Your search keyword '"G Beaune"' showing total 72 results

1. Évaluation d'une stratégie d'exclusion d'un syndrome coronarien aigu non ST+ basé sur une unique mesure de troponine de haute sensibilité à partir d'un prélèvement effectué entre 3 et 6 heures après le début de la douleur

Author

V. Thomas, K. Yayehd, Loic Belle, H. Madiot, C. Ricard, G. Beaune, N. Noirclerc, A. Douair, and T. Rocher

Subjects

Gynecology, medicine.medical_specialty, business.industry, medicine, Cardiology and Cardiovascular Medicine, business

Abstract

Resume Contexte Selon les recommandations actuelles, en presence d'une douleur thoracique suspecte, le diagnostic d'infarctus sans sus-decalage du segment ST (IDMST-) peut etre exclu en presence d'un resultat negatif de troponine cardiaque ultrasensible sur un prelevement unique realise au moins 6 heures apres le debut de la douleur. Le but de cette etude est d'evaluer une strategie d'exclusion de l'IDMST- base sur un taux plasmatique de Troponine I ultrasensible (TnIc-HS) inferieur a la limite de quantification, a partir d'un prelevement unique effectue entre 3 et 6 heures apres le debut de la douleur. Methodes Cette etude observationnelle retrospective a inclus 432 patients consecutifs vus aux Urgences pour douleurs thoraciques suspectes d'IDMST-, avec un dosage unique de TnIc-HS Resultats L’âge moyen etait de 48,5 ± 5,6 ans et 51 % etaient des hommes. La probabilite pre-test d'IDMST- etait faible (70 %) ou intermediaire (21 %). Sur les 419 patients suivis (13 perdus de vue, 3 %) il n'y a eu ni deces ni evenement cardiovasculaire ; 38 patients (9,2 %) ont ete hospitalises dans le 1er mois, aucun pour raison cardiaque. Conclusions Les resultats de cette etude confirment la validite d'une strategie d'exclusion de l'IDMST- aux urgences, basee sur un prelevement unique de troponine cardiaque effectue 3 a 6 heures apres le debut de la douleur thoracique.

Published

2021

2. [Evaluation of rule out strategy for patients with non-ST-elevation acute coronary syndrome with single measurement of high-sensitivity cardiac troponin I from one sample tested beetween 3 and 6 hours after chest pain onset]

Author

G, Beaune, K, Yayehd, T, Rocher, V, Thomas, H, Madiot, C, Ricard, N, Noirclerc, A, Douair, and L, Belle

Subjects

Adult, Male, Chest Pain, Troponin T, Predictive Value of Tests, Troponin I, Humans, Female, Acute Coronary Syndrome, Middle Aged, Biomarkers

Abstract

Guidelines recommend to consider excluding non-ST-segment elevation myocardial infarction (NSTEMI) when high-sensitivity cardiac troponin is below the limit of quantification and a single blood sample is taken6 h after the onset of chest pain. The aim of our study was to assess such exclusion when a single blood sample was taken 3-6 h after the onset of permanent chest pain.This observational study included consecutive patients admitted into the emergency room of our hospital with chest pain and suspected NSTEMI, with non-contributive electrocardiograms and a single high-sensitivity cardiac troponin I (hs-cTnI) blood sample taken 3-6 h after the onset of chest pain and hs-cTnI4 ng/l (Abbott Diagnostic). Clinical follow-up was undertaken 1 month after admission.The mean age of the 432 patients was 48.5 ± 5.6 years and 51% were male. Based on a clinical algorithm, the pre-test probability of NSTEMI was low in 70%, and intermediate in 21% of patients. Among 419 patients with available 1-month follow-up data, there were no myocardial infarctions or deaths. Thirty-eight patients (9%) were admitted into hospital but none for cardiac reasons.Our results suggest that exclusion of NSTEMI in patients with a non-contributive electrocardiogram and a single "negative" troponin test in a blood sample taken 3-6 h after the onset of symptoms is valid.

Published

2021

3. Dépistage de l’hypercholestérolémie familiale à partir du LDL cholestérol à l’admission en unité de soins intensifs cardiologiques

Author

C. Palette, A. Grenier, Loic Belle, G. Beaune, C. Legagneur, R. Boulestreau, P. Chemaly, O. Nallet, H. Courtade, N. Delarche, J.-L. Georges, and I. Reibel

Subjects

Gynecology, 03 medical and health sciences, medicine.medical_specialty, 0302 clinical medicine, business.industry, medicine, 030212 general & internal medicine, 030204 cardiovascular system & hematology, Cardiology and Cardiovascular Medicine, business

Abstract

Resume Contexte L’hypercholesterolemie familiale (HF) est une maladie genetique frequente qui expose a une atherosclerose precoce, en particulier coronaire. Cependant, l’HF reste encore meconnue des cardiologues et est largement sous-diagnostiquee en France. Elle doit etre suspectee pour des taux de LDL cholesterol (LDLc) ≥ 1,9 g/L en l’absence de traitement. Objectif L’objectif de cette etude multicentrique retro- et prospective etait de preciser la prevalence des patients admis en USIC avec un taux eleve de LDLc et l’impact sur leur suivi lipidique personnel et familial. Methodes Analyse retrospective de tous les bilans lipidiques preleves a l’admission en USIC dans 4 centres en 2017. Analyse descriptive des caracteristiques demographiques, des motifs d’hospitalisation et du statut coronaire des patients consecutifs avec taux de LDLc ≥ 1,9 g/L (4,9 mmol/L). Suivi prospectif a un an portant sur le traitement hypocholesterolemiant, le suivi biologique et l’existence d’un depistage familial de l’HF. Resultats Un dosage de lipides a ete realise chez 2172 patients et 108 (5 %) avaient un taux de LDLc ≥ 1,9 g/L (âge moyen 64 ± 14 ans, hommes 51 %). L’hospitalisation etait liee a un syndrome coronaire aigu dans 78 % des cas et une cardiopathie non ischemique dans 22 %. Un traitement hypocholesterolemiant etait prescrit chez 9 % des patients a l’entree et 84 % a la sortie, par fortes doses de statine. Au suivi a un an, 20 % n’avaient pas controle leur LDLc, la statine avait ete diminuee (36 %) ou arretee (7 %) chez 43 %. Au moins un relatif du premier degre (fratrie ou enfants) avait eu un dosage de cholesterol dans 37 % des cas, et l’exploration genetique a ete realisee chez 3 patients. Conclusions Le depistage de l’HF en USIC necessite le calcul systematique du score DUTCH chez les patients a risque dont le taux de LDLc est superieur a 1,9 g/L, ce critere biologique n’etant pas suffisant en soi. Cette etude montre qu’il existe une marge importante d’optimisation de la prise en charge therapeutique et de l’exploration familiale chez les patients a risque d’HF depistes en USIC.

Published

2018

4. [Screening for familial hypercholesterolemia from low-density lipoprotein cholesterol levels at admission in the coronary care unit]

Author

P, Chemaly, O, Nallet, N, Delarche, C, Legagneur, R, Boulestreau, I, Reibel, C, Palette, A, Grenier, H, Courtade, G, Beaune, L, Belle, and J-L, Georges

Subjects

Aged, 80 and over, Male, Anticholesteremic Agents, Cholesterol, HDL, Coronary Care Units, Cholesterol, LDL, Middle Aged, Hospitalization, Hyperlipoproteinemia Type II, Humans, Mass Screening, Female, France, Prospective Studies, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Triglycerides, Aged, Follow-Up Studies, Retrospective Studies

Abstract

Familial hypercholesterolemia (FH) is a frequent genetic disorder that leads to premature atherosclerosis and coronary artery disease. However, knowledge of FH by cardiologists is weak, and FH remains underdiagnosed in France. FH should be suspected when low-density lipoprotein cholesterol (LDLc) levels exceed 1.9g/L (4.9mmol/L) without lipid lowering therapy.This multicenter retro- and prospective observational study aimed at estimating the prevalence of high LDLc levels in patients admitted in coronary care units, and the impact for the personal and familial follow-up for lipid status.Retrospective analysis of all plasma lipid measurements performed at admission in coronary care unit of 4 hospitals in 2017. Retrospective analyses of demographic, clinical, and coronary data of consecutive patients with LDLc levels≥1.9g/L. Prospective 1 year follow-up focused on lipid levels, treatments, and personal and familial screening for FH.Lipid measurement has been performed in 2172 consecutive patients, and 108 (5%) had LDLc level≥1.9g/L (mean age 64±14 years, men 51%). The primary cause of the hospitalisation was acute coronary syndrome (78%), and 22% of patients were free off coronary artery disease. Lipid lowering therapy was present in 9% of patients at admission, and 84% at discharge, with high statins regimen. At 1-year follow-up, control of LDLc level was not performed in 20% of patients, and statin dose was decreased (36%) or withdrawn (7%) in 43%. Lipid measurement has been performed in at least one first degree relative in 37% of patients, and genetic exploration has been done for 3 patients.Screening of FH in CCU should be routinely performed using the Dutch Score when LDLc is above 1.9g/L. Individual and familial management of patients at high risk for FH screened in CCU should be optimized, both for diagnosis and therapeutic purposes.

Published

2018

5. Screening for familial hypercholesterolemia from low-density lipoprotein cholesterol levels at admission in the coronary care unit

Author

H. Courtade, C. Palette, R. Boulestreau, Nicolas Delarche, Loic Belle, O. Nallet, C. Legagneur, I. Reibel, P. Chemaly, J.-L. Georges, and G. Beaune

Subjects

medicine.medical_specialty, Acute coronary syndrome, Statin, medicine.drug_class, business.industry, Familial hypercholesterolemia, Lipid Measurement, medicine.disease, Coronary artery disease, Regimen, Internal medicine, medicine, Coronary care unit, First-degree relatives, Cardiology and Cardiovascular Medicine, business

Abstract

Background Familial hypercholesterolemia (FH) is a frequent genetic disorder that leads to premature atherosclerosis and coronary artery disease. However, knowledge of FH by cardiologists is weak, and FH remains underdiagnosed in France. FH should be suspected when low-density lipoprotein cholesterol (LDLc) levels exceed 1.9 g/L (4.9 mmol/L) without lipid lowering therapy. Purpose This multicenter retro- and prospective observational study aimed at estimating the prevalence of high LDLc levels in patients admitted in coronary care units, and the impact for the personal and familial follow-up for lipid status. Methods Retrospective analysis of all plasma lipid measurements performed at admission in coronary care unit of 4 hospitals in 2017. Retrospective analyses of demographic, clinical, and coronary data of consecutive patients with LDLc levels ≥ 1.9 g/L, whatever the reason for hospitalisation. Prospective 1-year follow-up focused on lipid levels, treatments, and personal and familial screening for FH. Results Lipid measurement has been performed in 2172 consecutive patients, and 108 (5%) had LDLc level ≥ 1.9 g/L (mean age 64 ± 14 years, men 51%). The primary cause of the hospitalisation was acute coronary syndrome (78%), and 22% of patients were free off coronary artery disease. Lipid lowering therapy was present in 9% of patients at admission, and 84% at discharge, with high statins regimen. At 1-year follow-up, control of LDLc level was not performed in 20% of patients, and statin dose was decreased (36%) or withdrawn (7%) in 43%. Lipid measurement has been performed in at least one first degree relative in 37% of patients, and genetic exploration has been done for 3 patients only. Conclusions Screening of FH in CCU should be routinely performed using the Dutch Score when LDLc is above 1.9 g/L. Individual and familial management of patients at high risk for FH screened in CCU should be optimized, both for diagnosis and therapeutic purposes.

Published

2020

6. Les doses de cefazoline actuellement recommandées permettent-elles d’obtenir des concentrations plasmatiques suffisantes ?

Author

E. Piet, V. Tolsma, M. Sirodot, C. Janssen, S. Bland, J.P. Bru, S. Cohen, G. Beaune, and A.L. Destrem

Subjects

Infectious Diseases

Abstract

Introduction Dans le contexte de rupture de stock de la penicilline M injectable, la SPILF a propose la cefazoline en alternative pour le traitement des infections presumees ou documentees a staphylocoques sensibles a la meticilline, a la dose de 80 a 100 mg/kg/j, avec une adaptation posologique en cas de clairance inferieure a 50 ml/min. Il n’y a actuellement pas de donnees recentes dans la litterature qui confirme l’obtention de concentrations plasmatiques suffisantes a ces doses. Materiels et methodes Nous avons realise une etude pharmacologique monocentrique, prospective, pendant l’annee 2016 avec des dosages de cefazoline par methode HPLC (chromatographie liquide haute pression) chez les patients traites par cefazoline en perfusion continue dans les services de maladies infectieuses et reanimation. Nous avons recueilli, pour chaque patient, la dose administree sur 24 heures, le poids, la fonction renale, la pathologie et le germe responsable. Resultats Vingt dosages ont ete fait, chez 16 patients (2 dosages pour 4 patients). Cinq d’entre eux avaient une clairance de la creatinine inferieure a 50 ml/min avec une posologie adaptee selon les recommandations. Les patients avec une fonction renale normale recevaient une dose de 100 mg/kg/j. Quinze patients avaient une infection documentee a SAMS, dont 4 endocardites, 2 infections liees a un catheter, 6 infections osteoarticulaires, 2 bacteriemies et 1 pneumonie. La concentration plasmatique moyenne etait de 61,9 mg/l (ET = 28,9, min = 22,17, max = 135), et de 60,7 mg/l chez les patients avec une clairance Conclusion Cette etude confirme que les concentrations plasmatiques de cefazoline obtenues aux doses actuellement recommandees sont nettement suffisantes, pour des infections potentiellement difficiles a traiter, y compris avec des doses faibles chez l’insuffisant renal. La variabilite interindividuelle et les valeurs hautes retrouvees conduisent a recommander un monitorage des concentrations plasmatiques afin d’adapter au mieux les posologies.

Published

2017

7. Etude du profil protéique de 45 enfants drépanocytaires homozygotes congolais

Author

N Borel Giraud, L Tshilolo, and G Beaune

Subjects

Gynecology, medicine.medical_specialty, business.industry, medicine, General Medicine, business

Abstract

La drepanocytose, maladie genetique tres repandue en Afrique, associe une anemie hemolytique chronique et des complications vaso-occlusives et infectieuses. Nous avons etudie, dans un contexte tropical ou les sujets sont continuellement soumis a un contact avec des agents infectieux, le profil proteique de 45 patients drepanocytaires homozygotes (15 garcons et 30 filles de mediane d’âge a 7 ans) compare a un groupe controle congolais de 43 patients non drepanocytaires en bonne sante, de statut AA ou heterozygote AS (18 filles, 25 garcons de mediane d’âge a 18 ans). La confrontation des resultats des dosages de 10 proteines constituant le profil proteique contribue a evaluer les statuts immunitaires (IgA, IgG et IgM), inflammatoires (C3, CRP, A1GP : α1-glycoproteine acide, et haptoglobine) et nutritionnels (transferrine, transthyretine, albumine) des patients. Les resultats ont montre une hyperstimulation de la reponse humorale chez les patients drepanocytaires avec une augmentation significative des 3 fractions A, G et M des patients par rapport a celles du groupe controle. La fraction IgA etait particulierement discriminante entre les deux groupes (p < 0,001). Nous avons note aussi une hemolyse intravasculaire illustree par une diminution tres significative du rapport haptoglobine/A1GP du groupe des enfants drepanocytaires. Au sein de ce groupe, nous constatons une diminution tres significative (p < 0,001) du rapport haptoglobine/A1GP chez les patients avec syndrome inflammatoire par rapport aux patients sans syndrome inflammatoire. Ceci confirme le lien etroit existant entre inflammation et hemolyse dans la drepanocytose. Enfin, les moyennes des parametres de la nutrition des patients drepanocytaires etaient tres significativement diminuees par rapport aux valeurs des temoins congolais.

Published

2009

8. Evaluation d’une technique de détermination de l’HBA1C sur Architect CI8200 (Abbott Diagnostic). Comparaison avec la technique HPLC D-10 Bio-Rad

Author

S Favre, J Ducruet, J Jund, and G Beaune

Subjects

medicine.medical_specialty, endocrine system diseases, business.industry, nutritional and metabolic diseases, Hemoglobin variants, General Medicine, medicine.disease, Gastroenterology, High-performance liquid chromatography, Hemoglobinopathy, Internal medicine, Medicine, business, Immunoturbidimetry

Abstract

The aim of this study is to present an evaluation of HbA(1c) Assay on Architect CI8200 (Abbott Diagnostic). The measurement includes Hb assay by colorimetry and HbA(1c) by immunoturbidimetry. The percentage of HbA(1c) is the report HbA(1c)/complete Hb with a conversion coefficient. Repetability (n = 30; CV: 1.15-1.91%) and reproductibility (n = 30; CV: 2.09-2.64%) are good. Abbott results cannot be returned above 12%. Comparison between HbA(1c) Abbott and HbA(1c) Bio-Rad is performed on 161 patients samples ranging from 4.7 and 12%. Results show a correlation coefficient of 0.9847 (N = 161) with a regression equation: [Abbott] = 1.02x [Bio-Rad]-0,636]. Differences between two methods are normally distributed. 95% of differences lie between limits (-0.61%; +0.61%). Such differences are clinically important and interchangability of two measurements can't be possible now because lack of agreement. We hope that IFCC standardization will reduce these differences. Presence of a jaundice and carbamylation of haemoglobin do not interfer with Abbott assay. Hemoglobin variants are not detected. Therefore, monitoring of diabetic patients with HbA(1c) is possible only if hemoglobinopathy has been identified before.

Published

2008

9. Dosage du BNP sur ADVIA Centaur (Bayer HealthCare) : corrélation avec la technique Triage (Biosite) et application au diagnostic étiologique d’une dyspnée

Author

G BEAUNE, A MERCIERVILLET, J STEIDEL, S HOMINAL, T DIDI, L BELLE, C LEBRUN, and J JUND

Subjects

Biochemistry (medical), Clinical Biochemistry

Published

2004

10. La porphyrie aiguë intermittente : une urgence métabolique

Author

M Sirodot, H Puy, J C Deybach, and G Beaune

Subjects

medicine.medical_specialty, Photosensitivity, business.industry, Gastroenterology, medicine, General Medicine, business, medicine.disease, Dermatology, Acute intermittent porphyria

Published

2009

11. The role of antitissue transglutaminase assay for the diagnosis and monitoring of coeliac disease: A French-Italian multicentre study

Author

Tonutti E., Visentini D., Bizzaro N., Caradonna M., Cerni L., Villalta D., Tozzoli R. F Ferrara, M Barraco, E Migali, D Mariotti, G Danzi, ML Martino, M Danzi, M Baldassarre, G Di Bitonto, M Ciccarelli, D Riello, G Bertiato, G Pedicini, RC Bocchino, F Moccia, G Alessio, P Amboni, C Ottomano, U Volta, A Granito, N Carabellese, R Amato, G Aurnia, C Spagnulo, P Clemen, F Coppola, G Spagnoletti, M Spina, T Trigilia, F Branciforte, L Giancotti, M Apollini, B Malamisura, A Sofia, M Boffardi, F Antico, P Arigliano, G Marcer, E Sala, ML Grassi, G Giana, C Staffa, V Cova, M Martinelli, A Calabrò, D Renzi, D Nigro, D Macchia, M Manfredi, E Cammelli, G Castellucci, L Ferraro, L Marchetti, G Garelli, M Colombo, E Castellano, M Cingolani, A Sabatino, A Di Blasi, M Golato, A Carlucci, G Spagnuolo, G Trivisonno, V Castelli, S Babbini, V Marrè, G Meli, S Amoroso, M Montesanti, E Mei, S Armelloni, C Gerosa, C Marcellino, C Gallo, R Pozzoli, M Peracchi, MT Bardella, C Trovato, VS Arosio, R Malberti, F Rea, MR Di Domenico, A Sergio, P Iardino, V Formicola, G Tamburro, A Massari, M Cirella, E Rondinella, A Pignero, D Scognamiglio, S Spagnuolo, S Orefice, V Romano, B Pennucci, A Maglione, S Lavecchia, A Rubino, O Leone, N Cantieri, F Michelutti, G Guariso, D Basso, S Teresi, E Gucciardino, M Di Gregorio, MA Trippiedi, P Greco, R Guadagna, E Maltese, T Imbastaro, G Lombardi, A Rossi, E Savi, L Spada, D Villalta, G Tabellini, M Saccarola, P Palumbo, G Marinucci, PM Strappini, F Viola, M Barbato, Roma, N Bizzaro, P Pasini, F Minetti, M Scogna, M Vascotto, G Morgese, F Bascietto, P Cantelmi, F Bulacanti, D Bassetti, S Santer, D Prizzon, S Loperfido, S Martelossi, T Not, A Ventura, E Tonutti, D Visentini, S Finazzi, S Salvatore, GV Melzi d’Eril, D Wolf, M Montesanto, M Negri, MG Azzeni, R Giordano, M Farina, S Micieli, V Gouilleux, O Bandin, A Tridon, M Meyer, F Bienvenu, G Beaune, S Jego, M San Marco, D Bernard, J Sarles, J Sahel, D Carre, S Benzaken, JF Demarquay, C Johanet, JJ Baudon., Tonutti E., Visentini D., Bizzaro N., Caradonna M., Cerni L., Villalta D., Tozzoli R. F Ferrara, M Barraco, E Migali, D Mariotti, G Danzi, ML Martino, M Danzi, M Baldassarre, G Di Bitonto, M Ciccarelli, D Riello, G Bertiato, G Pedicini, RC Bocchino, F Moccia, G Alessio, P Amboni, C Ottomano, U Volta, A Granito, N Carabellese, R Amato, G Aurnia, C Spagnulo, P Clemen, F Coppola, G Spagnoletti, M Spina, T Trigilia, F Branciforte, L Giancotti, M Apollini, B Malamisura, A Sofia, M Boffardi, F Antico, P Arigliano, G Marcer, E Sala, ML Grassi, G Giana, C Staffa, V Cova, M Martinelli, A Calabrò, D Renzi, D Nigro, D Macchia, M Manfredi, E Cammelli, G Castellucci, L Ferraro, L Marchetti, G Garelli, M Colombo, E Castellano, M Cingolani, A Sabatino, A Di Blasi, M Golato, A Carlucci, G Spagnuolo, G Trivisonno, V Castelli, S Babbini, V Marrè, G Meli, S Amoroso, M Montesanti, E Mei, S Armelloni, C Gerosa, C Marcellino, C Gallo, R Pozzoli, M Peracchi, MT Bardella, C Trovato, VS Arosio, R Malberti, F Rea, MR Di Domenico, A Sergio, P Iardino, V Formicola, G Tamburro, A Massari, M Cirella, E Rondinella, A Pignero, D Scognamiglio, S Spagnuolo, S Orefice, V Romano, B Pennucci, A Maglione, S Lavecchia, A Rubino, O Leone, N Cantieri, F Michelutti, G Guariso, D Basso, S Teresi, E Gucciardino, M Di Gregorio, MA Trippiedi, P Greco, R Guadagna, E Maltese, T Imbastaro, G Lombardi, A Rossi, E Savi, L Spada, D Villalta, G Tabellini, M Saccarola, P Palumbo, G Marinucci, PM Strappini, F Viola, M Barbato, Roma, and N Bizzaro, P Pasini, F Minetti, M Scogna, M Vascotto, G Morgese, F Bascietto, P Cantelmi, F Bulacanti, D Bassetti, S Santer, D Prizzon, S Loperfido, S Martelossi, T Not, A Ventura, E Tonutti, D Visentini, S Finazzi, S Salvatore, GV Melzi d’Eril, D Wolf, M Montesanto, M Negri, MG Azzeni, R Giordano, M Farina, S Micieli, V Gouilleux, O Bandin, A Tridon, M Meyer, F Bienvenu, G Beaune, S Jego, M San Marco, D Bernard, J Sarles, J Sahel, D Carre, S Benzaken, JF Demarquay, C Johanet, JJ Baudon.

Subjects

Immunoglobulin A, Adult, Male, Adolescent, Tissue transglutaminase, Reproducibility of Result, Enzyme-Linked Immunosorbent Assay, Autoantigens, Sensitivity and Specificity, Coeliac disease, Pathology and Forensic Medicine, Serology, Antigen, Autoantigen, Immunopathology, Humans, Medicine, Age Factor, Child, Autoantibodies, Transglutaminases, biology, business.industry, Age Factors, Reproducibility of Results, Infant, Original Articles, General Medicine, Biomarker, medicine.disease, Autoantibodie, Celiac Disease, Child, Preschool, Immunoglobulin G, Immunology, biology.protein, Gluten free, Female, Antibody, business, Biomarkers, Human

Abstract

Aims: Tissue transglutaminase (tTG) was recently identified as the major autoantigen in coeliac disease. The aim of this multicentre study was to evaluate the impact of a new immunoenzymatic assay for the detection of IgA anti-tGT antibodies. Methods: Seventy four Italian and French clinical laboratories participated in this study; anti-tTG IgA with an enzyme linked immunosorbent assay (ELISA) method using guinea pig liver extract as the coating antigen, anti-endomysium IgA autoantibodies (EMA), and total serum IgA were determined in 7948 patients, 1162 of whom had coeliac disease (737 untreated cases and 425 on a gluten free diet). A proportion of the sera were then sent to a reference laboratory for anti-tTG retesting with an ELISA method using recombinant human tTG antigen. Results: Seven thousand four hundred and fifty eight (93.8%) sera were EMA/antiguinea pig tTG concordant (positive or negative); 490 (6.2%) were non-concordant. The sensitivity of EMA and antiguinea pig tTG in the 737 untreated patients with coeliac disease was 92.1% and 94.8%, respectively, and the specificity was 99.8% and 99.2%, respectively. Retesting of the discordant sera showed that of the 162 sera classified as EMA negative/antiguinea pig tTG positive, only 49 were positive for human recombinant anti-tTG, and that 39 of these were also EMA positive. Furthermore, of the 36 sera classified as EMA positive/antiguinea pig tTG negative, only two were confirmed as EMA positive. Conclusions: The antiguinea pig tTG assay is more sensitive but less specific than EMA, whereas the antihuman recombinant tTG assay is far more specific and just as sensitive as antiguinea pig tTG. Testing for EMA presents considerable interpretative problems and is difficult to standardise.

Published

2003

12. [Protein profile in 45 Congolese children with sickle cell anaemia]

Author

G, Beaune, N Borel, Giraud, and L, Tshilolo

Subjects

Inflammation, Male, Adolescent, Transferrin, Nutritional Status, Anemia, Sickle Cell, Complement System Proteins, Immunoglobulin A, Congo, Immunoglobulin M, Reference Values, Immunoglobulin G, Humans, Prealbumin, Female, Child, Serum Albumin

Abstract

Sickle cell anemia (SCA) is a genetic disorder characterized by severe hemolytic anemia, frequent vaso-occlusive events and infections. In tropical environment, people are continuously in contact with infection agents. The present study was undertaken to measure 10 protein parameters in order to test humoral immunity, nutrition status and the relation between inflammation and hemolysis in sickle cell anemia patients in 45 Congolese sickle cell children (15 females and 30 males, median age: 7 yrs) and a control group of 43 well healthy congolese group (18 females, 25 males; median age 18 yrs). Mean values for immunoglobulins (IgG, IgM, IgA), nutrition proteins (albumin, transthyretin and transferrin) and inflammatory and hemolysis markers (C3, CRP, A1GP: alpha1-Glycoprotein acid and haptoglobin) were compared between two groups. Hyperstimulation of humoral immunity was observed in the SCA group. Most significative difference was found with IgA (p0,001). Intravascular hemolysis was illustrated by a significant decrease of the haptoglobin/A1GP ratio, and was constantly present in SCA patients. We also described a significative decrease (p0,001) of haptoglobin/A1GP ratio between SCA patients with inflammatory syndrom when compared to those without inflammation. All data confirm that haemolysis is quite linked to inflammation in SCA. In addition, nutrition parameters were significantly decreased in SCA group vs healthy congolese group.

Published

2009

13. [Evaluation of HBA1C measurement on Architect CI8200 (Abbott Diagnostic). Comparison with HPLC D-10 Bio-Rad assay]

Author

G, Beaune, J, Ducruet, J, Jund, and S, Favre

Subjects

Glycated Hemoglobin, Hemoglobinopathies, Hemoglobins, Nephelometry and Turbidimetry, Diabetes Mellitus, Humans, Reproducibility of Results, Sensitivity and Specificity, Blood Chemical Analysis, Chromatography, High Pressure Liquid

Abstract

The aim of this study is to present an evaluation of HbA(1c) Assay on Architect CI8200 (Abbott Diagnostic). The measurement includes Hb assay by colorimetry and HbA(1c) by immunoturbidimetry. The percentage of HbA(1c) is the report HbA(1c)/complete Hb with a conversion coefficient. Repetability (n = 30; CV: 1.15-1.91%) and reproductibility (n = 30; CV: 2.09-2.64%) are good. Abbott results cannot be returned above 12%. Comparison between HbA(1c) Abbott and HbA(1c) Bio-Rad is performed on 161 patients samples ranging from 4.7 and 12%. Results show a correlation coefficient of 0.9847 (N = 161) with a regression equation: [Abbott] = 1.02x [Bio-Rad]-0,636]. Differences between two methods are normally distributed. 95% of differences lie between limits (-0.61%; +0.61%). Such differences are clinically important and interchangability of two measurements can't be possible now because lack of agreement. We hope that IFCC standardization will reduce these differences. Presence of a jaundice and carbamylation of haemoglobin do not interfer with Abbott assay. Hemoglobin variants are not detected. Therefore, monitoring of diabetic patients with HbA(1c) is possible only if hemoglobinopathy has been identified before.

Published

2009

14. [BNP or NT-proBNP: 'that is the question']

Author

C, Lebrun, Y, Neuder, C, Pison, N, Chouri, D, Barnoud, L, Belle, and G, Beaune

Subjects

Aged, 80 and over, Heart Failure, Lung Diseases, Male, Time Factors, Laboratories, Hospital, Peptide Fragments, Diagnosis, Differential, Dyspnea, Patient Admission, Creatinine, Natriuretic Peptide, Brain, Humans, False Positive Reactions, Female, Natriuretic Agents, Protein Precursors, Emergency Service, Hospital, False Negative Reactions, Biomarkers

Abstract

Blood measurements of BNP and NT-proBNP, its catabolite, improve diagnosis for patients admitted to emergency departments with dyspnoea. In this paper, we have compared the BNP to the NT-proBNP for 119 dyspnoeic patients using at random clear clinical status. Among the test group of 119 patients, 57 showed coherent biological results for the 2 markers. These results confirm the final clinical diagnosis. Nine patients with congestive heart failure had abnormally low BNP and NT-proBNP rates. Six of these patients experienced long delays (longer than 48 hours and less than 72 hours) between their admission in emergency and the biological measurement of the natriuretic biomarkers. Three of the other patients could be not only flash OAP cases with a fast growth and a fast normalisation of BNP but also could have existing genetical factors. These genetical factors leading to high variability in BNP synthesis are not related to physiological or cardiac factors. 43 patients showed a mismatch between BNP and NT-proBNP. BNP appeared to be unstable in vitro. The lack of stability in whole blood or plasma samples is increased by sampling in a glass EDTA collection tube and too long delays in transferring the samples from the emergency area and the laboratory in a big hospital. Ten patients showed a mismatch with abnormally high NT-proBNP or false positive results. Among these 10 patients, 5 had renal dysfunction with a high level of creatinine concentration. It is clear that all Diagnostics Manufacturers should now propose different cut-off for natriuretic peptides tests according to the degree of patients' renal impairment.

Published

2007

15. [Vitamin C measurements in vulnerable populations: 4 cases of scurvy]

Author

G, Beaune, C, Martin, D, Martin, J P, Deplante, F, Heluwaert, and F, Ducret

Subjects

Aged, 80 and over, Male, Depression, Malnutrition, Ascorbic Acid, Vitamins, Middle Aged, Vulnerable Populations, Alcoholism, Social Isolation, Alzheimer Disease, Humans, Female, Scurvy

Abstract

Hypovitaminose C, at the origin of the scurvy, did not disappear. We report 4 cases of desocialized patients and whose very unbalanced diet was at the origin of the vitamin deficit. In addition to the hemorrhagic demonstrations described among 4 patients, one finds a modification of the superficial body growths. Physiologically, the vitamin C takes part in the stability of the collagen of the vascular wall and the bone. The biological assessment of the 4 patients was normal apart from the low ascorbemy, a syndrome of denutrition and anaemia related to the haemorrhage. The quality of the vitamin C determination requires to respect the recommended pre-analytical conditions. The treatment quickly effective, consists of an oral administration of ascorbic acid. The evolution for 3 of the 4 described patients was favorable without after-effects. The proportioning of the vitamin C should be more often prescribed in geriatrics, psychiatry and cancerology. It should systematically form part of the biological assessment of the people living alone and/or homelessness.

Published

2006

16. Description of 10 new mutations in platelet glycoprotein IIb (alphaIIb) and glycoprotein IIIa (beta3) genes

Author

Christine Vinciguerra, G Beaune, Jean-Claude Bordet, Claude Negrier, C Grenier, and Marc Dechavanne

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Mutation, Nonsense mutation, Intron, Hematology, General Medicine, Exons, Platelet Glycoprotein GPIIb-IIIa Complex, Sequence Analysis, DNA, Biology, medicine.disease_cause, Molecular biology, Polymerase Chain Reaction, Exon, Thrombasthenia, hemic and lymphatic diseases, medicine, Missense mutation, Humans, Electrophoresis, Polyacrylamide Gel, Gene

Abstract

In this study we have used denaturing gradient gel electrophoresis (DGGE) for identifying sequence alterations in glycoprotein (GP) IIb and IIIa genes from 20 patients affected by Glanzmann's thrombasthenia. These patients were from 16 different families. Using computer modelling, we divided the promoters, coding sequences and flanking splicing regions, in 31 segments for the GPIIb gene and 19 domains for the GPIIIa gene. We were able to find a mutation potentially affecting GPIIb-IIIa expression or function in 16 patients out of 20. In six patients from three families, the gypsy mutation modifying the splice donor site of intron 15 of the GPIIb gene was detected. In the other patients, 10 novel mutations were characterised, which were located either in the GPIIb gene (nine cases) or in the GPIIIa gene (one case). The type of mutation was nonsense mutation (one case), missense mutation (five cases), small insertion of 1 bp (one case) and splicing modifications (three cases). Among these genetic events, three were directly responsible for Glanzmann's thrombasthenia, four were localised in regions known to be involved in GPIIb-IIIa complex expression and three mutations were potentially responsible for Glanzmann's thrombasthenia.

Published

2002

17. [Etiologic diagnosis of malnutrition in pediatrics: reflections about a case]

Author

C, Frainais, G, Beaune, and B, Massenavette

Subjects

Male, Parenteral Nutrition, Time Factors, Ceftriaxone, Hemophilia B, Anti-Bacterial Agents, Cephalosporins, Diet, Nutrition Disorders, Enteral Nutrition, Anti-Infective Agents, Vancomycin, Child, Preschool, Metronidazole, Humans, Drug Therapy, Combination, Amikacin, Respiratory Tract Infections, Follow-Up Studies

Published

2001

18. [A case of congenital nephrotic syndrome]

Author

G, Beaune, F O, Mallaval, S, Gimbert, F, Dijoud, A, Vialle, and B, Parchoux

Subjects

Nephrotic Syndrome, Aspirin, Streptococcus pyogenes, Infant, Newborn, Bacteremia, Anti-Bacterial Agents, Glomerular Mesangium, Enalapril, Adrenal Cortex Hormones, Streptococcal Infections, Cyclosporine, Humans, Female, Diuretics, Antihypertensive Agents, Infant, Premature, Platelet Aggregation Inhibitors, Calcifediol, Follow-Up Studies

Published

1998

19. Serum procalcitonin rise is only slight in two cases of disseminated aspergillosis

Author

G. Beaune, C. Pondarré, F Bienvenu, J Bienvenu, G. Souillet, and G. Monneret

Subjects

Microbiology (medical), Calcitonin, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Anemia, Calcitonin Gene-Related Peptide, Biology, Aspergillosis, Procalcitonin, Aspergillus fumigatus, Diagnosis, Differential, Fatal Outcome, hemic and lymphatic diseases, parasitic diseases, medicine, Humans, Protein Precursors, Mycosis, Bone Marrow Transplantation, Lung Diseases, Fungal, General Medicine, bacterial infections and mycoses, medicine.disease, biology.organism_classification, Disseminated aspergillosis, Pathophysiology, Infectious Diseases, Immunology, Female, hormones, hormone substitutes, and hormone antagonists

Abstract

High serum concentrations of procalcitonin (PCT) have been found during bacterial and parasitic infections. This is a report of two cases of disseminated aspergillosis with moderate PCT increase in two 14-year-old girls after bone marrow transplantation (BMT) for myelodysplastic syndrome and Fanconi's anemia, respectively. In contrast, the important rise of serum CRP observed in these patients tends to demonstrate that the synthesis of these two proteins is under different control mechanisms.

Published

1998

20. Prise en charge des AC d'origine cardiaque récupérés, orientation et survie

Author

G. Beaune, S. Wurtz, Dominique Savary, Loic Belle, K. Fouquet-Guerot, and J.-P. Perfus

Subjects

Emergency Medicine, Critical Care and Intensive Care Medicine

Published

2007

21. [Acute transverse myelitis: important role of biology in diagnosis]

Author

A, Villet, E, Nalet, C, Lebrun, G, Beaune, C, Santre, D, Dorez, J-P, Deplante, P, Giraud, and M, Sirodot

Subjects

Paraplegia, Anemia, Hemolytic, Adolescent, Fever, Urticaria, Pancytopenia, Anti-Inflammatory Agents, Headache, Myelitis, Transverse, Magnetic Resonance Imaging, Abdominal Pain, Diagnosis, Differential, Predictive Value of Tests, Hypergammaglobulinemia, Lymphopenia, Humans, Prednisone, Female, Confusion, Hydroxychloroquine

22. Recombinant silk protein condensates show widely different properties depending on the sample background.

Author

Tersteegen J, Tunn I, Sand M, Välisalmi T, Malkamäki M, Gandier JA, Beaune G, Sanz-Velasco A, Anaya-Plaza E, and Linder MB

Subjects

Animals, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Silk chemistry, Spiders chemistry

Abstract

There is an increasing understanding that condensation is a crucial intermediate step in the assembly of biological materials and for a multitude of cellular processes. To apply and to understand these mechanisms, in vitro biophysical characterisation techniques are central. The formation and biophysical properties of protein condensates depend on a multitude of factors, such as protein concentration, pH, temperature, salt concentration, and presence of other biomolecules as well as protein purification and storage conditions. Here we show how critical the procedures for preparing protein samples for in vitro studies are. We compare two purification methods of the recombinant spider silk protein CBM-AQ12-CBM and study the effect of background molecules, such as DNA, on the formation and properties of the condensates. We characterize the condensates using aggregation induced emitters (AIEs), coalescence studies, and micropipette aspiration. The condensated sample containing background molecules exhibit a lower threshold concentration for condensate formation accompanied by a lower surface tension and longer coalescence time when compared to the pure protein condensates. Furthermore, the partitioning of small AIEs is enhanced in the presence of background molecules. Our results highlight that the purification method and remaining background molecules strongly affect the biophysical properties of spider silk condensates. Using the acquired knowledge about spider silk protein purification we derive guidelines for reproducible condensate formation that will foster the use of spider silk proteins as adhesives or carriers for biomedical applications.

Published

2024

23. pH-Responsive Near-Infrared Emitting Gold Nanoclusters.

Author

Zhou S, Gustavsson L, Beaune G, Chandra S, Niskanen J, Ruokolainen J, Timonen JVI, Ikkala O, Peng B, and Ras RHA

Abstract

Near-infrared (NIR) fluorophores with pH-responsive properties suggest merits in biological analyses. This work establishes a general and effective method to obtain pH-responsive NIR emissive gold nanoclusters by introducing aliphatic tertiary amine (TA) groups into the ligands. Computational study suggests that the pH-responsive NIR emission is associated with electronic structure change upon protonation and deprotonation of TA groups. Photo-induced electron transfer between deprotonated TA groups and the surface Au-S motifs of gold nanoclusters can disrupt the radiative transitions and thereby decrease the photoluminescence intensity in basic environments (pH=7-11). By contrast, protonated TA groups curb the electron transfer and restore the photoluminescence intensity in acidic environments (pH=4-7). The pH-responsive NIR-emitting gold nanoclusters serve as a specific and sensitive probe for the lysosomes in the cells, offering non-invasive emissions without interferences from intracellular autofluorescence., (© 2023 The Authors. Angewandte Chemie International Edition published by Wiley-VCH GmbH.)

Published

2023

24. [Help sheets for ordonnance in biochemistry: proposal].

Author

Beaune G, Oris C, Boizot HT, Annette-Reisch M, Pecquet M, and Schmitt F

Subjects

Humans, Biochemistry

Published

2023

25. Compressibility and porosity modulate the mechanical properties of giant gas vesicles.

Author

Al-Terke HH, Beaune G, Junaid M, Seitsonen J, Paananen A, Timonen JVI, Joensuu J, Brochard-Wyart F, and Ras RHA

Subjects

Porosity

Abstract

Gas vesicles used as contrast agents for noninvasive ultrasound imaging must be formulated to be stable, and their mechanical properties must be assessed. We report here the formation of perfluoro- n -butane microbubbles coated with surface-active proteins that are produced by filamentous fungi (hydrophobin HFBI from Trichoderma reesei ). Using pendant drop and pipette aspiration techniques, we show that these giant gas vesicles behave like glassy polymersomes, and we discover novel gas extraction regimes. We develop a model to analyze the micropipette aspiration of these compressible gas vesicles and compare them to incompressible liquid-filled vesicles. We introduce a sealing parameter to characterize the leakage of gas under aspiration through the pores of the protein coating. Utilizing this model, we can determine the elastic dilatation modulus, surface viscosity, and porosity of the membrane. These results demonstrate the engineering potential of protein-coated bubbles for echogenic and therapeutic applications and extend the use of the pipette aspiration technique to compressible and porous systems.

Published

2023

26. Recombinant protein condensation inside E. coli enables the development of building blocks for bioinspired materials engineering - Biomimetic spider silk protein as a case study.

Author

Gabryelczyk B, Sammalisto FE, Gandier JA, Feng J, Beaune G, Timonen JVI, and Linder MB

Abstract

Recombinant expression of proteins destined to form biological materials often results in poor production yields or loss of their function due to premature aggregation. Recently, liquid-liquid phase separation has been proposed as a mechanism to control protein solubility during expression and accumulation in the cytoplasm. Here, we investigate this process in vivo during the recombinant overexpression of the mimetic spider silk mini-spidroin NT2RepCT in Escherichia coli . The protein forms intracellular liquid-like condensates that shift to a solid-like state triggered by a decrease in their microenvironmental pH. These features are also maintained in the purified sample in vitro both in the presence of a molecular crowding agent mimicking the bacterial intracellular environment, and during a biomimetic extrusion process leading to fiber formation. Overall, we demonstrate that characterization of protein condensates inside E. coli could be used as a basis for selecting proteins for both materials applications and their fundamental structure-function studies., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2022 The Authors.)

Published

2022

27. Correction: β-1,3-Glucan synthesis, novel supramolecular self-assembly, characterization and application.

Author

Pylkkänen R, Mohammadi P, Liljeström V, Płaziński W, Beaune G, Timonen JVI, and Penttilä M

Abstract

Correction for 'β-1,3-Glucan synthesis, novel supramolecular self-assembly, characterization and application' by Robert Pylkkänen et al. , Nanoscale , 2022, https://doi.org/10.1039/D2NR02731C.

Published

2022

28. β-1,3-Glucan synthesis, novel supramolecular self-assembly, characterization and application.

Author

Pylkkänen R, Mohammadi P, Liljeström V, Płaziński W, Beaune G, Timonen JVI, and Penttilä M

Subjects

Glucans chemistry, Crystallization, Protein Structure, Secondary, beta-Glucans chemistry

Abstract

β-1,3-Glucans are ubiquitously observed in various biological systems with diverse physio-ecological functions, yet their underlying assembly mechanism and multiscale complexation in vitro remains poorly understood. Here, we provide for the first-time evidence of unidentified β-1,3-glucan supramolecular complexation into intricate hierarchical architectures over several length scales. We mediated these unique assemblies using a recombinantly produced β-1,3-glucan phosphorylase ( Ta 1,3BGP) by fine-tuning solution conditions during particle nucleation and growth. We report a synthesis of interconnected parallel hexagonal lamellae composed of 8 nm thick sheets of highly expanded paracrystals. The architecture consists of β-1,3-glucan triple-helices with considerable inter-intra hydrogen bonding within, as well as in between adjacent triple-helices. The results extend our understanding of β-1,3-glucan molecular organization and shed light on different aspects of the crystallization processes of biomolecules into structures unseen by nature. The presented versatile synthesis yields new materials for diverse medical and industrial applications.

Published

2022

29. Fusion Dynamics of Hybrid Cell-Microparticle Aggregates: A Jelly Pearl Model.

Author

Beaune G, Sinkkonen L, Gonzalez-Rodriguez D, Timonen JVI, and Brochard-Wyart F

Subjects

Hybrid Cells

Abstract

We study the fusion of homogeneous cell aggregates and of hybrid aggregates combining cells and microparticles. In all cases, we find that the contact area does not vary linearly over time, as observed for liquid drops, but rather it follows a power law in t 2/3 . This result is interpreted by generalizing the fusion model of soft viscoelastic solid balls to viscoelastic liquid balls, akin to jelly pearls. We also explore the asymmetric fusion between a homogeneous aggregate and a hybrid aggregate. This latter experiment allows the determination of the self-diffusion coefficient of the cells in a tissue by following the spatial distribution of internalized particles in the cells.

Published

2022

30. [Bioclinical comparison of two high sensitivity cardiac troponin I assays: Siemens ADVIA Centaur versus Mitsubishi PathFast].

Author

Arrivé C, Rocher T, Belle L, Boutruche S, and Beaune G

Subjects

Biomarkers, Humans, Laboratories, Point-of-Care Systems, Sensitivity and Specificity, Biological Assay, Troponin I

Abstract

High-sensitivity troponin has become an essential emergency biomarker for diagnosing or ruling out an ACS. The establishment of a point of care biology related to the reorganization and fusion of laboratories raise a question about transferability of results between techniques. In this study, we propose to compare the bioclinical performances of high-sensitivity troponin measured by two different techniques on laboratory immunoanalyzer (Siemens Advia Centaur XPT) and on point of care device (Mitsubishi Pathfast). The assay of high-sensitivity troponin (n = 90 patients), according to our study, show consistent clinical results with both method.

Published

2021

31. Bilateral posterior cerebral artery territory infarction in a SARS-Cov-2 infected patient: discussion about an unusual case.

Author

Bonardel C, Bonnerot M, Ludwig M, Vadot W, Beaune G, Chanzy B, Cornut L, Baysson H, Farines M, Combes I, Macheda G, and Bing F

Subjects

Adenosine Monophosphate analogs & derivatives, Adenosine Monophosphate therapeutic use, Alanine analogs & derivatives, Alanine therapeutic use, Antiviral Agents therapeutic use, COVID-19, Coronavirus Infections diagnosis, Coronavirus Infections drug therapy, Coronavirus Infections virology, Diagnosis, Differential, Fatal Outcome, Host-Pathogen Interactions, Humans, Infarction, Posterior Cerebral Artery diagnostic imaging, Infarction, Posterior Cerebral Artery therapy, Male, Middle Aged, Pandemics, Pneumonia, Viral diagnosis, Pneumonia, Viral drug therapy, Pneumonia, Viral virology, Predictive Value of Tests, Risk Factors, SARS-CoV-2, Thrombolytic Therapy, Treatment Outcome, COVID-19 Drug Treatment, Betacoronavirus pathogenicity, Coronavirus Infections complications, Infarction, Posterior Cerebral Artery complications, Pneumonia, Viral complications

Abstract

In time of SARS-Cov2 pandemic, neurologists need to be vigilant for cerebrovascular complications of Covid-19. We present a case of bilateral occipito-temporal infarction revealed by a sudden cortical blindness with haemorrhagic transformation after intravenous thrombolysis in a diabetic patient infected by Covid-19. Differential diagnoses are discussed in front of this unusual presentation and evolution., Competing Interests: Declaration of Competing Interest The authors report no disclosures. Informed consent for publication has been signed by the wife of the patient., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

32. Ferrofluid Microdroplet Splitting for Population-Based Microfluidics and Interfacial Tensiometry.

Author

Latikka M, Backholm M, Baidya A, Ballesio A, Serve A, Beaune G, Timonen JVI, Pradeep T, and Ras RHA

Abstract

Ferrofluids exhibit a unique combination of liquid properties and strong magnetic response, which leads to a rich variety of interesting functional properties. Here, the magnetic-field-induced splitting of ferrofluid droplets immersed in an immiscible liquid is presented, and related fascinating dynamics and applications are discussed. A magnetic field created by a permanent magnet induces instability on a mother droplet, which divides into two daughter droplets in less than 0.1 s. During the splitting process, the droplet undergoes a Plateau-Rayleigh-like instability, which is investigated using high-speed imaging. The dynamics of the resulting satellite droplet formation is shown to depend on the roughness of the supporting surface. Further increasing the field results in additional splitting events and self-assembly of microdroplet populations, which can be magnetically actuated. The effects of magnetization and interfacial tension are systematically investigated by varying magnetic nanoparticles and surfactant concentrations, and a variety of outcomes from labyrinthine patterns to discrete droplets are observed. As the splitting process depends on interfacial tension, the droplet splitting can be used as a measure for interfacial tension as low as 0.1 mN m -1 . Finally, a population-based digital microfluidics concept based on the self-assembled microdroplets is presented., Competing Interests: The authors declare no conflict of interest., (© 2020 The Authors. Published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

33. Controllable coacervation of recombinantly produced spider silk protein using kosmotropic salts.

Author

Mohammadi P, Jonkergouw C, Beaune G, Engelhardt P, Kamada A, Timonen JVI, Knowles TPJ, Penttila M, and Linder MB

Subjects

Animals, Fibroins genetics, Fibroins metabolism, Microfluidics, Recombinant Proteins genetics, Recombinant Proteins metabolism, Salts chemistry, Fibroins chemistry, Recombinant Proteins chemistry, Salts metabolism, Spiders chemistry

Abstract

Recent developments suggest that the phase transition of natural and synthetic biomacromolecules represents an important and ubiquitous mechanism underlying structural assemblies toward the fabrication of high-performance materials. Such a transition results in the formation of condensed liquid droplets, described as condensates or coacervates. Being able to effectively control the assembly of such entities is essential for tuning the quality and their functionality. Here we describe how self-coacervation of genetically engineered spidroin-inspired proteins can be preceded by a wide range of kosmotropic salts. We studied the kinetics and mechanisms of coacervation in different conditions, from direct observation of initial phase separation to the early stage of nucleation/growth and fusion into large fluid assemblies. We found that coacervation induced by kosmotropic salts follows the classical nucleation theory and critically relies on precursor clusters of few weak-interacting protein monomers. Depending on solution conditions and the strength of the supramolecular interaction as a function of time, coacervates with a continuum of physiochemical properties were observed. We observed similar characteristics in other protein-based coacervates, which include having a spherical-ellipsoid shape in solution, an interconnected bicontinuous network, surface adhesion, and wetting properties. Finally, we demonstrated the use of salt-induced self-coacervates of spidroin-inspired protein as a cellulosic binder in dried condition., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

34. Phthalocyanine-Virus Nanofibers as Heterogeneous Catalysts for Continuous-Flow Photo-Oxidation Processes.

Author

Anaya-Plaza E, Aljarilla A, Beaune G, Nonappa, Timonen JVI, de la Escosura A, Torres T, and Kostiainen MA

Abstract

The generation of highly reactive oxygen species (ROS) at room temperature for application in organic synthesis and wastewater treatment represents a great challenge of the current chemical industry. In fact, the development of biodegradable scaffolds to support ROS-generating active sites is an important prerequisite for the production of environmentally benign catalysts. Herein, the electrostatic cocrystallization of a cationic phthalocyanine (Pc) and negatively charged tobacco mosaic virus (TMV) is described, together with the capacity of the resulting crystals to photogenerate ROS. To this end, a novel peripherally crowded zinc Pc (1) is synthesized. With 16 positive charges, this photosensitizer shows no aqueous aggregation, and is able to act as a molecular glue in the unidimensional assembly of TMV. A step-wise decrease of ionic strength in mixtures of both components results in exceptionally long fibers, constituted by hexagonally bundled viruses thoroughly characterized by electron and confocal microscopy. The fibers are able to produce ROS in a proof-of-concept microfluidic device, where they are immobilized and irradiated in several cycles, showing a resilient performance. The bottom-up approach also enables the light-triggered disassembly of fibers after use. This work represents an important example of a biohybrid material with projected application in light-mediated heterogeneous catalysis., (© 2019 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

35. Polymeric Nanoparticles Limit the Collective Migration of Cellular Aggregates.

Author

Beaune G, Nagarajan U, Brochard-Wyart F, and Winnik FM

Subjects

Animals, Cell Line, Tumor, Mice, Viscosity, Cell Aggregation drug effects, Cell Movement drug effects, Nanoparticles chemistry, Polymers chemistry, Polymers pharmacology

Abstract

Controlling the propagation of primary tumors is fundamental to avoiding the epithelial to mesenchymal transition process leading to the dissemination and seeding of tumor cells throughout the body. Here we demonstrate that nanoparticles (NPs) limit the propagation of cell aggregates of CT26 murine carcinoma cells used as tumor models. The spreading behavior of these aggregates incubated with NPs is studied on fibronectin-coated substrates. The cells spread with the formation of a cell monolayer, the precursor film, around the aggregate. We study the effect of NPs added either during or after the formation of aggregates. We demonstrate that, in both cases, the spreading of the cell monolayer is slowed down in the presence of NPs and occurs only above a threshold concentration that depends on the size and surface chemistry of the NPs. The density of cells in the precursor films, measured by confocal microscopy, shows that the NPs stick cells together. The mechanism of slowdown is explained by the increase in cell-cell interactions due to the NPs adsorbed on the membrane of the cells. The present results demonstrate that NPs can modulate the collective migration of cells; therefore, they may have important implications for cancer treatment.

Published

2019

36. Spreading of Cell Aggregates on Zwitterion-Modified Chitosan Films.

Author

Qi B, Feng H, Qiu X, Beaune G, Guo X, Brochard-Wyart F, and Winnik FM

Subjects

Adsorption drug effects, Animals, Betaine chemical synthesis, Betaine chemistry, Cattle, Cell Aggregation drug effects, Cell Line, Tumor, Chitosan chemical synthesis, Mice, Serum Albumin, Bovine chemistry, Betaine analogs & derivatives, Chitosan analogs & derivatives

Abstract

The sulfobetaine (SB) moiety, which comprises a quaternary ammonium group linked to a negatively charged sulfonate ester, is known to impart nonfouling properties to interfaces coated with polysulfobetaines or grafted with SB-polymeric brushes. Increasingly, evidence emerges that the SB group is, overall, a better antifouling group than the phosphorylcholine (PC) moiety extensively used in the past. We report here the synthesis of a series of SB-modified chitosans (CH-SB) carrying between 20 and 40 mol % SB per monosaccharide unit. Chitosan (CH) itself is a naturally derived copolymer of glucosamine and N-acetyl-glucosamine linked with a β-1,4 bond. Analysis by quartz crystal microbalance with dissipation (QCM-D) indicates that CH-SB films (thickness ∼ 20 nm) resist adsorption of bovine serum albumin (BSA) with increasing efficiency as the SB content of the polymer augments (surface coverage ∼ 15 μg cm -2 for films of CH with 40 mol % SB). The cell adhesivity of CH-SB films coated on glass was assessed by determining the spreading dynamics of CT26 cell aggregates. When placed on chitosan films, known to be cell-adhesive, the CT26 cell aggregates spread by forming a cell monolayer around them. The spreading of CT26 cell aggregates on zwitterion-modified chitosans films is thwarted remarkably. In the cases of CH-SB30 and CH-SB40 films, only a few isolated cells escape from the aggregates. The extent of aggregate spreading, quantified based on the theory of liquid wetting, provides a simple in vitro assay of the nonfouling properties of substrates toward specific cell lines. This assay can be adopted to test and compare the fouling characteristics of substrates very different from the chemical viewpoint.

Published

2019

37. Spontaneous migration of cellular aggregates from giant keratocytes to running spheroids.

Author

Beaune G, Blanch-Mercader C, Douezan S, Dumond J, Gonzalez-Rodriguez D, Cuvelier D, Ondarçuhu T, Sens P, Dufour S, Murrell MP, and Brochard-Wyart F

Subjects

Animals, Cell Communication, Cell Culture Techniques, Cells, Cultured, Mice, Spheroids, Cellular physiology, Cell Aggregation, Cell Movement, Spheroids, Cellular cytology

Abstract

Despite extensive knowledge on the mechanisms that drive single-cell migration, those governing the migration of cell clusters, as occurring during embryonic development and cancer metastasis, remain poorly understood. Here, we investigate the collective migration of cell on adhesive gels with variable rigidity, using 3D cellular aggregates as a model system. After initial adhesion to the substrate, aggregates spread by expanding outward a cell monolayer, whose dynamics is optimal in a narrow range of rigidities. Fast expansion gives rise to the accumulation of mechanical tension that leads to the rupture of cell-cell contacts and the nucleation of holes within the monolayer, which becomes unstable and undergoes dewetting like a liquid film. This leads to a symmetry breaking and causes the entire aggregate to move as a single entity. Varying the substrate rigidity modulates the extent of dewetting and induces different modes of aggregate motion: "giant keratocytes," where the lamellipodium is a cell monolayer that expands at the front and retracts at the back; "penguins," characterized by bipedal locomotion; and "running spheroids," for nonspreading aggregates. We characterize these diverse modes of collective migration by quantifying the flows and forces that drive them, and we unveil the fundamental physical principles that govern these behaviors, which underscore the biological predisposition of living material to migrate, independent of length scale.

Published

2018

38. Self-Coacervation of a Silk-Like Protein and Its Use As an Adhesive for Cellulosic Materials.

Author

Mohammadi P, Beaune G, Stokke BT, Timonen JVI, and Linder MB

Abstract

Liquid-liquid phase separation of biomacromolecules plays a critical role in many of their functions, both as cellular components and in structural assembly. Phase separation is also a key mechanism in the assembly of engineered recombinant proteins for the general aim to build new materials with unique structures and properties. Here the phase separation process of an engineered protein with a block-architecture was studied. As a central block, we used a modified spider silk sequence, predicted to be unstructured. In each terminus, folded globular blocks were used. We studied the kinetics and mechanisms of phase formation and analyzed the evolving structures and their viscoelastic properties. Individual droplets were studied with a micropipette technique, showing both how properties vary between individual drops and explaining overall bulk rheological properties. A very low surface energy allowed easy deformation of droplets and led to efficient infiltration into cellulosic fiber networks. Based on these findings, we demonstrated an efficient use of the phase-separated material as an adhesive for cellulose. We also conclude that the condensed state is metastable, showing an ensemble of properties in individual droplets and that an understanding of protein phase behavior will lead to developing a wider use of proteins as structural polymers., Competing Interests: The authors declare no competing financial interest.

Published

2018

39. Reentrant wetting transition in the spreading of cellular aggregates.

Author

Beaune G, Duclos G, Khalifat N, Stirbat TV, Vignjevic DM, and Brochard-Wyart F

Subjects

Acrylic Resins chemistry, Biomechanical Phenomena, Cell Line, Tumor, Extracellular Matrix metabolism, Glass chemistry, Humans, Phase Transition, Cell Aggregation, Wettability

Abstract

We study spreading on soft substrates of cellular aggregates using CT26 cells that produce an extracellular matrix (ECM). Compared to our previous work on the spreading of S180 cellular aggregates, which did not secrete ECMs, we found that the spreading velocity of the precursor film is also maximal for intermediate rigidities, but new striking features show up. First, we observed a cascade of liquid-gas-liquid (L/G/L) transitions of the precursor film as the substrate rigidity is decreased. We attribute the L/G transition to a decrease of cell/cell adhesion resulting from the weakening of the cell/substrate adhesion. We attribute the reentrant liquid phase (G/L) observed on soft substrates to the slow spreading of the aggregates on ultra-soft substrates, which gives time to the cells to secrete more ECM proteins and stick together. Second, a nematic order appears in the cohesive (liquid) states of the precursor film, attributed to the gradient of cell's velocities.

Published

2017

40. How gluttonous cell aggregates clear substrates coated with microparticles.

Author

Beaune G, Lam AYW, Dufour S, Winnik FM, and Brochard-Wyart F

Subjects

Animals, Cadherins metabolism, Cell Aggregation drug effects, Cell Line, Tumor, Cell Nucleus drug effects, Cell Nucleus metabolism, Cell Size drug effects, Fibronectins pharmacology, Green Fluorescent Proteins metabolism, Mice, Cell-Derived Microparticles metabolism

Abstract

We study the spreading of cell aggregates deposited on adhesive substrates decorated with microparticles (MPs). A cell monolayer expands around the aggregate. The cells on the periphery of the monolayer take up the MPs, clearing the substrate as they progress and forming an aureole of cells filled with MPs. We study the dynamics of spreading and determine the width of the aureole and the level of MP internalization in cells as a function of MP size, composition, and density. From the radius and width of the aureole, we quantify the volume fraction of MPs within the cell, which leads to an easy, fast, and inexpensive measurement of the cell - particle internalization.

Published

2017

41. Rationalising BNP prescription in the Emergency Department.

Author

Saligari E, Pagani L, Jund J, Desjoyaux E, and Beaune G

Subjects

Adult, Aged, Aged, 80 and over, Biomarkers blood, Dyspnea diagnosis, Emergency Service, Hospital standards, Female, Humans, Male, Middle Aged, Retrospective Studies, Clinical Laboratory Techniques standards, Dyspnea blood, Natriuretic Peptide, Brain blood

Published

2017

42. A one-pot synthesis of water soluble highly fluorescent silica nanoparticles.

Author

Chandra S, Beaune G, Shirahata N, and Winnik FM

Abstract

We report a one-pot synthesis of water dispersible fluorescent silica nanoparticles (NPs) functionalized with terminal amine groups, starting from silicon tetrabromide (SiBr 4 ) and aminopropyltriethoxy silane (APTES). The NPs range from 1 to 2 nm in diameter, and exhibit an intense blue emission with a quantum yield (QY) of around 34% in water. They were characterized using XRD, XPS, TEM and FTIR spectroscopy for structural analysis. A tentative mechanism explaining the origin of the NPs emission in the blue region is presented based on the distinctive features of their low temperature photoluminescence (PL), photoluminescence excitation (PLE) spectrum and time correlated single photon counting lifetime decay profiles. The outstanding PL QY and photostability of the NPs, together with their water dispersibility and biocompatibility, constitute a unique set of properties among existing silica NPs and enable the application of the NPs in various fields.

Published

2017

43. An Addison disease revealed with a serious hyponatremia.

Author

Maguet H, Carreau A, Hautefeuille S, Bonnin P, and Beaune G

Subjects

Addison Disease blood, Addison Disease complications, Adrenocorticotropic Hormone analysis, Adrenocorticotropic Hormone blood, Autoantibodies blood, Coma blood, Coma diagnosis, Coma etiology, Diagnosis, Differential, Humans, Hydrocortisone analysis, Hydrocortisone blood, Hyponatremia blood, Hyponatremia complications, Male, Middle Aged, Severity of Illness Index, Steroid 21-Hydroxylase immunology, Addison Disease diagnosis, Hyponatremia diagnosis

Abstract

We present the case of an Addison's disease revealed by a serious hyponatremia. The serum concentration of ACTH and 21-hydroxylase antibodies were increased and lead to the diagnosis. The cortisol blood level was lowered but required to take into account the stress induced by the hospitalisation of the patient. Addison's disease is characterized by the destruction of the adrenal cortex. Autoimmune adrenalitis is the main cause of adrenal insufficiency. Treatment involves normalisation of sodium concentration and corticosteroids replacement. With a good patient compliance, the survival rate of Addisonian patient is similar to that of the normal population. Management of patient requires vigilance because of the occurrence of others autoimmunes diseases during patient life.

Published

2017

44. Exposure to metal oxide nanoparticles administered at occupationally relevant doses induces pulmonary effects in mice.

Author

Présumé M, Simon-Deckers A, Tomkiewicz-Raulet C, Le Grand B, Tran Van Nhieu J, Beaune G, Duruphty O, Doucet J, Coumoul X, Pairon JC, Boczkowski J, Lanone S, and Andujar P

Subjects

Animals, Lung immunology, Lung pathology, Macrophages drug effects, Macrophages immunology, Male, Metal Nanoparticles chemistry, Mice, Mice, Inbred C57BL, Occupational Exposure analysis, Oxides toxicity, Pneumonia immunology, Pneumonia pathology, Inhalation Exposure adverse effects, Lung drug effects, Metal Nanoparticles toxicity, Occupational Exposure adverse effects, Pneumonia chemically induced, Welding

Abstract

In spite of the great promises that the development of nanotechnologies can offer, concerns regarding potential adverse health effects of occupational exposure to nanoparticle (NP) is raised. We recently identified metal oxide NP in lung tissue sections of welders, located inside macrophages infiltrated in fibrous regions. This suggests a role of these NP in the lung alterations observed in welders. We therefore designed a study aimed to investigate the pulmonary effects, in mice, of repeated exposure to NP administered at occupationally relevant doses. We therefore chose four metal oxide NPs representative of those found in the welder's lungs: Fe 2 O 3 , Fe 3 O 4 , MnFe 2 O 4 and CrOOH. These NPs were administered weekly for up to 3 months at two different doses: 5 μg, chosen as occupationally relevant to welding activity, and 50 μg, chosen as occupationally relevant to the context of an NP-manufacturing facility. Our results show that 3 month-repeated exposures to 5 μg NP induced limited pulmonary effects, characterized by the development of a mild peribronchiolar fibrosis observed for MnFe 2 O 4 and CrOOH NP only. This fibrotic event was further extended in terms of intensity and localization after the repeated administration of 50 μg NP: all but Fe 2 O 3 NP induced the development of peribronchiolar, perivascular and alveolar fibrosis, together with an interstitial inflammation. Our data demonstrate for the first time a potential risk for respiratory health posed by repeated exposure to NP at occupationally relevant doses. Given these results, the development of occupational exposure limits (OELs) specifically dedicated to NP exposure might therefore be an important issue to address.

Published

2016

45. Nanostickers for cells: a model study using cell-nanoparticle hybrid aggregates.

Author

Brunel B, Beaune G, Nagarajan U, Dufour S, Brochard-Wyart F, and Winnik FM

Subjects

Animals, Cell Line, Mice, Models, Theoretical, Polystyrenes chemistry, Silicon Dioxide chemistry, Cell Membrane, Nanoparticles chemistry

Abstract

We present direct evidence that nanoparticles (NPs) can stick together cells that are inherently non-adhesive. Using cadherin-depleted S180 murine cells lines, which exhibit very low cell-cell adhesion, we show that NPs can assemble dispersed single cells into large cohesive aggregates. The dynamics of aggregation, which is controlled by diffusion and collision, can be described as a second-order kinetic law characterized by a rate of collision that depends on the size, concentration, and surface chemistry of the NPs. We model the cell-cell adhesion induced by the "nanostickers" using a three-state dynamical model, where the NPs are free, adsorbed on the cell membrane or internalized by the cells. We define a "sticking efficiency parameter" to compare NPs and look for the most efficient type of NP. We find that 20 nm carboxylated polystyrene NPs are more efficient nanostickers than 20 nm silica NPs which were reported to induce fast wound healing and to glue soft tissues. Nanostickers, by increasing the cohesion of tissues and tumors, may have important applications for tissue engineering and cancer treatment.

Published

2016

46. Functional double-shelled silicon nanocrystals for two-photon fluorescence cell imaging: spectral evolution and tuning.

Author

Chandra S, Ghosh B, Beaune G, Nagarajan U, Yasui T, Nakamura J, Tsuruoka T, Baba Y, Shirahata N, and Winnik FM

Subjects

Animals, HEK293 Cells, Humans, Mice, NIH 3T3 Cells, Nanoparticles ultrastructure, Optical Phenomena, Particle Size, Quantum Dots chemistry, Quantum Dots ultrastructure, Spectroscopy, Fourier Transform Infrared, Spectroscopy, Near-Infrared, Microscopy, Fluorescence, Multiphoton methods, Nanoparticles chemistry, Silicon chemistry

Abstract

Functional near-IR (NIR) emitting nanoparticles (NPs) adapted for two-photon excitation fluorescence cell imaging were obtained starting from octadecyl-terminated silicon nanocrystals (ncSi-OD) of narrow photoluminescence (PL) spectra having no long emission tails, continuously tunable over the 700-1000 nm window, PL quantum yields exceeding 30%, and PL lifetimes of 300 μs or longer. These NPs, consisting of a Pluronic F127 shell and a core made up of assembled ncSi-OD kept apart by an octadecyl (OD) layer, were readily internalized into the cytosol, but not the nucleus, of NIH3T3 cells and were non-toxic. Asymmetrical field-flow fractionation (AF4) analysis was carried out to determine the size of the NPs in water. HiLyte Fluor 750 amine was linked via an amide link to NPs prepared with Pluronic-F127-COOH, as a first demonstration of functional NIR-emitting water dispersible ncSi-based nanoparticles.

Published

2016

47. Formation of Tethers from Spreading Cellular Aggregates.

Author

Beaune G, Winnik FM, and Brochard-Wyart F

Subjects

Cell Line, Tumor, Fibronectins chemistry, Glass chemistry, Humans, Male, Cell Adhesion physiology, Cell Movement physiology

Abstract

Membrane tubes are commonly extruded from cells and vesicles when a point-like force is applied on the membrane. We report here the unexpected formation of membrane tubes from lymph node cancer prostate (LNCaP) cell aggregates in the absence of external applied forces. The spreading of LNCaP aggregates deposited on adhesive glass substrates coated with fibronectin is very limited because cell-cell adhesion is stronger than cell-substrate adhesion. Some cells on the aggregate periphery are very motile and try to escape from the aggregate, leading to the formation of membrane tubes. Tethered networks and exchange of cargos between cells were observed as well. Growth of the tubes is followed by either tube retraction or tube rupture. Hence, even very cohesive cells are successful in escaping aggregates, which may lead to epithelial mesenchymal transition and tumor metastasis. We interpret the dynamics of formation and retraction of tubes in the framework of membrane mechanics.

Published

2015

48. Phosphorylcholine-modified chitosan films as effective promoters of cell aggregation: correlation between the films properties and cellular response.

Author

Qi B, Kujawa P, Toita S, Beaune G, and Winnik FM

Subjects

Chitosan chemistry, Human Umbilical Vein Endothelial Cells, Humans, MCF-7 Cells, Phosphorylcholine chemistry, Tissue Engineering, Cell Aggregation drug effects, Chitosan pharmacology, Phosphorylcholine pharmacology

Abstract

This study describes chitosan-phosphorylcholine (CH-PC) films able to support the formation of cell aggregates (spheroids), which are important for tissue engineering and pharmacological studies. The surface topography, charge, thickness, and rheology of CH-PC thin films were characterized by AFM, zeta-potential measurements, SPR spectroscopy, and QCM-D measurements. The CH-PC films are highly hydrated gels, independently of the level of PC incorporation (15-40 mol-% PC/glucosamine units). QCM-D studies established that the amount of fibrinogen adsorbed on CH-PC films decreased with increasing PC content. CH-PC surfaces underwent a transition from moderately cell-adhesive (CH-PC15) to non-adhesive (CH-PC40). Optical micrographs of HUVEC and MCF-7 cell lines cultured on CH-PC surfaces showed that they form spheroids on CH-PC25 and CH-PC40 films., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

49. How cells flow in the spreading of cellular aggregates.

Author

Beaune G, Stirbat TV, Khalifat N, Cochet-Escartin O, Garcia S, Gurchenkov VV, Murrell MP, Dufour S, Cuvelier D, and Brochard-Wyart F

Subjects

Acrylic Resins, Adhesives, Animals, Cadherins metabolism, Cell Line, Tumor, Disease Progression, Friction, Green Fluorescent Proteins metabolism, Lipid A analogs & derivatives, Luminescent Proteins metabolism, Mechanotransduction, Cellular physiology, Mice, Microscopy, Confocal methods, Sarcoma metabolism, Wetting Agents, Red Fluorescent Protein, Cell Adhesion physiology, Cell Communication physiology, Cell Movement physiology, Models, Biological, Sarcoma pathology

Abstract

Like liquid droplets, cellular aggregates, also called "living droplets," spread onto adhesive surfaces. When deposited onto fibronectin-coated glass or polyacrylamide gels, they adhere and spread by protruding a cellular monolayer (precursor film) that expands around the droplet. The dynamics of spreading results from a balance between the pulling forces exerted by the highly motile cells at the periphery of the film, and friction forces associated with two types of cellular flows: (i) permeation, corresponding to the entry of the cells from the aggregates into the film; and (ii) slippage as the film expands. We characterize these flow fields within a spreading aggregate by using fluorescent tracking of individual cells and particle imaging velocimetry of cell populations. We find that permeation is limited to a narrow ring of width ξ (approximately a few cells) at the edge of the aggregate and regulates the dynamics of spreading. Furthermore, we find that the subsequent spreading of the monolayer depends heavily on the substrate rigidity. On rigid substrates, the migration of the cells in the monolayer is similar to the flow of a viscous liquid. By contrast, as the substrate gets softer, the film under tension becomes unstable with nucleation and growth of holes, flows are irregular, and cohesion decreases. Our results demonstrate that the mechanical properties of the environment influence the balance of forces that modulate collective cell migration, and therefore have important implications for the spreading behavior of tissues in both early development and cancer.

Published

2014

50. Role of metal oxide nanoparticles in histopathological changes observed in the lung of welders.

Author

Andujar P, Simon-Deckers A, Galateau-Sallé F, Fayard B, Beaune G, Clin B, Billon-Galland MA, Durupthy O, Pairon JC, Doucet J, Boczkowski J, and Lanone S

Subjects

Aged, Cell Movement drug effects, Cytokines metabolism, Female, Fibroblasts drug effects, Humans, Immunohistochemistry, Inhalation Exposure, Lung metabolism, Macrophages drug effects, Male, Middle Aged, Occupational Exposure, Smoking adverse effects, Smoking pathology, Tissue Fixation, Lung pathology, Metal Nanoparticles toxicity, Occupational Diseases pathology, Oxides toxicity, Welding

Abstract

Background: Although major concerns exist regarding the potential consequences of human exposure to nanoparticles (NP), no human toxicological data is currently available. To address this issue, we took welders, who present various adverse respiratory outcomes, as a model population of occupational exposure to NP.The aim of this study was to evaluate if welding fume-issued NP could be responsible, at least partially, in the lung alterations observed in welders., Methods: A combination of imaging and material science techniques including ((scanning) transmission electron microscopy ((S)TEM), energy dispersive X-ray (EDX), and X-ray microfluorescence (μXRF)), was used to characterize NP content in lung tissue from 21 welders and 21 matched control patients. Representative NP were synthesized, and their effects on macrophage inflammatory secretome and migration were evaluated, together with the effect of this macrophage inflammatory secretome on human lung primary fibroblasts differentiation., Results: Welding-related NP (Fe, Mn, Cr oxides essentially) were identified in lung tissue sections from welders, in macrophages present in the alveolar lumen and in fibrous regions. In vitro macrophage exposure to representative NP (Fe2O3, Fe3O4, MnFe2O4 and CrOOH) induced the production of a pro-inflammatory secretome (increased production of CXCL-8, IL-1ß, TNF-α, CCL-2, -3, -4, and to a lesser extent IL-6, CCL-7 and -22), and all but Fe3O4 NP induce an increased migration of macrophages (Boyden chamber). There was no effect of NP-exposed macrophage secretome on human primary lung fibroblasts differentiation., Conclusions: Altogether, the data reported here strongly suggest that welding-related NP could be responsible, at least in part, for the pulmonary inflammation observed in welders. These results provide therefore the first evidence of a link between human exposure to NP and long-term pulmonary effects.

Published

2014