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Featured researches published by Christina Hausl.


British Journal of Haematology | 2007

Mechanisms of action of immune tolerance induction against factor VIII in patients with congenital haemophilia A and factor VIII inhibitors

Birgit M. Reipert; Pauline M. W. van den Helden; Hans-Peter Schwarz; Christina Hausl

In its most severe form, haemophilia A is a life‐threatening haemorrhagic bleeding disorder that is caused by mutations in the factor VIII (FVIII) gene. About 25% of patients who receive replacement therapy with intravenous FVIII products develop neutralising antibodies (FVIII inhibitors) that inhibit the function of substituted FVIII. Long‐term application of high or low doses of FVIII has evolved as an effective strategy for eradicating antibodies and inducing long‐lasting immune tolerance. Despite clinical experience with the therapy, little is known about the immunological mechanisms that cause the downmodulation of FVIII‐specific immune responses or the induction of long‐lasting immune tolerance against FVIII. This review summarises current knowledge of the immunological mechanisms that might be involved in the induction of immune tolerance against FVIII in patients with haemophilia A who have FVIII inhibitors. In addition to data from patients with haemophilia A, data from patients who have had organ transplants or have immune‐related disorders, such as autoimmune diseases, are considered as well as data from animal models.


Thrombosis and Haemostasis | 2006

Tolerance to factor VIII in a transgenic mouse expressing human factor VIII cDNA carrying an Arg593 to Cys substitution

Wendy S. Bril; Pauline M. van Helden; Christina Hausl; Marleen G. Zuurveld; Rafi U. Ahmad; Martine J. Hollestelle; Pieter H. Reitsma; Karin Fijnvandraat; Rene A. W. Van Lier; Hans Peter Schwarz; Koen Mertens; Birgit M. Reipert; Jan Voorberg

Inhibitory antibodies develop in approximately 25% of patients with severe hemophilia. A following treatment with factorVIII. In E-16KO or E-17KO mice, in which the factor VIII gene has been inactivated by insertion of a neo cassette, inhibitors develop following administration of factor VIII. Here, we describe the generation of transgenic mice expressing human factor VIII-R593C (huFVIII-R593C). Human factor VIII-R593C cDNA under control of a mouse albumin enhancer/promoter was injected into fertilized oocytes. Analysis of transgenic mice revealed that human factor VIII-R593C was expressed in the liver. Transgenic mice were crossed with factor VIII-deficient mice (E-16KO mice). In plasma of E-16KO mice antibodies were detected after five serial intravenous injections of factor VIII, while plasma of huFVIII-R593C/E-16KO mice did not contain detectable levels of antibodies. No antibody secreting cells were observed in either spleen or bone marrow of huFVIII-R593C/E-16KO mice. Also, factor VIII-specific memory B cells were not observed in the spleen of huFVIII-R593C/E-16KO mice. Analysis of T cell responses revealed that splenocytes derived of E-16KO mice secreted IL-10 and IFN-gamma following restimulation with factor VIII in vitro. In contrast, no factor VIII-specific T cell responses were observed in huFVIII-R593C/E-16KO mice. These results indicate that huFVIII-R593C/E-16KO mice are tolerant to intravenously administered factor VIII. It is anticipated that this model may prove useful for studying immune responses in the context of factor VIII gene therapy.


Blood | 2005

High-dose factor VIII inhibits factor VIII–specific memory B cells in hemophilia A with factor VIII inhibitors

Christina Hausl; Rafi U. Ahmad; Maria Sasgary; Christopher B. Doering; Pete Lollar; Günter Richter; Hans Peter Schwarz; Peter Turecek; Birgit M. Reipert


Blood | 2004

Preventing restimulation of memory B cells in hemophilia A: a potential new strategy for the treatment of antibody-dependent immune disorders

Christina Hausl; Rafi U. Ahmad; Hans Peter Schwarz; Eva M. Muchitsch; Peter Turecek; Friedrich Dorner; Birgit M. Reipert


Thrombosis and Haemostasis | 2002

Long-term Persistence of Anti-factor VIII Antibody-secreting Cells in Hemophilic Mice after Treatment with Human Factor VIII

Christina Hausl; Elisabeth Maier; Hans Peter Schwarz; Rafi U. Ahmad; Peter Turecek; Friedrich Dorner; Birgit M. Reipert


Blood | 2008

Requirements for Co-Stimulation in T-Cell Dependent and T-Cell Independent Re-Stimulation of FVIII-Specific Memory B Cells

Aniko Ginta Pordes; Christina Hausl; Peter Allacher; Rafi U. Ahmad; Eva M. Muchitsch; Hartmut J. Ehrlich; Hans Peter Schwarz; Birgit M. Reipert


Blood | 2005

Toll-Like Receptor Triggering Modulates Factor VIII-Specific Immune Memory in Murine Hemophilia A with Factor VIII Inhibitors.

Peter Allacher; Christina Hausl; Rafi U. Ahmad; Hans Peter Schwarz; Peter Turecek; Birgit M. Reipert


Blood | 2007

Humanized E17 Hemophilic Mice Are a Major Breakthrough in the Design of New Preclinical Models for Developing Factor VIII Products with Reduced Immunogenicity.

Birgit M. Reipert; Christina Hausl; Maria Sasgary; Maria Schuster; Rafi U. Ahmad; Bernhard Baumgartner; J. Ilas; Natalie Bauer; Hartmut J. Ehrlich; Hans Peter Schwarz


Blood | 2006

Comparable Long-Term Persistence of Anti-FVIII Antibodies in Hemophilic E17 Mice on Different Genetic Backgrounds Despite Significant Differences in the Amplitude of the Immune Responses.

Natalie Bauer; Christina Hausl; Rafi U. Ahmad; Bernhard Baumgartner; Hans Peter Schwarz; Birgit M. Reipert


Blood | 2007

Single-Cell Analysis of FVIII-Specific Memory B Cells in Murine Hemophilia A.

Christina Hausl; Rafi U. Ahmad; Bernhard Baumgartner; Hans Peter Schwarz; Hartmut J. Ehrlich; Birgit M. Reipert

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Pieter H. Reitsma

Université catholique de Louvain

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