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| ProtIG is an NIH Special Interest Group (SIG) that organizes seminars and workshops in relevant areas of proteomics, including talks on separation and protein identification methods, determination of post-translational modifications, protein-protein interactions, and bioinformatics and data management. A monthly seminar series is usually held at 12 pm on the Second Thursday of each month (always check the Mtgs/Seminars button on this page for these and other PROTIG announced meetings). To receive email announcements of ProtIG events, join the listserv (Join the SIG button on this page) |
| January ProtIG Seminar |
| Thursday, January 15th, 2026 |
| 11:00 am - 12:00 pm ET |
| NIH Building 50 |
| Room 1227/1233 |
| Peter Lund, Ph.D. |
| Assistant Professor Department of Nutrition Department of Pharmacology School of Medicine, Case Western Reserve University Member, Molecular Oncology Program, Case Comprehensive Cancer Center |
| "Fatty acid metabolism as a symbiotic link between the gut microbiota and host epithelial cells" |
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The intestinal epithelium is a critical mucosal barrier that confines the gut microbiota to the lumen, preventing these generally beneficial microbes from invading host tissues and triggering overt inflammation. While gut homeostasis requires this physical separation of the microbiota and host, it also depends on symbiotic interactions between them, which often occur through small molecule metabolites. For instance, by converting indigestible fiber into short-chain fatty acids (SCFA), the microbiota provides colonic epithelial cells with a fuel source to power fatty acid oxidation (FAO) and energy production. Accordingly, intestinal tissues from germ-free mice show signs of energy deprivation, and the clinical significance of this metabolic integration is evident from studies correlating inflammatory bowel disease (IBD) with impaired FAO and changes in microbiota composition. However, the mechanisms by which these alterations could contribute to IBD remain unclear, highlighting the need to understand the pathways linking epithelial cell metabolism with microbial metabolism and whether disruptions in this symbiosis could promote inflammation. In a recent study to investigate metabolic contributions from the microbiota to the host, we performed stable isotope tracing in a mouse model and found that acetylated histones and numerous metabolites in epithelial cells contain microbiota-derived carbon. Treatment with DSS, a chemical irritant that induces inflammation, suppressed the isotopic labeling of molecules bearing fatty acid chains, coinciding with shifts in microbiota composition and decreased expression of genes related to FAO. In ongoing work, we are employing cell and organoid models to trace the anabolic and catabolic pathways by which epithelial cells metabolize microbiota-derived carbon. Overall, we aim to generate mechanistic insight into how metabolic interactions between the gut microbiota and host promote tissue homeostasis and how a disruption in this symbiosis may contribute to the development of IBD.
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This seminar will be videocast on
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Seminars will be webcast online and available on the
Proteomics Interest Group website http://proteome.nih.gov as an archived presentation unless otherwise noted. |
This site was updated on January 12th, 2026. Please contact Renee Olano at olanol(at)mail.nih.gov with questions or suggestions.