This project sought to investigate hepatic macrophage responses to microbes and microbial products focusing on the heterogeneity, fate, activation profile and tissue context of these cells. The objectives proposed were divided in three independent work packages (WP). In
WP1 we have profiled the different macrophage populations in the liver and have determined their fate, location, origin and specific responses during microbial insult (WP1). In WP2 we have focused on the Kupffer cells (KCs) and have investigated their specific function during microbial inflammation. Having analysed the specific response of KCs to microbial component, we have started to uncover the crosstalk between KC and their cellular in environment in WP3.
We could show that the number of resident KCs (resKCs) decreased upon exposure to the bacterial component lipopolysaccharide (LPS) which was accompanied by a concomitant increase of non-KC macrophages in the liver. While with time recruited macrophages were progressively lost from the liver, resident KC numbers recovered and reached homeostatic levels within a month after LPS challenge. Investigating the origin of these macrophages we demonstrated that the resident KCs present the liver after microbial insult were not monocyte-derived indicating that the remaining cells may have proliferated to repopulate the liver. Preliminary data showed that mice lacking an important regulatory factor specifically in KCs develop excessive systemic inflammation and display significantly decreased survival in response to LPS challenge. Here, we have identified the cellular and molecular mediators responsible for these excessive inflammatory responses. Furthermore, by using cell-specific knock-out mice we have been able to provide a better understanding of the crosstalk between KCs and endothelial cells.
We are currently preparing a manuscript to publish the findings obtained during this fellowship in a relevant journal in the coming months. In the context of his work the fellow has published a review article discussing the distinct macrophage populations present in the liver and their plasticity during hepatic inflammation (Zwicker, Bujko, Scott, Front Immunology 2021). Moreover, fellow has contributed as a co-author to a paper identifying several distinct macrophage populations and their niche in the mouse and human liver (Guilliams, Cell 2022).
Data generated during this fellowship was presented at two international conference and at departmental seminars to other experts in the field. Moreover, to reach a wider public audience the fellow has used his twitter account (@ChriZwi) to advertise publications and inform about activities of the host lab.