| Literature DB >> 18078521 |
Veronica Zaga-Clavellina1, Guadalupe Garcia-Lopez, Hector Flores-Herrera, Aurora Espejel-Nuñez, Arturo Flores-Pliego, Diana Soriano-Becerril, Rolando Maida-Claros, Horacio Merchant-Larios, Felipe Vadillo-Ortega.
Abstract
BACKGROUND: Chorioamniotic membranes infection is a pathologic condition in which an abnormal secretion of proinflammatory cytokines halts fetal immune tolerance. The aim of the present study was to evaluate the functional response of human chorioamniotic membranes, as well as the individual contribution of the amnion and choriodecidua after stimulation with Escherichia coli, a pathogen associated with preterm labor.Entities:
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Year: 2007 PMID: 18078521 PMCID: PMC2175507 DOI: 10.1186/1477-7827-5-46
Source DB: PubMed Journal: Reprod Biol Endocrinol ISSN: 1477-7827 Impact factor: 5.211
Figure 1Experimental model. The fetal membranes are held together with silicone rubber rings in the upper chamber of a Transwell® device. In this system, the choriodecidua region delimits the upper chamber and the amnion region, the lower chamber.
Figure 2In vitro secretion of IL-1β in amnion and choriodecidua regions after selective stimulation with . IL-1β secreted to the culture medium after 24 h of infection with 1 × 106 CFU of E. coli. Data were normalized in function of protein concentration (pg/μg protein) and each bar represents the 95% confidence intervals and the median (solid line) of 10 different experiments. Significant difference between basal and stimulated values is indicated (*P < 0.05) C. Choriodecidua; A. Amnion.
Figure 3In vitro secretion of IL-6 in amnion and choriodecidua regions after selective infection with . IL-6 secreted to the culture medium after 24 h of infection with 1 × 106CFU of E. coli. Data were normalized in function of protein concentration (pg/μg protein) and each bar represents the 95% confidence intervals and the median (solid line) of 10 different experiments. Significant difference between basal and stimulated values is indicated (*P < 0.05) C. Choriodecidua; A. Amnion.
Figure 4In vitro secretion of IL-10 in amnion and choriodecidua regions after selective infection with . IL-10 secreted to the culture medium after 24 h of infection with 1 × 106CFU of E. coli. Data were normalized in function of protein concentration (pg/μg protein) and each bar represents the 95% confidence intervals and the median (solid line) of 10 different experiments. Significant difference between basal and stimulated values is indicated (*P < 0.05) C. Choriodecidua; A. Amnion.
Figure 5In vitro secretion of TNF-α in amnion and choriodecidua regions after selective infection with . TNF-α secreted to the culture medium after 24 h of infection with 1 × 106 CFU of E. coli. Data were normalized in function of protein concentration (pg/μg protein) and each bar represents the 95% confidence intervals and the median (solid line) of 10 different experiments. Significant difference between basal and stimulated values is indicated (*P < 0.05) C. Choriodecidua; A. Amnion.
Figure 6In vitro secretion of IL-8 in amnion and choriodecidua regions after selective infection with . IL-8 secreted to the culture medium after 24 h of infection with 1 × 106CFU of E. coli. Data were normalized in function of protein concentration (pg/μg protein) and each bar represents the 95% confidence intervals and the median (solid line) of 10 different experiments. Significant difference between basal and stimulated values is indicated (*P < 0.05) C. Choriodecidua; A. Amnion.