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8 results on '"Thomas J. Christopherson"'

1. The Effect of a Platelet Activating Factor Antagonist (BN 52021) on Neurologic Outcome and Histopathology in a Canine Model of Complete Cerebral Ischemia

Author

James H. Milde, Bernd W. Scheithauer, Roger E. Hofer, Thomas J. Christopherson, and William L. Lanier

Subjects
medicine.medical_specialty, Ischemia, Placebo, Brain Ischemia, Cerebral edema, Central nervous system disease, Lactones, chemistry.chemical_compound, Dogs, medicine, Animals, Platelet, Platelet Activating Factor, Platelet-activating factor, business.industry, Hemodynamics, Antagonist, medicine.disease, Disease Models, Animal, Ginkgolides, Anesthesiology and Pain Medicine, chemistry, Anesthesia, Injections, Intravenous, Histopathology, Diterpenes, business
Abstract

Background Research has demonstrated that platelet activating factor may modulate, in part, the severity of postischemic neurologic injury. The proposed mechanism involves a platelet activating factor-mediated release of cerebral cellular lipids and free fatty acids, resulting in increased cerebral edema and cell injury. The present study tested the hypothesis that a specific platelet activating factor antagonist, BN 52021, would improve neurologic outcome after 12 min of complete global cerebral ischemia in a canine model. Methods Using an established canine model of complete cerebral ischemia, dogs were assigned randomly to receive, in a blinded fashion, either 20 mg/kg BN 52021 intravenously (N = 8) or placebo (N = 7) 5 min before cerebral ischemia. After cerebral ischemia and recovery, neurologic assessment was performed by a blinded observer for 72 h. Immediately thereafter, the brains were harvested and later were evaluated histologically by a neuropathologist blinded to the treatment groups. Results Dogs were well matched for systemic physiologic variables during all portions of the study. One placebo-treated dog and one BN 52021-treated dog were not included in the statistical analysis because of failure to meet preestablished protocol criteria. BN 52021, when compared to placebo, affected neither neurologic functional recovery nor overall histopathology scores. Regional histopathology was improved in BN 52021-treated dogs in only 1 of 18 brain regions studied (i.e., the parietal cortex). When both treatment groups were combined, there was a significant correlation between neurologic function rank and histopathology rank. Conclusions The present data demonstrate that the platelet activating factor antagonist BN 52021, at a dose of 20 mg/kg intravenously given 5 min before cerebral ischemia, did not protect the brain from injury in this canine model of complete global ischemia.

Published
1993
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2. Cerebral Vascular Autoregulation and CO2 Reactivity following Onset of the Delayed Postischemic Hypoperfusion State in Dogs

Author

John D. Michenfelder, James H. Milde, and Thomas J. Christopherson

Subjects
Male, Ischemia, Brain Ischemia, Brain ischemia, Cerebral circulation, Dogs, Cerebrospinal fluid, medicine, Animals, Homeostasis, Autoregulation, business.industry, Brain, Carbon Dioxide, medicine.disease, Blood pressure, Neurology, Cerebral blood flow, Cerebrovascular Circulation, Anesthesia, Reperfusion, Female, Neurology (clinical), Animal studies, Cardiology and Cardiovascular Medicine, business
Abstract

A small number of animal studies have suggested that during the delayed postischemic hypoperfusion state, CO2 reactivity of the cerebral vasculature is lost whereas autoregulation is retained. These findings, however, are inconsistent with the bulk of experimental evidence which demonstrates that CO2 reactivity is more robust and may be retained in pathologic circumstances which abolish autoregulation. These opposing viewpoints were therefore further evaluated in 18 dogs in which complete global ischemia was induced by cerebrospinal fluid (CSF) compression for periods of 12 ( n = 12) and 18 ( n = 6) min. Following 45 min of reperfusion and with onset of the delayed postischemic hypoperfusion state, autoregulation and CO2 reactivity were evaluated using a continuous measurement of CBF (by sagittal sinus outflow). CO2 reactivity was tested over a Paco2 range of 20 to 60 mm Hg; autoregulation was tested over a blood pressure range of 60 to 140 mm Hg. Results demonstrated that after both 12 and 18 min of complete global ischemia, autoregulation and CO2 reactivity of the cerebral vasculature were both present, but attenuated. In the case of CO2 reactivity, the slope of the CBF response was decreased approximately 75%. In the case of autoregulation, the response in some dogs was incomplete as compared with their preischemic response.

Published
1993
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6. CONTRIBUTORS

Author

Martin D. Abel, Roxann D. Barnes, David R. Becker, Eric A. Bedell, Richard Belmont, Keith H. Berge, Ines H. Berger, William G. Binegar, Michael L. Bishop, Susan Black, Daniel R. Brown, Pamela Jensen-Bundy, Paul E. Carns, Renee E. Caswell, Thomas J. Christopherson, David J. Cook, Robert M. Craft, Frank D. Crowl, Roy F. Cucchiara, David R. Danielson, William J. Davis, Maria DeCastro, Ann E. Decker, Martin L. DeRuyter, Niki M. Dietz, Jerry A. Dorsch, Douglas A. Dubbink, Beth A. Elliott, John K. Erie, Scott A. Eskuri, Ronald J. Faust, Neil G. Feinglass, James Findlay, Randall P. Flick, Robert J. Friedhoff, Scott A. Gammel, Stephen T. Gott, Robert E. Grady, Brian A. Hall, Jerry A. Hall, James D. Hannon, Barry A. Harrison, Roger E. Hofer, Terese T. Horlocker, Michael P. Hosking, Paul J. Hubbell, Daniel J. Janik, Christopher J. Jankowski, Mary B. Jedd, Michael E. Johnson, Robert V. Johnson, Michael J. Joyner, Mark T. Keegan, Brian C. Kerr, Michelle A.O. Kinney, Tim J. Lamer, Theresia L. Lee, Scott A. Lockwood, Noel Lumpkin, Robert J. Lunn, Carlos B. Mantilla, David P. Martin, Brian P. McGlinch, John C. McMichan, K.A. Kelly McQueen, Pamela A. Mergens, Linda K. Miller, David R. Mumme, Donald A. Muzzi, Bradly J. Narr, Gregory A. Nuttall, Doris B. Ockert, William C. Oliver, Steven G. Peters, Susanne D. Pfeffer, Christopher Powers, Mary M. Raja la, Karen S. Reed, Guy S. Reeder, Kent H. Rehfeldt, Edwin H. Rho, Richard H. Rho, Kevin P. Ronan, Steven H. Rose, Joseph J. Sandor, Timothy S.J. Shine, Peter A. Southorn, Thomas N. Spackman, Wolf H. Stapelfeldt, Paul E. Stensrud, Michael D. Taylor, Norman E. Torres, Mark F. Trankina, Terrence L. Trentman, Claude A. Vachon, Jerald O. Van Beck, John M. Van Erdewyk, G.M.S. Vasdev, Pamela Vick, Wayne H. Wallender, David O. Warner, Mark A. Warner, Mary Ellen Warner, C. Thomas Wass, Joseph G. Weber, Mary B. Weber, Denise J. Wedel, Margaret R. Weglinski, Roger D. White, Jack L. Wilson, Lawrence J. Winikur, Gilbert Y. Wong, and Glenn E. Woodworth

Published
2002
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