Differential expression of c-fos in a mouse model of fetal alcohol syndrome - 28/08/11
, Katie M Goodwin, MS b, Joanna M Hill, PhD b, Douglas E Brenneman, PhD b, Elisabetta Tendi, PhD b, Sergio Schninelli, PhD b, Catherine Y Spong, MD b
Reprint requests: Sarah H. Poggi, MD, Department of Obstetrics and Gynecology, 3PHC, 3800 Reservoir Rd, Washington, DC 20007.Washington, DC, and Bethesda, Md
Abstract |
Objective |
Fetal alcohol syndrome (FAS) results in stillbirth, fetal growth restriction, and mental retardation with injury attributed to oxidative stress. Our objective was to identify signal transduction pathways expressed in a model of FAS and to quantify expression of c-fos, a gene in the stress signal pathway.
Study design |
Timed, pregnant C57Bl6/J mice were injected on E8 with saline solution or alcohol. RNA was extracted from decidua and embryo 6 and 24 hours later. Microarray analysis was used to screen gene pathways. Differential gene expression was confirmed using real-time polymerase chain reaction with results presented as the ratio of c-fos concentration to that of glyceraldehyde-3-phosphate dehydrogenase (GAPDH).
Results |
Differential gene expression between alcohol and control was noted for stress signal pathway genes including c-fos. Real-time polymerase chain reaction demonstrated that c-fos messenger RNA expression was greater in the alcohol than control decidua at 6 hours after injection (P<.01). This effect persisted at 24 hours (P<.01). There was no difference in c-fos expression in embryos whose mothers received alcohol versus control after 6 hours (P=.12) or 24 hours (P=.89).
Conclusion |
Alcohol administration during pregnancy results in differential gene expression in the stress signal pathway, particularly in c-fos. C-fos expression in the decidua increases from 6 to 24 hours after alcohol injection, but does not change in the embryo, which may contribute to alcohol-induced damage in FAS.
Le texte complet de cet article est disponible en PDF.Keywords : Fetal alcohol syndrome, c-fos, oxidative stress, mouse
Plan
 | Presented at the Twenty-Third Annual Meeting of the Society for Maternal-Fetal Medicine, San Francisco, Calif, February 2003. |
Vol 189 - N° 3
P. 786-789 - septembre 2003 Retour au numéro
Article précédent
- Neonatal outcome after exposure to indomethacin in utero: a retrospective case cohort study
- Soraya Abbasi, Jeffrey S Gerdes, Harish M Sehdev, Sara S Samimi, Jack Ludmir
- The role of activity-dependent neuroprotective protein in a mouse model of fetal alcohol syndrome
- Sarah H Poggi, Katie Goodwin, Joanna M Hill, Douglas E Brenneman, Elizabetta Tendi, Sergio Schinelli, Daniel Abebe, Catherine Y Spong
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