Eric Wolford
Research Triangle Park
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Publication
Featured researches published by Eric Wolford.
International Journal of Clinical Practice | 2007
M. Naslund; Alicia Gilsenan; Kirk Midkiff; A. Bown; Eric Wolford; J. Wang
Purpose: Men with lower urinary tract symptoms (LUTS) from benign prostatic hyperplasia often do not discuss their symptoms with their primary care physicians (PCPs). The primary objectives of this study were to estimate the prevalence of LUTS, prostate enlargement, and prostate‐specific antigen (PSA) ≥ 1.5 ng/ml in men visiting their PCP and to assess patients’ intent to discuss LUTS with their PCP.
International Journal of Antimicrobial Agents | 2002
Iris H. Hall; Ute Schwab; E. Stacy Ward; John D. Butts; Eric Wolford; Timothy J. Ives
Uptake of [14C]-azithromycin into THP-1 human monocytes was determined at pH 7.4, 6.8 or 5.5 over 4-log antibiotic concentrations for 24 h under a number of conditions. Stimulation of cells was with bacteria, latex beads, lipopolysaccharide (LPS), or zymogen A. Subcellular organelle disposition was determined after isolation by ultracentrifugation or sucrose gradients. Hydrolytic enzyme activities and mediators of intracellular inflammation (IL-1, IL-6, IL-8, and TNFalpha) were assessed. Azithromycin uptake into human THP-1 monocytes was initially linear achieving approximately 2% of the extracellular concentration. At pH 7.4, uptake was both passive- and carrier-mediated, but as the pH became more acidic, the uptake was exclusively passive. The intracellular concentration was not pH-dependent over 24 h. Uptake was dependent upon temperature but not the presence of foetal calf serum. Intracellular disposition in zymogen A-stimulated and unstimulated cells was throughout all compartments of the cell, but was higher in the nucleus and cell sap. Phagosomes of stimulated cells contained higher level of the antibiotic. Efflux from THP-1 monocytes was complete between 3 and 4 h. After 1 h treatment with zymogen A, THP-1 monocytes demonstrated an increase in intracellular acidity, protein kinase C, SOD and NAG activities, and NO, H(2)O(2), TNFalpha and IL-1 release over the 1st h. After 2-4 h the pH became alkaline, activities of NADPH reductase, NAG and cathepsin were reduced, and the release of NO, H(2)O(2), TNFalpha and IL-6 were suppressed. Protein synthesis and killing of the bacteria was evident in bacteria kept in monocyte-free medium and those phagocytized by the THP-1 monocytes moderately at 2 h, but more significantly at 24 h. The early killing of the bacteria appears to be a cidal mechanism whereas later, a standard bacteriostatic mechanism was evident. Nevertheless, suppression of these chemical mediators and hydrolytic enzyme activities would reduce the infection and the spread to adjacent areas.
Urology | 2004
Claus G. Roehrborn; Leonard S. Marks; Tom Fenter; Sheldon Freedman; John P. Tuttle; Marc Gittleman; Betsy Morrill; Eric Wolford
Contemporary Clinical Trials | 2007
Neil Fleshner; Leonard G. Gomella; Michael S. Cookson; Antonio Finelli; Andrew Evans; Samir S. Taneja; M. Scott Lucia; Eric Wolford; Matthew C. Somerville; Roger S. Rittmaster
The Journal of Urology | 2007
Leonard S. Marks; Claus G. Roehrborn; Eric Wolford; Timothy H. Wilson
AORN Journal | 1997
John D. Butts; Eric Wolford
The Journal of Urology | 2006
Claus G. Roehrborn; Michael Marberger; Eric Wolford; Timothy H. Wilson
The Journal of Urology | 1999
Claus G. Roehrborn; Peter Boyle; Hoda Gabriel; Stuart Hobbs; Timothy H. Wilson; Eric Wolford; Richard V. Clark
The Journal of Urology | 2007
Michael J. Naslund; Alicia Gilsenan; Kirk Midkiff; Eric Wolford; Aileen Bown; Jianmin Wang
Urology | 2006
Claus G. Roehrborn; M. Marberger; Eric Wolford; Timothy Wilson