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Hendrikx Group

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  4. Hendrikx Group

Tim Hendrikx, PhD

© private

Group Leader

Medical University of Vienna,
Department of Laboratory Medicine, KILM
Anna Spiegel Research Building
Lazarettgasse 14, AKH BT25.2, Level 6
1090 Vienna, Austria

ORCID: 0000-0002-3381-210

Tim Hendrikx is a molecular biologist who obtained his degree in Biomedical Sciences at the University of Hasselt, Belgium, in 2010. After his studies, he joined the lab of Prof. R. Shiri-Sverdlov at Maastricht University, where he investigated underlying molecular mechanisms of non-alcoholic fatty liver disease, and obtained his PhD degree in 2015.
Following a primary postdoctoral training period in the lab of Prof. C. Binder at the Medical University of Vienna, he joined the lab of Prof. B. Schnabl at the University of California in San Diego in early 2017 for a second postdoctoral period as part of an Erwin-Schrödinger Fellowship.
Since his return in 2019, Tim became Group Leader at the Department of Laboratory Medicine at the Medical University of Vienna.

know-how and research interests

In his work, Tim aims to improve patient healthcare by studying fundamental research questions underlying chronic liver disease pathology and working in close collaboration with clinical experts to translate his findings from animal models. In particular, his research focuses at the interface of nutrition, microbiome-host interactions and host immunity during non-alcoholic and alcohol-associated fatty liver disease, with the aim to identify novel targets for better treatment strategies and diagnostic tools. As such, he recently discovered a novel pathway by which intestinal dysbiosis affects alcohol-induced liver disease in mice and men, and showed the potential of using engineered bacteria to modulate disease outcome (Hendrikx et al., 2019). Moreover, he previously identified that IgM antibodies targeting malondialdehyde epitopes are protective in murine steatohepatitis (Hendrikx et al., 2016; Gruber et al., 2016) and that circulatory IgM titers targeting oxidation-specific epitopes are lower in patients with NAFLD (Hendrikx et al., 2016). In recent work, he described the functional role of TREM2-expressing macrophages during NAFLD and discovered that circulatory soluble TREM2 levels are useful to distinguish the different stages of fatty liver hepatitis and could serve as marker of non-alcoholic fatty liver disease (Hendrikx et al., 2022). So far, he has obtained several prestigious fellowships and awards, including an Erwin-Schrödinger Fellowship (FWF), the Dutch Veni grant (NWO), and the Zukunftkollegs grant (FWF; www.peptaides.com), and published numerous publications in high-ranked journals, including Gut, Gastroenterology, Journal of Hepatology and Hepatology.

Main Research Interests

  • Decipher the cellular and molecular mechanisms involved in the progression of chronic fatty liver diseases
  • Study the gut-liver axis during (non-)alcoholic liver disease
  • Peptide therapeutics as tool to modulate immunity during fatty liver disease