Your search keyword '"Castaman Giancarlo"' showing total 29 results

1. Surgical Experience from the STASEY Study of Emicizumab Prophylaxis in People with Hemophilia A with Factor VIII Inhibitors

Author

Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Infection & Immunity, Castaman, Giancarlo, Peyvandi, Flora, Kremer Hovinga, Johanna A, Schutgens, Roger E G, Robson, Susan, Moreno, Katya, Jiménez-Yuste, Víctor, Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Infection & Immunity, Castaman, Giancarlo, Peyvandi, Flora, Kremer Hovinga, Johanna A, Schutgens, Roger E G, Robson, Susan, Moreno, Katya, and Jiménez-Yuste, Víctor

Published

2024

2. Stable and durable factor IX levels in patients with hemophilia B over 3 years after etranacogene dezaparvovec gene therapy

Author

Leebeek, Frank, von Drygalski, Annette, Gomez, Esteban, Giermasz, Adam, Castaman, Giancarlo, Key, Nigel S., Lattimore, Susan U., Miesbach, Wolfgang, Recht, Michael P., Gut, Robert, Dolmetsch, Ricardo E., Monahan, Paul E., Le Quellec, Sandra, Pipe, Steven W., Leebeek, Frank, von Drygalski, Annette, Gomez, Esteban, Giermasz, Adam, Castaman, Giancarlo, Key, Nigel S., Lattimore, Susan U., Miesbach, Wolfgang, Recht, Michael P., Gut, Robert, Dolmetsch, Ricardo E., Monahan, Paul E., Le Quellec, Sandra, and Pipe, Steven W.

Abstract

Etranacogene dezaparvovec (AMT-061) is a recombinant adeno-associated virus serotype 5 (AAV5) vector containing a codon-optimized Padua variant human factor IX (FIX) transgene with a liver-specific promoter. Here, we report 3-year outcomes from a phase 2b, open-label, single-dose, single-arm, multicenter trial conducted among adults with severe or moderately severe hemophilia B (FIX ≤2%). All participants (n = 3) received a single intravenous dose (2 × 10 13 gene copies per kg) and will be followed up for 5 years. The primary end point of FIX activity ≥5% at 6 weeks was met. Secondary end points included bleed frequency, FIX concentrate use, joint health, and adverse events (AEs). All participants required routine FIX prophylaxis and had neutralizing antibodies to AAV5 before etranacogene dezaparvovec treatment. After administration, FIX activity rose to a mean of 40.8% in year 1 and was sustained in year 3 at 36.9%. All participants discontinued FIX prophylaxis. Bleeding was completely eliminated in 2 out of 3 participants. One participant required on-demand FIX replacement therapy per protocol because of elective surgical procedures, for 2 reported bleeding episodes, and twice for a single self-administered infusion because of an unreported reason. One participant experienced 2 mild, self-limiting AEs shortly after dosing. During the 3-year study period, there were no clinically significant elevations in liver enzymes, no requirement for steroids, no FIX inhibitor development, and no late-emergent safety events in any participant. Etranacogene dezaparvovec was safe and effective in adults with hemophilia B over 3 years after administration. This trial was registered at www.clinicaltrials.gov as #NCT03489291.

Published

2023

3. Translational readthrough at F8 nonsense variants in factor VIII B domain contributes to residual expression and lowers inhibitor association

Author

Testa, M, Lombardi, S, Bernardi, F, Ferrarese, M, Belvini, D, Radossi, P, Castaman, G, Pinotti, M, Branchini, A, Testa, Maria Francesca, Lombardi, Silvia, Bernardi, Francesco, Ferrarese, Mattia, Belvini, Donata, Radossi, Paolo, Castaman, Giancarlo, Pinotti, Mirko, Branchini, Alessio, Testa, M, Lombardi, S, Bernardi, F, Ferrarese, M, Belvini, D, Radossi, P, Castaman, G, Pinotti, M, Branchini, A, Testa, Maria Francesca, Lombardi, Silvia, Bernardi, Francesco, Ferrarese, Mattia, Belvini, Donata, Radossi, Paolo, Castaman, Giancarlo, Pinotti, Mirko, and Branchini, Alessio

Abstract

In hemophilia A, F8 nonsense variants, and particularly those affecting the large factor VIII (FVIII) B domain that is dispensable for coagulant activity, display lower association with replacement therapy-related anti-FVIII inhibitory antibodies as retrieved from multiple international databases. Since null genetic conditions favor inhibitor development, we hypothesized that translational readthrough over premature termination codons (PTC) may contribute to immune tolerance by producing full-length proteins through the insertion of amino acid subset(s). To quantitatively evaluate the readthrough output in vitro, we developed a very sensitive luciferase-based system to detect very low full-length FVIII synthesis from a wide panel (n=45; ~60% patients with PTC) of F8 nonsense variants. PTC not associated with inhibitors displayed higher readthrough-driven expression levels than inhibitor-associated PTC, a novel observation. Particularly, higher levels were detected for B-domain variants (n=20) than for variants in other domains (n=25). Studies on plasma from six hemophilia A patients with PTC, integrated by expression of the corresponding nonsense and readthrough-deriving missense variants, consistently revealed higher FVIII levels for B-domain variants. Only one B-domain PTC (Arg814*) was found among the highly represented PTC not sporadically associated with inhibitors, but with the lowest proportion of inhibitor cases (4 out of 57). These original insights into the molecular genetics of hemophilia A, and particularly into genotype-phenotype relationships related with disease treatment, demonstrate that B-domain features favor PTC readthrough output. This provides a potential molecular mechanism contributing to differential PTC-associated inhibitor occurrence, with translational implications for a novel, experimentally based classification of F8 nonsense variants.

Published

2023

4. Antithrombotic Treatment in Patients With Hemophilia:an EHA-ISTH-EAHAD-ESO Clinical Practice Guidance

Author

Schutgens, Roger E.G., Jimenez-Yuste, Victor, Escobar, Miguel, Falanga, Anna, Gigante, Bruna, Klamroth, Robert, Lassila, Riitta, Leebeek, Frank W.G., Makris, Michael, Owaidah, Tarek, Sholzberg, Michelle, Tiede, Andreas, Werring, David J., Van Der Worp, H. Bart, Windyga, Jerzy, Castaman, Giancarlo, Schutgens, Roger E.G., Jimenez-Yuste, Victor, Escobar, Miguel, Falanga, Anna, Gigante, Bruna, Klamroth, Robert, Lassila, Riitta, Leebeek, Frank W.G., Makris, Michael, Owaidah, Tarek, Sholzberg, Michelle, Tiede, Andreas, Werring, David J., Van Der Worp, H. Bart, Windyga, Jerzy, and Castaman, Giancarlo

Abstract

Cardiovascular disease is an emerging medical issue in patients with hemophilia (PWH) and its prevalence is increasing up to 15% in PWH in the United States. Atrial fibrillation, acute and chronic coronary syndromes, venous thromboembolism, and cerebral thrombosis are frequent thrombotic or prothrombotic situations, which require a careful approach to fine-tune the delicate balance between thrombosis and hemostasis in PWH when using both procoagulant and anticoagulant treatments. Generally, PWH could be considered as being naturally anticoagulated when clotting factors are <20 IU/dL, but specific recommendations in patients with very low levels according to the different clinical situations are lacking and mainly based on the anecdotal series. For PWH with baseline clotting factor levels >20 IU/dL in need for any form of antithrombotic therapy, usually treatment without additional clotting factor prophylaxis could be used, but careful monitoring for bleeding is recommended. For antiplatelet treatment, this threshold could be lower with single-antiplatelet agent, but again factor level should be at least 20 IU/dL for dual antiplatelet treatment. In this complex growing scenario, the European Hematology Association in collaboration with the International Society on Thrombosis and Haemostasis, the European Association for Hemophilia and Allied Disorders, the European Stroke Organization, and a representative of the European Society of Cardiology Working Group on Thrombosis has produced this current guidance document to provide clinical practice recommendations for health care providers who care for PWH.

Published

2023

5. Prophylaxis with recombinant von Willebrand factor in patients with type 3 von Willebrand disease:Results of a post hoc analysis from a phase 3 trial

Author

Leebeek, Frank W.G., Peyvandi, Flora, Tiede, Andreas, Castaman, Giancarlo, Escobar, Miguel, Wang, Michael, Zülfikar, Bulent, Susen, Sophie, Miesbach, Wolfgang, Wang, Scarlett, Wang, Yi, Zhang, Jingmei, Özen, Gülden, Leebeek, Frank W.G., Peyvandi, Flora, Tiede, Andreas, Castaman, Giancarlo, Escobar, Miguel, Wang, Michael, Zülfikar, Bulent, Susen, Sophie, Miesbach, Wolfgang, Wang, Scarlett, Wang, Yi, Zhang, Jingmei, and Özen, Gülden

Abstract

Objectives: To describe efficacy/safety of recombinant von Willebrand factor (rVWF) prophylaxis in patients with type 3 von Willebrand disease (VWD). Methods: This post hoc analysis of a phase 3 open-label trial provides a more detailed analysis of adults with type 3 VWD, categorized based on prior treatment at screening: “Prior On-Demand (OD)” (OD VWF; ≥3 documented spontaneous bleeding events [BEs] requiring VWF in previous 12 months) or “Switch” (plasma-derived [pd] VWF prophylaxis for ≥12 months). Annualized bleeding rates (ABRs) were evaluated during 12 months of rVWF prophylaxis versus historical data from medical records. Results: In the Prior OD group (n = 10), mean spontaneous ABR (sABR) for treated BEs was reduced by 91.6% (ratio, 0.08; 95% CI, 0.02–0.45) versus mean historical sABR. In the Switch group (n = 8), mean sABR for treated BEs was reduced by 47% (ratio, 0.53; 95% CI, 0.08–3.62). One non-serious adverse event (AE) was considered possibly related to rVWF. No treatment-related, fatal, or life-threatening serious AEs were reported, and no patient developed VWF inhibitors. Conclusions: rVWF prophylaxis reduced sABR in type 3 VWD patients previously treated with OD VWF therapy, and maintained a similar level of hemostatic control in those switching from pdVWF prophylaxis to rVWF prophylaxis.

Published

2023

6. Bleeding and thrombotic events in a patient with lupus anticoagulant-associated hypoprothrombinemia and antiphospholipid antibody syndromes: managing hemostasis between Scylla and Charybdis

Author

Lipari, Alice, Sorrentino, Silvia, Tamburini, Carlo, Castaman, Giancarlo, Prisco, Domenico, De Candia, Erica, De Candia, Erica (ORCID:0000-0003-0942-2819), Lipari, Alice, Sorrentino, Silvia, Tamburini, Carlo, Castaman, Giancarlo, Prisco, Domenico, De Candia, Erica, and De Candia, Erica (ORCID:0000-0003-0942-2819)

Abstract

N/A

Published

2023

7. Antithrombotic Treatment in Patients With Hemophilia: an EHA-ISTH-EAHAD-ESO Clinical Practice Guidance

Author

Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Infection & Immunity, Neurologen, Brain, Stroke, Schutgens, Roger E.G., Jimenez-Yuste, Victor, Escobar, Miguel, Falanga, Anna, Gigante, Bruna, Klamroth, Robert, Lassila, Riitta, Leebeek, Frank W.G., Makris, Michael, Owaidah, Tarek, Sholzberg, Michelle, Tiede, Andreas, Werring, David J., Van Der Worp, H. Bart, Windyga, Jerzy, Castaman, Giancarlo, Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Infection & Immunity, Neurologen, Brain, Stroke, Schutgens, Roger E.G., Jimenez-Yuste, Victor, Escobar, Miguel, Falanga, Anna, Gigante, Bruna, Klamroth, Robert, Lassila, Riitta, Leebeek, Frank W.G., Makris, Michael, Owaidah, Tarek, Sholzberg, Michelle, Tiede, Andreas, Werring, David J., Van Der Worp, H. Bart, Windyga, Jerzy, and Castaman, Giancarlo

Published

2023

8. Gene Therapy with Etranacogene Dezaparvovec for Hemophilia B

Author

Poli Van Creveldkliniek Medisch, Pipe, Steven W, Leebeek, Frank W G, Recht, Michael, Key, Nigel S, Castaman, Giancarlo, Miesbach, Wolfgang, Lattimore, Susan, Peerlinck, Kathelijne, Van der Valk, Paul, Coppens, Michiel, Kampmann, Peter, Meijer, Karina, O'Connell, Niamh, Pasi, K John, Hart, Daniel P, Kazmi, Rashid, Astermark, Jan, Hermans, Cedric R J R, Klamroth, Robert, Lemons, Richard, Visweshwar, Nathan, von Drygalski, Annette, Young, Guy, Crary, Shelley E, Escobar, Miguel, Gomez, Esteban, Kruse-Jarres, Rebecca, Quon, Doris V, Symington, Emily, Wang, Michael, Wheeler, Allison P, Gut, Robert, Liu, Ying P, Dolmetsch, Ricardo E, Cooper, David L, Li, Yanyan, Goldstein, Brahm, Monahan, Paul E, Poli Van Creveldkliniek Medisch, Pipe, Steven W, Leebeek, Frank W G, Recht, Michael, Key, Nigel S, Castaman, Giancarlo, Miesbach, Wolfgang, Lattimore, Susan, Peerlinck, Kathelijne, Van der Valk, Paul, Coppens, Michiel, Kampmann, Peter, Meijer, Karina, O'Connell, Niamh, Pasi, K John, Hart, Daniel P, Kazmi, Rashid, Astermark, Jan, Hermans, Cedric R J R, Klamroth, Robert, Lemons, Richard, Visweshwar, Nathan, von Drygalski, Annette, Young, Guy, Crary, Shelley E, Escobar, Miguel, Gomez, Esteban, Kruse-Jarres, Rebecca, Quon, Doris V, Symington, Emily, Wang, Michael, Wheeler, Allison P, Gut, Robert, Liu, Ying P, Dolmetsch, Ricardo E, Cooper, David L, Li, Yanyan, Goldstein, Brahm, and Monahan, Paul E

Published

2023

9. Cost-minimization analysis of recombinant factor VIII Fc versus emicizumab for treating patients with hemophilia A without inhibitors in Europe

Author

Mancuso, Maria Elisa, Castaman, Giancarlo, Pochopien, Michal, Aballéa, Samuel, Drzewiecka, Aleksandra, Hakimi, Zalmai, Nazir, Jameel, Fatoye, Francis, Mancuso, Maria Elisa, Castaman, Giancarlo, Pochopien, Michal, Aballéa, Samuel, Drzewiecka, Aleksandra, Hakimi, Zalmai, Nazir, Jameel, and Fatoye, Francis

Abstract

Background and objective: A cost-minimization model was developed to compare recombinant factor VIII Fc (rFVIIIFc) and emicizumab as prophylaxis for hemophilia A without inhibitors. Methods: The model was based on 100 patients from the healthcare payer perspective in the UK, France, Italy, Spain, and Germany (5-year time horizon). Costs included: drug acquisition; emicizumab wastage by bodyweight (manufacturer’s dosing recommendations); and additional FVIII for breakthrough bleeds. Scenario analyses (UK only): reduced emicizumab dosing frequency; and emicizumab maximum wastage. Results: Total incremental 5-year savings for rFVIIIFc rather than emicizumab use range from €89,320,131 to €149,990,408 in adolescents/adults (≥12 years) and €173,417,486 to €253,240,465 in children (<12 years). Emicizumab wastage accounts for 6% of its total cost in adolescents/adults and 26% in children. Reducing the emicizumab dosing frequency reduces the incremental cost savings with rFVIIIFc, but these remain substantial (adolescents/adults, >€92 million; children >€32 million). Maximum emicizumab wastage increases by 86% and 106%, respectively, increasing the incremental cost savings with rFVIIIFc to €125,352,125 and €105,872,727, respectively. Conclusion: Based on cost-minimization modeling, rFVIIIFc use for hemophilia A prophylaxis in patients without inhibitors is associated with substantial cost savings in Europe, reflecting not only higher acquisition costs of emicizumab, but also other costs including wastage related to available vial sizes.

Published

2022

10. EHA Guidelines on Management of Antithrombotic Treatments in Thrombocytopenic Patients With Cancer

Author

Falanga, Anna, Leader, Avi, Ambaglio, Chiara, Bagoly, Zsuzsa, Castaman, Giancarlo, Elalamy, Ismail, Lecumberri, Ramon, Niessner, Alexander, Pabinger, Ingrid, Szmit, Sebastian, Trinchero, Alice, Ten Cate, Hugo, Rocca, Bianca, Rocca, Bianca (ORCID:0000-0001-8304-6423), Falanga, Anna, Leader, Avi, Ambaglio, Chiara, Bagoly, Zsuzsa, Castaman, Giancarlo, Elalamy, Ismail, Lecumberri, Ramon, Niessner, Alexander, Pabinger, Ingrid, Szmit, Sebastian, Trinchero, Alice, Ten Cate, Hugo, Rocca, Bianca, and Rocca, Bianca (ORCID:0000-0001-8304-6423)

Abstract

In cancer patients, thrombocytopenia can result from bone marrow infiltration or from anticancer medications and represents an important limitation for the use of antithrombotic treatments, including anticoagulant, antiplatelet, and fibrinolytic agents. These drugs are often required for prevention or treatment of cancer-associated thrombosis or for cardioembolic prevention in atrial fibrillation in an increasingly older cancer population. Data indicate that cancer remains an independent risk factor for thrombosis even in case of thrombocytopenia, since mild-to-moderate thrombocytopenia does not protect against arterial or venous thrombosis. In addition, cancer patients are at increased risk of antithrombotic drug-associated bleeding, further complicated by thrombocytopenia and acquired hemostatic defects. Furthermore, some anticancer treatments are associated with increased thrombotic risk and may generate interactions affecting the effectiveness or safety of antithrombotic drugs. In this complex scenario, the European Hematology Association in collaboration with the European Society of Cardiology has produced this scientific document to provide a clinical practice guideline to help clinicians in the management of patients with cancer and thrombocytopenia. The Guidelines focus on adult patients with active cancer and a clear indication for anticoagulation, single or dual antiplatelet therapy, their combination, or reperfusion therapy, who have concurrent thrombocytopenia because of either malignancy or anticancer medications. The level of evidence and the strength of the recommendations were discussed according to a Delphi procedure and graded according to the Oxford Centre for Evidence-Based Medicine.

Published

2022

11. The p.P1127S pathogenic variant lowers von Willebrand factor levels through higher affinity for the macrophagic scavenger receptor LRP1: Clinical phenotype and pathogenic mechanisms

Author

Sacco, Monica, Lancellotti, Stefano, Branchini, Alessio, Tardugno, Maira, Testa, Maria Francesca, Lunghi, Barbara, Bernardi, Francesco, Pinotti, Mirko, Giusti, Betti, Castaman, Giancarlo, De Cristofaro, Raimondo, De Cristofaro, Raimondo (ORCID:0000-0002-8066-8849), Sacco, Monica, Lancellotti, Stefano, Branchini, Alessio, Tardugno, Maira, Testa, Maria Francesca, Lunghi, Barbara, Bernardi, Francesco, Pinotti, Mirko, Giusti, Betti, Castaman, Giancarlo, De Cristofaro, Raimondo, and De Cristofaro, Raimondo (ORCID:0000-0002-8066-8849)

Abstract

Background The index case is a 21-year-old Italian woman with a mild hemorrhagic syndrome and von Willebrand factor antigen (VWF:Ag) = 34.3 U/dl, VWF recombinant glycoprotein Ib (VWF:GpIbR) = 32.8 U/dl, and factor VIII (FVIII) = 55.3 IU/dl. Aims The aim of this study is to characterize from a genetic and biochemical standpoint this low VWF phenotype. Methods Coagulation and biochemical methods were used to study the structural and functional pattern of VWF multimers in the index case's plasma. Recombinant wild-type and p.P1127S VWF variants were produced using human embryonic kidney (HEK)-293 cells. In addition, genetic screening was carried out to detect single nucleotide variants of some scavenger VWF/FVIII receptor genes such as CLEC4M, STAB2, and ASGR2. Results Genetic investigation revealed that the index case inherited from her mother the heterozygous missense mutation c.3379C > T (VWF exon 25), causing the p.P1127S substitution in the VWF D ' D3 domain. The index case was also homozygous for the scavenger receptor ASGR2 c.-95 CC-genotype. Desmopressin normalized the VWF level of the patient, although its clearance was faster (t(1/2) = 6.7 h) than in normal subjects (t(1/2) = 12 +/- 0.7 h). FVIII-VWF interaction, A Disintegrin And Metalloprotease with ThromboSpondin type 1 motif-13 levels, ristocetin-induced-platelet-aggregation, and VWF multimeric pattern were normal. The p.P1127S variant was normally synthesized and secreted by HEK-293 cells, and molecular modeling predicts a conformational change showing higher affinity for the macrophagic scavenger receptor lipoprotein receptor-related protein 1 (LRP1), as also experimentally verified. Conclusions The p.P1127S variant may cause a low VWF phenotype, stemming from an increased VWF affinity for the scavenger receptor LRP1 and, consequently, an accelerated clearance of VWF.

Published

2022

12. The bleeding phenotype in people with nonsevere hemophilia

Author

Kloosterman, Fabienne R., Zwagemaker, Anne Fleur, Bagot, Catherine N., Beckers, Erik A.M., Castaman, Giancarlo, Cnossen, Marjon H., Collins, Peter, Hay, Charles, Hof, Michel, Gorkom, Britta Laros Van, Leebeek, Frank W.G., Male, Christoph, Meijer, Karina, Pabinger, Ingrid, Shapiro, Susan, Coppens, Michiel, Fijnvandraat, Karin, Gouw, Samantha C., Kloosterman, Fabienne R., Zwagemaker, Anne Fleur, Bagot, Catherine N., Beckers, Erik A.M., Castaman, Giancarlo, Cnossen, Marjon H., Collins, Peter, Hay, Charles, Hof, Michel, Gorkom, Britta Laros Van, Leebeek, Frank W.G., Male, Christoph, Meijer, Karina, Pabinger, Ingrid, Shapiro, Susan, Coppens, Michiel, Fijnvandraat, Karin, and Gouw, Samantha C.

Abstract

Detailed information on the onset, frequency, and severity of bleeding in nonsevere hemophilia is limited. We aimed to assess the bleeding phenotype of persons with nonsevere hemophilia and to analyze the association between baseline factor VIII/IX (FVIII/IX) levels and the joint bleeding rate. In the DYNAMO (Dynamic Interplay Between Bleeding Phenotype and Baseline Factor Level in Moderate and Mild Hemophilia A and B) study, an international multicenter cohort, we included males with nonsevere hemophilia (FVIII/IX, 0.02-0.35 IU/mL) aged 12 to 55 years. Information on age at first treated (joint) bleed, annual bleeding rates (ABRs), and annual joint bleeding rates (AJBRs) was collected from the medical files. The association between baseline FVIII/IX levels and the joint bleeding rate was assessed by using a frailty model for recurrent events. In total, 304 persons (70 with moderate hemophilia and 234 with mild hemophilia) were included. The median age was 38 years (interquartile range [IQR], 25-49 years), and the median baseline FVIII/IX level was 0.12 IU/mL (IQR, 0.05-0.21 IU/mL). In total, 245 (81%) persons had experienced at least 1 bleed, and 156 (51%) had experienced at least 1 joint bleed. The median age at first bleed and first joint bleed was 8 and 10 years, respectively. The median ABR and AJBR was 0.2 (IQR, 0.1-0.5) and 0.0 (IQR, 0.0-0.2). From baseline FVIII/IX levels 0.02 to 0.05 IU/mL to >0.25 IU/mL, the median ABR decreased from 0.6 (IQR, 0.2-1.4) to 0.1 (IQR, 0.0-0.2) and the AJBR from 0.2 (IQR, 0.0-0.4) to 0.0 (IQR, 0.0-0.0). Baseline FVIII/IX was inversely associated with the joint bleeding rate (P < .001). Low bleeding rates were observed in persons with nonsevere hemophilia. However, one-half of all adolescents and adults had experienced a joint bleed.

Published

2022

13. Recombinant von Willebrand factor prophylaxis in patients with severe von Willebrand disease:phase 3 study results

Author

Leebeek, Frank W.G., Peyvandi, Flora, Escobar, Miguel, Tiede, Andreas, Castaman, Giancarlo, Wang, Michael, Wynn, Tung, Baptista, Jovanna, Wang, Yi, Zhang, Jingmei, Mellgård, Björn, Özen, Gülden, Leebeek, Frank W.G., Peyvandi, Flora, Escobar, Miguel, Tiede, Andreas, Castaman, Giancarlo, Wang, Michael, Wynn, Tung, Baptista, Jovanna, Wang, Yi, Zhang, Jingmei, Mellgård, Björn, and Özen, Gülden

Abstract

International guidelines conditionally recommend long-term prophylaxis in patients with von Willebrand disease (VWD) and severe and frequent bleeding. As recombinant von Willebrand factor (rVWF; vonicog alfa) may reduce the frequency of treated spontaneous bleeding events (BEs), we investigated the efficacy and safety of rVWF prophylaxis in adults with severe VWD. Patients with BEs requiring VWF therapy in the past year (on-demand VWF therapy [prior on-demand group] or plasma-derived VWF prophylaxis [pdVWF; switch group]) were enrolled in a prospective, open-label, nonrandomized, phase 3 study. The planned duration of rVWF prophylaxis was 12 months; starting rVWF dose was 50 ± 10 VWF: ristocetin cofactor (VWF:RCo) IU/kg twice weekly (prior on-demand group) or based on prior pdVWF weekly dose/dosing frequency (switch group). The primary endpoint was annualized bleeding rate (ABR) of treated spontaneous BEs (sABR) during rVWF prophylaxis. Over the 12-month study period, treated sABR decreased by 91.5% on-study vs historical sABR in 13 patients in the prior on-demand group, and by 45.0% in 10 patients in the switch group (model-based analysis ratio, 0.085; 95% confidence interval [CI], 0.021-0.346 and 0.550; 95% CI, 0.086-3.523, respectively). No treated spontaneous BEs were recorded in 84.6% (11/13) and 70.0% (7/10) of patients, respectively. The safety profile of rVWF was consistent with the previously established profile, with no new adverse drug reactions identified. Findings suggest that rVWF prophylaxis can reduce treated spontaneous BEs in patients previously receiving on-demand VWF therapy and maintains at least the same level of hemostatic control in patients who switch from prophylaxis with pdVWF to rVWF, with a favorable safety profile. This trial was registered at www.clinicaltrials.gov (#NCT02973087) and www.clinicaltrialsregister.eu (#EudraCT 2016-001478-14).

Published

2022

14. Desmopressin for bleeding in non-severe hemophilia A:Suboptimal use in a real-world setting

Author

Zwagemaker, Anne Fleur, Kloosterman, Fabienne R., Coppens, Michiel, Gouw, Samantha C., Boyce, Sara, Bagot, Catherine N., Beckers, Erik A.M., Brons, Paul, Castaman, Giancarlo, Eikenboom, Jeroen, Jackson, Shannon, Kruip, Marieke J.H.A., Leebeek, Frank W.G., Meijer, Karina, Nieuwenhuizen, Laurens, Pabinger, Ingrid, Fijnvandraat, Karin, Zwagemaker, Anne Fleur, Kloosterman, Fabienne R., Coppens, Michiel, Gouw, Samantha C., Boyce, Sara, Bagot, Catherine N., Beckers, Erik A.M., Brons, Paul, Castaman, Giancarlo, Eikenboom, Jeroen, Jackson, Shannon, Kruip, Marieke J.H.A., Leebeek, Frank W.G., Meijer, Karina, Nieuwenhuizen, Laurens, Pabinger, Ingrid, and Fijnvandraat, Karin

Abstract

Background: Desmopressin is an important treatment option in nonsevere hemophilia A because it has several benefits compared with factor (F) concentrates, including no inhibitor risk and much lower costs. Despite these advantages, data are limited on the real-world use of desmopressin in the treatment of bleeds. Objective: To describe the clinical use of desmopressin in relation to other therapeutic modalities in the treatment of bleeding episodes in patients with nonsevere hemophilia A. Methods: Patients with nonsevere hemophilia A aged 12–55 years were included from the DYNAMO cohort study. Data on the desmopressin test response and treated bleeding events in the period January 2009 to July 2020 were retrospectively collected from medical files. An adequate desmopressin test response was defined based on a peak FVIII level of ≥30 IU/dl. Results: A total of 248 patients with a median age of 38 years (interquartile range 25–49) were included. An adequate desmopressin test response was documented in 25% and 73% of patients with moderate and mild hemophilia, respectively. In adequate responders, 51% of bleeds were exclusively treated with FVIII concentrates, 24% exclusively with desmopressin, 21% with a combination of both and 4% with other treatments. In 54% of bleeds treated with a single dose of factor concentrates, the expected FVIII level after desmopressin exceeded the level targeted. Conclusion: Most bleeds in patients with an adequate response to desmopressin are treated with factor concentrates. These findings may indicate a suboptimal use of desmopressin and that barriers to the use of desmopressin should be explored.

Published

2022

15. EHA Guidelines on Management of Antithrombotic Treatments in Thrombocytopenic Patients With Cancer

Author

Falanga, Anna, Leader, Avi, Ambaglio, Chiara, Bagoly, Zsuzsa, Castaman, Giancarlo, Elalamy, Ismail, Lecumberri, Ramon, Niessner, Alexander, Pabinger, Ingrid, Szmit, Sebastian, Trinchero, Alice, Ten Cate, Hugo, Rocca, Bianca, Falanga, Anna, Leader, Avi, Ambaglio, Chiara, Bagoly, Zsuzsa, Castaman, Giancarlo, Elalamy, Ismail, Lecumberri, Ramon, Niessner, Alexander, Pabinger, Ingrid, Szmit, Sebastian, Trinchero, Alice, Ten Cate, Hugo, and Rocca, Bianca

Abstract

In cancer patients, thrombocytopenia can result from bone marrow infiltration or from anticancer medications and represents an important limitation for the use of antithrombotic treatments, including anticoagulant, antiplatelet, and fibrinolytic agents. These drugs are often required for prevention or treatment of cancer-associated thrombosis or for cardioembolic prevention in atrial fibrillation in an increasingly older cancer population. Data indicate that cancer remains an independent risk factor for thrombosis even in case of thrombocytopenia, since mild-to-moderate thrombocytopenia does not protect against arterial or venous thrombosis. In addition, cancer patients are at increased risk of antithrombotic drug-associated bleeding, further complicated by thrombocytopenia and acquired hemostatic defects. Furthermore, some anticancer treatments are associated with increased thrombotic risk and may generate interactions affecting the effectiveness or safety of antithrombotic drugs. In this complex scenario, the European Hematology Association in collaboration with the European Society of Cardiology has produced this scientific document to provide a clinical practice guideline to help clinicians in the management of patients with cancer and thrombocytopenia. The Guidelines focus on adult patients with active cancer and a clear indication for anticoagulation, single or dual antiplatelet therapy, their combination, or reperfusion therapy, who have concurrent thrombocytopenia because of either malignancy or anticancer medications. The level of evidence and the strength of the recommendations were discussed according to a Delphi procedure and graded according to the Oxford Centre for Evidence-Based Medicine.

Published

2022

16. Treatment-related risk factors for inhibitor development in non-severe hemophilia A after 50 cumulative exposure days: A case-control study

Author

Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, Gouw, Samantha C., Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, and Gouw, Samantha C.

Abstract

Item does not contain fulltext

Published

2021

17. Treatment-related risk factors for inhibitor development in non-severe hemophilia A after 50 cumulative exposure days: a case-control study.

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, Abdi, Amal, Eckhardt, Corien L, van Velzen, Alice S, Vuong, Caroline, Coppens, Michiel, Castaman, Giancarlo, Hart, Dan P, Hermans, Cédric, Laros-van Gorkom, Britta, Leebeek, Frank W G, Mancuso, Maria Elisa, Mazzucconi, Maria G, McRae, Simon, Oldenburg, Johannes, Male, Christoph, van der Bom, Johanna G, Fijnvandraat, Karin, Gouw, Samantha C, INSIGHT Study Group, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, Abdi, Amal, Eckhardt, Corien L, van Velzen, Alice S, Vuong, Caroline, Coppens, Michiel, Castaman, Giancarlo, Hart, Dan P, Hermans, Cédric, Laros-van Gorkom, Britta, Leebeek, Frank W G, Mancuso, Maria Elisa, Mazzucconi, Maria G, McRae, Simon, Oldenburg, Johannes, Male, Christoph, van der Bom, Johanna G, Fijnvandraat, Karin, Gouw, Samantha C, and INSIGHT Study Group

Abstract

BACKGROUND: Non-severe hemophilia A patients have a life-long inhibitor risk. Yet, no studies analyzed risk factors for inhibitor development after 50 factor VIII (FVIII) exposure days (EDs). OBJECTIVES: This case-control study investigated treatment-related risk factors for inhibitor development in non-severe hemophilia A and assessed whether these risk factors were different for early versus late inhibitor development. PATIENTS/METHODS: Non-severe hemophilia A patients (FVIII:C 2-40%) were selected from the INSIGHT study. Inhibitor-positive patients were defined as early (<50 EDs) or late (> 50EDs) cases and matched to 1-4 inhibitor-negative controls by year of birth, cumulative number of EDs and center/country. We investigated treatment intensity during the last 10 EDs prior to inhibitor development. Intensive treatment was defined as: surgery, peak treatment (10 consecutive EDs) and high mean FVIII dose (>45 IU/kg/ED). Odds ratios (OR) were calculated by logistic regression. RESULTS: Of 2,709 patients, we analyzed 63 early and 26 late cases and 195 and 71 respectively matched controls. Peak treatment was associated with early and late inhibitor risk (crude OR 1.8, 95%CI 1.0-3.4; 4.0, 95%CI 1.1-14.3). This association was slightly less pronounced after adjustment for mean FVIII dose. High mean FVIII dose was also associated with early and late inhibitor risk (crude OR 2.8, 95%CI 1.5-5.1; 4.5, 95%CI 1.2-16.6). Surgery increased inhibitor risk for early cases. This was less pronounced for late cases. CONCLUSIONS: Our findings suggest that intensive FVIII treatment remains a risk factor for inhibitor development in non-severe hemophilia A after more than 50 EDs. Therefore, persistent caution is required throughout the life-time treatment course.

Published

2021

18. Treatment-related risk factors for inhibitor development in non-severe hemophilia A after 50 cumulative exposure days: A case-control study

Author

Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, Gouw, Samantha C., Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, and Gouw, Samantha C.

Abstract

Contains fulltext : 237770.pdf (Publisher’s version ) (Open Access)

Published

2021

19. Treatment-related risk factors for inhibitor development in non-severe hemophilia A after 50 cumulative exposure days: A case-control study

Author

Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, Gouw, Samantha C., Abdi, Amal, Eckhardt, C.L., Velzen, A.S. van, Vuong, C., Coppens, M., Castaman, Giancarlo, Laros-van Gorkom, B.A.P., Fijnvandraat, Karin, and Gouw, Samantha C.

Abstract

Contains fulltext : 237770.pdf (Publisher’s version ) (Open Access)

Published

2021

20. Obstacles to Early Diagnosis and Treatment of Inherited von Willebrand Disease: Current Perspectives

Author

Castaman,Giancarlo, Linari,Silvia, Castaman,Giancarlo, and Linari,Silvia

Abstract

Giancarlo Castaman, Silvia Linari Center for Bleeding Disorders and Coagulation, Department of Oncology, Careggi University Hospital, Florence, ItalyCorrespondence: Giancarlo CastamanCenter for Bleeding Disorders and Coagulation, Department of Oncology, Careggi University Hospital, Largo G. Brambilla 3, Florence, 50134, ItalyTel +39 055 7947587Fax +39 055 7947794Email giancarlo.castaman@unifi.itAbstract: Von Willebrand disease (VWD), the most common inherited bleeding disorder, is highly heterogeneous, and its early diagnosis may be difficult, especially for mild cases and in qualitative von Willebrand factor (VWF) defects. Appropriate VWD diagnosis requires the combination of personal and/or family history of bleeding and abnormal VWF laboratory testing. The use of bleeding assessment tools has been helpful in standardizing bleeding history collection and quantification of bleeding symptoms to select patients who may benefit of further hemostatic testing. Type 1 and 3 VWD which represent quantitative VWD variants are relatively easy to diagnose. The diagnosis of type 2 VWD requires multiple assessments to evaluate the effects induced by the responsible abnormality on the heterogeneous functions of VWF. Sensitive and reproducible tests are needed to evaluate different VWF activities, starting from measuring VWF-platelet interaction. In the recent years, several increasingly sensitive, rapid and automated assays have been developed, but they are not widely available so far. Genetic testing for VWD diagnosis is not a common practice because VWF gene is very large and highly polymorphic and therefore it is used only in specific cases. It is evident that the early and correct VWD diagnosis allows optimal management of bleeding and situations at risk. Tranexamic acid, desmopressin, replacement therapy with plasma-derived concentrates with a variable content of VWF and FVIII, or the new recombinant VWF are the different therapeutic options available. Careful VWD classific

Published

2021

21. Variability of treatment modalities and intensity in patients with severe haemophilia A on prophylaxis: results from the Italian national registry

Author

Cortesi, P, Giampaolo, A, Abbonizio, F, Molinari, A, Castaman, G, Biffoni, M, Mantovani, L, Cortesi, Paolo Angelo, Giampaolo, Adele, Abbonizio, Francesca, Molinari, Angelo Claudio, Castaman, Giancarlo, Biffoni, Mauro, Mantovani, Lorenzo Giovanni, Cortesi, P, Giampaolo, A, Abbonizio, F, Molinari, A, Castaman, G, Biffoni, M, Mantovani, L, Cortesi, Paolo Angelo, Giampaolo, Adele, Abbonizio, Francesca, Molinari, Angelo Claudio, Castaman, Giancarlo, Biffoni, Mauro, and Mantovani, Lorenzo Giovanni

Abstract

Background: A shift from a standard to a personalized prophylaxis has been increasingly adopted in patients with severe haemophilia A (SHA). This approach has raised the likelihood of a significant variability in the prophylactic approaches and the relative Factor VIII (FVIII) consumptions. The aim of our study was to assess the treatment variability of SHA patients without inhibitors and on prophylaxis regimen in Italy. Material and methods: Data reported in the National Registry of Congenital Coagulopathies (NRCC) were analysed to assess treatment distribution within SHA patients without inhibitors, focussing on FVIII consumption in 2017, associated with prophylaxis regimen. The analysis was stratified based on age groups and Italian regions to describe the variability of FVIII consumption in Italy. Results: In 2017, the Registry reported the therapeutic plans of 1068 SHA patients without inhibitors on prophylaxis. The mean (95% CI) individual consumption ranges from 123 127 IU (99 736-146 518) in the age group 0-6 years to 345 000 IU (336 000-354 000) in the age group >20 years. A significant FVIII consumption variability was identified within the adult population. Regions with less than 50 patients reported the higher variability in mean FVIII consumption per patient-year within the different age groups. Similar difference in FVIII consumption variability was reported also in the age groups comparing “low,” “middle” and “high” patient volume regions. Discussion: A reliable estimation of FVIII consumption for patients’ treatment is necessary to manage and plan the appropriate budget and keep treatment's costs affordable. However, without the implementation of a methodology aiming to assess the overall value produced by these FVIII consumptions, the scenario will keep driven by FVIII consumptions, its costs and the budget available. An effort by haemophilic community, haemophilia treatment centres and institutions is required to develop and share this cultural

Published

2021

22. Concomitant Use of rFVIIa and Emicizumab in People with Hemophilia A with Inhibitors: Current Perspectives and Emerging Clinical Evidence

Author

Linari,Silvia, Castaman,Giancarlo, Linari,Silvia, and Castaman,Giancarlo

Abstract

Silvia Linari, Giancarlo Castaman Department of Oncology, Center for Bleeding Disorders and Coagulation, Careggi University Hospital, Florence, ItalyCorrespondence: Giancarlo CastamanDepartment of Oncology, Center for Bleeding Disorders and Coagulation, Careggi University Hospital, Largo G. Brambilla 3, Florence 50134, ItalyTel +39 055 7947587Fax +39 055 7947794Email giancarlo.castaman@unifi.itAbstract: Emicizumab, a humanized, bi-specific, monoclonal antibody subcutaneously administered, mimicking the function of FVIIIa, represents a milestone in treatment of patients affected by hemophilia A complicated with inhibitors. The HAVEN 1 and 2 studies have clearly established its superiority compared to bypassing agents for routine prophylaxis in preventing or reducing bleeding episodes in adult and pediatric patients with inhibitors. However, its protection against bleeding is only partial, and concomitant use of a bypassing agent may be required with potential prothrombotic risk. The emicizumab Phase III trials (HAVEN 1, 2 and 4) have shown that the traditional bypassing agents, activated prothrombin complex concentrates or recombinant activated factor VII (rFVIIa), may be necessary for the treatment of breakthrough bleeds or surgery management. A post hoc analysis in particular has shown that the concomitant use of emicizumab and rFVIIa is safe and no thrombotic events have been described. The review describes the state of the art of the concomitant use of emicizumab and rFVIIa for treating acute bleeding and surgeries, its efficacy and safety and the lack of thrombotic events associated with this treatment modality. Data still derive mainly from HAVEN trials; however, the availability of emicizumab in clinical practice is progressively increasing the number of patients treated and no adverse events directly attributed to this agent have occurred . The availability of guidelines for the use and dosing of rFVIIa during emicizumab prophylaxis is useful in clinical prac

Published

2020

23. The factor VIII treatment history of non-severe hemophilia A

Author

Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Abdi, Amal, Kloosterman, Fabienne R., Eckhardt, Corien L., Male, Christoph, Castaman, Giancarlo, Fischer, Kathelijn, Beckers, Erik A.M., Kruip, Marieke J.H.A., Peerlinck, Kathelijne, Mancuso, Maria Elisa, Santoro, Cristina, Hay, Charles R., Platokouki, Helen, van der Bom, Johanna G., Gouw, Samantha C., Fijnvandraat, Karin, Hart, Dan P., INSIGHT Study Group, Poli Van Creveldkliniek Medisch, Child Health, Circulatory Health, Abdi, Amal, Kloosterman, Fabienne R., Eckhardt, Corien L., Male, Christoph, Castaman, Giancarlo, Fischer, Kathelijn, Beckers, Erik A.M., Kruip, Marieke J.H.A., Peerlinck, Kathelijne, Mancuso, Maria Elisa, Santoro, Cristina, Hay, Charles R., Platokouki, Helen, van der Bom, Johanna G., Gouw, Samantha C., Fijnvandraat, Karin, Hart, Dan P., and INSIGHT Study Group

Published

2020

24. A phase III study comparing secondary long-term prophylaxis versus on-demand treatment with vWF/FVIII concentrates in severe inherited von Willebrand disease

Author

Peyvandi, Flora, Castaman, Giancarlo, Gresele, Paolo, De Cristofaro, Raimondo, Schinco, Piercarla, Bertomoro, Antonella, Morfini, Massino, Gamba, Gabriella, Barillari, Giovanni, Jiménez-Yuste, Víctor, Königs, Cristoph, Iorio, Alfonso, Federici, Augusto B, De Cristofaro, Raimondo (ORCID:0000-0002-8066-8849), Peyvandi, Flora, Castaman, Giancarlo, Gresele, Paolo, De Cristofaro, Raimondo, Schinco, Piercarla, Bertomoro, Antonella, Morfini, Massino, Gamba, Gabriella, Barillari, Giovanni, Jiménez-Yuste, Víctor, Königs, Cristoph, Iorio, Alfonso, Federici, Augusto B, and De Cristofaro, Raimondo (ORCID:0000-0002-8066-8849)

Abstract

BACKGROUND: There is a lack of prospective clinical trials specifically designed to evaluate the benefits of prophylaxis with vWF/FVIII concentrates in patients with inherited von Willebrand disease (vWD). The aim of the study was to compare efficacy of secondary long-term prophylaxis (PRO) with vWF/FVIII in the prevention of bleeding episodes in severe vWD patients to standard of care (on-demand treatment; ODT). MATERIALS AND METHODS: In this 12-month, phase III, open-label study (PRO.WILL), vWD patients (aged ≥6 years) were randomised to PRO (n=9; 5 completed) or ODT (n=10; 7 completed) treatment with Fanhdi®/Alphanate® (Grifols) according to current licensing status for use in vWD. We assessed the proportion of patients who did not present any spontaneous bleeding episode, adverse events (AEs) or thrombotic events. RESULTS: All patients on ODT had vWD type 2 or 3 vs 70% of patients on PRO. All ODT patients experienced bleeds vs 60% on PRO. PRO patients showed fewer bleeds (n=32 vs n=172 [112 in the same patient, mostly mucosal]; p<0.0001) and lower risk of bleeding (relative attributable risk estimate: -0.667; 95% CI: -2.374, -0.107; p<0.001). Most frequent bleeds in ODT and PRO groups were, respectively, epistaxis (n=52 vs n=15) and gastrointestinal (n=13 [9 in the same patient] vs n=1). While most bleeds lasted one day under ODT (31/32), only epistaxis did so in PRO group (14/15). No AEs due to study medication were observed. DISCUSSION: Despite the small sample size and the heterogeneity of the study population, patients on vWF/FVIII prophylaxis showed a reduction in bleeding risk and rate compared to on-demand treatment.

Published

2019

25. European retrospective study of real-life haemophilia treatment.

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, Berntorp, Erik, Dolan, Gerry, Hay, Charles, Linari, Sylvia, Santagostino, Elena, Tosetto, Alberto, Castaman, Giancarlo, Álvarez-Román, María Teresa, Parra Lopez, Rafael, Oldenburg, Johannes, Albert, Thilo, Scholz, Ute, Holmström, Margareta, Schved, Jean-François, Trossaërt, Marc, Hermans, Cédric, Boban, Ana, Ludlam, Christopher, Lethagen, Stefan, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, Berntorp, Erik, Dolan, Gerry, Hay, Charles, Linari, Sylvia, Santagostino, Elena, Tosetto, Alberto, Castaman, Giancarlo, Álvarez-Román, María Teresa, Parra Lopez, Rafael, Oldenburg, Johannes, Albert, Thilo, Scholz, Ute, Holmström, Margareta, Schved, Jean-François, Trossaërt, Marc, Hermans, Cédric, Boban, Ana, Ludlam, Christopher, and Lethagen, Stefan

Abstract

INTRODUCTION: Haemophilia treatment varies significantly between individuals, countries and regions and details of bleed rates, factor consumption and injection frequency are often not available. AIM: To provide an overview of the FVIII/FIX treatment practice and outcome for patients with haemophilia A (HA) or haemophilia B (HB) across Europe. METHODS: Non-interventional, 12-month retrospective study where anonymized data were retrieved from haemophilia centres/registers in Belgium, France, Germany, Italy, Spain, Sweden and the United Kingdom. Male patients (all ages) receiving coagulation factor treatment 24 months prior to the study, with basal FVIII/FIX levels ≤5 IU dL-1 , without inhibitors, were included. Data were summarized descriptively. RESULTS: In total, 1346 patients with HA and 312 with HB were included in the analysis; 75% and 57% had severe disease (FVIII/FIX < 1 IU dL-1 ) respectively. Prophylaxis was most common for severe haemophilia, especially for children, whereas on-demand treatment was more common for moderate haemophilia in most countries. The mean (SD) prescribed prophylactic treatment ranged from 67.9 (30.4) to 108.4 (78.1) (HA) and 32.3 (10.2) to 97.7 (32.1) (HB) IU kg-1 per week, across countries. Most patients on prophylaxis were treated ≥3 times/week (HA) or two times/week (HB). The median annual bleeding rate (ABR) for patients on prophylaxis ranged from 1.0 to 4.0 for severe HA, and from 1.0 to 6.0 for severe HB, while those with moderate haemophilia generally had slightly higher ABRs. Median ABRs for on-demand-treated severe HA ranged from 4.5 to 18.0, and for HB, 1.5 to 14.0. CONCLUSION: Treatment practice varied greatly between centres and countries and patients treated on-demand and prophylactically both experienced bleeds, emphasizing the need for further optimization of care.

Published

2017

26. Italian daily platelet transfusion practice for haematological patients undergoing high dose chemotherapy with or without stem cell transplantation: A survey by the GIMEMA Haemostasis and Thrombosis Working Party

Author

Tagariello, Giuseppe, Castaman, Giancarlo, Falanga, Anna, Santoro, Rita, Napolitano, Mariasanta, Storti, Sergio, Veneri, Dino, Basso, Marco, Candiotto, Laura, Tassinari, Cristina, Federici, Augusto B., De Stefano, Valerio, Storti, Sergio (ORCID:0000-0002-4374-3985), De Stefano, Valerio (ORCID:0000-0002-5178-5827), Tagariello, Giuseppe, Castaman, Giancarlo, Falanga, Anna, Santoro, Rita, Napolitano, Mariasanta, Storti, Sergio, Veneri, Dino, Basso, Marco, Candiotto, Laura, Tassinari, Cristina, Federici, Augusto B., De Stefano, Valerio, Storti, Sergio (ORCID:0000-0002-4374-3985), and De Stefano, Valerio (ORCID:0000-0002-5178-5827)

Abstract

Background. Following high-dose chemotherapy/bone marrow transplantation, patients are routinely, prophylactically transfused with platelet concentrates (PC) if they have a platelet count ≤10×109/L or higher in the presence of risk factors for bleeding. However, whether such transfusions are necessary in clinically stable patients with no bleeding, or whether a therapeutic transfusion strategy could be sufficient and safe, is still debated. Materials and methods. The GIMEMA Haemostasis and Thrombosis Working Party sent a questionnaire to Italian haematology departments to survey several aspects of daily platelet transfusion practice, such as the cut-off platelet count for transfusion, the evaluation of refractoriness and the type of PC administered. Results. The questionnaire was answered by 18 out of 31 centres (58%). A total of 23,162 PC were transfused in 2,396 patients in 2013. The vast majority of centres (95%) transfused PC according to Italian and international guidelines; only a few transfused always at platelet counts ≤20×109/L. The broad agreement on platelet count cut-off for transfusion (≤10×109/L) was not confirmed when the World Health Organization (WHO) bleeding score was considered: only a third of centres (33%) used transfusions as recommended when the bleeding grade was ≥2. Platelet refractoriness was poorly monitored and most centres (89%) evaluated, mostly empirically (67%), response to transfusion only 24 hours later. Thirty percent of centres transfused platelets in asymptomatic refractory patients. Discussion. Although most Italian haematology departments transfuse PC according to Italian and international guidelines, our survey shows that in routine daily practice physicians do not comply closely with the WHO recommendations on platelet transfusions and monitoring platelet refractoriness. This causes excessive platelet transfusions, with a resulting increase of costs and waste of public health resources.

Published

2016

27. Human von Willebrand factor/factor VIII concentrates in the management of pediatric patients with von Willebrand disease/hemophilia A

Author

Castaman,Giancarlo, Linari,Silvia, Castaman,Giancarlo, and Linari,Silvia

Abstract

Giancarlo Castaman, Silvia Linari Department of Oncology, Center for Bleeding Disorders, Careggi University Hospital, Florence, ItalyAbstract: Several plasma-derived intermediate and high-purity concentrates containing von Willebrand factor (VWF) and factor VIII (FVIII) are currently available. The main role of these products in the management of pediatric the population is represented by the replacement therapy in patients with severe or intermediate forms of von Willebrand disease, in whom other treatments are ineffective or contraindicated. Another important role of VWF/FVIII concentrates in children may be their use in immune tolerance induction (ITI) protocols. ITI is particularly recommended for hemophilia A children who have developed an inhibitor against FVIII, currently the most serious complication of substitutive treatment in hemophilia. Although recombinant concentrates may represent the preferred option in children with hemophilia A, VWF/FVIII concentrates may offer an advantage in rescuing patients who failed previous ITI.Keywords: von Willebrand factor, factor VIII, plasma-derived concentrates, children, von Willebrand disease, hemophilia A

Published

2016

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

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, UCL - (SLuc) Centre de malformations vasculaires congénitales, Eckhardt, Corien L., Van Velzen, Alice S., Peters, Marjolein, Astermark, Jan, Brons, Paul P., Castaman, Giancarlo, Cnossen, Marjon H., Dors, Natasja, Escuriola-Ettingshausen, Carmen, Hamulyak, Karly, Hart, Daniel P., Hay, Charles R. M., Haya, Saturnino, Van Heerde, Waander L., Hermans, Cédric, Holmström, Margareta, Jimenez-Yuste, Victor, Keenan, Russell D., Klamroth, Robert, Laros-van Gorkom, Britta A. P., Leebeek, Frank W. G., Liesner, Ri, Mäkipernaa, Anne, Male, Christoph, Mauser-Bunschoten, Evelien, Mazzucconi, Maria G., McRae, Simon, Meijer, Karina, Mitchell, Michael, Morfini, Massimo, Nijziel, Marten, Oldenburg, Johannes, Peerlinck, Kathelijne, Petrini, Pia, Platokouki, Helena, Reitter-Pfoertner, Sylvia E., Santagostino, Elena, Schinco, Piercarla, Smiers, Frans J., Siegmund, Berthold, Tagliaferri, Annarita, Yee, Thynn T., Kamphuisen, Pieter Willem, Van Der Bom, Johanna G., Fijnvandraat, Karin, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service d'hématologie, UCL - (SLuc) Centre de malformations vasculaires congénitales, Eckhardt, Corien L., Van Velzen, Alice S., Peters, Marjolein, Astermark, Jan, Brons, Paul P., Castaman, Giancarlo, Cnossen, Marjon H., Dors, Natasja, Escuriola-Ettingshausen, Carmen, Hamulyak, Karly, Hart, Daniel P., Hay, Charles R. M., Haya, Saturnino, Van Heerde, Waander L., Hermans, Cédric, Holmström, Margareta, Jimenez-Yuste, Victor, Keenan, Russell D., Klamroth, Robert, Laros-van Gorkom, Britta A. P., Leebeek, Frank W. G., Liesner, Ri, Mäkipernaa, Anne, Male, Christoph, Mauser-Bunschoten, Evelien, Mazzucconi, Maria G., McRae, Simon, Meijer, Karina, Mitchell, Michael, Morfini, Massimo, Nijziel, Marten, Oldenburg, Johannes, Peerlinck, Kathelijne, Petrini, Pia, Platokouki, Helena, Reitter-Pfoertner, Sylvia E., Santagostino, Elena, Schinco, Piercarla, Smiers, Frans J., Siegmund, Berthold, Tagliaferri, Annarita, Yee, Thynn T., Kamphuisen, Pieter Willem, Van Der Bom, Johanna G., and Fijnvandraat, Karin

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

29. Phenotype and genotype of a cohort of families historically diagnosed with type 1 von Willebrand disease in the European study, Molecular and Clinical Markers for the Diagnosis and Management of Type 1 von Willebrand Disease (MCMDM-1VWD)

Author

Goodeve, Anne, Eikenboom, Jeroen, Castaman, Giancarlo, Rodeghiero, Francesco, Federici, Augusto B., Batlle, Javier, Meyer, Dominique, Mazurier, Claudine, Goudemand, Jenny, Schneppenheim, Reinhard, Budde, Ulrich, Ingerslev, Jorgen, Habart, David, Vorlova, Zdena, Holmberg, Lars, Lethagen, Stefan, Pasi, John, Hill, Frank, Hashemi Soteh, Mohammad, Baronciani, Luciano, Halldén, Christer, Guilliatt, Andrea, Lester, Will, Peake, Ian, Goodeve, Anne, Eikenboom, Jeroen, Castaman, Giancarlo, Rodeghiero, Francesco, Federici, Augusto B., Batlle, Javier, Meyer, Dominique, Mazurier, Claudine, Goudemand, Jenny, Schneppenheim, Reinhard, Budde, Ulrich, Ingerslev, Jorgen, Habart, David, Vorlova, Zdena, Holmberg, Lars, Lethagen, Stefan, Pasi, John, Hill, Frank, Hashemi Soteh, Mohammad, Baronciani, Luciano, Halldén, Christer, Guilliatt, Andrea, Lester, Will, and Peake, Ian

Abstract

Type 1 von Willebrand disease (VWD) is characterized by a personal and family history of bleeding coincident with reduced levels of normal plasma von Willebrand factor (VWF). The molecular basis of the disorder is poorly understood. The aims of this study were to determine phenotype and genotype and their relationship in patients historically diagnosed with type 1 VWD. Families were recruited in 9 European countries based on previous type 1 VWD diagnosis. Bleeding symptoms were recorded, plasma phenotype analyzed, and VWF mutation analysis performed in all index cases (ICs). Phenotypic and molecular analysis stratified patients into those with or without phenotypes suggestive of qualitative VWF defects (abnormal multimers) and with or without mutations. A total of 105 of 150 ICs (70%) had mutations identified. A subgroup with abnormal multimers (38% of ICs, 57 of 150) showed a high prevalence of VWF gene mutations (95% of ICs, 54 of 57), whereas in those with qualitatively normal VWF, fewer mutations were identified (55% of ICs, 51 of 93). About one third of the type 1 VWD cases recruited could be reconsidered as type 2. The remaining group could be considered "true" type 1 VWD, although mutations were found in only 55%.

Published

2007