ReFacto®<sup>1</sup> and Advate®<sup>2</sup>: a single‐dose, randomized, two‐period crossover pharmacokinetics study in subjects with haemophilia A

Paola, Jorge Di; Smith, Mark; Klamroth, Robert; Mannucci, P.M.; Kollmer, Carl; Feingold, J.; Kessler, C. M.; Pollmann, H.; Morfini, Massimo; Udata, Chandrasekhar; Rothschild, Chantal; Hermans, Cédric; Janco, Robert L.

doi:10.1111/j.1365-2516.2006.01420.x

Cited by 49 publications

(49 citation statements)

References 15 publications

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“…As expected, most of the rFVIII dispensed (89.1%) was administered to severe When not controlling for any other variables, severe patients treated on-demand utilized less FVIII than those on prophylaxis (median 1442 and 4060 IU kg )1 year )1 , respectively, P < 0.0001). After separating treatment regimen cohorts by age, there were significant differences in utilization between paediatric (<13 years old), adolescent (13)(14)(15)(16)(17)(18), and adult ( ‡19) patients receiving either episodic treatment or prophylaxis (Fig. 1, all P < 0.0001).…”

Section: Overall Fviii Utilizationmentioning

confidence: 84%

“…This reformulation of BDD-rFVIII was completed well before 2006 and would not interfere with the results. Although a pharmacokinetic crossover study [18] for the second generation BDD-rFVII product (ReFacto, Pfizer) showed BDD-rFVIII to be bioequivalent to a FL-rFVIII, half-life measurements were not provided. The follow-on BDD-rFVIII product (Xyntha in US, Refacto AF in EU, Pfizer) showed a 2-h difference in half-life between BDD-rFVIII and FL-rFVIII (11 h vs. 13 h, respectively) [19] although statistical significance was not provided.…”

Section: Discussionmentioning

confidence: 99%

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Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Xiong

Woo

et al. 2011

Haemophilia

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Finding differences in drug utilization patterns within rare patient populations is challenging without access to a large sample. Our objective was to identify patient and treatment-related factors associated with differences in annual recombinant factor VIII (rFVIII) utilization in a large cohort of haemophilia A patients. This retrospective analysis utilized a large, US specialty pharmacy dispensing database from January 2006 to September 2009. Differences in median annual FVIII utilization (IU kg(-1) year(-1)) by age, severity, treatment regimen, rFVIII product type and health insurance plan were tested using non-parametric statistics and regression analysis. A total of 1011 haemophilia A patients were included in the overall analysis. Severe haemophilia patients had higher median annual FVIII utilization than mild/moderate patients (P < 0.0001). Median annual FVIII utilization was also significantly different between treatment regimens (episodic = 1429 IU kg(-1) year(-1) vs. prophylaxis = 3993 IU kg(-1) year(-1) for severe patients, P < 0.0001). Children (0-12 years old), adolescents (13-18 years old) and adults (19+ years old) with severe haemophilia A receiving prophylaxis utilized 4588, 4082 and 3223 IU kg(-1) year(-1) (P < 0.0001). After controlling for age, severity, treatment regimen and insurance type, regression analysis revealed B domain-deleted recombinant FVIII (BDD-rFVIII) was associated with 33% higher FVIII consumption compared with full-length recombinant FVIII (FL-rFVIII) (P = 0.0172). Similar results were also seen when matching BDD-rFVIII and FL-rFVIII patients. Health insurance type was not associated with annual FVIII utilization. As expected, age, severity and treatment regimen were significantly associated with FVIII utilization. After controlling for confounders, patients receiving FL-rFVIII prophylactically were associated with lower annual FVIII utilization compared with patients receiving BDD-rFVIII prophylactically.

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Section: Overall Fviii Utilizationmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Xiong

Woo

et al. 2011

Haemophilia

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“…Such direct comparison studies were performed using plasma-derived factor VIII (Hemophil M) and separately using full length recombinant factor VIII (Advate ® ; Baxter Healthcare). The direct pharmacokinetic comparisons showed that the factor VIII products are bioequivalent to each other 68,71…”

Section: Are All Currently Available Recombinant Factor VIII Productsmentioning

confidence: 99%

Recombinant factor VIII in the management of hemophilia A: current use and future promise

Powell

2009

TCRM

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Hemophilia A is a rare inherited bleeding disorder due to mutation of the gene that encodes the coagulation protein factor VIII. Historically, prior to the availability of treatment with factor VIII preparations, most boys died from uncontrolled bleeding, either spontaneous bleeding or after injury, before reaching 20 years of age. One of the most impressive triumphs of modern medicine is that with current recombinant factor VIII replacement therapy, a boy born in the 21st century with severe hemophilia A can anticipate a normal life expectancy with essentially no permanent complications from bleeding. For severe hemophilia A, current optimal treatment should have two goals: first, to provide sufficient factor VIII to prevent spontaneous bleeding, and second, to provide sufficient factor VIII to have normal coagulation function after any trauma. However, the replacement therapy requires tremendous resources for effective use, and remains extraordinarily expensive. Thus there are opportunities for further advances in therapy for hemophilia A. Two major concerns continue to trouble current optimal treatment approaches: some patients will develop neutralizing antibodies during the first 50 infusions of therapeutic factor VIII, and second, to administer therapeutic factor VIII every other day in young boys often requires placement of a central venous access device, and such use carries the life-threatening risks of infection and thrombosis. Because of the effectiveness of current therapy, any new developments in treatment will require significant concerns for safety, both immediate and in the long term. A number of research groups seek to prolong the biological efficacy of infused recombinant factor VIII. Currently, one such promising development is in the advanced stages of clinical trial. The goals will be to improve further the quality of life of an individual with severe hemophilia A, and to reduce the burden of current treatment strategies on families and medical resources. Hopefully, the hemophilia community will continue to participate actively in the clinical trials needed to address these new challenges.

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“…Di Paola et al conducted a clinical study using BDD-rFVIII, rAFH-PMF, and pdFVIII to compare pharmacokinetic profiles using a chromogenic substrate assay for the measurement of FVIII:C. The results indicated that BDD-rFVIII and rAFH-PMF were equivalent [22].…”

Section: Efficacy and Safety In Postmarketing Clinical Studiesmentioning

confidence: 99%

Products Used to Treat Hemophilia: Recombinant Products

Yoshioka

2014

Textbook of Hemophilia

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ReFacto®¹ and Advate®²: a single‐dose, randomized, two‐period crossover pharmacokinetics study in subjects with haemophilia A

Cited by 49 publications

References 15 publications

Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Recombinant factor VIII in the management of hemophilia A: current use and future promise

Products Used to Treat Hemophilia: Recombinant Products

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ReFacto®1 and Advate®2: a single‐dose, randomized, two‐period crossover pharmacokinetics study in subjects with haemophilia A

Cited by 49 publications

References 15 publications

Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Retrospective analysis of differences in annual factor VIII utilization among haemophilia A patients

Recombinant factor&nbsp;VIII in the management of hemophilia A: current use and future promise

Products Used to Treat Hemophilia: Recombinant Products

Contact Info

Product

Resources

About

ReFacto®¹ and Advate®²: a single‐dose, randomized, two‐period crossover pharmacokinetics study in subjects with haemophilia A

Recombinant factor VIII in the management of hemophilia A: current use and future promise