Biphasic modulation by galanin of excitatory synaptic transmission in substantia gelatinosa neurons of adult rat spinal cord slices

Yue, Haosong; Fujita, Teizo; Kumamoto, Eiichi

doi:10.1152/jn.00991.2010

Cited by 26 publications

(40 citation statements)

References 62 publications

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“…This effect appears to be mediated by GAL 2 , presumably located on terminals of primary afferents and DH neurons, because it is mimicked by low-dose galanin (2-11), but not the GAL 1 preferential agonist M617 (Yue et al, 2011). Conversely, it was demonstrated that galanin (2-11) decreases spontaneous EPSC frequency (Alier et al, 2008).…”

Section: Painmentioning

confidence: 95%

“…Ablation of primary afferent innervation into the spinal cord does not appear to significantly decrease galanin binding (indicative of galanin receptor expression/levels) in the spinal cord, suggesting galanin receptors are present mainly on postsynaptic neurons (Kar and Quirion, 1994;Zhang et al, 1998). However, more recent studies imply that galanin also functions presynaptically in the DH, likely via GAL 2 (Alier et al, 2008;Yue et al, 2011). It is noteworthy that galanin and galanin receptor binding have also been detected in monkey DRG and spinal cord (Zhang et al, 1993a(Zhang et al, , 1995a, and galanin is expressed in human DRG (Landry et al, 2003).…”

Section: Painmentioning

confidence: 98%

“…Conversely, it was demonstrated that galanin (2-11) decreases spontaneous EPSC frequency (Alier et al, 2008). Furthermore, galanin or galanin (2-11) both reduce nociceptor stimulation-evoked EPSC amplitudes, indicative of decreased primary afferent glutamate release (Alier et al, 2008;Yue et al, 2011). Galanin produces variable dose-dependent effects on postsynaptic currents in both excitatory and inhibitory lamina II neurons; GAL 1 agonism appears to predominantly cause hyperpolarization (Yue et al, 2011), and highdose galanin (2-11) decreases membrane excitability (Alier et al, 2008;Yue et al, 2011).…”

Section: Painmentioning

confidence: 99%

“…Furthermore, galanin or galanin (2-11) both reduce nociceptor stimulation-evoked EPSC amplitudes, indicative of decreased primary afferent glutamate release (Alier et al, 2008;Yue et al, 2011). Galanin produces variable dose-dependent effects on postsynaptic currents in both excitatory and inhibitory lamina II neurons; GAL 1 agonism appears to predominantly cause hyperpolarization (Yue et al, 2011), and highdose galanin (2-11) decreases membrane excitability (Alier et al, 2008;Yue et al, 2011). Overall, the effect of galanin in the spinal cord is likely to be determined by several factors, including the sensitivity of the receptors to galanin, the phenotype of the receptorbearing neurons (e.g., neurotransmitter content and electrophysiological properties), and the local circuitry in the DH.…”

Section: Painmentioning

confidence: 99%

See 3 more Smart Citations

Physiology, Signaling, and Pharmacology of Galanin Peptides and Receptors: Three Decades of Emerging Diversity

et al. 2014

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Section: Painmentioning

confidence: 95%

Section: Painmentioning

confidence: 98%

Section: Painmentioning

confidence: 99%

Section: Painmentioning

confidence: 99%

See 2 more Smart Citations

Physiology, Signaling, and Pharmacology of Galanin Peptides and Receptors: Three Decades of Emerging Diversity

et al. 2014

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“…Galanin produced a biphasic dose-dependent effect on spinal nociceptive excitability. In pain processing, the activation of postsynaptic GAL1 extent anti-nociceptive actions with decrease membrane excitability of dorsal horn neurons at high doses, while the activation of presynaptic GAL2 media pro-nociceptive action at low doses (28,29). Spinal parvalbumin(PV) positive cells mainly distribute in lamina I-III.…”

Section: Gabaergic Neuronal Circuit In Spinal Dorsal Hornmentioning

confidence: 99%

The Inhibitory Neuronal Circuit of Spinal Cord in Neuropathic Pain

Fu¹,

Wang²

2016

J Anesth Perioper Med

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Aim of review:Inhibitory interneurons, including GABAergic neurons and glycine neurons, regulate nociceptive information and non-nociceptive information in spinal dorsal horn. Emerging evidence showed that disinhibition of inhibitory interneurons of neuronal circuit in spinal dorsal horn is a pivotal mechanism of neuropathic pain after nerve injury. Method: In this view, we summarized the recent researches of the structure of inhibitory neurons in spinal dorsal horn and disinhibition of inhibitory interneurons after nerve injury and discussed the primary mechanism. Recent findings: Much progress has been made with the construction of inhibitory neuronal network in spinal dorsal horn and the dysfunction of inhibitory interneurons in these networks since inhibitory interneurons in spinal dorsal horn firstly integrate nociceptive information and non-nociceptive information from primary afferent fiber and separate non-nociceptive stimuli from nociceptive information. Disinhibitory of inhibitory interneurons underlies hyperalgesia and allodynia after nerve injury. Summary: Loss of inhibitory function of neurons in inhibitory network in the dorsal horn contributes to hyperalgesia and allodynia. The findings of these inhibitory networks provide a new evidence for preventing and curing neuropathic pain.ABSTRACT N europathic pain is a challenge for clinicians because the treatment of neuropathic pain is still unsatisfactory. Therefore, increasing understanding of the mechanisms that underlie neuropathic pain will be beneficial for the discovery of new molecular therapy targets. The gate control theory of pain is one of important mechanisms of pain. The theory is the idea that physical pain is modulated by interaction between different neurons. According to the postulate of Melzack and Wall (1), the nerve fibers project to the substantia gelatinosa (SG) of the dorsal horn and the first central transmission cells of the spinal cord. Inhibitory interneurons in the SG act as the gate and determine which signals should reach the T cells and then go further through the spinothalamic tract to reach the brain. Thus, spinal inhibitory interneurons play an important role in maintaining normal pain. Spinal dorsal horn is the first site of integration of nociceptive and nonnociceptive information within the central nervous system (CNS). Under normal physiological conditions, spinal inhibitory interneurons, including gammaaminobutyric acid (GABA) neurons and glycine neurons, form axo-axonic contacts with the termination of primary afferent fiber (PAF), exerting presynaptic inhibition control over sensory transmission. Meanwhile, these inhibitory interneurons generate postsynaptic inhibi-

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Actions of a novel water-soluble benzodiazepine-receptor agonist JM-1232(−) on synaptic transmission in adult rat spinal substantia gelatinosa neurons

Uemura

Fujita

Saito³

et al. 2012

Biochemical and Biophysical Research Communications

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Biphasic modulation by galanin of excitatory synaptic transmission in substantia gelatinosa neurons of adult rat spinal cord slices

Cited by 26 publications

References 62 publications

Physiology, Signaling, and Pharmacology of Galanin Peptides and Receptors: Three Decades of Emerging Diversity

Physiology, Signaling, and Pharmacology of Galanin Peptides and Receptors: Three Decades of Emerging Diversity

The Inhibitory Neuronal Circuit of Spinal Cord in Neuropathic Pain

Actions of a novel water-soluble benzodiazepine-receptor agonist JM-1232(−) on synaptic transmission in adult rat spinal substantia gelatinosa neurons

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