Jennifer Wolstenholme
- Position:
Graduate Student - Ph.D.
Pharmacology and Toxicology
Neuroscience
Virginia Commonwealth University (Richmond, VA)
- Advisor:
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Degrees:
Ph.D. (in progress), Neuroscience, Virginia Commonwealth University (Richmond, VA)
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Past Advisors:
Steven E Hyman (as Technician)Robert L Chevalier (as Technician)
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Research:
I am currently researching individual variation in ethanol drinking behaviors in mice and the effects of social stress on ethanol drinking behaviors.
Alcoholism is a complex, polygenic disease affecting many neurotransmitter pathways in the brain. Both genetic and environmental factors contribute to this development of alcohol abuse. It has been estimated that genetics contributes to about half of the vulnerability to drink excessively. Studies in our laboratory and others have found persistent individual variability in rodent models of ethanol self-administration. These differences in ethanol intake and preference, in a laboratory model, may be affected by social stress since subordinate or defeated animals increase their ethanol consumption as compared to their aggressive, dominant counterparts. Inbred strains of mice, which are virtually genetically identical, have also shown such individual variation in drinking behaviors. Our experiments use an inbred mouse strain to "clamp" the genetic factors allowing us to study the effects of social stress on the individual variation of ethanol drinking behavior. It is our hypothesis that social stress causes long-lasting signaling changes in the brain that influence ethanol drinking. The proposed study uses a two-pronged approach, behavioral (two-bottle choice drinking, social stress and anxiety measurements) and molecular (DMA microarrays) assays to identify the gene networks affecting ethanol drinking behavior. Experiments will utilize a within and between subjects design. The goals of these experiments are: 1) to characterize a model of social stress in mice; 2) to identify the effects of social stress and anxiety on ethanol drinking; and 3) to identify the gene networks involved in both individual variation of drinking and the effects of social stress on the variation of drinking behavior. Using the proposed model to investigate the non-genetic factors involved in excessive alcohol drinking, we may identify novel therapeutic targets for treating alcohol abuse and alcoholism.
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Honors:
2006 Student Merit Award, Research Society on Alcoholism
2001 Public Health Service Award; NIH, NINDS, Molecular Plasticity Section
2000 Quality Step Increase; NIH, NINDS, Molecular Plasticity Section
2000 Staff Recognition Award; NIH, NINDS, Molecular Plasticity Section
Jennifer Wolstenholme's Genealogy
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Jennifer Wolstenholme's Publications (9)
Jennifer Wolstenholme's Posters and Presentations (15)
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Behavioral, genomic and genetic analysis of responses to repeated social defeat in inbred mice. (poster)
Wolstenholme JT and Miles MF
Society for Neuroscience; 11/2007 -
Brief repeated social defeat alters ethanol drinking patterns in C57BL/6 mice. (poster)
Wolstenholme JT and Miles MF
Research Society on Alcoholism; 07/2007 -
Identification of candidate genes related to individual variation in ethanol consumption. (poster)
Wolstenholme JT and Miles MF
Research Society on Alcoholism; 07/2006 -
Ania4 a dopamine-induced gene that shares high homology with doublecortin-like kinase, a microtubule-associated protein. (poster)
Lavoie, B, Wolstenholme JT, and Hyman SE
American Society for Cell Biology; 12/2001 -
Characterization of Ania-4, a dopamine-induced gene that shares high homology with the doublecortin- and CAM kinase-like family (KIAA0369). (poster)
Lavoie, B, Wolstenholme JT, and Hyman SE
Society for Neuroscience; 11/2001 -
In vivo and in vitro characterization of Ania-4, a dopamine induced gene in striatal neurons. (poster)
Lavoie B, Berke JD, Wolstenholme JT, Hyman SE.
Society for Neuroscience; 10/2000 -
Characterization of Homer (Vesl) expression in transfected organotypic striatal-cortical slices (poster)
Voulalas PJ, Wolstenholme JT, Hyman SE
Society for Neuroscience; 10/1999 -
Temporary unilateral ureteral obstruction in early development delays glomerular maturation and reduces nephron number (poster)
Kim A, Thornhill BA, Wolstenholme JT, Chevalier RL:
Society for Pediatric Research; 05/1998 -
Unilateral ureteral obstruction early development alters renal growth: dependence on duration of obstruction (poster)
Chevalier RL, Thornhill BA, Wolstenholme JT, Rudrapatna H, Kim A
American Society for Nephrology; 11/1997 -
Unique cellular responses of the developing kidney to unilateral ureteral obstruction: Role of angiotensin II. (poster)
Chevalier RL, Thornhill BA, Wolstenholme JT
American Society for Nephrology; 11/1997 -
Regulation of renal tubular cell proliferation and apoptosis by angiotensin II in the neonatal rat kidney with unilateral ureteral obstruction. (presentation)
Wolstenholme JT, Thornhill BA, Chevalier RL
Society for Pediatric Research; 05/1997 -
Sequelae of obstructive nephropathy in the neonate are attenuated by exogenous epidermal growth factor. (poster)
Goyal S, Thornhill BA, Wolstenholme JT, Chevalier RL
Society for Pediatric Research; 05/1997 -
Unilateral ureteral obstruction impairs renal antioxidant enzyme activation during sodium depletion. (poster)
Kinter M, Wolstenholme JT, Thornhill BA, Newton E, Chevalier RL:
Society for Pediatric Research; 05/1997 -
Sodium deprivation increases apoptosis resulting from unilateral ureteral obstruction in the rat. (poster)
Chevalier RL, Smith CD, Thornhill BA, Wolstenholme JT
Society for Pediatric Research; 05/1996 -
Interferon gamma may act as an autocrine or pancreatic growth factor in Burkitt’s Lymphoma by upregulating c-myc transcription via the juxtaposed immunoglobulin enhancer (poster)
Jain VK, Wolstenholme JT, Magrath IT
American Society of Hematology; 08/1992
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