idw – Informationsdienst Wissenschaft

Nachrichten, Termine, Experten

Grafik: idw-Logo
Science Video Project
idw-Abo

idw-News App:

AppStore

Google Play Store



Instanz:
Teilen: 
24.04.2020 11:54

New active ingredient against allergic asthma: Parasite larvae could help fight allergies

Dr. Ulrich Marsch Corporate Communications Center
Technische Universität München

    Our immune system protects us against pathogens. However, an excessive immune reaction can trigger allergies or chronic asthma. Scientists at the Technical University of Munich (TUM) and Helmholtz Zentrum München have discovered an active ingredient taken from the larvae of a worm parasite that could help diminish immune reactions.

    The larvae of the roundworm Heligmosomoides polygyrus bakeri (Hpb) need a very special environment in order to survive: They have to invade the mucosal layer of the intestine in rodents, the only place where they can then develop into adult worms capable of reproduction. To do this, the tiny larvae have to outdo the host's immune system, which defends the host against the intruders with inflammatory reactions, the secretion of fluids and muscle contractions. “Normally the larvae of the parasitic worm would have no chance of withstanding these immune responses. But they use active molecules to specifically modulate the immune response of the host,” explains Dr. Julia Esser-von Bieren, researcher at the Center of Allergy and Environment (ZAUM) at Technical University of Munich and Helmholtz Zentrum München. “We want to harness these evolutionarily matured active ingredients to treat chronic inflammatory diseases.”

    A worm protein alters the immune response

    Together with her team Esser-von Bieren has succeeded in isolating, identifying and analyzing a substance that the worm larvae use to trick the immune system of their host: The protein Hpb glutamate dehydrogenase activates various immunoregulatory metabolic pathways. These pathways ensure the formation of anti-inflammatory mediators in the immune cells of the host organism. At the same time the number of inflammatory mediators is reduced.

    “The ability of Hpb glutamate dehydrogenase to weaken the immune response makes it a promising candidate for treatment of chronic airway inflammation,” says Esser-von Bieren. Respiratory illnesses such as allergic asthma are often the result of an over-reaction by the immune system due to an overproduction of inflammatory mediators known as leukotrienes, which can trigger asthma attacks. However, the medications currently given to patients, usually cortisone, hardly have any effect on these mediators at all.

    Active ingredient for new asthma medications

    The researchers used a mouse model of allergic asthma to successfully show that the larval protein can be used to suppress inflammatory reactions. Investigations using human cell cultures also provided encouraging results, says Esser-von Bieren: “We paid particular attention to the effects on certain human immune cells known as macrophages. Constant activation of macrophages results in chronic inflammation. By adding Hpb glutamate dehydrogenase we were able to significantly reduce the pro-inflammatory activity of the macrophages. Here the substance turns out to have greater efficacy than cortisone.”

    However, Esser-von Bieren points out that there is still a long way to go before a finished medication can be produced: “We're in the pre-clinical phase and still have to address a number of questions, for example how the worm protein is received by cells in the respiratory tract and what the overall effects on the human immune system are.”

    More information:

    In addition to scientists from TUM and the Helmholtz Zentrum München, researchers from Goethe University Frankfurt, Germany, Karolinska Institutet Stockholm, Sweden, Friedrich-Alexander-Universität Erlangen-Nürnberg (FAU), Germany, and Monash University, Australia, also participated in the project. The project was funded by the German Research Foundation (Deutsche Forschungsgemeinschaft (DFG)), the Else Kröner-Fresenius-Stiftung foundation, the Fritz Thyssen Foundation and received Helmholtz Young Investigator Group Funding from the Helmholtz Association.


    Wissenschaftliche Ansprechpartner:

    Dr. Julia Esser-von Bieren
    Technical University of Munich
    Center of Allergy and Environment (ZAUM)
    phone: +49 89 4140 3454
    julia.esser-von-bieren@tum.de


    Originalpublikation:

    M. de los Reyes Jiménez, A. Lechner, F. Alessandrini, S. Bohnacker, S. Schindela, A. Trompette, P. Haimerl, D. Thomas, F. Henkel, A. Mourão, A. Geerlof, C. Prazeres da Costa, A. M. Chaker, B. Brüne, R. Nüsing, P.-J. Jakobsson, W. A. Nockher, M. J. Feige, M. Haslbeck, C. Ohnmacht, B. J. Marsland, D. Voehringer, N. L. Harris, C. B. Schmidt-Weber, J. Esser-von Bieren: An anti-inflammatory eicosanoid switch mediates the suppression of type-2 inflammation by helminth larval products. In: Science Translational Medicine, 22 April 2020. DOI: 10.1126/scitranslmed.aay0605


    Weitere Informationen:

    https://www.tum.de/nc/en/about-tum/news/press-releases/details/35994/


    Bilder

    Merkmale dieser Pressemitteilung:
    Journalisten
    Medizin
    überregional
    Forschungsergebnisse
    Englisch


     

    Hilfe

    Die Suche / Erweiterte Suche im idw-Archiv
    Verknüpfungen

    Sie können Suchbegriffe mit und, oder und / oder nicht verknüpfen, z. B. Philo nicht logie.

    Klammern

    Verknüpfungen können Sie mit Klammern voneinander trennen, z. B. (Philo nicht logie) oder (Psycho und logie).

    Wortgruppen

    Zusammenhängende Worte werden als Wortgruppe gesucht, wenn Sie sie in Anführungsstriche setzen, z. B. „Bundesrepublik Deutschland“.

    Auswahlkriterien

    Die Erweiterte Suche können Sie auch nutzen, ohne Suchbegriffe einzugeben. Sie orientiert sich dann an den Kriterien, die Sie ausgewählt haben (z. B. nach dem Land oder dem Sachgebiet).

    Haben Sie in einer Kategorie kein Kriterium ausgewählt, wird die gesamte Kategorie durchsucht (z.B. alle Sachgebiete oder alle Länder).