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Featured researches published by Horst Blum.


Journal of Immunology | 2005

A small molecule alpha 4 beta 1 antagonist prevents development of murine Lyme arthritis without affecting protective immunity.

Joachim Gläsner; Horst Blum; Volkmar Wehner; Hans Ulrich Stilz; Jonathan D. Humphries; G. Paul Curley; A. Paul Mould; Martin J. Humphries; Rupert Hallmann; Martin Röllinghoff; André Gessner

After infection with Borrelia burgdorferi, humans and mice under certain conditions develop arthritis. Initiation of inflammation is dependent on the migration of innate immune cells to the site of infection, controlled by interactions of a variety of adhesion molecules. In this study, we used the newly synthesized compound S18407, which is a prodrug of the active drug S16197, to analyze the functional importance of α4β1-dependent cell adhesion for the development of arthritis and for the antibacterial immune response. S16197 is shown to interfere specifically with the binding of α4β1 integrin to its ligands VCAM-1 and fibronectin in vitro. Treatment of B. burgdorferi-infected C3H/HeJ mice with the α4β1 antagonist significantly ameliorated the outcome of clinical arthritis and the influx of neutrophilic granulocytes into ankle joints. Furthermore, local mRNA up-regulation of the proinflammatory mediators IL-1, IL-6, and cyclooxygenase-2 was largely abolished. Neither the synthesis of spirochete-specific Igs nor the development of a Th1-dominated immune response was altered by the treatment. Importantly, the drug also did not interfere with Ab-mediated control of spirochete load in the tissues. These findings demonstrate that the pathogenesis, but not the protective immune response, in Lyme arthritis is dependent on the α4β1-mediated influx of inflammatory cells. The onset of inflammation can be successfully targeted by treatment with S18407.


Journal of Immunology | 1996

Two distinct stimulus-dependent pathways lead to production of soluble murine interleukin-4 receptor.

Horst Blum; M Wolf; K Enssle; Martin Röllinghoff; André Gessner


Blood | 2001

A soluble form of the murine common γ chain is present at high concentrations in vivo and suppresses cytokine signaling

Udo Meissner; Horst Blum; Markus Schnare; Martin Röllinghoff; André Gessner


Journal of Immunology | 1998

Specific Antagonism of Type I IL-4 Receptor with a Mutated Form of Murine IL-4

Markus Schnare; Horst Blum; Stefan Jüttner; Martin Röllinghoff; André Gessner


Synthesis | 2002

Aromatic β-Amino Acids as Asp-Phg Mimics in LDV Derived VLA-4 Antagonists­

Volkmar Wehner; Horst Blum; Michael Kurz; Hans Ulrich Stilz


Archive | 2002

Novel imidazolidine derivatives, their preparation and their use as vla-4 antagonists

Volkmar Wehner; Stefanie Flohr; Horst Blum; Hartmut Rütten; Hans Ulrich Stilz


Archive | 2002

Imidazolidine derivatives, their preparation and their use

Volkmar Wehner; Stefanie Flohr; Horst Blum; Hartmut Rütten; Hans Ulrich Stilz


Archive | 2013

concentrations in vivo and suppresses cytokine signaling chain is present at high γ A soluble form of the murine common

Horst Blum; André Gessner


Archive | 2002

Novel imidazolidine derivatives, their preparation and their use

Volkmar Wehner; Stefanie Flohr; Horst Blum; Hartmut Rütten; Hans Ulrich Stilz


Archive | 2002

Neue imidazolidinderivate, deren herstellung und verwendung als vla4-antagonisten New imidazolidine derivatives, their preparation and use as VLA4 antagonists

Horst Blum; Stefanie Flohr; Hartmut Rütten; Hans Ulrich Stilz; Volkmar Wehner

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André Gessner

University of Erlangen-Nuremberg

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Markus Schnare

University of Erlangen-Nuremberg

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Joachim Gläsner

University of Erlangen-Nuremberg

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