Nabila Moussaoui
Institut national de la recherche agronomique
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Publication
Featured researches published by Nabila Moussaoui.
PLOS ONE | 2014
Nabila Moussaoui; Viorica Braniste; Afifa Ait-Belgnaoui; Mélissa Gabanou; Soraya Sekkal; Maïwenn Olier; Vassilia Theodorou; Pascal Martin; Eric Houdeau
Glucocorticoids (GC) contribute to human intestine ontogeny and accelerate gut barrier development in preparation to birth. Rat gut is immature at birth, and high intestinal GC sensitivity during the first two weeks of life resembles that of premature infants. This makes suckling rats a model to investigate postpartum impact of maternal separation (MS)-associated GC release in preterm babies, and whether GC sensitivity may shape MS effects in immature gut. A 4 hours-MS applied once at postnatal day (PND)10 enhanced plasma corticosterone in male and female pups, increased by two times the total in vivo intestinal permeability (IP) to oral FITC-Dextran 4 kDa (FD4) immediately after the end of MS, and induced bacterial translocation (BT) to liver and spleen. Ussing chamber experiments demonstrated a 2-fold increase of permeability to FD4 in the colon immediately after the end of MS, but not in the ileum. Colonic permeability was not only increased for FD4 but also to intact horseradish peroxidase 44 kDa in MS pups. In vivo, the glucocorticoid receptor (GR) antagonist RU486 or ML7 blockade of myosin light chain kinase controlling epithelial cytoskeleton contraction prevented MS-induced IP increase to oral FD4 and BT. In addition, the GR agonist dexamethasone dose-dependently mimicked MS-increase of IP to oral FD4. In contrast, MS effects on IP to oral FD4 and BT were absent at PND20, a model for full-term infant, characterized by a marked drop of IP to FD4 in response to dexamethasone, and decreased GR expression in the colon only compared to PND10 pups. These results show that high intestinal GC responsiveness in a rat model of prematurity defines a vulnerable window for a post-delivery MS, evoking immediate disruption of epithelial integrity in the large intestine, and increasing susceptibility to macromolecule passage and bacteremia.
Neurogastroenterology and Motility | 2018
Muriel H. Larauche; Nabila Moussaoui; Mandy Biraud; Won Ki Bae; Henri Duboc; Mulugeta Million; Yvette Taché
Water avoidance stress (WAS) induces a naloxone‐independent visceral analgesia in male rats under non‐invasive conditions of monitoring. The objective of the study was to examine the role of brain CRF signaling in acute stress‐induced visceral analgesia (SIVA).
Gastroenterology | 2017
Muriel H. Larauche; Nabila Moussaoui; Mandy Biraud; Won Ki Bae; Wendy Walwyn; Yvette Taché
Gastroenterology | 2017
Izumi Kaji; Artem Minalyan; Nabila Moussaoui; Yasutada Akiba; Jonathan D. Kaunitz; Yvette Taché; Lixin Wang
Gastroenterology | 2016
Nabila Moussaoui; Muriel H. Larauche; Mandy Biraud; Jenny Molet; Mulugeta Million; Emeran A. Mayer; Yvette Taché
Gastroenterology | 2016
Muriel H. Larauche; Mandy Biraud; Won Ki Bae; Nabila Moussaoui; Jenny Molet; Mulugeta Million; Yvette Taché
Gastroenterology | 2016
Won Ki Bae; Muriel H. Larauche; Mandy Biraud; Nabila Moussaoui; Mulugeta Million; Yvette Taché
Gastroenterology | 2016
Hung Pham; Suwan Oh; Shuping S. Wu; Nabila Moussaoui; Mandy Biraud; Muriel H. Larauche; Oscar U. Scremin; Mulugeta Million
Gastroenterology | 2016
Jonathan P. Jacobs; Nabila Moussaoui; Muriel H. Larauche; Mandy Biraud; Yvette Taché
Gastroenterology | 2016
Muriel H. Larauche; Mandy Biraud; Nabila Moussaoui; Won Ki Bae; Henri Duboc; Mulugeta Million; Honghui Liang; Yvette Taché