P01 Haller, Schwerd
Impact of exclusive enteral nutrition on microbiome signatures and function in pediatric Crohn’s disease
Crohn’s disease (CD) is one of the two main entities of idiopathic inflammatory bowel disease (IBD). Exclusive enteral nutrition (EEN) alters microbial composition and efficiently induces remission in active pediatric CD. In this tandem project, clinical trials, gnotobiotic mouse models and ex vivo organoid culture systems are implemented to understand the molecular mechanisms and functional relevance of microbiome signatures for the clinical effects of EEN. The perspective of this project is to develop a microbiome-based maintenance therapy for pediatric CD patients.
P02 Jost, Zeissig
Microbial triggers of intestinal inflammation in hosts deficient in X-linked inhibitor of apoptosis protein
Host-microbial interactions play critical roles in the pathogenesis of inflammatory bowel disease (IBD). We have recently demonstrated that loss-of-function variants in the gene encoding X-linked inhibitor of apoptosis protein (XIAP) provide the basis for a prevalent Mendelian form of IBD. Further, we observed that mice deficient in XIAP can develop spontaneous, microbiota-induced intestinal inflammation. Here, we aim to study XIAP-deficient mice as a model system to identify specific microbial triggers of intestinal inflammation in a genetically susceptible host and to delineate host pathways involved in this process.
Circadian control of microbial function in chronic intestinal inflammation
Kiessling, Silke, TUM
Disruption of intrinsic clocks, e.g. by mismatch of the external and internal daytime in shift worker, as well as microbiota dysbiosis promote the development of gastrointestinal diseases. This project examines whether the circadian clock controls daytime-dependent fluctuations of microbiota composition and function. Microbiota transfer from will test whether the loss of microbiota fluctuations plays a key role in the development of IBD. Enhancing the clock in an IBD-relevant mouse model will determine whether the circadian clock can be a target for future strategies to treat shift-work associated syndromes.
P04 Busch, Holler
T cell skewing in relation to intestinal dysbiosis and GvHD in allogeneic stem cell transplantation
The key hypothesis of this project is that microbiota dysbiosis skews the reconstitution of a regulatory immune response in the gut and both contribute to development of graft-versus-host disease (GvHD) after allogeneic stem cell transplantation (aHSTC). This connection provides the rationale for reverting dysbiosis and the loss of regulatory T cells as a potent treatment of GvHD. We aim to identify changes in microbiota signatures, mucosal lymphocyte populations and T cell receptor repertoire composition associated with clinical outcome, taking advantage of a unique collection of gut biopsies longitudinally collected over the course of GvHD onset and development, including patients before and after fecal transplantation (FMT).
P05 Poeck, Ruland
Role of innate immune signals and microbiota on intestinal epithelial regeneration in graft-versus-host disease
Innate immune signaling and gut microbiota considerably affect the outcome of graft-versus-host disease (GvHD) after allogeneic hematopoietic stem cell transplantation. Using antifungal/antibacterial regimens and unique gnotobiotic animal models in an experimental setting of GvHD, we aim to understand the contribution of specific innate immune pathways and microbiota-dependent factors on intestinal stem cell function and epithelial barrier regeneration.
P06 Biedermann, Schnieke
Mechanisms underlying intestinal microbiome orchestrated induction, maintenance and breaking of tolerance to non-self-antigens
Although humans do not express α-galactose-α-1-3-galactose (α-Gal), only a few develop allergies to α-Gal+ meat. Therefore, the role of the α Gal+ intestinal microbiome for this immune tolerance in
α-Gal-/- mice and pigs will be investigated. Using gnotobiotic animals, it will be analyzed how tolerance-associated commensals modulate the immune response and allergy to α-gal. α-Gal-allergic and tolerant adults and a cohort of newborns will be investigated for α-Gal specific immune phenotypes in dependence on the intestinal microbiome composition. The long-term goal is to develop prevention or treatment strategies against food allergies by modulating the intestinal microbiome.
P07 Ohnmacht, Zehn
Microbiota-mediated modulation of adaptive immunity
In P07, we make use of a viral infection model (LCMV) to investigate how microbial particularities of the microbiota impact the adaptive immune response to viral infections. For this purpose, we will use gnotobiotic mice colonized with natural variations of complex microbial communities and defined minimal consortia (Oligo-MM) and assess in parallel how changes in the mucosal immune system including innate immune cells and Foxp3+ regulatory T cells mechanistically impact the antigen-specific cytotoxic T cell response during acute and chronic LCMV infections.
P08 Jung, Stecher
The role of primary metabolites in the intestinal ecosystem under normal and inflamed conditions
Inflammatory processes create metabolic and trophic niches in the gut that, in turn, affect the composition and function of the microbial ecosystem. The project P08 will investigate the role of primary luminal metabolites, specifically pyruvate, and characterize the impact of pyruvate sensing and uptake on fitness and growth of Salmonella and the individual species of the microbiota using germ-free or gnotobiotic mice colonized with the minimal bacterial consortium Oligo-MM and other mouse models of gut inflammation.
P09 Deng, Gerhard
Helicobacter infection and microbiota-dependent colonic pathologies
Helicobacter pylori not only induces gastric cancer but also appears to impact colonic carcinogenesis. We hypothesize that chronic H. pylori infection induces changes in the composition of the gastrointestinal microbiota, thereby promoting carcinogenesis. We will characterize the influence of
H. pylori infection on intestinal/colonic inflammation and tumorigenesis and decipher the microbiome signatures involved. These will be further explored in H. pylori-infected patients with colonic pathologies. As a therapeutic approach, we will identify specific bacteriophages using a “viral tagging” approach and test lytic phages for the treatment of H. pylori infection in mice without disruption of the endogenous microbiota.
P10 Janssen, Zeissig
Microbiota- and TLR-dependent regulation of intestinal tumor development
Microbial factors can either promote or inhibit intestinal tumor development through activation of various TLR (toll-like-receptor)-dependent pathways. Here we aim to analyze whether specific microbial taxa are responsible for promoting tumor compared to tumor-suppressive effects in mouse models of colorectal cancer (CRC). We also aim to dissect the tumor-suppressive effects of TRIF/TLR3 signaling with the help of genetically engineered mouse models. The translational relevance of the preclinical findings will be evaluated using two large, independent human CRC cohorts.
Deciphering the role of tumor-site specific dysbiosis in subtypes of colorectal cancer
Tschurtschenthaler, Markus, TUM
We aim to decipher colorectal cancer subtype-specific bacterial risk profiles and to delineate host-microbiota interactions that are relevant for tumor-initiation and progression using mouse models of BrafV637E, KrasG12D, Pik3caH1047R and Apc1638N-driven tumors. Orthotopic transplantations of organoids derived from these mice will be performed to functionally analyze the impact of various environments, i.e. SPF, germ-free and inflammatory conditions, on tumor initiation and progression with the long-term aim of targeting tumor-promoting taxa and bacterial signals.
P12 Saur, Schnieke
Temporal and spatial analysis of the microbiome in a porcine model for colorectal cancer
An existing APC1311 porcine model of colorectal cancer will be used to study causal relationships between changes in gut microbial composition and cancer progression and regression. We will experimentally manipulate the mutational load in individual polyps by in vivo and ex vivo CRISPR/Cas9 gene editing and monitor changes in microbiome composition and in lipid and bile acid metabolism during disease progression. We will also generate a new model of inflammatory bowel disease based on the TnfDARE mouse by modifying the porcine TNF gene.
P13 Ecker, Klingenspor
We aim to reveal the role of dietary fat / microbiota interaction on lipid metabolism. Mouse models with different microbiota status and intestinal cancer susceptibility will receive diets with varying dietary fat content and lipid composition. Obesity and cancer progression will be determined and bioactive lipids identified by mass-spectrometric lipid analytics, also applying stable isotope labeled tracers. Our goal is to define dietary lipid compositions and gut microbiota communities beneficial in the suppression of obesity-driven metabolic diseases and intestinal cancer.
P14 Clavel, Stecher
Targeted design and manipulation of minimal bacterial consortia for microbial ecology of bile acid metabolism
In P14 we will study the diversity of gut bacteria involved in secondary bile acid production and investigate their impact on the host using targeted experimental models. Using defined communities of cultured bacteria and corresponding phages to manipulate them, we will dissect microbe-microbe and microbe-host interactions underlying bile acid conversion in continuous culture and gnotobiotic mouse models. We focus on testing the causal role of secondary bile acids in colorectal carcinogenesis, with further applications in chronic inflammatory models by CRC partners.
P16 Gulder, Zeller
Functional characterization of carcinogenic small molecules from the intestinal microbiota
P16 will systematically identify biosynthetic gene clusters (BGCs) in gut microbiota through in silico mining of genomic and metagenomic resources. To infer pro-inflammatory or carcinogenic effects of the encoded metabolites, we will determine statistical enrichment in metagenomes of colorectal cancer and inflammatory bowel disease patients. Promising candidate BGCs will be cloned, heterologously expressed and characterized in cell-based assays. The impact of the identified biologically relevant metabolites on the host will be evaluated in animal models with partners of the CRC. Ultimately, this project will elucidate new links between gut microbial metabolism and host disease development.
INF01 Baumbach, Lagkouvardos, Prasser
Secure integrated big data analytics
In this subproject, state-of-the-art open source software solutions will be extended and integrated to build a central platform for the secure collection and processing of clinical, para-clinical and experimental data to accelerate research and to leverage synergies. The main focuses are the characterization of microbial communities (16S rRNA and metabolomic profiling), translational data integration and analysis, systems biology as well as network biology methods for knowledge extraction, biomarker discovery and hypothesis generation.
Z01 Bleich, Clavel, Haller
Gnotobiotic mouse models and minimal bacterial consortia
Germ-free animals can be utilized to unravel the functionality of individual murine or human bacterial species, synthetic consortia or human fecal transplants in health and disease, implementing highly defined experimental conditions. In this core project, the two well-established facilities at TUM (PI Haller) and Hannover (PI Bleich) generate and maintain gnotobiotic mice. This expertise will be complemented by anaerobic bacterial cultivation techniques (PI Clavel) with the aim of tailoring novel bacterial consortia that are adapted to the specific needs of consortium members and to their implementation in gnotobiotic models.
Z02 Gessner, Quante, Steiger
Clinical integration of microbiome research
The Z02 clinical core unit supports integrative research into the clinical impact of microbiome signatures and provides a prospective, systematic and standardized sampling of biomaterial from patients to enable potential therapeutic options (e.g. FMT). Human material and datasets comprising all relevant information (i.e. nutritional, metabolic, microbiotic and immunologic), will be presented in a ready-to-use fashion in collaboration with INF01. We offer a comprehensive multiscale collection of patient data combined with digitalized histopathology, microbiome analyses of stool and tissue samples and, as well as optionally, human tissue sequencing data in a pseudonymized, research-applicable manner.
Integrated Research Training Group
Klingenspor, Martin, TUM
The Integrated Research Training Group (IRTG) will provide PhD students and postdocs with a project-related qualification program dedicated to the integration of knowledge and methodologies from multiple disciplines. It will offer training opportunities to enable cross-disciplinary approaches and promote rapid progress of the individual research projects. The IRTG will foster interaction and collaboration of CRC teams at local or distant sites. Our diverse agenda of excellent academic and hands-on training will promote self-reliance in experimental and clinical research, originality in thinking, and innovation in research.
Central tasks of the Collaborative Research Centre
Haller, Dirk, TUM
Central tasks of the CRC 1371 are coordinated and supervised by Dirk Haller in agreement with the CRC executive board. Tasks in Z04 include administrative coordination of the scientific consortia and IRTG, including the organization of CRC office, retreats, symposia, summer school, and guest lectures as well as all public relations and dissemination activities. An important task is ensuring gender equality, family and early career support. The CRC office closely interacts with the CRC-specific Gender Equality Team. Furthermore, Z04 coordinates scientific services for microbiome and metabolite profiling.