| Literature DB >> 31042485 |
Kacy Greenhalgh1, Javier Ramiro-Garcia1, Almut Heinken1, Pit Ullmann2, Tamara Bintener2, Maria Pires Pacheco2, Joanna Baginska1, Pranjul Shah1, Audrey Frachet1, Rashi Halder1, Joëlle V Fritz1, Thomas Sauter2, Ines Thiele3, Serge Haan2, Elisabeth Letellier2, Paul Wilmes4.
Abstract
By modulating the human gut microbiome, prebiotics and probiotics (combinations of which are called synbiotics) may be used to treat diseases such as colorectal cancer (CRC). Methodological limitations have prevented determining the potential combinatorial mechanisms of action of such regimens. We expanded our HuMiX gut-on-a-chip model to co-culture CRC-derived epithelial cells with a model probiotic under a simulated prebiotic regimen, and we integrated the multi-omic results with in silico metabolic modeling. In contrast to individual prebiotic or probiotic treatments, the synbiotic regimen caused downregulation of genes involved in procarcinogenic pathways and drug resistance, and reduced levels of the oncometabolite lactate. Distinct ratios of organic and short-chain fatty acids were produced during the simulated regimens. Treatment of primary CRC-derived cells with a molecular cocktail reflecting the synbiotic regimen attenuated self-renewal capacity. Our integrated approach demonstrates the potential of modeling for rationally formulating synbiotics-based treatments in the future.Entities:
Keywords: colorectal cancer; gut microbiome; gut-on-a-chip; modeling; nutritional therapy; prebiotic; probiotic; symbiotic
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Year: 2019 PMID: 31042485 DOI: 10.1016/j.celrep.2019.04.001
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423