Fetal Origin of Chronic Immune Disease: Role of Prenatal Stress Challenge

Jago, Caitlin A.

Please use this identifier to cite or link to this item: http://hdl.handle.net/11375/12068

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DC Field	Value	Language
dc.contributor.advisor	Arck, Petra	en_US
dc.contributor.advisor	Ashkar, Ali	en_US
dc.contributor.advisor	Khalil Karimi, Mark Larché	en_US
dc.contributor.author	Jago, Caitlin A.	en_US
dc.date.accessioned	2014-06-18T16:58:08Z	-
dc.date.available	2014-06-18T16:58:08Z	-
dc.date.created	2012-04-05	en_US
dc.date.issued	2012	en_US
dc.identifier.other	opendissertations/6985	en_US
dc.identifier.other	7937	en_US
dc.identifier.other	2728461	en_US
dc.identifier.uri	http://hdl.handle.net/11375/12068	-
dc.description	<p>NB: I had another committee member, Dr. Mark Larché; and would like to have his name included in the document.</p> <p>Thank you.</p>	en_US
dc.description.abstract	<p><strong>Introduction: </strong>Increasing incidence of chronic immune diseases are mirrored by changing disease risk factors, which include maternal stress during pregnancy. To date, no studies have investigated the impact of prenatal stress challenge (PNS) on the fetal immune system. Fetal liver and bone marrow represent major sources of hematopoietic stem cells (HSC) at mid gestation, which differentiate and mature in the thymus. Disturbance of immune development may cause immune impairment in later life. Further, progesterone is recognized as a critical part of feto-maternal interaction. This study aimed to determine if PNS interferes with normal fetal immune development in mice and the impact of progesterone supplementation on stress effects. <strong>Methods: </strong>DBA/2J-mated BALB/c dams were sorted into three groups: control, PNS (gestation days (GDs) 12.5 and 14.5) and PNS plus progesterone supplementation (DHD). Fetal tissue was collected on GDs 16.5 and 18.5. Flow cytometric analysis examined frequency and phenotype of fetal immune cell populations: HSC in fetal liver and bone marrow, and different stages of T cell maturation and regulatory T (Treg) cells in the thymus. Fetal tails were collected to determine fetal sex by PCR analysis. <strong>Results: </strong>PNS induced a decrease in organ size on GD16.5, which was not seen on GD18.5 and was reversed by DHD treatment. PNS altered the percentage and absolute number of HSC within the liver and bone marrow populations, on GD16.5 and 18.5. There was a significant lag in T cell maturation as demonstrated by the altered expression of CD3 and skewed CD3-:CD3+ ratio. There was a significant decrease in Treg cells within CD3+ thymic cells in response to PNS. PNS effects in the thymus were ameliorated by DHD treatment. There was no PNS-induced sex bias. <strong>Conclusions: </strong>These results indicate that PNS compromises the developing fetal immune system, which could account for impaired immune responses in adults with chronic immune disease, and provide evidence for a therapeutic role of progesterone supplementation.</p>	en_US
dc.subject	Fetal Programming	en_US
dc.subject	Progesterone	en_US
dc.subject	Immune Ontogeny	en_US
dc.subject	Regulatory T Cells	en_US
dc.subject	Hematopoietic Stem Cells	en_US
dc.subject	Allergy and Immunology	en_US
dc.subject	Biological Phenomena, Cell Phenomena, and Immunity	en_US
dc.subject	Hemic and Immune Systems	en_US
dc.subject	Immune System Diseases	en_US
dc.subject	Maternal and Child Health	en_US
dc.subject	Medical Immunology	en_US
dc.subject	Other Immunology and Infectious Disease	en_US
dc.subject	Allergy and Immunology	en_US
dc.title	Fetal Origin of Chronic Immune Disease: Role of Prenatal Stress Challenge	en_US
dc.type	thesis	en_US
dc.contributor.department	Medical Sciences	en_US
dc.description.degree	Master of Science (MSc)	en_US
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