Kirk Johnson
Novartis
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Publication
Featured researches published by Kirk Johnson.
Shock | 1998
Roy D. Goldfarb; Dana Glock; Kirk Johnson; Abla A. Creasey; Christina Carr; Robert J. McCarthy; Marian Matushek; Imran Akhter; Gordon M. Trenholme; Joseph E. Parrillo
ABSTRACT This study tested the hypothesis that tissue factor pathway inhibitor (TFPI) would improve mortality and morbidity evoked by peritonitis-induced bacteremia in pigs. Secondarily, it sought to determine if TFPI treatment would attenuate cardiodynamic abnormalities produced by this septic model. 32 pigs were chronically instrumented with intracardiac transducers to measure left ventricular pressure and diameter, pulmonary and aortic pressures, and cardiac output. At least 5 days after surgery to implant transducers, basal cardiovascular readings and blood samples were obtained. Using a randomized, blinded study design, either purified, reconstituted TFPI (1 mg/kg bolus, 10 mg/kg/min for 48 h), placebo (arginine buffer), or saline was administered to pigs immediately after Escherichia coli 0111.B4 (3.0–11 ± 109 colony-forming U/kg)-laden fibrin clots were implanted intraperitoneally, producing peritonitis and bacteremia. Pigs did not receive antibiotics or supportive therapy. No significant differences in primary or secondary endpoints were noted between the arginine and saline groups, so these data were combined into a control group (N = 20). 5 of 12 TFPI pigs survived (42%), while 5 of 20 control pigs survived (25%); this difference was not significant (p = .714, Fishers exact test). TFPI treatment augmented cardiac output in surviving pigs, but did not affect any other cardiovascular performance variable (heart rate, % diameter shortening, or systemic and pulmonary vascular resistance). In controls, peritonitis induced rapid increase in plasma tumor necrosis factor-± (428 ± 771 to 5,933 ± 559 pg/mL at 2 h) and interleukin-8 (180 ± 153 to 1,393 ± 145 pg/mL at 2 h). TFPI treatment significantly attenuated cytokine responses to sepsis, reducing peak tumor necrosis factor-± to 2,103 ± 813 pg/mL and reducing peak interleukin-8 levels to 534 ± 211 pg/mL at 2 h (p < .05, Tukey test, two-way ANOVA). In conclusion, TFPI treatment attenuated important mediator components of the inflammatory response but did not provide significant survival benefit.
Diabetes | 2002
Gary W. Cline; Kirk Johnson; Werner Regittnig; Pascale Perret; Effie Tozzo; Linda Xiao; Christine Damico; Gerald I. Shulman
Proceedings of the National Academy of Sciences of the United States of America | 1993
Carol Beadling; Kirk Johnson; Kendall A. Smith
Proceedings of the National Academy of Sciences of the United States of America | 1988
Kirk Johnson; Bruce H Davis; Kendall A. Smith
Archive | 1995
Kirk Johnson; Abla A. Creasey; Lucien A. Aarden
Methods | 1994
Kirk Johnson; Russ Granzow; Abla A. Creasey; Thomas L. Ciardelli
Thrombosis and Haemostasis | 1998
Kirk Johnson; Isabel Zaror; Diane Bauer; Yoon Choi; Abla A. Creasey; Michael A. Innis
Archive | 2003
David Duhl; William H. Ii Frey; Kirk Johnson; Jian Luo; Effie Tozzo; Linda Li Xiao; Baoji Xu
Archive | 2003
David Duhl; William H. Ii Frey; Kirk Johnson; Jian Luo; Effie Tozzo; Linda Li Xiao; Baoji Xu
Archive | 2001
Paul A. Renhowe; Daniel Chu; Rustum Boyce; Zhi-Jie Ni; David Duhl; Effie Tozzo; Kirk Johnson; David Myles