, and Hermine, Olivier

Subjects

BETA-Thalassemia, ERYTHROPOIESIS, ERYTHROCYTES, HEMOGLOBINS, HEMOGLOBINOPATHY, GENE expression

Published

2013

22. Determination of the best method to estimate glomerular filtration rate from serum creatinine in adult patients with sickle cell disease: a prospective observational cohort study.

Author

Arlet, Jean-Beno�t, Ribeil, Jean-Antoine, Chatellier, Gilles, Eladari, Dominique, De Seigneux, Sophie, Souberbielle, Jean-Claude, Friedlander, G�rard, de Montalembert, Marianne, Pouchot, Jacques, Pri�, Dominique, and Courbebaisse, Marie

Subjects

SICKLE cell anemia, GLOMERULAR filtration rate, HYPOXEMIA, KIDNEY diseases, CREATININE

Abstract

Background: Sickle cell disease (SCD) leads to tissue hypoxia resulting in chronic organ dysfunction including SCD associated nephropathy. The goal of our study was to determine the best equation to estimate glomerular filtration rate (GFR) in SCD adult patients. Methods: We conducted a prospective observational cohort study. Since 2007, all adult SCD patients in steady state, followed in two medical departments, have had their GFR measured using iohexol plasma clearance (gold standard). The Cockcroft-Gault, MDRD-v4, CKP-EPI and finally, MDRD and CKD-EPI equations without adjustment for ethnicity were tested to estimate GFR from serum creatinine. Estimated GFRs were compared to measured GFRs according to the graphical Bland and Altman method. Results: Sixty-four SCD patients (16 men, median age 27.5 years [range 18.0-67.5], 41 with SS-genotype were studied. They were Sub-Saharan Africa and French West Indies natives and predominantly lean (median body mass index: 22 kg/m2 [16-33]). Hyperfiltration (defined as measured GFR >110 mL/min/1.73 m2) was detected in 53.1% of patients. Urinary albumin/creatinine ratio was higher in patients with hyperfiltration than in patients with normal GFR (4.05 mg/mmol [0.14-60] versus 0.4 mg/mmol [0.7-81], p = 0.01). The CKD-EPI equation without adjustment for ethnicity had both the lowest bias and the greatest precision. Differences between estimated GFRs using the CKPEPI equation and measured GFRs decreased with increasing GFR values, whereas it increased with the Cockcroft-Gault and MDRD-v4 equations. Conclusions: We confirm that SCD patients have a high rate of glomerular hyperfiltration, which is frequently associated with microalbuminuria or macroalbuminuria. In non-Afro-American SCD patients, the best method for estimating GFR from serum creatinine is the CKD-EPI equation without adjustment for ethnicity. This equation is particularly accurate to estimate high GFR values, including glomerular hyperfiltration, and thus should be recommended to screen SCD adult patients at high risk for SCD nephropathy. [ABSTRACT FROM AUTHOR]

Published

2012

23. Polymeric IgA1 controls erythroblast proliferation and accelerates erythropoiesis recovery in anemia.

Author

Coulon, Séverine, Dussiot, Michaël, Grapton, Damien, Maciel, Thiago Trovati, Wang, Pamella Huey Mei, Callens, Celine, Tiwari, Meetu Kaushik, Agarwal, Saurabh, Fricot, Aurelie, Vandekerckhove, Julie, Tamouza, Houda, Zermati, Yael, Ribeil, Jean-Antoine, Djedaini, Kamel, Oruc, Zeliha, Pascal, Virginie, Courtois, Geneviève, Arnulf, Bertrand, Alyanakian, Marie-Alexandra, and Mayeux, Patrick

Subjects

ANEMIA, ERYTHROPOIETIN, KIDNEY diseases, CANCER, ERYTHROPOIESIS

Abstract

Anemia because of insufficient production of and/or response to erythropoietin (Epo) is a major complication of chronic kidney disease and cancer. The mechanisms modulating the sensitivity of erythroblasts to Epo remain poorly understood. We show that, when cultured with Epo at suboptimal concentrations, the growth and clonogenic potential of erythroblasts was rescued by transferrin receptor 1 (TfR1)-bound polymeric IgA1 (pIgA1). Under homeostatic conditions, erythroblast numbers were increased in mice expressing human IgA1 compared to control mice. Hypoxic stress of these mice led to increased amounts of pIgA1 and erythroblast expansion. Expression of human IgA1 or treatment of wild-type mice with the TfR1 ligands pIgA1 or iron-loaded transferrin (Fe-Tf) accelerated recovery from acute anemia. TfR1 engagement by either pIgA1 or Fe-Tf increased cell sensitivity to Epo by inducing activation of mitogen-activated protein kinase (MAPK) and phosphatidylinositol 3-kinase (PI3K) signaling pathways. These cellular responses were mediated through the TfR1-internalization motif, YXX?. Our results show that pIgA1 and TfR1 are positive regulators of erythropoiesis in both physiological and pathological situations. Targeting this pathway may provide alternate approaches to the treatment of ineffective erythropoiesis and anemia. [ABSTRACT FROM AUTHOR]

Published

2011

24. Protective Effect of Systemic Administration of Erythropoietin on Auditory Brain Stem Response and Compound Action Potential Thresholds in an Animal Model of Cochlear Implantation.

Author

Ouesnel, Stephanie, Nguyen, Yann, Campo, Pierre, Hermine, Olivier, Ribeil, Jean-Antoine, Elmaleh, Monique, Bozorg Grayeli, Alexis, Ferrary, Evelyne, Sterkers, Olivier, and Couloigner, Vincent

Subjects

ACTION potentials, ANALYSIS of variance, ANIMAL experimentation, AUDITORY evoked response, BRAIN stem, COCHLEA, COCHLEAR implants, DRUG administration, ERYTHROPOIETIN, GUINEA pigs, HEARING disorders, HEARING levels, PERITONEUM, STATISTICS, T-test (Statistics), TOMOGRAPHY, DATA analysis, THERAPEUTICS

Abstract

Objectives: An animal model of cochlear implantation has been developed, and the hearing threshold was evaluated after different surgical procedures. The effect of perioperative systemic administration of erythropoietin on the hearing loss induced by cochlear implantation was tested. Methods: Twenty-nine guinea pigs with normal hearing underwent implantation of a 254-uxn-diameter array through a cochleostomy. The effects on hearing of cochleostomy and transient and long-term array implantation (21 days) were assessed by testing of the auditory brain stem responses and compound action potentials. Eleven implanted animals received intraperitoneal administration of erythropoietin. Selected computed tomographic scans and cochlear histologic studies were performed 1 month after implantation to confirm proper placement of the array. The erythropoietin concentration at the time of surgery was assessed in samples of perilymph, cerebrospinal fluid, and blood. Results: The cochleostomy and transient array insertion had no effect on hearing thresholds. Long-term array implantation induced a stable decrease of hearing threshold (30 dB), a decrease that was reduced by 12 dB in erythropoietin-treated animals. The erythropoietin-treated animals had better hearing preservation at higher frequencies. Fibrosis surrounding the array was seen in both groups. Conclusions: The hearing loss observed was probably due to the presence of the array in the cochlea. The intraperitoneal injection of erythropoietin improved the hearing threshold shift induced by implantation. [ABSTRACT FROM AUTHOR]

Published

2011

25. Vitronectin dictates intraglomerular fibrinolysis in immune-mediated glomerulonephritis.

Author

Mesnard, Laurent, Rafat, Cédric, Vandermeersch, Sophie, Hertig, Alexandre, Cathelin, Dominique, Xu-Dubois, Yi-Chun, Jouanneau, Chantal, Keller, Alexandre Castro, Ribeil, Jean-Antoine, Leite-de-Moraes, Maria C., and Rondeau, Eric

Abstract

During human glomerulonephritis, the severity of injuries correlates with glomerular fibrin deposits, which are tightly regulated by the intraglomerular fibrinolytic system. Here, we evaluated the role of vitronectin (VTN; also known as complement S protein), the principal cofactor of the plasminogen activator inhibitor-1 (PAI-1), in a mouse model of acute glomerulonephritis. We found that in mice subjected to nephrotoxic serum, the absence of VTN resulted in a lower glomerular PAI-1 activity and a higher glomerular fibrinolytic activity. Challenged VTN-/- mice displayed significantly less fibrin deposits, proteinuria, and renal failure than their wild-type counterparts. Notably, this protective effect afforded by VTN deficiency was still observed after a C3 depletion. Finally, the injection of VTN+/+ serum in VTN-/- mice induced the glomerular deposition of VTN, increased PAI-1 deposition, decreased glomerular fibrinolytic activity, and aggravated glomerular injury. As in mice, abundant glomerular VTN deposits were also observed in patients with severe glomerulonephritis. Here, we show that plasma-exchange therapy, admittedly beneficial in this clinical context, induces a significant depletion in circulating VTN, which might modulate PAI-1 activity locally and accelerate the clearance of fibrin deposits in the glomeruli. Collectively, these results demonstrate that VTN exerts a deleterious role independently from complement, by directing PAI-dependent fibrinolysis in the glomerular compartment. [ABSTRACT FROM AUTHOR]

Published

2011

26. First experience of autologous peripheral blood stem cell mobilization with biosimilar granulocyte colony-stimulating factor.

Author

Lefrère, François, Brignier, Anne-Colette, Elie, Caroline, Ribeil, Jean-Antoine, Bernimoulin, Michael, Aoun, Charbel, Dal Cortivo, Liliane, Delarue, Richard, Hermine, Olivier, and Cavazzana-Calvo, Marina

Abstract

INTRODUCTION: Mobilization techniques for autologous peripheral blood stem cell (PBSC) collection include chemotherapy followed by hematopoietic growth factors, such as granulocyte colony-stimulating factor (G-CSF). Biosimilar versions of G-CSF are now available in Europe. METHODS: In this study, 40 patients with a hematological malignancy scheduled to receive biosimilar G-CSF (Zarzio((R)) Sandoz Biopharmaceuticals, Paris, France) following first-cycle chemotherapy for treatment and autologous PBSC mobilization were prospectively included at a single center. These patients were compared with a historical control group who had been treated with G-CSF (Neupogen((R)) Paris, France) at the same center according to the same clinical protocol. PBSC harvesting was considered successful if at least 3x10(6) CD34+ cells/kg were collected. If three consecutive CD34+ tests were below 10/[mu]L then PBSC harvesting was not performed. RESULTS: Patient characteristics were similar in both groups with no significant differences in age, diagnosis, previous chemotherapy, or chemotherapy mobilization regimen. No significant differences were observed between groups in median CD34+ cells mobilized and collected, or the number of G-CSF injections and leukaphereses required to obtain the minimal CD34+ cell count. Proportion of failures was also similar in both groups. CONCLUSION: Zarziois((R)) comparable to Neupogen((R)) for PBSC mobilization and collection after chemotherapy and so may provide a more cost-effective strategy. [ABSTRACT FROM AUTHOR]

Published

2011

27. First experience of autologous peripheral blood stem cell mobilization with biosimilar granulocyte colony- stimulating factor.

Author

Lefrère, François, Brignier, Anne-Colette, Elie, Caroline, Ribeil, Jean-Antoine, Bernimoulin, Michael, Aoun, Charbel, Cortivo, Liliane, Delarue, Richard, Hermine, Olivier, and Cavazzana-Calvo, Marina

Abstract

Introduction: Mobilization techniques for autologous peripheral blood stem cell (PBSC) collection include chemotherapy followed by hematopoietic growth factors, such as granulocyte colony-stimulating factor (G-CSF). Biosimilar versions of G-CSF are now available in Europe. Methods: In this study, 40 patients with a hematological malignancy scheduled to receive biosimilar G-CSF (Zarzio® Sandoz Biopharmaceuticals, Paris, France) following first-cycle chemotherapy for treatment and autologous PBSC mobilization were prospectively included at a single center. These patients were compared with a historical control group who had been treated with G-CSF (Neupogen® Paris, France) at the same center according to the same clinical protocol. PBSC harvesting was considered successful if at least 3×10 CD34+ cells/kg were collected. If three consecutive CD34+ tests were below 10/μL then PBSC harvesting was not performed. Results: Patient characteristics were similar in both groups with no significant differences in age, diagnosis, previous chemotherapy, or chemotherapy mobilization regimen. No significant differences were observed between groups in median CD34+ cells mobilized and collected, or the number of G-CSF injections and leukaphereses required to obtain the minimal CD34+ cell count. Proportion of failures was also similar in both groups. Conclusion: Zarziois® comparable to Neupogen® for PBSC mobilization and collection after chemotherapy and so may provide a more cost-effective strategy. [ABSTRACT FROM AUTHOR]

Published

2011

28. Decreased transfusion needs associated with hydroxyurea therapy in Algerian patients with thalassemia major or intermedia.

Author

Bradai, Mohamed, Pissard, Serge, Abad, Mohand Tayeb, Dechartres, Agnes, Ribeil, Jean-Antoine, Landais, Paul, and de Montalembert, Mariane

Subjects

THALASSEMIA, HEMOGLOBINOPATHY, HEMOLYTIC anemia, BLOOD transfusion, SURGERY

Abstract

BACKGROUND: Studies of evolution of transfusion requirements in thalassemic patients treated with hydroxyurea have produced somewhat conflicting results, especially in patients with thalassemia major. Our aims were to determine the proportion of good responders to hydroxyurea in a population of transfusion-dependent thalassemic patients and to identify the factors associated with a decrease of transfusion needs. STUDY DESIGN AND METHODS: Hydroxyurea treatment was initiated in 9 patients with thalassemia intermedia (TI) and 45 with thalassemia major (TM). Patients received transfusions when their hemoglobin (Hb) levels dropped below 6 g per dL. A decrease in annual transfusion requirements greater than 70 percent defined a good response, between 40 and 70 percent a partial response, and smaller than 40 percent no response. RESULTS: The response was good in 8 (90%) patients with TI and 20 (44.5%) with TM, partial in 9 (20%) patients with TM, and absent in 1 (10%) with TI and 16 (35.5%) with TM. In TM patients, transfusion needs decreased by 56 percent over the first year of hydroxyurea treatment. By univariate analysis, a better response to hydroxyurea was associated with older age at the first transfusion (p = 0.02), higher prehydroxyurea Hb (p = 0.0004), codon 6(–A) mutation (p = 0.002), TI (p = 0.03), and history of splenectomy (p = 0.05). Xmn1–/– was associated with a worse response (p = 0.0001). By multivariate analysis, a better response was associated with the Xmn1 polymorphism (p = 0.008). CONCLUSION: Hydroxyurea may be an alternative to transfusions for TI patients as well as for TM patients in countries that have limited blood supplies. [ABSTRACT FROM AUTHOR]

Published

2007

29. Evaluation of an algorithm based on peripheral blood hematopoietic progenitor cell and CD34+ cell concentrations to optimize peripheral blood progenitor cell collection by apheresis.

Author

Lefrère, François, Zohar, Sarah, Beaudier, Sandrine, Audat, Françoise, Ribeil, Jean-Antoine, Ghez, David, Varet, Bruno, Cavazzana-Calvo, Marina, Cortivo, Liliane Dal, Letestu, Rémi, McIntyre, Elizabeth, and Brouzes, Chantal

Subjects

HEMAPHERESIS, BLOOD collection, BLOOD transfusion, BLOOD cells

Abstract

BACKGROUND: Quantification of peripheral blood (PB) CD34+ cells is commonly used to plan peripheral blood progenitor cell (PBPC) collection but is time-consuming. Sysmex has developed a hematology analyzer that can quickly identify a population of immature hematopoietic cells (HPCs) according to cell size, cell density, and differential lysis resistance, which may indicate the presence of PBPCs in PB. This prospective study has evaluated the potential of such method to predict the PBPC mobilization. STUDY DESIGN AND METHODS: A total of 141 patients underwent PBPC mobilization. PB HPCs and PB CD34+ cells were simultaneously quantified with a hematology analyzer (SE2100, Sysmex) and flow cytometry, respectively. The number of blood volumes processed was then based on PB CD34+ cell concentration. RESULTS: The optimal PB HPC level able to predict a minimal level of 10 × 106 PB CD34+ cells per L was 5 × 106 per L with positive and negative predictive values of 0.93 and 0.36 percent, respectively. For this cutoff point, sensitivity and specificity were 0.81 and 0.65, respectively. The median number of blood volumes processed according to the PB CD34+ cell count allowed us to perform only one apheresis procedure for a majority of patients. CONCLUSION: PB HPC quantification is very useful to quickly determine the initiation of PBPC apheresis especially for patients with higher concentrations. For patients exhibiting a lower HPC count (<5 × 106/L), other parameters such as a CD34 test may be needed. Such a policy associated with a length of apheresis adapted to the richness in the PB CD34+ cells allows for optimizing the organization of centers with an improvement in patient comfort and economical savings. [ABSTRACT FROM AUTHOR]

Published

2007

30. Hsp70 regulates erythropoiesis by preventing caspase-3-mediated cleavage of GATA-1.

Author

Ribeil, Jean-Antoine, Zermati, Yael, Vandekerckhove, Julie, Cathelin, Severine, Kersual, Joelle, Dussiot, Michaël, Coulon, Séverine, Cruz Moura, Ivan, Zeuner, Ann, Kirkegaard-Sørensen, Thomas, Varet, Bruno, Solary, Eric, Garrido, Carmen, and Hermine, Olivier

Subjects

REGULATION of erythropoiesis, APOPTOSIS, TRANSCRIPTION factors, PROTEOLYSIS, PEPTIDES

Abstract

Caspase-3 is activated during both terminal differentiation and erythropoietin-starvation-induced apoptosis of human erythroid precursors. The transcription factor GATA-1, which performs an essential function in erythroid differentiation by positively regulating promoters of erythroid and anti-apoptotic genes, is cleaved by caspases in erythroid precursors undergoing cell death upon erythropoietin starvation or engagement of the death receptor Fas. In contrast, by an unknown mechanism, GATA-1 remains uncleaved when these cells undergo terminal differentiation upon stimulation with Epo. Here we show that during differentiation, but not during apoptosis, the chaperone protein Hsp70 protects GATA-1 from caspase-mediated proteolysis. At the onset of caspase activation, Hsp70 co-localizes and interacts with GATA-1 in the nucleus of erythroid precursors undergoing terminal differentiation. In contrast, erythropoietin starvation induces the nuclear export of Hsp70 and the cleavage of GATA-1. In an in vitro assay, Hsp70 protects GATA-1 from caspase-3-mediated proteolysis through its peptide-binding domain. The use of RNA-mediated interference to decrease the Hsp70 content of erythroid precursors cultured in the presence of erythropoietin leads to GATA-1 cleavage, a decrease in haemoglobin content, downregulation of the expression of the anti-apoptotic protein Bcl-XL, and cell death by apoptosis. These effects are abrogated by the transduction of a caspase-resistant GATA-1 mutant. Thus, in erythroid precursors undergoing terminal differentiation, Hsp70 prevents active caspase-3 from cleaving GATA-1 and inducing apoptosis. [ABSTRACT FROM AUTHOR]

Published

2007

31. CD34+ stem cell top-ups without conditioning after initial haematopoietic stem cell transplantation for correction of incomplete haematopoietic and immunological recovery in severe congenital immunodeficiencies.

Author

Booth, Claire, Ribeil, Jean-Antoine, Audat, Françoise, Dal-Cortivo, Liliane, Veys, Paul A., Thrasher, Adrian J., Davies, E. Graham, Lefrère, François, Fischer, Alain, Cavazzana-Calvo, Marina, and Gaspar, H. Bobby

Subjects

HEMATOPOIETIC stem cells, IMMUNODEFICIENCY, BONE marrow cells, CELL transplantation, CELLULAR therapy, IMMUNE system

Abstract

Haematopoietic stem cell transplantation can be limited by ineffective haematopoiesis and poor immune recovery. A CD34+ cell infusion without conditioning has the potential to improve stem cell function with limited toxicity. Eighteen patients with congenital immunodeficiencies received CD34+ boosts for various defects. When given <1 year after the original graft, six of seven cytopenic patients achieved transfusion independence. A second cohort ( n = 11) received boosts >1 year after the original graft; only minimal changes in immune function or chimaerism were noted. Unconditioned stem cell boosts have limited toxicity but should be given early after the original graft to be effective. [ABSTRACT FROM AUTHOR]

Published

2006

32. Rôle d'HSP70 dans l'érythropoïèse inefficace des β-thalassémies majeures.

Author

Arlet, Jean-Benoît, Ribeil, Jean-Antoine, Guillem, Flavia, Hermine, Olivier, and Courtois, Geneviève

Published

2015

33. Primary Hyperparathyroidism in Sickle Cell Disease: An Unknown Complication of the Disease in Adulthood.

Author

Denoix, Elsa, Bomahou, Charlène, Clavier, Lorraine, Ribeil, Jean-Antoine, Lionnet, François, Bartolucci, Pablo, Courbebaisse, Marie, Pouchot, Jacques, and Arlet, Jean-Benoît

Subjects

SICKLE cell anemia, HYPOPARATHYROIDISM, DISEASE complications, BONE density, HYPERPARATHYROIDISM, ADULTS

Abstract

Primary hyperparathyroidism (pHPT) is the third most common endocrine disorder and usually affects patients between 60 and 70 years of age. To our knowledge, this condition has never been studied in young patients with sickle cell disease (SCD). Our objective was to describe the clinical and biological characteristics of pHPT in adult patients with SCD and its management. We conducted a retrospective study that included SCD patients who were diagnosed with pHPT in four SCD referral centers. pHPT was defined by the presence of elevated serum calcium levels with inappropriate normal or increased parathyroid hormone (PTH) serum levels or histopathological evidence of parathyroid adenoma or hyperplasia. Patients with severe renal impairment (GFR <30 mL/min) were excluded. Twenty-eight patients (18 women, 64%; 22 homozygous genotype, 79%) were included. The median age at pHPT diagnosis was 41 years (interquartile range –IQR- 31.5–49.5). The median serum calcium and PTH concentration were, respectively, 2.62 mmol/L (IQR 2.60–2.78) and 105 pg/mL (IQR 69–137). Bone mineral density (BMD) revealed very low BMD (≤−2.5 SD) in 44% of patients explored (vs. 12.5% among 32 SCD patients matched for SCD genotype, sex, age, and BMI, p = 0.03). Fourteen patients (50%) received surgical treatment, which was successful in all cases, but four of these patients (29%) presented with pHPT recurrence after a median time of 6.5 years. Three of these patients underwent a second cervical surgery that confirmed the presence of a new parathyroid adenoma. These results suggest that SCD is a condition associated with pHPT in young subjects. SCD patients with pHPT have a high risk of very low BMD. A diagnosis of pHPT should be suspected in the presence of mild hypercalcemia or low BMD in SCD patients. [ABSTRACT FROM AUTHOR]

Published

2020

34. Cytoplasmic proliferating cell nuclear antigen connects glycolysis and cell survival in acute myeloid leukemia.

Author

Ohayon, Delphine, De Chiara, Alessia, Chapuis, Nicolas, Candalh, Céline, Mocek, Julie, Ribeil, Jean-Antoine, Haddaoui, Lamya, Ifrah, Norbert, Hermine, Olivier, Bouillaud, Frédéric, Frachet, Philippe, Bouscary, Didier, and Witko-Sarsat, Véronique

Published

2016

35. Ineffective erythropoiesis in β -thalassemia.

Author

Ribeil, Jean-Antoine, Arlet, Jean-Benoit, Dussiot, Michael, Cruz Moura, Ivan, Courtois, Geneviève, Hermine, Olivier, and Moura, Ivan Cruz

Abstract

In humans, β -thalassemia dyserythropoiesis is characterized by expansion of early erythroid precursors and erythroid progenitors and then ineffective erythropoiesis. This ineffective erythropoiesis is defined as a suboptimal production of mature erythrocytes originating from a proliferating pool of immature erythroblasts. It is characterized by (1) accelerated erythroid differentiation, (2) maturation blockade at the polychromatophilic stage, and (3) death of erythroid precursors. Despite extensive knowledge of molecular defects causing β -thalassemia, less is known about the mechanisms responsible for ineffective erythropoiesis. In this paper, we will focus on the underlying mechanisms leading to premature death of thalassemic erythroid precursors in the bone marrow. [ABSTRACT FROM AUTHOR]

Published

2013