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"Tag des Hundes“, 3. Juni 2018

Judit Fazekas-Singer aus dem Jensen-Jarolim Lab generierte in ihrer PhD Arbeit ein Immunglobulin der Klasse IgE, welches bei Hunden mit Krebserkrankung eingesetzt werden kann.[more]

 

Alum-adjuvanted allergoids induce functional blocking antibodies

Reithofer M, Böll SL, Kitzmüller C, Horak F, Sotoudeh M, Bohle B, Jahn-Schmid B. Clin Exp Allergy. 2018 Feb 12. doi: 10.1111/cea.13120[more]

 

Fusion proteins of flagellin and the major birch pollen allergen Bet v 1 show enhanced immunogenicity, reduced allergenicity, and intrinsic adjuvanticity.

Claudia Kitzmüller, Julia Kalser, Sonja Mutschlechner, Michael Hauser, Gerhard J. Zlabinger, Fatima Ferreira und Barbara Bohle J Allergy Clin Immunol. 2018 Jan;141(1):293-299.e6. [more]

 

Isolation of a high affinity Bet v 1-specific IgG-derived ScFv from a subject vaccinated with hypoallergenic Bet v 1 fragments

Elisabeth Gadermaier, Katharina Marth, Christian Lupinek, Raffaela Campana, Gerhard Hofer, Katharina Blatt, Dubravka Smiljkovic, Uwe Roder, Margarete Focke-Tejkl, Susanne Vrtala, Walter Keller, Peter Valent, Rudolf Valenta,...[more]

 

Franziska Roth-Walter from Erika Jensen-Jarolim´s team authored an article in Metallomics on the great impact of lipocalins and their interplay with iron from the blood.

LINK:http://xlink.rsc.org/?DOI=C7MT00241F)[more]

 

Interessante Neuigkeiten auf dem Gebiet AllergoOnkologie!

Mehrere MitarbeiterInnen des Instituts für Pathophysiologie und Allergieforschung sind an einem kürzlich erschienenen Positionspapier der EAACI TaskForce "AllergoOncology" beteiligt, die den aktuellen Wissensstand zum Thema...[more]

 

Characterization of the T cell response to Dau c 1, the Bet v 1-homolog in carrot.

Nora Zulehner, Birgit Nagl, Peter Briza, Anargyros Roulias, Barbara Ballmer-Weber, Gerhard J. Zlabinger, Fatima Ferreira und Barbara Bohle Allergy. 2017;72:244-251. doi: 10.1111/all.12938. Epub 2016 Jun 10. [more]

 
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Inhaltsbereich

AID/APOBECs among important factors in body’s defence against SARS-CoV-2

Research team comprising Anastasia Meshcheryakova, Diana Mechtcheriakova and Peter Pietschmann from the Institute of Pathophysiology and Allergy Research has addressed the potential interrelations between AID/APOBECs and the SARS-CoV-2 virus, particularly in connection with the course of COVID-19 in different patients. This could provide a starting point for future clinical strategies to improve and strengthen individual antiviral response.

Together with their multifaceted action mechanisms, activation-induced cytidine deaminase (AID) and so-called APOBEC proteins are important factors in the body's immune response and offer fast and effective protection against a large number of DNA and RNA viruses. The task of AID is to strengthen the human immune response, while APOBECs are able to block the virus.

The defence mechanisms associated with AID/APOBECs in response to the coronavirus were assessed on the basis of integrative data mining and gene expression analyses, as part of a study conducted with international partners. It was found that members of the APOBEC family are preferentially expressed in a particular type of cell or tissue: "However, this does not mean that a particular cell type only expresses a particular member of the APOBEC family but that each cell type exhibits its own characteristic APOBEC repertoire," explains Diana Mechtcheriakova.

What is completely new is that the researchers found that APOBEC4 is highly expressed in cells and tissues that are points of attack for SARS-CoV-2. These include epithelial cells in the bronchi, in the lungs, in the trachea and in the nose. It was also found that there is an extremely high level of expression of both molecules (one of the members of the APOBEC family and ACE2, the entry receptor for SARS-CoV-2), in the gastrointestinal tract, in the heart and in the testis.

"Based on this knowledge, the clinical challenge in the future will be to characterise the antiviral cell status attributed to AID/APOBECs specific to patients and/or patient groups and to correlate the cell-type-specific AID/APOBEC gene expression signature with the organs affected by SARS-CoV-2 infection and the severity of COVID-19," explains Mechtcheriakova.

A particular role in this process is attributed to AID, since it co-determines the strength of an adaptive immune response. "The AID-driven, highly coordinated sequence of events, which all occur in specialised immunological lymphoid structures with germinal centres, results in the production of high-affinity antibodies by plasma cells or memory B cells. These antibodies are directed against the pathogen causing the disease, such as SARS-CoV-2, either in the course of infection or of an immune response to a vaccine," explains Anastasia Meshcheryakova. The role of these complex lymphoid structures and of AID is of great importance for our further understanding of the pathobiology of COVID-19, and consequently for the development of new therapeutic approaches.

The results of the study have now been published in the journal "Frontiers in Immunology”. The study was funded by the "Medical and Scientific fund of the Mayor of the Federal Capital Vienna", the " Foundation Fund to Promote the Fight against Tuberculosis and other Lung Diseases" as part of the special SARS-CoV-2/COVID-19 call.

Service: Frontiers in Immunology, Viral Immunology
"AID and APOBECs as multifaceted intrinsic virus-restricting factors: emerging concepts in the light of COVID-19." Anastasia Meshcheryakova, Peter Pietschmann, Philip Zimmermann, Igor B. Rogozin and Diana Mechtcheriakova. Front. Immunol. doi:10.3389/fimmu.2021.690416.

Link to the paper

https://www.frontiersin.org/articles/10.3389/fimmu.2021.690416/full

Link to MedUni NEWS

https://www.meduniwien.ac.at/web/ueber-uns/news/2021/news-im-juli-2021/aid/apobecs-als-wichtiger-teil-der-koerpereigenen-abwehr-gegen-sars-cov-2/

 

 

 
 
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