Systemic administration of anti-NGF increases A-type potassium currents and decreases pancreatic nociceptor excitability in a rat model of chronic pancreatitis

Zhu, Yingdong; Mehta, Kshama; Li, Cuiping; Xu, Guiyun; Liu, Liansheng; Çolak, Tuğba Seda; Shenoy, Mohan; Pasricha, Pankaj J.

doi:10.1152/ajpgi.00053.2011

Cited by 29 publications

(26 citation statements)

References 28 publications

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“…For chronic pancreatitis, infusion of trinitrobenzene sulphonic acid (TNBS) into the pancreatic duct was used in several studies to investigate chronic-pancreatitisassociated neural alterations, particularly within the DRG. [62][63][64][65] By means of this model, substance P, CGRP, TRPV1, and the density of ion currents were shown to be augmented in the thoracic DRG that supply the pancreas, [62][63][64][65] and NGF was reported to be upregulated within the pancreas, 62 which has been previously shown in human chronic pancreatitis. 66 Electrophysiologically, the pancreas-innervating thoracic DRG neurons were reported to be hyperexcitable in the same model due to suppression of A type I (A) currents, 65 and this suppression and nociception were reversible upon systemic administration of anti-NGF antibodies.…”

Section: Th9mentioning

confidence: 53%

“…66 Electrophysiologically, the pancreas-innervating thoracic DRG neurons were reported to be hyperexcitable in the same model due to suppression of A type I (A) currents, 65 and this suppression and nociception were reversible upon systemic administration of anti-NGF antibodies. 64 Furthermore, retrograde tracing of pancreatic nerve fibres and anterograde tracing of DRG neurites in spontaneous chronic pancreatitis in the Wistar Bonn/Kobori (WBN/Kob) rat model showed that the amount of retrograde labelled DRG neurons decreased and the numbers of anterograde labelled nerve fibres in the pancreas increased during chronic pancreatitis. 67 Hence, evidence for altered and enhanced activity of sensory DRG neurons in chronic pancreatitis models exists.…”

Section: Th9mentioning

confidence: 99%

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Neural plasticity in pancreatitis and pancreatic cancer

Demir

Frieß

Ceyhan

2015

Nat Rev Gastroenterol Hepatol

169

146

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Pancreatic nerves undergo prominent alterations during the evolution and progression of human chronic pancreatitis and pancreatic cancer. Intrapancreatic nerves increase in size (neural hypertrophy) and number (increased neural density). The proportion of autonomic and sensory fibres (neural remodelling) is switched, and are infiltrated by perineural inflammatory cells (pancreatic neuritis) or invaded by pancreatic cancer cells (neural invasion). These neuropathic alterations also correlate with neuropathic pain. Instead of being mere histopathological manifestations of disease progression, pancreatic neural plasticity synergizes with the enhanced excitability of sensory neurons, with Schwann cell recruitment toward cancer and with central nervous system alterations. These alterations maintain a bidirectional interaction between nerves and non-neural pancreatic cells, as demonstrated by tissue and neural damage inducing neuropathic pain, and activated neurons releasing mediators that modulate inflammation and cancer growth. Owing to the prognostic effects of pain and neural invasion in pancreatic cancer, dissecting the mechanism of pancreatic neuroplasticity holds major translational relevance. However, current in vivo models of pancreatic cancer and chronic pancreatitis contain many discrepancies from human disease that overshadow their translational value. The present Review discusses novel possibilities for mechanistically uncovering the role of the nervous system in pancreatic disease progression.

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Section: Th9mentioning

confidence: 53%

Section: Th9mentioning

confidence: 99%

Neural plasticity in pancreatitis and pancreatic cancer

Demir

Frieß

Ceyhan

2015

Nat Rev Gastroenterol Hepatol

169

146

View full text Add to dashboard Cite

show abstract

“…Conversely, TGFβ1 antagonism can attenuate hypersensitivity and hyperalgesia in chronic pancreatitis, a painful inflammatory condition. These studies do not imply that TGFβ is the sole or even dominant contributor to nociceptive sensitization in chronic pancreatitis, where many other factors, such as NGF may also play a role [30,31]. Surprisingly, TGFβ antagonism caused hyperalgesia to noxious stimulation in naïve rats, suggesting that endogenous TGF plays a tonic modulatory effect in nociception signal processing and that the effects of TGF on nociception are likely to be complex and bimodal, as has been described for other biological consequences of TGF neutralization [32].…”

Section: Discussionmentioning

confidence: 99%

Transforming Growth Factor Beta Induces Sensory Neuronal Hyperexcitability, and Contributes to Pancreatic Pain and Hyperalgesia in Rats with Chronic Pancreatitis

Zhu¹,

Çolak

Shenoy

et al. 2012

Mol Pain

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BackgroundTransforming growth factor beta (TGFβ) is upregulated in chronic inflammation, where it plays a key role in wound healing and promoting fibrosis. However, little is known about the peripheral effects of TGFβ on nociception.MethodsWe tested the in vitro effects of TGFβ1 on the excitability of dorsal root ganglia (DRG) neurons and the function of potassium (K) channels. We also studied the effects of TGFβ1 infusion on pain responses to noxious electrical stimulation in healthy rats as well as the effects of neutralization of TGFβ1 on evoked pain behaviors in a rat model of chronic pancreatitis.ResultsExposure to TGFβ1 in vitro increased sensory neuronal excitability, decreased voltage-gated A-type K+ currents (IA) and downregulated expression of the Kv1.4 (KCNA4) gene. Further TGFβ1 infusion into the naïve rat pancreas in vivo induces hyperalgesia and conversely, neutralization of TGFβ1 attenuates hyperalgesia only in rats with experimental chronic pancreatitis. Paradoxically, TGFβ1 neutralization in naïve rats results in pancreatic hyperalgesia.ConclusionsTGFβ1 is an important and complex modulator of sensory neuronal function in chronic inflammation, providing a link between fibrosis and nociception and is a potentially novel target for the treatment of persistent pain associated with chronic pancreatitis.

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“…21 These findings emphasize a crucial role of Na v 1.7 protein which is dynamic and up-regulated in response to increased stresses. Similarly, the other cellular molecules such as KCNA4 22 and TRPV1 23 and cellular endogenous factors such as neural growth factor 23 and transforming growth factor 24 have been reported in relation to visceral hypersensitivity. Obviously, the present findings in which the molecules of Na v 1.7, Na v 1.8, KCNA4 and TRPV1 have been suggested to be associated with visceral hypersensitivity need for the further assessment under high salt feeding, based on the idea reported from Black et al 16 …”

Section: Commentmentioning

confidence: 85%

Upregulation of Na_v1.7 Through High Salt Loading

Zhu¹,

Zhu

2014

J Neurogastroenterol Motil

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Systemic administration of anti-NGF increases A-type potassium currents and decreases pancreatic nociceptor excitability in a rat model of chronic pancreatitis

Cited by 29 publications

References 28 publications

Neural plasticity in pancreatitis and pancreatic cancer

Neural plasticity in pancreatitis and pancreatic cancer

Transforming Growth Factor Beta Induces Sensory Neuronal Hyperexcitability, and Contributes to Pancreatic Pain and Hyperalgesia in Rats with Chronic Pancreatitis

Upregulation of Na_v1.7 Through High Salt Loading

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Systemic administration of anti-NGF increases A-type potassium currents and decreases pancreatic nociceptor excitability in a rat model of chronic pancreatitis

Cited by 29 publications

References 28 publications

Neural plasticity in pancreatitis and pancreatic cancer

Neural plasticity in pancreatitis and pancreatic cancer

Transforming Growth Factor Beta Induces Sensory Neuronal Hyperexcitability, and Contributes to Pancreatic Pain and Hyperalgesia in Rats with Chronic Pancreatitis

Upregulation of Nav1.7 Through High Salt Loading

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Upregulation of Na_v1.7 Through High Salt Loading