A systematic overview of the first pasteurised VWF/FVIII medicinal product, Haemate P/ Humate -P: history and clinical performance.

Berntorp, Erik; Archey, William; Auerswald, Günter; Federici, Augusto B; Franchini, Massimo; Knaub, Sigurd; Kreuz, Wolfhart; Lethagen, Stefan; Mannucci, Pier M; Pollmann, Hartmut; Scharrer, Inge; Hoots, Keith

A systematic overview of the first pasteurised VWF/FVIII medicinal product, Haemate P/ Humate -P: history and clinical performance.

Mark

Berntorp, Erik ^LU ; Archey, William ; Auerswald, Günter ; Federici, Augusto B ; Franchini, Massimo ; Knaub, Sigurd ; Kreuz, Wolfhart ; Lethagen, Stefan ^LU ; Mannucci, Pier M and Pollmann, Hartmut , et al. (2008) In European Journal of Haematology. Supplementum 80(s70). p.3-35

Abstract: Patients with von Willebrand disease (VWD) and haemophilia A (HA) lack, to varying degrees, the von Willebrand factor (VWF) and coagulation factor VIII (FVIII) that are critical for normal haemostasis. These conditions in turn make patients prone to uncontrolled bleeding. Historically, patients with severe forms of VWD or HA were crippled before adulthood and their life expectancy was significantly reduced. Over the past decades, specific coagulation factor replacement therapies including Haemate P, have been developed to help patients achieve and maintain normal haemostasis. Haemate P is a human, plasma-derived VWF/FVIII medicinal product, which was first licensed in Germany in 1981 for the treatment of HA-associated bleeding. It has... (More); Patients with von Willebrand disease (VWD) and haemophilia A (HA) lack, to varying degrees, the von Willebrand factor (VWF) and coagulation factor VIII (FVIII) that are critical for normal haemostasis. These conditions in turn make patients prone to uncontrolled bleeding. Historically, patients with severe forms of VWD or HA were crippled before adulthood and their life expectancy was significantly reduced. Over the past decades, specific coagulation factor replacement therapies including Haemate P, have been developed to help patients achieve and maintain normal haemostasis. Haemate P is a human, plasma-derived VWF/FVIII medicinal product, which was first licensed in Germany in 1981 for the treatment of HA-associated bleeding. It has since then come to be accepted as the gold standard for both the treatment and prophylaxis of bleeding in VWD, especially in cases where desmopressin [1-deamino-8-D-arginine vasopressin (DDAVP)] has been ineffective. Haemate P was the first effectively virus-inactivated (pasteurisation: 60 degrees C for 10 h in aqueous solution) FVIII product, whereby the risk of potentially threatening infective complications of plasma-derived products was reduced. Haemate P was also shown to have a VWF multimer profile remarkably close to that of normal plasma. This bibliographic review presents previously unpublished clinical data of Haemate P, based upon internal clinical study reports of the proprietor, CSL Behring, in addition to data already presented in other publications. The data demonstrate a predictable and well-characterised pharmacokinetic profile, and a proven record of short- and long-term safety, while effectively correcting the haemostatic defects in VWD and HA. Recently available data have also shown Haemate P to be of haemostatic value in exceptional clinical circumstances including surgical interventions. By virtue of its plasma-derived combination of VWF and FVIII, in addition to its high VWF:FVIII content ratio (2.4:1), Haemate P is also associated with successful immune tolerance induction in those patients developing inhibitor antibodies. Although the theoretical risk of thromboembolic complications does exist while receiving Haemate P, as it does with any FVIII replacement therapy, the incidence of such complications has remained notably low. Given the robust data that have accumulated for the use of Haemate P, dosing recommendations are also described in this review; the recommendations are tailored to patient-specific contexts including baseline VWF and FVIII levels in plasma and the type of surgical intervention being undertaken. A wide variety of studies have also provided data on paediatric and geriatric populations, all of which have suggested that Haemate P can be safely and effectively used in a wide variety of clinical circumstances. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1153835

author

Berntorp, Erik ^LU ; Archey, William ; Auerswald, Günter ; Federici, Augusto B ; Franchini, Massimo ; Knaub, Sigurd ; Kreuz, Wolfhart ; Lethagen, Stefan ^LU ; Mannucci, Pier M and Pollmann, Hartmut , et al. (More)

Berntorp, Erik ^LU ; Archey, William ; Auerswald, Günter ; Federici, Augusto B ; Franchini, Massimo ; Knaub, Sigurd ; Kreuz, Wolfhart ; Lethagen, Stefan ^LU ; Mannucci, Pier M ; Pollmann, Hartmut ; Scharrer, Inge and Hoots, Keith (Less)

organization

publishing date

2008

type

Contribution to journal

publication status

published

subject

Hematology

keywords

Haemate P, Humate-P, von Willebrand disease, von Willebrand factor, haemophilia, factor VIII

in

European Journal of Haematology. Supplementum

volume

80

issue

s70

pages

3 - 35

publisher

Wiley-Blackwell

external identifiers

wos:000255553400002
pmid:18380871
pmid:18380871
scopus:41749108922

ISSN

0902-4506

DOI

10.1111/j.1600-0609.2008.01049.x

language

English

LU publication?

yes

additional info

The information about affiliations in this record was updated in December 2015. The record was previously connected to the following departments: Emergency medicine/Medicine/Surgery (013240200), Clinical Coagulation Research Unit (013242510)

id

04f53bf7-d971-4c75-aeb1-da7b8f663c12 (old id 1153835)

alternative location

http://www.ncbi.nlm.nih.gov/pubmed/18380871?dopt=Abstract

date added to LUP

2016-04-01 14:40:11

date last changed

2022-01-28 01:52:36

@article{04f53bf7-d971-4c75-aeb1-da7b8f663c12,
  abstract     = {{Patients with von Willebrand disease (VWD) and haemophilia A (HA) lack, to varying degrees, the von Willebrand factor (VWF) and coagulation factor VIII (FVIII) that are critical for normal haemostasis. These conditions in turn make patients prone to uncontrolled bleeding. Historically, patients with severe forms of VWD or HA were crippled before adulthood and their life expectancy was significantly reduced. Over the past decades, specific coagulation factor replacement therapies including Haemate P, have been developed to help patients achieve and maintain normal haemostasis. Haemate P is a human, plasma-derived VWF/FVIII medicinal product, which was first licensed in Germany in 1981 for the treatment of HA-associated bleeding. It has since then come to be accepted as the gold standard for both the treatment and prophylaxis of bleeding in VWD, especially in cases where desmopressin [1-deamino-8-D-arginine vasopressin (DDAVP)] has been ineffective. Haemate P was the first effectively virus-inactivated (pasteurisation: 60 degrees C for 10 h in aqueous solution) FVIII product, whereby the risk of potentially threatening infective complications of plasma-derived products was reduced. Haemate P was also shown to have a VWF multimer profile remarkably close to that of normal plasma. This bibliographic review presents previously unpublished clinical data of Haemate P, based upon internal clinical study reports of the proprietor, CSL Behring, in addition to data already presented in other publications. The data demonstrate a predictable and well-characterised pharmacokinetic profile, and a proven record of short- and long-term safety, while effectively correcting the haemostatic defects in VWD and HA. Recently available data have also shown Haemate P to be of haemostatic value in exceptional clinical circumstances including surgical interventions. By virtue of its plasma-derived combination of VWF and FVIII, in addition to its high VWF:FVIII content ratio (2.4:1), Haemate P is also associated with successful immune tolerance induction in those patients developing inhibitor antibodies. Although the theoretical risk of thromboembolic complications does exist while receiving Haemate P, as it does with any FVIII replacement therapy, the incidence of such complications has remained notably low. Given the robust data that have accumulated for the use of Haemate P, dosing recommendations are also described in this review; the recommendations are tailored to patient-specific contexts including baseline VWF and FVIII levels in plasma and the type of surgical intervention being undertaken. A wide variety of studies have also provided data on paediatric and geriatric populations, all of which have suggested that Haemate P can be safely and effectively used in a wide variety of clinical circumstances.}},
  author       = {{Berntorp, Erik and Archey, William and Auerswald, Günter and Federici, Augusto B and Franchini, Massimo and Knaub, Sigurd and Kreuz, Wolfhart and Lethagen, Stefan and Mannucci, Pier M and Pollmann, Hartmut and Scharrer, Inge and Hoots, Keith}},
  issn         = {{0902-4506}},
  keywords     = {{Haemate P; Humate-P; von Willebrand disease; von Willebrand factor; haemophilia; factor VIII}},
  language     = {{eng}},
  number       = {{s70}},
  pages        = {{3--35}},
  publisher    = {{Wiley-Blackwell}},
  series       = {{European Journal of Haematology. Supplementum}},
  title        = {{A systematic overview of the first pasteurised VWF/FVIII medicinal product, Haemate P/ Humate -P: history and clinical performance.}},
  url          = {{http://dx.doi.org/10.1111/j.1600-0609.2008.01049.x}},
  doi          = {{10.1111/j.1600-0609.2008.01049.x}},
  volume       = {{80}},
  year         = {{2008}},
}

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A systematic overview of the first pasteurised VWF/FVIII medicinal product, Haemate P/ Humate -P: history and clinical performance.