AI Article Synopsis

  • The study investigated the effects of a lactococci strain that either produced or delivered the precursor to the antimicrobial peptide LL37 (hCAP18) in alleviating chemically induced colitis in mice.
  • Mice treated with LL-Probi-H1:hCAP18 experienced reduced colitis severity, with increased immune markers IL17A and IL10 observed in their lymph nodes.
  • Although L. lactis altered gut microbiota composition, a fecal transplant from treated mice did not improve colitis symptoms in new recipients.

Article Abstract

With its antimicrobial and immunomodulating properties, the cathelicidin (LL37) plays an important role in innate immune system. Here, we attempted to alleviate chemically induced colitis using a lactococci strain that either directly expressed the precursor to LL37, hCAP18 (LL-pSEC:hCAP18), or delivered hCAP18 cDNA to host cells under the control of the cytomegalovirus promoter (LL-Probi-H1:hCAP18). We also investigated whether the alleviation of symptoms could be explained through modification of the gut microbiota by hCAP18. Mice were administered daily doses of LL-pSEC:hCAP18 or LL-Probi-H1:hCAP18. On day 7, colitis was induced by DNBS. During autopsy, we assessed macroscopic tissue damage in the colon and collected tissue samples for the characterization of inflammation markers and histological analysis. Feces were collected at day 7 for 16S DNA sequencing. We also performed a fecal transplant experiment in which mice underwent colon washing and received feces from Lactococcus lactis-treated mice before DNBS-colitis induction. Treatment with LL-Probi-H1:hCAP18 reduced the severity of colitis symptoms. The protective effects were accompanied by increased levels of IL17A and IL10 in mesenteric lymph node cells. L. lactis administration altered the abundance of Lachnospiraceae and Muribaculaceae. However, fecal transplant from L. lactis-treated mice did not improve DNBS-induced symptoms in recipient mice.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9485145PMC
http://dx.doi.org/10.1038/s41598-022-19455-3DOI Listing

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