Evidence for a spinal origin of the effect of baclofen on the myocardial oxygen demand indexes

Monassier, Laurent; Tibiricca, Eduardo; Roegel, Jean Christophe; Feldman, Josiane; Bousquet, Pascal

doi:10.1007/bf00169390

Cited by 2 publications

(1 citation statement)

References 45 publications

(59 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The lowest therapeutic dose was chosen based on the literature. [30][31][32][33] For the GABA A/B receptor antagonists, 1,000 µg GABA A antagonist Bicuculline (Sigma-Aldrich, USA) or 3,000 µg GABA B antagonist CGP55845 (Sigma-Aldrich) was dissolved in 2 ml normal saline and warmed to 37°C, and was infused more than 5 minutes using a syringe pump. Given that the peak dorsal horn drug concentration occurs 30 min after intrathecal administrations, each antagonist was applied 30 min before starting ischemia-reperfusion and reapplied at 60-min intervals.…”

Section: Spinal Cord Stimulationmentioning

confidence: 99%

GABAergic Signaling during Spinal Cord Stimulation Reduces Cardiac Arrhythmias in a Porcine Model

et al. 2023

View full text Add to dashboard Cite

Background Neuraxial modulation, including spinal cord stimulation, reduces cardiac sympathoexcitation and ventricular arrhythmogenesis. There is an incomplete understanding of the molecular mechanisms through which spinal cord stimulation modulates cardiospinal neural pathways. We hypothesize that spinal cord stimulation reduces myocardial ischemia/reperfusion induced sympathetic excitation and ventricular arrhythmias through γ-aminobutyric acid (GABA) mediated pathways in the thoracic spinal cord. Methods Yorkshire pigs were randomized to Control (n=11), Ischemia/reperfusion (n=16), Ischemia/reperfusion+Spinal cord stimulation (n=17), Ischemia/reperfusion+Spinal cord stimulation +GABAA or GABAB receptor antagonist (GABAA, n=8, GABAB, n=8, and Ischemia/reperfusion+GABA transaminase inhibitor (GABAculine, n=8). A 4-pole spinal cord stimulation lead was placed epidurally (T1-T4) GABA modulating pharmacologic agents were administered intrathecally. Spinal cord stimulation at 50 Hertz was applied 30-min prior to ischemia. A 56-electrode epicardial mesh was used for high-resolution electrophysiological recordings, including activation recovery intervals and ventricular arrhythmia scores.. Immunohistochemistry and Western blots were performed to measure GABA receptor expression in the thoracic spinal cord. Results Cardiac ischemia led to myocardial sympathoexcitation with reduction in activation recovery interval (mean±SD: -42 ± 11%), which was attenuated by spinal cord stimulation (-21 ± 17%, P=0.001). GABAA and GABAB receptor antagonists abolished spinal cord stimulation attenuation of sympathoexcitation (GABAA -9.7 ± 9.7%, P=0.043 vs Ischemia/reperfusion + Spinal cord stimulation. GABAB -13 ± 14%, P=0.012 vs Ischemia/reperfusion + Spinal cord stimulation), while GABAculine alone caused a therapeutic effect similar to spinal cord stimulation (-4.1 ± 3.7%, P=0.038 vs Ischemia/Reperfusion). The ventricular arrhythmia score supported the above findings. Spinal cord stimulation during ischemia/reperfusion increased GABAA receptor expression with no change in GABAB receptor expression. Conclusions Thoracic spinal cord stimulation reduces ischemia/reperfusion-induced sympathoexcitation and ventricular arrhythmias through activation of GABA signaling pathways. These data support the hypothesis that spinal cord stimulation-induced release of GABA activates inhibitory interneurons to decrease primary afferent signaling from superficial dorsal horn to sympathetic output neurons in the intermediolateral nucleus.

show abstract

Section: Spinal Cord Stimulationmentioning

confidence: 99%

GABAergic Signaling during Spinal Cord Stimulation Reduces Cardiac Arrhythmias in a Porcine Model

et al. 2023

View full text Add to dashboard Cite

show abstract

Autonomic Nervous System as a Target for Cardiovascular Drugs

Bousquet

Monassier

Feldman

1998

Clin Exp Pharma Physio

View full text Add to dashboard Cite

1. Drugs acting within the autonomic nervous system (ANS) are of particular interest when autonomic abnormalities are implicated in the development and maintenance of various cardiovascular pathologies. For example, it has been documented that in the early stages of hypertensive disease (i.e. hyperkinetic borderline hypertension) a sympathetic hyperactivity associated with a decreased parasympathetic activity results in increased cardiac output and heart rate. 2. Several classes of drugs acting within the central, as well as the peripheral ANS, are very efficient in treating hypertensive disease. One of these classes of drugs, the second generation of centrally acting drugs, has proved beneficial in this respect because, in addition to their therapeutic efficacy, these drugs are well tolerated. 3. The central nervous system may also be the target for drugs with the potential to treat other cardiovascular diseases. Some recent experimental and clinical data supporting such new perspectives concerning idiopathic dysrhythmias, angina pectoris and congestive heart failure will be summarized.

show abstract

Evidence for a spinal origin of the effect of baclofen on the myocardial oxygen demand indexes

Cited by 2 publications

References 45 publications

GABAergic Signaling during Spinal Cord Stimulation Reduces Cardiac Arrhythmias in a Porcine Model

GABAergic Signaling during Spinal Cord Stimulation Reduces Cardiac Arrhythmias in a Porcine Model

Autonomic Nervous System as a Target for Cardiovascular Drugs

Contact Info

Product

Resources

About