Grantee Research Project Results
Validating a fetal membrane on a chip model for characterizing reproductive toxicant exposure risks
EPA Grant Number: R835736C003Subproject: this is subproject number 003 , established and managed by the Center Director under grant R835736
(EPA does not fund or establish subprojects; EPA awards and manages the overall grant for this center).
Center: Vanderbilt Pittsburgh Resource for Organotypic Models for Predictive Toxicology
Center Director: Hutson, Michael Shane
Title: Validating a fetal membrane on a chip model for characterizing reproductive toxicant exposure risks
Investigators: Osteen, Kevin G. , Bruner-Tran, Kaylon L. , Aronoff, David
Institution: University of Pittsburgh , Vanderbilt University
EPA Project Officer: Aja, Hayley
Project Period: December 1, 2014 through November 30, 2018 (Extended to November 30, 2019)
RFA: Organotypic Culture Models for Predictive Toxicology Center (2013) RFA Text | Recipients Lists
Research Category: Chemical Safety for Sustainability
Objective:
Leveraging the unique expertise available to us from the larger VPROMPT Center, the objective of Project 3 is to develop a micro-scaled, instrumented fetal membrane on a chip (IFMOC) system, which will enable higher throughput screening of multiple toxicants that may negatively impact pregnancy. We will validate this new technology using primary cultures of human fetal membranes. We have previously found that a prior toxicant exposure of human endometrial tissue exacerbates the immune response to infection. Thus, validation studies will include the examination of the IFMOC model in response to an inflammatory challenge after a toxicant exposure. We hypothesize that environmental toxicants prime the gravid uterus for exaggerated inflammatory responses to microbial invasion.
Approach:
We will initially use established human fetal membrane models (punch biopsies and within a transwell) exposed to TCDD (a toxicant known to disrupt pregnancy) to determine the optimum biomarkers indicating appropriate versus exaggerated inflammatory responses. Next, we will establish the IFMOC using commercially available human cell lines representing the heterogeneity of native human fetal membrane. The IFMOC will be exposed to >20 compounds (tested individually) and biomarkers identified above will be examined. Following these screening studies, a small subset of compounds will be analyzed again using the whole tissue fetal membrane transwell to compare to and validate the IFMOC results. Additional studies on these >20 compounds will be conducted using a liver organoid culture model placed directly upstream of the IFMOC to include the potential for hepatic detoxification and/or metabolic activation.
Expected Results:
Thousands of chemicals with unknown toxicity are present in our environment. It is not feasible to conduct human or animal studies on each of these compounds; thus higher-throughput models are needed. We expect that our IFMOC model will enable the rapid screening of a large number of toxicants which may negatively impact the maintenance of pregnancy. Prematurity is a leading cause of perinatal morbidity and mortality; thus, there is a need to understand the potential role of toxicant exposure on maternal response to infection.
Publications and Presentations:
Publications have been submitted on this subproject: View all 22 publications for this subproject | View all 169 publications for this centerJournal Articles:
Journal Articles have been submitted on this subproject: View all 11 journal articles for this subproject | View all 56 journal articles for this centerSupplemental Keywords:
toxicants, risk assessment, human health effects, reproductive effects, sensitive populations, pathophysiologyProgress and Final Reports:
Main Center Abstract and Reports:
R835736 Vanderbilt Pittsburgh Resource for Organotypic Models for Predictive Toxicology Subprojects under this Center: (EPA does not fund or establish subprojects; EPA awards and manages the overall grant for this center).
R835736C001 Mammosphere Bioreactor For Life-Stage Specific Toxicology
R835736C002 Organotypic Culture Model to Analyze DevelopmentalLimbMalformationsResulting from Toxicant/Teratogen Exposure
R835736C003 Validating a fetal membrane on a chip model for characterizing
reproductive toxicant exposure risks
R835736C004 Organotypic Liver Model for Predictive Human Toxicology and Metabolism
R835736C005 Systems Engineering & Analysis for Organotypic Culture Models
The perspectives, information and conclusions conveyed in research project abstracts, progress reports, final reports, journal abstracts and journal publications convey the viewpoints of the principal investigator and may not represent the views and policies of ORD and EPA. Conclusions drawn by the principal investigators have not been reviewed by the Agency.
Project Research Results
11 journal articles for this subproject
Main Center: R835736
169 publications for this center
56 journal articles for this center