Your search keyword '"Ouwerkerk, Janneke P."' showing total 4 results

1. Akkermansia muciniphila Reduces Peritonitis and Improves Intestinal Tissue Wound Healing after a Colonic Transmural Defect by a MyD88-Dependent Mechanism

Author

Bachmann, Radu, primary, Van Hul, Matthias, additional, Baldin, Pamela, additional, Léonard, Daniel, additional, Delzenne, Nathalie M., additional, Belzer, Clara, additional, Ouwerkerk, Janneke P., additional, Repsilber, Dirk, additional, Rangel, Ignacio, additional, Kartheuser, Alex, additional, Brummer, Robert Jan, additional, De Vos, Willem M., additional, and Cani, Patrice D., additional

Published

2022

2. Comparative Genomics and Physiology of Akkermansia muciniphila Isolates from Human Intestine Reveal Specialized Mucosal Adaptation

Author

Ouwerkerk, Janneke P., primary, Tytgat, Hanne L. P., additional, Elzinga, Janneke, additional, Koehorst, Jasper, additional, Van den Abbeele, Pieter, additional, Henrissat, Bernard, additional, Gueimonde, Miguel, additional, Cani, Patrice D., additional, Van de Wiele, Tom, additional, Belzer, Clara, additional, and de Vos, Willem M., additional

Published

2022

3. Comparative Genomics and Physiology of Akkermansia muciniphila Isolates from Human Intestine Reveal Specialized Mucosal Adaptation

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, Ouwerkerk, Janneke P., Tytgat, Hanne L. P., Elzinga, Janneke, Koehorst, Jasper, Van den Abbeele, Pieter, Henrissat, Bernard, Gueimonde, Miguel, Cani, Patrice D., Van de Wiele, Tom, Belzer, Clara, de Vos, Willem M., UCL - SSS/LDRI - Louvain Drug Research Institute, Ouwerkerk, Janneke P., Tytgat, Hanne L. P., Elzinga, Janneke, Koehorst, Jasper, Van den Abbeele, Pieter, Henrissat, Bernard, Gueimonde, Miguel, Cani, Patrice D., Van de Wiele, Tom, Belzer, Clara, and de Vos, Willem M.

Abstract

Akkermansia muciniphila is a champion of mucin degradation in the human gastrointestinal tract. Here, we report the isolation of six novel strains from healthy human donors and their genomic, proteomic and physiological characterization in comparison to the type-strains A. muciniphila MucT and A. glycaniphila PytT. Complete genome sequencing revealed that, despite their large genomic similarity (>97.6%), the novel isolates clustered into two distinct subspecies of A. muciniphila: Amuc1, which includes the type-strain MucT, and AmucU, a cluster of unassigned strains that have not yet been well characterized. CRISPR analysis showed all strains to be unique and confirmed that single healthy subjects can carry more than one A. muciniphila strain. Mucin degradation pathways were strongly conserved amongst all isolates, illustrating the exemplary niche adaptation of A. muciniphila to the mucin interface. This was confirmed by analysis of the predicted glycoside hydrolase profiles and supported by comparing the proteomes of A. muciniphila strain H2, belonging to the AmucU cluster, to MucT and A. glycaniphila PytT (including 610 and 727 proteins, respectively). While some intrinsic resistance was observed among the A. muciniphila straind, none of these seem to pose strain-specific risks in terms of their antibiotic resistance patterns nor a significant risk for the horizontal transfer of antibiotic resistance determinants, opening the way to apply the type-strain MucT or these new A. muciniphila strains as next generation beneficial microbes.

Published

2022

4. Akkermansia muciniphila Reduces Peritonitis and Improves Intestinal Tissue Wound Healing after a Colonic Transmural Defect by a MyD88-Dependent Mechanism.

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - (SLuc) Service de chirurgie et transplantation abdominale, UCL - (SLuc) Service d'anatomie pathologique, Bachmann, Radu, Van Hul, Matthias, Baldin, Paméla, Léonard, Daniel, Delzenne, Nathalie M., Belzer, Clara, Ouwerkerk, Janneke P, Repsilber, Dirk, Rangel, Ignacio, Kartheuser, Alex, Brummer, Robert Jan, De Vos, Willem M, Cani, Patrice D., UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - (SLuc) Service de chirurgie et transplantation abdominale, UCL - (SLuc) Service d'anatomie pathologique, Bachmann, Radu, Van Hul, Matthias, Baldin, Paméla, Léonard, Daniel, Delzenne, Nathalie M., Belzer, Clara, Ouwerkerk, Janneke P, Repsilber, Dirk, Rangel, Ignacio, Kartheuser, Alex, Brummer, Robert Jan, De Vos, Willem M, and Cani, Patrice D.

Abstract

Anastomotic leakage is a major complication following colorectal surgery leading to peritonitis, complications, and mortality. has shown beneficial effects on the gut barrier function. Whether reduces peritonitis and mortality during colonic leakage is unknown. Whether can directly modulate the expression of genes in the colonic mucosa in humans has never been studied. We investigated the effects of a pretreatment (14 days) with live prior to surgical colonic perforation on peritonitis, mortality, and wound healing. We used mice with an inducible intestinal-epithelial-cell-specific deletion of MyD88 (IEC-MyD88 KO) to investigate the role of the innate immune system in this context. In a proof-of-concept pilot study, healthy humans were exposed to for 2 h and colonic biopsies taken before and after colonic instillation for transcriptomic analysis. Seven days after colonic perforation, -treated mice had significantly lower mortality and severity of peritonitis. This effect was associated with significant improvements of wound histological healing scores, higher production of IL22, but no changes in the mucus layer thickness or genes involved in cell renewal, proliferation, or differentiation. All these effects were abolished in IEC-MyD88 KO mice. Finally, human subjects exposed to exhibited an increased level of the bacterium at the mucus level 2 h after instillation and significant changes in the expression of different genes involved in the regulation of cell cycling, gene transcription, immunity, and inflammation in their colonic mucosa. improves wound healing during transmural colonic wall defect through mechanisms possibly involving IL22 signaling and requiring MyD88 in the intestinal cells. In healthy humans, colonic administration of is well tolerated and changes the expression of genes involved in the immune pathways.

Published

2022