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1. Minimal factor XIII activity level to prevent major spontaneous bleeds

Author

Menegatti, M., Palla, R., Boscarino, M., Bucciarelli, P., Muszbek, L., Katona, E., Makris, M., Peyvandi, F., Halimeh, S., Lachmann, B., Bidlingmaier, C., Platokouki, H., Pergantou, H., Siboni, S.M., Schutgens, R.E.G., Borhany, M., Fatima, N., Mikovic, D., Saracevic, M., De Moerloose, P., Casini, A., Ozdemir, N., Ay, Y., Mumford, A., Harvey, A., Payne, J., Shapiro, A.D., Williamson, A., Chapin, J., and Hsu, F.

Published
2017
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2. Inhibitor development and mortality in non‐severe hemophilia A

Author

Eckhardt, C.L., Loomans, J.I., van Velzen, A.S., Peters, M., Mauser‐Bunschoten, E.P., Schwaab, R., Mazzucconi, M.G., Tagliaferri, A., Siegmund, B., Reitter‐Pfoertner, S.E., van der Bom, J.G., Fijnvandraat, K., Kamphuisen, P.W., Peerlinck, K., Oldenburg, J., Santagostino, E., Astermark, J., Eckhardt, C.L, van Velzen, A.S, Streefkerk, N., Loomans, J.L., van Eijkelenburg, A., Jansen, A.J., Kruijt, C.C., van Tienoven, B., van Baar, A.C.G., Corten, I.W., Meijer, K., Nijziel, M.R., Dors, N., Hamulyak, K., Beckers, E., Brons, P.P., Laros‐van Gorkom, B.A.P., van Heerde, W.L., Leebeek, F., Kruip, M., Cnossen, M.H., Mauser‐Bunschoten, E., Fischer, K., Smiers, F.J., Hermans, C., Klamroth, R., Escuriola‐Ettingshausen, C., Königs, C., Petrini, P., Holmström, M., Mäkipernaa, A., Male, C., Pabinger, I., Keenan, R.D., Liesner, R., Khair, K., Yee, T.T., Hart, D.P., Rangarajan, S., Mitchell, M., Thompson, G., Haya, S., Moret, A., Cid, A.R., Jimenez‐Yuste, V., Mancuso, M.E., Mazzuconni, M.G., Santoro, C., Morfini, M., Castaman, G., Schinco, P., Rivolta, G.F., Platokouki, H., and McRae, S.

Published
2015
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3. The factor VIII treatment history of non-severe hemophilia A

Author

Abdi, A., Kloosterman, F.R., Eckhardt, C.L., Male, C., Castaman, G., Fischer, K., Beckers, E.A.M., Kruip, M.J.H.A., Peerlinck, K., Mancuso, M.E., Santoro, C., Hay, C.R., Platokouki, H., Bom, J.G. van der, Gouw, S.C., Fijnvandraat, K., Hart, D.P., INSIGHT Study Grp, Interne Geneeskunde, MUMC+: MA Hematologie (9), RS: Carim - B01 Blood proteins & engineering, Graduate School, ACS - Pulmonary hypertension & thrombosis, Paediatric Haematology, ARD - Amsterdam Reproduction and Development, Landsteiner Laboratory, and Hematology

Subjects
Fviii activity, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, CHILDREN, 030204 cardiovascular system & hematology, Severe hemophilia A, Severity of Illness Index, Hemostatics, DEFINITIONS, 03 medical and health sciences, 0302 clinical medicine, Primary outcome, Interquartile range, Internal medicine, hemic and lymphatic diseases, Hemarthrosis, medicine, Humans, In patient, Treatment history, Treatment timing, RISK, MILD HEMOPHILIA, Factor VIII, joint bleed, treatment, business.industry, HAEMOSTASIS, Hematology, Original Articles, factor VIII, Cohort, INHIBITOR DEVELOPMENT, Original Article, hemophilia A, hemorrhage, business, IX
Abstract

BACKGROUND: In patients with non-severe hemophilia A, we lack detailed knowledge on the timing of treatment with factor VIII (FVIII) concentrates. This knowledge could provide information about the expected treatment timing in patients with severe hemophilia A treated with non-replacement therapies. OBJECTIVE: To assess the FVIII treatment history in patients with non-severe hemophilia A. METHODS: Patients with non-severe hemophilia (baseline FVIII activity [FVIII:C] 2-40 IU/dL) were included from the INSIGHT study. The primary outcome was median age at first FVIII exposure (ED1). In a subgroup of patients for whom more detailed information was available, we analyzed the secondary outcomes: median age at first 20 EDs, annualized bleeding rate for all bleeds (ABR), joint bleeds (AJBR), and major spontaneous bleeds (ASmBR). RESULTS: In the total cohort (n = 1013), median baseline FVIII activity was 8 IU/dL (interquartile range [IQR] 4-15) and the median age at ED1 was 3.7 years (IQR 1.4-7.7). Median age at ED1 rose from 2.5 years (IQR 1.2-5.7) in patients with FVIII:C 2-5 IU/dL to 9.7 years (IQR 4.8-16.0) in patients with FVIII:C 25-40 IU/dL. In the subgroup (n = 104), median age at ED1, ED5, ED10, and ED20 was 4.0 years (IQR 1.4-7.6), 5.6 years (IQR 2.9-9.3), 7.5 years (IQR 4.4-11.3), and 10.2 years (IQR 6.5-14.2), respectively. Median ABR, AJBR, and ASmBR were 1.1 (IQR 0.5-2.6), 0.3 (IQR 0.1-0.7), and 0 (IQR 0-0), respectively. CONCLUSION: This study demonstrates that in non-severe hemophilia A, the age at first FVIII exposure increases with baseline FVIII:C and that major spontaneous bleeds rarely occur. ispartof: JOURNAL OF THROMBOSIS AND HAEMOSTASIS vol:18 issue:12 pages:3203-3210 ispartof: location:England status: published

Published
2020

9. Coagulation factor activity and clinical bleeding severity in rare bleeding disorders: results from the European Network of Rare Bleeding Disorders

Author

PEYVANDI, F., PALLA, R., MENEGATTI, M., SIBONI, S. M., HALIMEH, S., FAESER, B., PERGANTOU, H., PLATOKOUKI, H., GIANGRANDE, P., PEERLINCK, K., CELKAN, T., OZDEMIR, N., BIDLINGMAIER, C., INGERSLEV, J., GIANSILY-BLAIZOT, M., SCHVED, J. F., GILMORE, R., GADISSEUR, A., BENEDIK-DOLNIČAR, M., KITANOVSKI, L., MIKOVIC, D., MUSALLAM, K. M., and ROSENDAAL, F. R.

Published
2012
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10. Desmopressin in moderate hemophilia A patients: a treatment worth considering

Author

Loomans, J.I., Kruip, M.J.H.A., Carcao, M., Jackson, S., Velzen, A.S. van, Peters, M., Santagostino, E., Platokouki, H., Beckers, E., Voorberg, J., Bom, J.G. van der, Fijnvandraat, K., RISE Consortium, Graduate School, ARD - Amsterdam Reproduction and Development, ACS - Amsterdam Cardiovascular Sciences, General Paediatrics, Paediatric Infectious Diseases / Rheumatology / Immunology, Other departments, ACS - Microcirculation, ACS - Pulmonary hypertension & thrombosis, Hematology, MUMC+: MA Hematologie (9), and RS: CARIM - R1.01 - Blood proteins & engineering

Subjects
Adult, medicine.medical_specialty, Adolescent, VONWILLEBRANDS-DISEASE, medicine.medical_treatment, VON-WILLEBRANDS DISEASE, 030204 cardiovascular system & hematology, Hemophilia A, Gastroenterology, Young Adult, 03 medical and health sciences, BLEEDING DISORDERS, 0302 clinical medicine, Predictive Value of Tests, hemic and lymphatic diseases, Internal medicine, von Willebrand Factor, medicine, Humans, Deamino Arginine Vasopressin, Young adult, Child, Desmopressin, INTRANASAL SPRAY, DDAVP, Factor VIII, FACTOR-VIII, TRANSPLANTATION, business.industry, Moderate hemophilia A, Hematology, Middle Aged, MILD, Prognosis, ENDOTHELIAL-CELLS, Transplantation, Treatment Outcome, Editorial, Nasal spray, Predictive value of tests, Mutation, Factor VIII level, business, NASAL SPRAY, hormones, hormone substitutes, and hormone antagonists, 030215 immunology, medicine.drug, Cohort study
Abstract

Desmopressin increases endogenous factor VIII levels in hemophilia A. Large inter-individual variation in the response to desmopressin is observed. Patients with a lower baseline factor VIII activity tend to show a reduced response, therefore, desmopressin is less frequently used in moderate hemophilia A patients (baseline factor VIII activity 1-5 international units/deciliter), even though factor VIII levels may rise substantially in some of them. We aim to describe the response to desmopressin in moderate hemophilia A patients and to identify predictors. We selected data on 169 patients with moderate hemophilia from the multicenter Response to DDAVP In non-severe hemophilia A patients: in Search for dEterminants (RISE) cohort study. Adequate response to desmopressin was defined as a peak factor VIII level ≥ 30, and excellent response as ≥ 50 international units/deciliter after desmopressin administration. We used univariate and multiple linear regression techniques to analyze predictors of the peak factor VIII level. Response was considered adequate in 68 patients (40%), of whom 25 showed excellent response (15%). Intravenous administration, age, pre-desmopressin factor VIII activity and von Willebrand factor antigen, peak von Willebrand factor activity and desmopressin-induced rise in von Willebrand factor antigen were significant predictors of peak factor VIII level and explained 65% of the inter-individual variation. In 40% of moderate hemophilia A patients, desmopressin response was adequate, thus it is important not to with-hold this group of patients from desmopressin responsiveness. Among the six predictors that we identified for desmopressin-induced factor VIII rise, factor VIII activity and desmopressin-induced rise in von Willebrand factor antigen had the strongest effect.

Published
2018
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11. The factor VIII treatment history of non-severe hemophilia A

Author

Abdi, A, Kloosterman, FR, Eckhardt, CL, Male, C, Castaman, G, Fischer, K, Beckers, EAM, Kruip, Marieke, Peerlinck, K, Mancuso, ME, Santoro, C, Hay, CRM, Platokouki, H, Bom, Josine, Gouw, SC, Fijnvandraat, K, Hart, DP, Abdi, A, Kloosterman, FR, Eckhardt, CL, Male, C, Castaman, G, Fischer, K, Beckers, EAM, Kruip, Marieke, Peerlinck, K, Mancuso, ME, Santoro, C, Hay, CRM, Platokouki, H, Bom, Josine, Gouw, SC, Fijnvandraat, K, and Hart, DP

Published
2020

12. Mode of delivery in hemophilia: vaginal delivery and Cesarean section carry similar risks for intracranial hemorrhages and other major bleeds

Author

Andersson, NG, Chalmers, EA, Kenet, G, Ljung, R, Makipernaa, A, Chambost, H, Roca, CA, Roman, MTA, Buhrlen, M, van den Berg, HM, Chalmers, E, Cid, AR, Claeyssens, S, Escuriola, C, Fischer, K, Van Geet, C, Kobelt, R, Konigs, C, Kurnik, K, Liesner, R, Molinari, A, Muntean, W, Nolan, B, Oldenburg, J, Garrido, RP, Platokouki, H, Rafowicz, A, Ranta, S, Santagostino, E, Mancuso, ME, Bonomi, AB, Mikkelsen, TS, Thomas, A, Williams, M, Carcao, M, Rivard, G, and PedNet Haemophilia Res Fdn

Abstract

The optimal mode of delivery for a pregnant hemophilia carrier is still a matter of debate. The aim of the study was to determine the incidence of intracranial hemorrhage and other major bleeds in neonates with moderate and severe hemophilia in relationship to mode of delivery and known family history. A total of 926 neonates, 786 with severe and 140 with moderate hemophilia were included in this PedNet multicenter study. Vaginal delivery was performed in 68.3% (n=633) and Cesarean section in 31.6% (n=293). Twenty intracranial hemorrhages (2.2%) and 44 other major bleeds (4.8%) occurred. Intracranial hemorrhages occurred in 2.4% of neonates following vaginal delivery compared to 1.7% after Cesarean section (P=not significant); other major bleeds occurred in 4.2% born by vaginal delivery and in 5.8% after Cesarean section (P=not significant). Further analysis of subgroups (n=813) identified vaginal delivery with instruments being a significant risk factor for both intracranial hemorrhages and major bleeds (Relative Risk: 4.78-7.39; P

Published
2019

16. Desmopressin in moderate hemophilia a patients: A treatment worth considering

Author

Loomans, J.I. (Janneke I.), Kruip, M.J.H.A. (Marieke), Carcao, M. (M.), Jackson, S. (Shannon), Velzen, A.S. (Alice) van, Peters, M.A.D. (Marjolein), Santagostino, E. (Elena), Platokouki, H. (Helen), Beckers, E.A.M. (Erik), Voorberg, J. (Jan), Bom, J.G. (Anske) van der, Fijnvandraat, K., Loomans, J.I. (Janneke I.), Kruip, M.J.H.A. (Marieke), Carcao, M. (M.), Jackson, S. (Shannon), Velzen, A.S. (Alice) van, Peters, M.A.D. (Marjolein), Santagostino, E. (Elena), Platokouki, H. (Helen), Beckers, E.A.M. (Erik), Voorberg, J. (Jan), Bom, J.G. (Anske) van der, and Fijnvandraat, K.

Abstract

Desmopressin increases endogenous factor VIII levels in hemophilia A. Large inter-individual variation in the response to desmopressin is observed. Patients with a lower baseline factor VIII activity tend to show a reduced response, therefore, desmopressin is less frequently used in moderate hemophilia A patients (baseline factor VIII activity 1-5 international units/deciliter), even though factor VIII levels may rise substantially in some of them. We aim to describe the response to desmopressin in moderate hemophilia A patients and to identify predictors. We selected data on 169 patients with moderate hemophilia from the multicenter Response to DDAVP In non-severe hemophilia A patients: in Search for dEterminants (RISE) cohort study. Adequate response to desmopressin was defined as a peak factor VIII level ≥ 30, and excellent response as ≥ 50 international units/deciliter after desmopressin administration. We used univariate and multiple linear regression techniques to analyze predictors of the peak factor VIII level. Response was considered adequate in 68 patients (40%), of whom 25 showed excellent response (15%). Intravenous administration, age, pre-desmopressin factor VIII activity and von Willebrand factor antigen, peak von Willebrand factor activity and desmopressin-induced rise in von Willebrand factor antigen were significant predictors of peak factor VIII level and explained 65% of the inter-individual variation. In 40% of moderate hemophilia A patients, desmopressin response was adequate, thus it is important not to withhold this group of patients from desmopressin responsiveness. Among the six predictors that we identified for desmopressin-induced factor VIII rise, factor VIII activity and desmopressin-induced rise in von Willebrand factor antigen had the strongest effect.

Published
2018
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18. Vaccinations are not associated with inhibitor development in boys with severe haemophilia A

Author

Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Datamanagement 1, Platokouki, H., Fischer, K., Gouw, S. C., Rafowicz, A., Carcao, M., Kenet, G., Liesner, R., Kurnik, K., Rivard, G. E., van den Berg, H. M., Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Datamanagement 1, Platokouki, H., Fischer, K., Gouw, S. C., Rafowicz, A., Carcao, M., Kenet, G., Liesner, R., Kurnik, K., Rivard, G. E., and van den Berg, H. M.

Published
2018

19. Desmopressin in moderate hemophilia A patients: a treatment worth considering

Author

Loomans, JI, Kruip, Marieke, Carcao, M, Jackson, S, van Velzen, AS, Peters, M, Santagostino, E, Platokouki, H, Beckers, E, Voorberg, J, van der Bom, JG, Fijnvandraat, K, Loomans, JI, Kruip, Marieke, Carcao, M, Jackson, S, van Velzen, AS, Peters, M, Santagostino, E, Platokouki, H, Beckers, E, Voorberg, J, van der Bom, JG, and Fijnvandraat, K

Published
2018

21. Factor VIII gene (F8) mutation and risk of inhibitor development in nonsevere hemophilia A

Author

Eckhardt, C.L., Velzen, A.S. van, Peters, M., Astermark, J., Brons, P.P., Castaman, G., Cnossen, M.H., Dors, N., Escuriola-Ettingshausen, C., Hamulyak, K., Hart, D.P., Hay, C.R.M., Haya, S., Heerde, W.L. van, Hermans, C., Holmstrom, M., Jimenez-Yuste, V., Keenan, R.D., Klamroth, R., Gorkom, B.A.P., Leebeek, F.W.G., Liesner, R., Makipernaa, A., Male, C., Mauser-Bunschoten, E., Mazzucconi, M.G., Mcrae, S., Meijer, K., Mitchell, M., Morfini, M., Nijziel, M., Oldenburg, J., Peerlinck, K., Petrini, P., Platokouki, H., Reitter-Pfoertner, S.E., Santagostino, E., Schinco, P., Smiers, F.J., Siegmund, B., Tagliaferri, A., Yee, T.T., Kamphuisen, P.W., Bom, J.G. van der, Fijnvandraat, K., INSIGHT Study Grp, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, UCL - (SLuc) Centre de malformations vasculaires congénitales, Cardiovascular Centre (CVC), Vascular Ageing Programme (VAP), RS: CARIM School for Cardiovascular Diseases, Biochemie, Interne Geneeskunde, Pediatrics, Hematology, Epidemiology, Other departments, Paediatric Infectious Diseases / Rheumatology / Immunology, ACS - Amsterdam Cardiovascular Sciences, and AII - Amsterdam institute for Infection and Immunity

Subjects
Invasive mycoses and compromised host Translational research [N4i 2], Adult, medicine.medical_specialty, Age-related aspects of cancer [ONCOL 2], Time Factors, Adolescent, Genotype, Immunology, Mutation, Missense, Kaplan-Meier Estimate, Hemophilia A, DIAGNOSIS, Biochemistry, Gastroenterology, Young Adult, Interquartile range, Risk Factors, Internal medicine, medicine, Missense mutation, Humans, Cumulative incidence, Desmopressin, Genotyping, POLYMORPHISMS, Retrospective Studies, Hematology, Factor VIII, Cardiovascular diseases [NCEBP 14], business.industry, Incidence (epidemiology), DESMOPRESSIN, Cell Biology, Middle Aged, MILD, Antibodies, Neutralizing, Confidence interval, Treatment Outcome, business, medicine.drug, Follow-Up Studies
Abstract

Neutralizing antibodies (inhibitors) toward factor VIII form a severe complication in nonsevere hemophilia A, profoundly aggravating the bleeding pattern. Identification of high-risk patients is hampered by lack of data that take exposure days to therapeutic factor VIII concentrates into account. In the INSIGHT study, we analyzed the association between F8 mutation and inhibitor development in patients with nonsevere hemophilia A (factor VIII 2-40 IU/dL). This analysis included 1112 non-severe hemophilia A patients from 14 centers in Europe and Australia that had genotyped at least 70% of their patients. Inhibitor risk was calculated as Kaplan-Meier incidence with cumulative number of exposure days as the time variable. During 44 800 exposure days (median, 24 exposure days per patient; interquartile range [IQR], 7-90), 59 of the 1112 patients developed an inhibitor; cumulative incidence of 5.3% (95% confidence interval [CI], 4.0-6.6) after a median of 28 exposure days (IQR, 12-71). The inhibitor risk at 50 exposure days was 6.7% (95% CI, 4.5-8.9) and at 100 exposure days the risk further increased to 13.3% (95% CI, 9.6-17.0). Among a total of 214 different F8 missense mutations 19 were associated with inhibitor development. These results emphasize the importance of F8 genotyping in nonsevere hemophilia A. ( Blood . 2013; 122(11):1954-1962) © 2013 by The American Society of Hematology.

Published
2013
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22. MYH9-Related Disease: A Novel Prognostic Model to Predict the Clinical Evolution of the Disease Based on Genotype-Phenotype Correlations

Author

Pecci, A, Klersy, C, Gresele, P, Lee, K, De Rocco, D, Bozzi, V, Russo, G, Heller, Pg, Loffredo, G, Ballmaier, M, Fabris, F, Beggiato, E, Kahr, Wha, Pujol-Moix, N, Platokouki, H, Matthijs, G, Noris, P, Yerram, P, Hermans, C, Batzios, S, De Groot, M, Zieger, B, De Candia, E, Fraticelli, V, Kersseboom, R, Piccoli, Gb, Zimmermann, S, Zaninetti, C, Nicchia, E, Baronci, C, Seri, M, Knight, Pj, Balduini, Cl, Savoia, A, Van Geet, C, Geber, B, Economou, M, Fierro, T, Glembotsky, Ac, Vianello, F, Guthner, C., Pecci, A, Klersy, C, Gresele, P, Lee, Kj, De Rocco, D, Bozzi, V, Russo, G, Heller, Pg, Loffredo, G, Ballmaier, M, Fabris, F, Beggiato, E, Kahr, Wh, Pujol-Moix, N, Platokouki, H, Van Geet, C, Noris, P, Yerram, P, Hermans, C, Gerber, B, Economou, M, De Groot, M, Zieger, B, De Candia, E, Fraticelli, V, Kersseboom, R, Piccoli, Gb, Zimmermann, S, Fierro, T, Glembotsky, Ac, Vianello, F, Zaninetti, C, Nicchia, E, Güthner, C, Baronci, C, Seri, M, Knight, Pj, Balduini, Cl, Savoia, A., DE ROCCO, Daniela, Pujol Moix, N, Nicchia, Elena, Savoia, Anna, and University of Zurich

Subjects
Male, Oncology, thrombocytopenia, Medicina Clínica, Disease, Malattia MYH9 associata, Myh9 related disease, MYH9 RELATED DISEASE, Myh9, MYH9, Risk Factors, purl.org/becyt/ford/3.2 [https], Genotype, Genetics(clinical), CRYSTAL-STRUCTURE, Age of Onset, IIA, Genetics (clinical), deafne, MYOSIN HEAVY-CHAIN, EPSTEIN-SYNDROME, Molecular Motor Proteins, FECHTNER SYNDROMES, Trombocitopenia, Penetrance, POWER STROKE STATE, Phenotype, Italy, nephropathy, Female, purl.org/becyt/ford/3 [https], Miosina No Muscular Iia, Adult, 2716 Genetics (clinical), medicine.medical_specialty, CIENCIAS MÉDICAS Y DE LA SALUD, MOTOR DOMAIN, Hearing Loss, Sensorineural, Genetic counseling, 610 Medicine & health, Biology, nonmuscle myosin, Article, Cataract, Nephropathy, 1311 Genetics, Internal medicine, deafness, Genetics, medicine, Humans, Hematología, Gene, Genetic Association Studies, Hereditaria, Myosin Heavy Chains, MUTATIONS, Settore MED/09 - MEDICINA INTERNA, medicine.disease, Amino Acid Substitution, Epstein Syndrome, Mutation, 10032 Clinic for Oncology and Hematology, Linear Models, SMOOTH-MUSCLE MYOSIN
Abstract

MYH9-related disease (MYH9-RD) is a rare autosomal-dominant disorder caused by mutations in the gene for nonmuscle myosin heavy chain IIA (NMMHC-IIA). MYH9-RD is characterized by a considerable variability in clinical evolution: patients present at birth with only thrombocytopenia, but some of them subsequently develop sensorineural deafness, cataract, and/or nephropathy often leading to end-stage renal disease (ESRD). We searched for genotype–phenotype correlations in the largest series of consecutive MYH9-RD patients collected so far (255 cases from 121 families). Association of genotypes with noncongenital features was assessed by a generalized linear regression model. The analysis defined disease evolution associated to seven different MYH9 genotypes that are responsible for 85% of MYH9-RD cases. Mutations hitting residue R702 demonstrated a complete penetrance for early-onset ESRD and deafness. The p.D1424H substitution associated with high risk of developing all the noncongenital manifestations of disease. Mutations hitting a distinct hydrophobic seam in the NMMHC-IIA head domain or substitutions at R1165 associated with high risk of deafness but low risk of nephropathy or cataract. Patients with p.E1841K, p.D1424N, and C-terminal deletions had low risk of noncongenital defects. These findings are essential to patients' clinical management and genetic counseling and are discussed in view of molecular pathogenesis of MYH9-RD. Fil: Pecci, Alessandro. University of Pavia; Italia Fil: Klersy, Catherine. IRCCS Policlinico San Matteo Foundation; Italia Fil: Gresele, Paolo. Università di Perugia; Italia Fil: Lee, Kieran J. D.. University of Leeds; Reino Unido Fil: De Rocco, Daniela. Università degli Studi di Trieste; Italia Fil: Bozzi, Valeria. University of Pavia; Italia Fil: Russo, Giovanna. University of Catania; Italia Fil: Heller, Paula Graciela. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto de Investigaciones Médicas. Universidad de Buenos Aires. Facultad de Medicina. Instituto de Investigaciones Médicas; Argentina Fil: Loffredo, Giuseppe. Pausilipon Hospital. Department of Oncology; Italia Fil: Ballmaier, Matthias. Hannover Medical School; Alemania Fil: Fabris, Fabrizio. Università di Padova; Italia Fil: Beggiato, Eloise. Hospital “Città della Salute e Della Scienza”; Italia Fil: Kahr, Walter H. A.. University of Toronto; Canadá. Hospital for Sick Children. Division of Hematology/Oncology; Canadá Fil: Pujol Moix, Nuria. Universitat Autònoma de Barcelona; España Fil: Platokouki, Helen. “Aghia Sophia” Children's Hospital; Grecia Fil: Van Geet, Christel. University of Leuven. Center for Molecular and Vascular Biology; Bélgica Fil: Noris, Patrizia. University of Pavia; Italia Fil: Yerram, Preethi. University of Missouri; Estados Unidos Fil: Hermans, Cedric. St-Luc University Hospital; Bélgica Fil: Gerber, Bernhard. University Hospital Zurich, Division of Hematology; Suiza Fil: Economou, Marina. Aristotle University; Grecia Fil: De Groot, Marco. University of Groningen; Países Bajos Fil: Zieger, Barbara. University Medical Center Freiburg; Alemania Fil: De Candia, Erica. Catholic University of Rome; Italia Fil: Fraticelli, Vincenzo. Giovanni Paolo II Foundation; Italia Fil: Kersseboom, Rogier. Erasmus Medical Centre; Países Bajos Fil: Piccoli, Giorgina B.. Università di Torino; Italia Fil: Zimmermann, Stefanie. Goethe Universitat Frankfurt; Alemania Fil: Fierro, Tiziana. Università di Perugia; Italia Fil: Glembotsky, Ana Claudia. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto de Investigaciones Médicas. Universidad de Buenos Aires. Facultad de Medicina. Instituto de Investigaciones Médicas; Argentina Fil: Vianello, Fabrizio. Università di Padova; Italia Fil: Zaninetti, Carlo. University of Pavia; Italia Fil: Nicchia, Elena. Università degli Studi di Trieste; Italia Fil: Güthner, Christiane. Stadtspital Triemli. Department of Medical Oncology and Hematology; Italia Fil: Baronci, Carlo. Pediatric Hospital "Bambino Gesù"; Italia Fil: Seri, Marco. Università di Bologna; Italia Fil: Knight, Peter J.. University of Leeds; Reino Unido Fil: Balduini, Carlo L.. University of Pavia; Italia Fil: Savoia, Anna. Università degli Studi di Trieste; Italia

Published
2014

25. Intensity of factor VIII treatment and inhibitor development in children with severe hemophilia A: the RODIN study

Author

Gouw, S.C., Berg, H.M. van den, Fischer, K., Auerswald, G., Carcao, M., Chalmers, E., Chambost, H., Kurnik, K., Liesner, R., Petrini, P., Platokouki, H., Altisent, C., Oldenburg, J., Nolan, B., Garrido, R.P., Mancuso, M.E., Rafowicz, A., Williams, M., Clausen, N., Middelburg, R.A., Ljung, R., Bom, J.G. van der, PedNet, Res Determinants INhibitor Dev, AII - Amsterdam institute for Infection and Immunity, and Paediatric Infectious Diseases / Rheumatology / Immunology

Subjects
Adult, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Immunology, Hemorrhage, Hemophilia A, Biochemistry, Gastroenterology, Chemoprevention, Severity of Illness Index, Cohort Studies, Young Adult, Risk Factors, Internal medicine, hemic and lymphatic diseases, Severity of illness, medicine, Humans, Young adult, Child, Hematology, Factor VIII, Blood Coagulation Factor Inhibitors, Dose-Response Relationship, Drug, business.industry, Incidence (epidemiology), Hazard ratio, Cell Biology, Confidence interval, Surgery, Dose–response relationship, business, Cohort study
Abstract

The objective of this study was to examine the association of the intensity of treatment, ranging from high-dose intensive factor VIII (FVIII) treatment to prophylactic treatment, with the inhibitor incidence among previously untreated patients with severe hemophilia A. This cohort study aimed to include consecutive patients with a FVIII activity < 0.01 IU/mL, born between 2000 and 2010, and observed during their first 75 FVIII exposure days. Intensive FVIII treatment of hemorrhages or surgery at the start of treatment was associated with an increased inhibitor risk (adjusted hazard ratio [aHR], 2.0; 95% confidence interval [CI], 1.3-3.0). High-dose FVIII treatment was associated with a higher inhibitor risk than low-dose FVIII treatment (aHR, 2.3; 95% CI, 1.0-4.8). Prophylaxis was only associated with a decreased overall inhibitor incidence after 20 exposure days of FVIII. The association with prophylaxis was more pronounced in patients with low-risk F8 genotypes than in patients with high-risk F8 genotypes (aHR, 0.61, 95% CI, 0.19-2.0 and aHR, 0.85, 95% CI, 0.51-1.4, respectively). In conclusion, our findings suggest that in previously untreated patients with severe hemophilia A, high-dosed intensive FVIII treatment increases inhibitor risk and prophylactic FVIII treatment decreases inhibitor risk, especially in patients with low-risk F8 mutations.

Published
2013

27. Continuous infusion of recombinant factor VIII formulated with sucrose in surgery: non-interventional, observational study in patients with severe haemophilia A

Author

Poli Van Creveldkliniek Medisch, Circulatory Health, Meijer, K, Rauchensteiner, S, Santagostino, E, Platokouki, H, Schutgens, R E G, Brunn, M, Tueckmantel, C, Valeri, F, Schinco, P C, Poli Van Creveldkliniek Medisch, Circulatory Health, Meijer, K, Rauchensteiner, S, Santagostino, E, Platokouki, H, Schutgens, R E G, Brunn, M, Tueckmantel, C, Valeri, F, and Schinco, P C

Published
2015

28. Assessment of the progression of haemophilic arthropathy in children

Author

Pergantou, H. Platokouki, H. Matsinos, G. Papakonstantinou, O. Papadopoulos, A. Xafaki, P. Petratos, D. Aronis, S.

Abstract

Arthropathy is considered as an irreversible and progressive complication in patients with haemophilia, even in children on prophylaxis. To estimate the progression of haemophilic arthropathy, 85 joints of 24 boys with severe (n = 18) and moderate (n = 6) haemophilia (A: 22, B: 2) were investigated with clinical examination, X-rays and magnetic resonance imaging (MRI) at two time periods (time 0 and 1). Patients' age at time 0 was 10.5 ± 3.6 years and time elapsed to time 1 was 3.8 ± 1.4 years. At time 0: all investigated joints had more than three bleeds. Sixteen boys were on secondary prophylaxis for 5.4 ± 2.8 years. Clinical score (a modification of World Federation of Haemophilia's scale): 2.0 ± 3.6, X-ray score (Pettersson): 2.1 ± 2.8, MRI score (Denver): 4.5 ± 3.8. After the first evaluation, prophylaxis was intensified in 11 children and initiated in four. At time 1: clinical score: 1.5 ± 3.1, X-ray: 1.7 ± 2.7, MRI score: 5.1 ± 4.1. On average, the clinical and X-ray scores showed a significant improvement (26% and 40% of the joints respectively, P < 0.01) and the number of haemarthroses evidenced a threefold reduction from time 0 to 1 (P < 0.01), findings that could be associated with the modification of prophylaxis after time 0. MRI findings showed deterioration in 34% of the joints. Conversely, 14 joints (16.5%) with mild or moderate synovitis without cartilage degradation at time 0 showed an improvement at time 1. The information carried by the three scales could be divided into information shared by the three scores and information specific to each score, thus giving a more complete picture of joint damage caused by bleedings. © 2009 Blackwell Publishing Ltd.

Published
2010

29. Assessment of bone mineral density and markers of bone turnover in children under long-term oral anticoagulant therapy

Author

Avgeri, M. Papadopoulou, A. Platokouki, H. Douros, K. Rammos, S. Nicolaidou, P. Aronis, S.

Subjects
musculoskeletal diseases
Abstract

Oral anticoagulants antagonize vitamin K action and potentially impair the carboxylation of osteocalcin, a protein essential for normal bone matrix formation. In the present study, bone mineral density (BMD) and bone turnover markers were evaluated in 23 children under long-term oral anticoagulant therapy. BMD of the lumbar spine was assessed (Dual Energy x-ray Absorptiometry) and reported as z score. Osteoblast [bone alkaline phosphatase, osteocalcin (Gla-Oc), amino-terminal procollagen 1 extension peptide] and osteoclast (urinary calcium and deoxypyridinoline, serum cross-linked C telopeptide) activity markers were measured. Vitamin D ([25(OH) D], parathormone, calcium, phosphorus, magnesium) and vitamin K status [factors II, VII, IX, X, protein C, protein S, undercarboxylated osteocalcin (Glu-Oc)] were determined. The above parameters were also evaluated in 25 healthy controls. Patients presented with higher levels in Glu-Oc, parathormone, and bone resorption markers, lower levels in bone formation markers and 25(OH) D, whereas 52% of them showed signs of osteopenia (-1> BMD z score > -2.5). Statistical analysis demonstrated that anticoagulant therapy was an independent predictor of alterations in Glu-Oc, Gla-Oc, bone alkaline phosphatase, amino-terminal procollagen 1 extension peptide, and serum cross-linked C telopeptide levels. It seems that long-term use of coumarin derivatives may cause osteopenia in children with the risk of developing osteoporosis later in life. © 2008 by Lippincott Williams & Wilkins.

Published
2008

30. Mutations and polymorphisms in genes affecting haemostasis components in children with thromboembolic events

Author

Komitopoulou, A. Platokouki, H. Kapsimali, Z. Moschovi, M. and Kattamis, A. Pergantou, H. Aronis, S.

Abstract

The distribution of mutations/polymorphisms in genes affecting haemostasis [factor V Leiden (FVL), FV H1298R (FVR2), FII 20210A, b-Fib 455G -> A, FXIII V34L, PAI-1 4G, HPA-1b] among 141 children with thrombosis at various sites and 103 controls was compared. Additionally, the carriage of these mutations/polymorphisms was associated with the levels of their corresponding proteins in thrombosed children. Thrombosis was more frequent in boys (p = 0.021). No studied mutation/polymorphism was found to be a risk factor for thrombosis, except for FVL (odds ratio 3.8, 95% CI 1.4-10.6). The risk of thrombosis for FVL carriers was twice as high in children with an idiopathic thrombosis (odds ratio 5.4) than in thrombosed children with an underlying disease or a triggering event (odds ratio 2.7). FVL carriers had an odds ratio of 5.9 (95% CI 1.8-19.6) when FVR2 was absent. In thrombosed children, the activated protein C resistance ratio was significantly lower in the presence of FVL ( p < 0.001). Prothrombin and fibrinogen levels, although higher in FII 20210A and b-Fib 455G -> A carriers, did not reach statistical significance. Copyright (c) 2006 S. Karger AG, Basel.

Published
2006

31. Rituximab in the treatment of high responding inhibitors in severe haemophilia A

Author

Moschovi, M Aronis, S Trimis, G Platokouki, H Salavoura, K Tzortzatou-Stathopoulou, F

Abstract

The development of antibodies to factor VIII (FVIII) in severely affected haemophilia A patients is a serious complication associated with increased morbidity and mortality. Bypassing agents are used to treat acute bleeding episodes; however, elimination of the inhibitors can only be achieved with immune tolerance therapy (ITT) in 60-80% of cases. High responding (HR) inhibitors are more likely to respond to ITT if the titre is decreased to < 5 BU over time or in selected cases after the administration of immunosuppressive drugs, plasmapheresis or immunoabsorption, techniques difficult to apply in children. Anti-CD20 (rituximab), a monoclonal antibody, was given as an alternative treatment in two haemophilic children with HR inhibitors and impaired quality of life, due to recurrent haemarthrosis. Rituximab was given at the dose of 375 mg m(-2), once weekly for four consecutive weeks. Both patients showed a partial response to rituximab reducing the inhibitor titre to < 5 BU, thus facilitating ITT initiation; however, only the older patient eradicated the inhibitor within 21 days after application of ITT. The second patient, despite depletion of B cells, did not respond to ITT. No long-term side effects have been observed in both patients for a follow-up period of 20 and 18 months respectively. In conclusion, rituximab appears to be an alternative effective therapy to rapidly reduce or eliminate the inhibitor in selected cases of severely affected haemophiliacs before further proceeding to ITT. However, the dose and appropriate schedule, as well as long-term side effects need further investigation.

Published
2006

32. Clinical remission following monoclonal anti-CD20 therapy in two children with chronic refractory idiopathic thrombocytopenic purpura

Author

Moschovi, M Trimis, G Pergantou, H Platokouki, H and Vrachnou, E Tzortzatou-Stathopoulou, F

Abstract

Two patients, a 4-year-old boy and a 6-year-old girl who had a 2-year and a 3-year history of idiopathic thrombocytopenic purpura, respectively, were referred to our Department. Both patients had frequent haemorrhagic events. They received i.v. immunoglobulin, corticosteroids, cyclosporine, interferon alpha-2b and azathioprine, but no clinical remission was established. The girl also underwent splenectomy. Anti-CD20 antibody was administered to both patients at a dose of 375 mg/m(2) once weekly for 4 weeks. No side-effects were detected. During the 18-month follow-up period the patients received no other drug and remained in clinical remission. The B lymphocytes remained undetectable in peripheral blood for 3 months and they progressively increased during the following 4 months. Rituximab is a novel, quite effective, safe treatment of chronic refractory idiopathic thrombocytopenic purpura in childhood. More studies and follow up of patients for longer periods are necessary.

Published
2005

34. Factor VIII gene (F8) mutation and risk of inhibitor development in nonsevere hemophilia A

Author

Eckhardt, CL, van Velzen, AS, Peters, M, Astermark, J, Brons, PP, Castaman, G, Cnossen, Marjon, Dors, N, Escuriola-Ettingshausen, C, Hamulyak, K, Hart, DP, Hay, CRM, Haya, S, van Heerde, WL, Hermans, C, Holmstrom, M, Jimenez-Yuste, V, Keenan, RD, Klamroth, R, Laros-Van Gorkom, BAP, Leebeek, Frank, Liesner, R, Makipernaa, A, Male, C, Mauser-Bunschoten, E, Mazzucconi, MG, Mcrae, S, Meyer, K, Mitchell, M, Morfini, M, Nijziel, M, Oldenburg, J, Peerlinck, K, Petrini, P, Platokouki, H, Reitter-Pfoertner, SE, Santagostino, E, Schinco, P, Smiers, FJ, Siegmund, B, Tagliaferri, A, Yee, TT, Kamphuisen, PW, van der Bom, JG (Anske), Fijnvandraat, K, Eckhardt, CL, van Velzen, AS, Peters, M, Astermark, J, Brons, PP, Castaman, G, Cnossen, Marjon, Dors, N, Escuriola-Ettingshausen, C, Hamulyak, K, Hart, DP, Hay, CRM, Haya, S, van Heerde, WL, Hermans, C, Holmstrom, M, Jimenez-Yuste, V, Keenan, RD, Klamroth, R, Laros-Van Gorkom, BAP, Leebeek, Frank, Liesner, R, Makipernaa, A, Male, C, Mauser-Bunschoten, E, Mazzucconi, MG, Mcrae, S, Meyer, K, Mitchell, M, Morfini, M, Nijziel, M, Oldenburg, J, Peerlinck, K, Petrini, P, Platokouki, H, Reitter-Pfoertner, SE, Santagostino, E, Schinco, P, Smiers, FJ, Siegmund, B, Tagliaferri, A, Yee, TT, Kamphuisen, PW, van der Bom, JG (Anske), and Fijnvandraat, K

Published
2013

35. Diffuse splenic and visceral hemangiomas complicated by chronic consumption coagulopathy

Author

Platokouki, H. Aronis, S. Mitsika, A. Keramidas, D. Harokopos, E.

Abstract

The case of a 7-year-old girl with a 2 year history of easy bruising associated with thrombocytopenia is reported. On admission she presented with ecchymoses, abdominal distention and splenomegaly. Hemostasis investigation revealed a consumption coagulopathy. Several radiological studies failed to confirm the diagnosis of diffuse splenic and visceral hemangiomatosis, which was eventually estasblished by an explorative laparotomy. Platelet count and the other coagulation abnormalities progressively returned to normal after splenectomy, although the remaining hemangiomas were extensive. © 1998 Wiley. All rights reserved.

Published
1998

36. Correlation between phenotype and genotype in a large unselected cohort of children with severe hemophilia A

Author

Carcao, Manuel D., primary, van den Berg, H. Marijke, additional, Ljung, Rolf, additional, Mancuso, Maria Elisa, additional, Altisent, C, additional, Auerswald, G, additional, Chalmers, E, additional, Chambost, H, additional, Cid, A, additional, Claeyssens, S, additional, Clausen, N, additional, Fischer, K, additional, Kliniek, Van Creveld, additional, van Geet, Ch, additional, Peerlinck, K, additional, Kobelt, R, additional, Kreuz, W, additional, Escuriola, C, additional, Kurnik, K, additional, Liesner, R, additional, Ljung, R, additional, Mäkipernaa, A, additional, Molinari, A, additional, Muntean, W, additional, Oldenburg, J, additional, Garrido, R Pérez, additional, Petrini, P, additional, Platokouki, H, additional, Rafowicz, A, additional, Santagostino, E, additional, Mancuso, ME, additional, Thomas, A, additional, Williams, M, additional, Gouw, SC, additional, van den Berg, HM, additional, Kenet, G, additional, Carcao, M, additional, and Rivard, G, additional

Published
2013
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38. 17 YEARS OF EXPERIENCE WITH CHRONIC IDIOPATHIC THROMBOCYTOPENIC PURPURA IN CHILDHOOD - IS THERAPY ALWAYS BETTER

Author

ARONIS, S PLATOKOUKI, H MITSIKA, A HAIDAS, S and CONSTANTOPOULOS, A

Subjects
hemic and lymphatic diseases
Abstract

Between 1975 and 1992 450 children with idiopathic thrombocytopenic purpura (ITP) were diagnosed, and of those 100 (22%) developed the chronic form of the disease. Approximately half the patients with chronic ITP presented with mild to moderate hemorrhagic manifestations at the onset of purpura (30 cases) and/or later during the course of the disease (25 cases). The incidence of intracranial hemorrhage was 1%, and the mortality rate due to overwhelming septicemia after splenectomy was also 1%. Overall one-third of the patients received no therapy; two-thirds of them went into spontaneous remission within 8 months to 8 years from the onset of ITP. Steroids given in conventional or high doses (51 cases) achieved a transient (if any) rise in platelet count, but in no case were steriods curative. Remission related to intravenous immune globulin (IVIG) therapy was noticed in 38.5% of the children (10 of 26) after variable courses. The response rate to splenectomy was 95.0%. Ultimately the long-term outcome in children with chronic ITP was as follows: remission, 58 cases (spontaneous, 30; after IVIG therapy, 10; after splenectomy, 18); hemostatic platelet values, 22 cases (spontaneous, 16; after IVIG, 5; after splenectomy, 1). Thirteen children were lost in follow-up, and 7 remain thrombocytopenic but asymptomatic. These data indicate that chronic ITP in childhood runs a benign course in most cases and may remit with or without therapy even several years from onset. Therefore, therapeutic intervention has to be individualized, and splenectomy, which is not always safe, should be reserved for problematic cases that fail to respond to conventional therapeutic modalities.

Published
1994

39. EUROPEAN THROMBOSIS REGISTRY. THE ATHEN'S EXPERIENCE

Author

Aronis, S, primary, Mantziou, Th, additional, Platokouki, H, additional, Karabelas, B, additional, Kapsimali, Z, additional, Adamtziki, E, additional, Kovanis, A, additional, Skardoutsou, A, additional, and Costantopoulos, A, additional

Published
1999
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42. Central Nervous System (CNS) Thrombosis

Author

Mantziou, Th, primary, Platokouki, H, additional, Karabelas, B, additional, Kapsimali, Z, additional, Adamtziki, E, additional, Covanis, A, additional, Skardoutsou, A, additional, Constantopoulos, A, additional, and Aronis, S, additional

Published
1999
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46. THROMBOTIC RISK IN VLBW NEONATES

Author

Aronis, S., Lipsou, N., Kapsimali, Z., Platokouki, H., Liossis, G., Fotopoulos, S., and Xanthou, M.

Published
2001

47. MYH9-related disease: Five novel mutations expanding the spectrum of causative mutations and confirming genotype/phenotype correlations

Author

Daniela De Rocco, Alessandro Pecci, Helen Pergantou, Annalisa Pastore, Barbara Zieger, Patrizia Noris, Roberta Bottega, Anna Savoia, Helen Platokouki, Paula G. Heller, Serena Barozzi, Ana C. Glembotsky, Carlo L. Balduini, DE ROCCO, Daniela, Zieger, B., Platokouki, H., Heller, P. G., Pastore, A., Bottega, Roberta, Noris, P., Barozzi, S., Glembotsky, A. C., Pergantou, H., Balduini, C. L., Savoia, Anna, Pecci, A., De Rocco, D., Bottega, R., Glembotsky, A., Balduini, C., and Savoia, A.

Subjects
Male, Models, Molecular, Genotype-phenotype correlation, Protein Conformation, Medicina Clínica, MYH9-related disease, Malattia MYH9 associata, medicine.disease_cause, Inclusion bodies, MYH9 related disease, Mutational screening, Exon, purl.org/becyt/ford/3.2 [https], Myosin, Missense mutation, Child, Genetics (clinical), Genes, Dominant, Genetics, Mutation, Genotype–phenotype correlation, Molecular Motor Proteins, Exons, Syndrome, General Medicine, Middle Aged, Phenotype, Pedigree, In frame deletion/duplication, Child, Preschool, Female, purl.org/becyt/ford/3 [https], Adult, CIENCIAS MÉDICAS Y DE LA SALUD, Adolescent, Molecular Sequence Data, MYH9 gene, Settore BIO/11 - Biologia Molecolare, Biology, Nephropathy, Young Adult, Clinical Research, in frame deletions/insertions, medicine, Humans, Hematología, Amino Acid Sequence, Gene, Genetic Association Studies, Base Sequence, Myosin Heavy Chains, medicine.disease, Thrombocytopenia, Molecular biology, Amino Acid Substitution, Sequence Alignment
Abstract

MYH9-related disease (MYH9-RD) is a rare autosomal dominant syndromic disorder caused by mutations in MYH9, the gene encoding for the heavy chain of non-muscle myosin IIA (myosin-9). MYH9-RD is characterized by congenital macrothrombocytopenia and typical inclusion bodies in neutrophils associated with a variable risk of developing sensorineural deafness, presenile cataract, and/or progressive nephropathy. The spectrum of mutations responsible for MYH9-RD is limited. We report five families, each with a novel MYH9 mutation. Two mutations, p.Val34Gly and p.Arg702Ser, affect the motor domain of myosin-9, whereas the other three, p.Met847_Glu853dup, p.Lys1048_Glu1054del, and p.Asp1447Tyr, hit the coiled-coil tail domain of the protein. The motor domain mutations were associated with more severe clinical phenotypes than those in the tail domain. Fil: de Rocco, Daniela. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia Fil: Zieger, Barbara. University of Freiburg; Alemania Fil: Platokouki, Helen. “Aghia Sophia” Children; Grecia Fil: Heller, Paula Graciela. Consejo Nacional de Investigaciones Cientificas y Tecnicas. Oficina de Coordinacion Administrativa Houssay. Instituto de Investigaciones Medicas; Argentina. Universidad de Buenos Aires. Facultad de Medicina. Instituto de Investigaciones Médicas; Argentina Fil: Pastore, Annalisa. National Institute for Medical Research; Reino Unido Fil: Bottega, Roberta. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia Fil: Noris, Patrizia. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia. University of Pavia; Italia Fil: Barozzi, Serena. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia. University of Pavia; Italia Fil: Glembotsky, Ana Claudia. Universidad de Buenos Aires. Facultad de Medicina. Instituto de Investigaciones Médicas; Argentina. Consejo Nacional de Investigaciones Cientificas y Tecnicas. Oficina de Coordinacion Administrativa Houssay. Instituto de Investigaciones Medicas; Argentina Fil: Pergantou, Helen. “Aghia Sophia” Children; Grecia Fil: Balduini, Carlo L.. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia. University of Pavia; Italia Fil: Savoia, Anna. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia. Universita Degli Studi Di Trieste; Italia Fil: Pecci, Alessandro. Istituto di Ricovero e Cura a Carattere Scientifico "Burlo Garofolo"; Italia. University of Pavia; Italia

Published
2013

48. Congenital fibrinogen disorders: a retrospective clinical and genetic analysis of the Prospective Rare Bleeding Disorders Database.

Author

Mohsenian S, Palla R, Menegatti M, Cairo A, Lecchi A, Casini A, Neerman-Arbez M, Asselta R, Scardo S, Siboni SM, Blatny J, Zapletal O, Schved JF, Giansily-Blaizot M, Halimeh S, Daoud MA, Platokouki H, Pergantou H, Schutgens REG, Van Haaften-Spoor M, Brons P, Laros-van Gorkom B, Van Pinxten E, Borhany M, Fatima N, Mikovic D, Saracevic M, Özdemir GN, Ay Y, Makris M, Lockley C, Mumford A, Harvey A, Austin S, Shapiro A, Williamson A, McGuinn C, Goldberg I, De Moerloose P, and Peyvandi F

Subjects
Humans, Female, Fibrinogen genetics, Prospective Studies, Retrospective Studies, Hemorrhage genetics, Afibrinogenemia epidemiology, Afibrinogenemia genetics, Afibrinogenemia complications, Hemostatics
Abstract

Abstract: Congenital fibrinogen deficiency (CFD) is a rare bleeding disorder caused by mutations in FGA, FGB, and FGG. We sought to comprehensively characterize patients with CFD using PRO-RBDD (Prospective Rare Bleeding Disorders Database). Clinical phenotypes, laboratory, and genetic features were investigated using retrospective data from the PRO-RBDD. Patients were classified from asymptomatic to grade 3 based on their bleeding severity. In addition, FGA, FGB, and FGG were sequenced to find causative variants. A total of 166 CFD cases from 16 countries were included, of whom 123 (30 afibrinogenemia, 33 hypofibrinogenemia, 55 dysfibrinogenemia, and 5 hypodysfibrinogenemia) were well characterized. Considering the previously established factor activity and antigen level thresholds, bleeding severity was correctly identified in 58% of the cases. The rates of thrombotic events among afibrinogenemic and hypofibrinogenemic patients were relatively similar (11% and 10%, respectively) and surprisingly higher than in dysfibrinogenemic cases. The rate of spontaneous abortions among 68 pregnancies was 31%, including 86% in dysfibrinogenemic women and 14% with hypofibrinogenemia. Eighty-six patients received treatment (69 on-demand and/or 17 on prophylaxis), with fibrinogen concentrates being the most frequently used product. Genetic analysis was available for 91 cases and 41 distinct variants were identified. Hotspot variants (FGG, p.Arg301Cys/His and FGA, p.Arg35Cys/His) were present in 51% of dysfibrinogenemia. Obstetric complications were commonly observed in dysfibrinogenemia. This large multicenter study provided a comprehensive insight into the clinical, laboratory, and genetic history of patients with CFDs. We conclude that bleeding severity grades were in agreement with the established factor activity threshold in nearly half of the cases with quantitative defects., (© 2024 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published
2024
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49. Efficacy and safety of von Willebrand factor concentrate almost devoid of factor VIII (Wilfactin ® ) in paediatric patients under 6 years of age with severe von Willebrand disease.

Author

Gouider E, Klukowska A, Maes P, Platokouki H, Pujol S, Henriet C, Bridey F, and Goudemand J

Subjects
Adult, Adolescent, Humans, Child, von Willebrand Factor adverse effects, Factor VIII adverse effects, Hemorrhage drug therapy, Hemorrhage prevention & control, Hemorrhage chemically induced, von Willebrand Diseases drug therapy, Hemostatics adverse effects, Anaphylaxis chemically induced
Abstract

Background: Plasma-derived von Willebrand factor (VWF) (Wilfactin ® , LFB, France) was developed for prophylaxis and treatment of haemorrhages in both adults and adolescents with von Willebrand disease (VWD). Replacement therapy in paediatric patients is a key element of the clinical trial programme., Material and Methods: Patients aged <6 years with severe VWD were enrolled in a multinational, open-label study to evaluate the in vivo recovery for Wilfactin ® , and its efficacy in preventing and treating bleeding episodes and during surgery. Overall haemostatic efficacy based on a 4-point scale was assessed by investigators. The treatment period ≥18 months investigated the long-term safety., Results: Nine patients, including 7 with type 3 VWD were exposed to treatment with Wilfactin ® for up to 4.2 years. Recovery of VWF in 7 patients (n=5 type 3, n=1 type 2, n=1 type 1) was 1.8±0.4 IU/dL per IU/kg. Of the 62 bleeds, 89% were controlled with one (73%) or two (16%) infusions of Wilfactin ® . The median dose per infusion was 54 IU/kg. A factor VIII dose was co-administered in 1.6% of bleeds. "Excellent"/"Good" haemostatic efficacy was achieved in 90.3% of episodes. Six patients underwent 11 minor surgical interventions. Treatment duration was 1 day (range: 1-6 days) with a dose administered 30-60 minutes before procedure of 56 IU/kg (range: 41-106 IU/kg). Haemostasis was rated as "Excellent" in all surgeries. During 4-year prophylactic treatment in one patient, breakthrough bleeds were reported in 2.2% of infusions. No VWF inhibitors, thromboembolic events or allergic/anaphylactic-type reactions were observed following a total exposure of 770 days., Discussion: The results show that Wilfactin ® provides a safe and effective treatment in patients <6 years of age with severe VWD.

Published
2023
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50. Inhibitor incidence in an unselected cohort of previously untreated patients with severe haemophilia B: a PedNet study.

Author

Male C, Andersson NG, Rafowicz A, Liesner R, Kurnik K, Fischer K, Platokouki H, Santagostino E, Chambost H, Nolan B, Königs C, Kenet G, Ljung R, and Van den Berg M

Subjects
Factor VIII, Humans, Incidence, Prospective Studies, Risk Factors, Hemophilia A, Hemophilia B drug therapy, Hemophilia B epidemiology, Hemophilia B genetics
Abstract

The incidence of FIX inhibitors in severe hemophilia B (SHB) is not well defined. Frequencies of 3-5% have been reported but most studies to date were small, including patients with different severities, and without prospective follow-up for inhibitor incidence. Study objective was to investigate inhibitor incidence in patients with SHB followed up to 500 exposure days (ED), the frequency of allergic reactions, and the relationship with genotypes. Consecutive previously untreated patients (PUPs) with SHB enrolled into the PedNet cohort were included. Detailed data was collected for the first 50 ED, followed by annual collection of inhibitor status and allergic reactions. Presence of inhibitors was defined by at least two consecutive positive samples. Additionally, data on factor IX gene mutation was collected. 154 PUPs with SHB were included; 75% were followed until 75 ED, and 43% until 500 ED. Inhibitors developed in 14 patients (7 high-titre). Median number of ED at inhibitor manifestation was 11 (IQR 6.5-36.5). Cumulative inhibitor incidence was 9.3% (95%CI 4.4-14.1) at 75 ED, and 10.2% (5.1-15.3) at 500 ED. Allergic reactions occurred in 4 (28.6%) inhibitor patients. Missense mutations were most frequent (46.8%) overall but not associated with inhibitors. Nonsense mutations and deletions with large structural changes comprised all mutations among inhibitor patients and were associated with an inhibitor risk of 26.9% and 33.3%, respectively. In an unselected, well-defined cohort of PUPs with SHB, cumulative inhibitor incidence was 10.2% at 500 ED. Nonsense mutations and large deletions were strongly associated with the risk of inhibitor development. The PedNet Registry is registered at clinicaltrials.gov; identifier: NCT02979119.

Published
2021
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