Elizabeth A. Clubbs
Ohio State University
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Publication
Featured researches published by Elizabeth A. Clubbs.
Wound Repair and Regeneration | 2003
Traci A. Wilgus; Yael Vodovotz; Elena Vittadini; Elizabeth A. Clubbs; Tatiana M. Oberyszyn
Adult wound repair occurs with an initial inflammatory response, reepithelialization, and the formation of a permanent scar. Although the inflammatory phase is often considered a necessity for successful adult wound healing, fetal healing studies have shown the ability to regenerate skin and to heal wounds in a scarless manner in the absence of inflammation. The cyclooxygenase‐2 (COX‐2) enzyme, a known mediator of inflammation, has been shown to contribute to a variety of inflammatory conditions and to the development of cancer in many organs. To examine the role of COX‐2 in the wound healing process, incisional wounds were treated topically with the anti‐inflammatory COX‐2 inhibitor celecoxib. Acutely, celecoxib inhibited several parameters of inflammation in the wound site. This decrease in the early inflammatory phase of wound healing had a significant effect on later events in the wound healing process, namely a reduction in scar tissue formation, without disrupting reepithelialization or decreasing tensile strength. Our data suggest that in the absence of infection, adult wound healing is able to commence with decreased inflammation and that anti‐inflammatory drugs may be used to improve the outcome of the repair process in the skin by limiting scar formation. (WOUND REP REG 2003;11:25–34)
Nutrition and Cancer | 2009
Elizabeth A. Clubbs; Joshua A. Bomser
Increased consumption of soy and soy isoflavones is associated with a reduced risk for prostate cancer (PCa). PCa progression is characterized, in part, by a loss of luminal/basal epithelial differentiation; however, the effects of soy isoflavones on cellular differentiation in the prostate are unknown. The present study examined the effects of the soy isoflavone glycitein on cellular differentiation in prostate epithelial cells (RWPE-1, WPE1-NB14, and RWPE-2). Glycitein significantly inhibited RWPE-1 cellular proliferation at concentrations ranging from 0.4 to 50 μ M. Expression of the luminal epithelial cell marker cytokeratin 18 was not affected by glycitein treatment in the WPE1-NB14 and RWPE-2 cell lines. However, expression of cytokeratin 18 and prostate specific antigen (PSA) was decreased in the RWPE-1 cell line in response to glycitein treatment, whereas the expression of the basal epithelial cell markers p63 and cytokeratin 5 remained unchanged. These data suggest that glycitein may induce basal cell differentiation in the RWPE-1 cell line.
Chemico-Biological Interactions | 2008
Daniel Albrecht; Elizabeth A. Clubbs; Mario G. Ferruzzi; Joshua A. Bomser
Journal of Nutritional Biochemistry | 2006
Xingya Wang; Elizabeth A. Clubbs; Joshua A. Bomser
Journal of Cereal Science | 2004
Elena Vittadini; Elizabeth A. Clubbs; T.H. Shellhammer; Yael Vodovotz
Journal of Nutritional Biochemistry | 2007
Elizabeth A. Clubbs; Joshua A. Bomser
Innovative Food Science and Emerging Technologies | 2005
Elizabeth A. Clubbs; Elena Vittadini; Thomas H. Shellhammer; Yael Vodovotz
Journal of Cereal Science | 2008
Elizabeth A. Clubbs; Elena Vittadini; Thomas H. Shellhammer; Yael Vodovotz
Lipids | 2008
Kyle D. Kent; Elizabeth A. Clubbs; W. James Harper; Joshua A. Bomser
international conference on evolvable systems | 2003
Elizabeth A. Clubbs; Yael Vodovotz; Elena Vittadini; Thomas H. Shellhammer