Tom Kiner
Medical College of Wisconsin
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Journal of Applied Physiology | 2009
Katie Krause; Hubert V. Forster; S. Davis; Tom Kiner; Joshua M. Bonis; L. G. Pan; B. Qian
There are widespread chemosensitive areas in the brain with varying effects on breathing. In the awake goat, microdialyzing (MD) 50% CO(2) at multiple sites within the medullary raphe increases pulmonary ventilation (Vi), blood pressure, heart rate, and metabolic rate (Vo(2)) (11), while MD in the rostral and caudal cerebellar fastigial nucleus has a stimulating and depressant effect, respectively, on these variables (17). In the anesthetized cat, the pre-Bötzinger complex (preBötzC), a hypothesized respiratory rhythm generator, increases phrenic nerve activity after an acetazolamide-induced acidosis (31, 32). To gain insight into the effects of focal acidosis (FA) within the preBötzC during physiological conditions, we tested the hypothesis that FA in the preBötzC during wakefulness would stimulate breathing, by increasing respiratory frequency (f). Microtubules were bilaterally implanted into the preBötzC of 10 goats. Unilateral MD of mock cerebral spinal fluid equilibrated with 6.4% CO(2) did not affect Vi, tidal volume (Vt), or f. Unilateral MD of 25 and 50% CO(2) significantly increased Vi and f by 10% (P < 0.05, n = 10, 17 trials), but Vt was unaffected. Bilateral MD of 6.4, 25, or 50% CO(2) did not significantly affect Vi, Vt, or f (P > 0.05, n = 6, 6 trials). MD of 80% CO(2) caused a 180% increase in f and severe disruptions in airflow (n = 2). MD of any level of CO(2) did not result in any significant changes in mean arterial blood pressure, heart rate, or Vo(2). Thus the data suggest that the preBötzC area is chemosensitive, but the responses to FA at this site are unique compared with other chemosensitive sites.
Journal of Applied Physiology | 2009
Katie Krause; Suzanne Neumueller; B. D. Marshall; Tom Kiner; Joshua M. Bonis; L. G. Pan; B. Qian; Hubert V. Forster
Opioids are clinically important in the alleviation of pain. An undesirable side effect of opioids is depression of breathing. Data from isolated preparations suggest this effect is due to attenuation of discharge activity of neurons in the pre-Bötzinger complex (preBötzC), a medullary area with respiratory rhythmogenic properties. The purpose of this study was to examine how [d-Ala(2),N-Me-Phe(4),Gly(5)-ol]-enkephalin (DAMGO), a mu-opioid receptor agonist, affected breathing after injection into the presumed preBötzC of the adult awake goat. We hypothesized that DAMGO would cause breathing to decrease and become irregular when injected into the presumed preBötzC and the surrounding region of the conscious animal. We further hypothesized that ventilatory sensitivity to CO(2) and hypoxia would be blunted after the injection of DAMGO. Microtubules were bilaterally implanted into the presumed preBötzC of 10 adult female goats. After recovery from the surgery, DAMGO (0.5-10 mul, 1 nM-10 muM) was injected into the presumed preBötzC during the awake state. DAMGO had no effect on pulmonary ventilation [inspiratory minute ventilation (Vi)], respiratory rhythm and pattern, the activation pattern of inspiratory and expiratory muscles, or arterial blood gases during eupneic breathing conditions (P > 0.10). However, DAMGO attenuated (P < 0.05) the evoked increase in breathing frequency when inspired CO(2) was increased, and DAMGO attenuated the Vi response to reduction of inspired O(2) to 10.8% (P < 0.05). We conclude that our data do not provide support for the concept that in awake mammals opioid depression of breathing is due to a directed action of opioids on preBötzC neurons.
Journal of Applied Physiology | 2010
Joshua M. Bonis; Suzanne Neumueller; Katie Krause; Tom Kiner; Al Smith; B. D. Marshall; B. Qian; L. G. Pan; Hubert V. Forster
For many years, acetylcholine has been known to contribute to the control of breathing and sleep. To probe further the contributions of cholinergic rostral pontine systems in control of breathing, we designed this study to test the hypothesis that microdialysis (MD) of the muscarinic receptor antagonist atropine into the pontine respiratory group (PRG) would decrease breathing more in animals while awake than while in NREM sleep. In 16 goats, cannulas were bilaterally implanted into rostral pontine tegmental nuclei (n = 3), the lateral (n = 3) or medial (n = 4) parabrachial nuclei, or the Kölliker-Fuse nucleus (KFN; n = 6). After >2 wk of recovery from surgery, the goats were studied during a 45-min period of MD with mock cerebrospinal fluid (mCSF), followed by at least 30 min of recovery and a second 45-min period of MD with atropine. Unilateral and bilateral MD studies were completed during the day and at night. MD of atropine into the KFN at night decreased pulmonary ventilation and breathing frequency and increased inspiratory and expiratory time by 12-14% during both wakefulness and NREM sleep. However, during daytime studies, MD of atropine into the KFN had no effect on these variables. Unilateral and bilateral nighttime MD of atropine into the KFN increased levels of NREM sleep by 63 and 365%, respectively. MD during the day or at night into the other three pontine sites had minimal effects on any variable studied. Finally, compared with MD of mCSF, bilateral MD of atropine decreased levels of acetylcholine and choline in the effluent dialysis fluid. Our data support the concept that the KFN is a significant contributor to cholinergically modulated control of breathing and sleep.
Advances in Experimental Medicine and Biology | 2010
Hubert V. Forster; Katie Krause; Tom Kiner; Suzanne Neumueller; Josh Bonis; B. Qian; L. G. Pan
Abrupt destruction of >70% of the pre-Bötzinger complex (preBötzC) in awake goats results in terminal apnea (Wenninger et al. 2004b). Herein we report data on awake and sleeping goats in which the preBötzC was incrementally destroyed by injection of ibotenic acid (IBO) in increasing volumes at weekly intervals. All injections resulted in an acute tachypnea and dysrhythmia featuring apneas and increased variation in breathing. In studies at night, 10-15 hours after the injections, apneas were nearly all central and occurred during the awake state and variation in breathing was greater while awake than during NREM sleep. However, one week after the final IBO injection, the breathing pattern, breath-to-breath variation, and arterial blood gases were unchanged from baseline, indicating recovery. Histology revealed more than 90% destruction of the preBötzC region, and greater than 80% destruction of the surrounding area. We conclude: (1) the dysrhythmic effects on breathing acutely after the injection are state-dependent, and (2) after incremental, near-complete destruction of the preBötzC region, time-dependent plasticity within the respiratory network provides a normal respiratory rhythm that sustains normal arterial blood gases.
Archive | 2015
Katie Krause; H. V. Forster; Tom Kiner; S. Davis; Joshua M. Bonis; B. Qian; John D. Bukowy; Asem O. Daghistany; Matthew R. Hodges; Hubert V. Forster; Justin Miller; Suzanne Neumueller; Samantha Olesiak; L. G. Pan; Clarissa Muere; Justin Robert Miller
Archive | 2015
L. G. Pan; Hubert V. Forster; Joshua M. Bonis; S. E. Neumueller; Katie Krause; Tom Kiner; Al Smith; B. D. Marshall; H. V. Forster; Clarissa Muere; Suzanne Neumueller; Justin Miller; Samantha Olesiak; Matthew R. Hodges
The FASEB Journal | 2010
Josh Bonis; Suzanne Neumueller; B. D. Marshall; Katie Krause; Tom Kiner; Alex J. Smith; L. G. Pan; Hubert V. Forster
The FASEB Journal | 2010
Josh Bonis; Suzanne Neumueller; Katie Krause; Tom Kiner; Alex J. Smith; B. D. Marshall; L. G. Pan; Hubert V. Forster
Archive | 2010
Matthew R. Hodges; Paul Martino; S. Davis; C. Opansky; L. G. Pan; Hubert V. Forster; Joshua M. Bonis; Suzanne Neumueller; Kurt L. Krause; Tom Kiner; Ashlee L. Smith; Brandon D. L. Marshall; Bin-Zhi Qian; George B. Richerson; Ryan W. Bavis; Kevin J. Barry; Matthew R. Boller; Eung Kweon Kim; Petra M. Klein; Alida R. Ovrutsky
The FASEB Journal | 2009
Joshua M. Bonis; Suzanne Neumueller; Katie Krause; Tom Kiner; Al Smith; B. Qian; L. G. Pan; Hubert V. Forster