Colon mustard oil instillation induced cross-organ reflex sensitization on the pelvic–urethra reflex activity in rats

Peng, Hsien Yu; Chen, Gin Den; Tung, Kwong‐Chung; Lai, Chih-Sheng; Hsien, Ming Chun; Chiu, Chien‐Liang; Lu, Hsiao Ting; Liao, Jiuan Miaw; Lee, Shin-Da; Lin, Tzer Bin

doi:10.1016/j.pain.2008.11.017

Cited by 44 publications

(36 citation statements)

References 78 publications

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“…The right lumbosacral (L6 -S2) dorsal horns were dissected out and were immediately snap-frozen on liquid nitrogen. The protocol for Western blotting has been described elsewhere (22,23); in brief, the sample was homogenized and the extracts were centrifuged to retain supernatants. The supernatant was separated on an acrylamide gel and transferred to a polyvinylidene difluoride membrane and then were incubated for 1 h at room temperature in either rabbit antiephrinB2 (1:2,000, Santa Cruz Biotechnology), anti-phosphorylated EphB1/2 (pEphB1/2l 1:2,000, Millipore), rabbit anti-phospho-Src antibody (1:1,000, Millipore), or rabbit anti-phosphotyr1336 or anti-phosphotyr1472-NR2B (1:1,000 Millipore).…”

Section: Western Blottingmentioning

confidence: 99%

“…At the lumbosacral spinal cord, our laboratory has recently demonstrated a novel form of pain-related central sensitization, cross-organ sensitization, in which instillation of mustard oil (MO) into the descending colon could sensitize the reflex activity of the urethra (21,22). Pharmacological investigations indicated spinal NR2B subunit phosphorylation is crucial in the induction of cross-organ sensitization (19,20,23).…”

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confidence: 99%

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Endogenous ephrinB2 mediates colon-urethra cross-organ sensitization via Src kinase-dependent tyrosine phosphorylation of NR2B

Peng

Chen²,

Lai

et al. 2010

American Journal of Physiology-Renal Physiology

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Endogenous ephrinB2 mediates colon-urethra cross-organ sensitization via Src kinase-dependent tyrosine phosphorylation of NR2B. Am J Physiol Renal Physiol 298: F109 -F117, 2010. First published October 28, 2009 doi:10.1152/ajprenal.00287.2009.-Recently, the role of EphB receptor (EphBR) tyrosine kinase and their ephrinB ligands in spinal pain-related neural plasticity has been identified. To test whether Src-family non-receptor tyrosine kinase-dependent glutamatergic Nmethyl-D-aspartate receptor (NMDAR) NR2B subunit phosphorylation underlies lumbosacral spinal EphBR activation to mediate crossorgan sensitization between the colon and the urethra, external urethra sphincter electromyogram activity evoked by pelvic nerve stimulation and protein expression in the lumbosacral (L6 -S2) dorsal horn were studied before and after intracolonic mustard oil (MO) instillation. We found MO instillation produced colon-urethra reflex sensitization along with an upregulation of endogenous ephrinB2 expression as well as phosphorylation of EphB1/2, Src-family kinase, and NR2B tyrosine residues. Intrathecal immunoglobulin fusion protein of EphB1 and EphB2 as well as PP2 reversed the reflex sensitization and NR2B phosphorylation caused by MO. All these results suggest that EphBR-ephrinB interactions, which provoke Src-family kinase-dependent NMDAR NR2B phosphorylation at the lumbosacral spinal cord level, are involved in cross-organ sensitization, contributing to the development of viscero-visceral referred pain between the bowel and the urethra. pelvic pain syndrome; urethra; irritable bowel syndrome; colon; NMDA ALTHOUGH THE ETIOLOGY IS NOT fully understood, patients with irritable bowel syndrome (IBS) have a higher prevalence of lower urinary tract dysfunction with pelvic pain compared with control groups (15). In addition, pelvic visceral pain might not only arise from an inflamed/injured organ itself but might also be referred from other diseased viscera, and thus results in viscero-visceral referred pain (6). Despite the fact that bowelto-urethra cross-organ sensitization has been demonstrated previously (25), little information is available to explain the underlying mechanism because it could involve complicated interactions in afferent inputs arising from different viscera, known as central sensitization (33).It is established that spinal glutamatergic N-methyl-D-aspartate receptor (NMDAR)-dependent neurotransmission underlies pain-related central sensitization (10, 11). The NMDAR NR2B subunit, as a major unit controlling NMDAR activity via phosphorylation mechanisms, was found to play a pivot role in the NMDA-dependent form of neural plasticity at the spinal cord level (10,11,17,19,20). Chronic inflammatory pain caused by Freund's adjuvant injections was shown to be associated with increases in spinal NR2B subunit phosphorylation (10). Moreover, Slack and colleagues (28) revealed that intrathecal administration of Src-family kinase inhibitors prevented hyperalgesia-related NR2B subunit phosphorylation in the spinal dorsa...

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Section: Western Blottingmentioning

confidence: 99%

mentioning

confidence: 99%

Endogenous ephrinB2 mediates colon-urethra cross-organ sensitization via Src kinase-dependent tyrosine phosphorylation of NR2B

Peng

Chen²,

Lai

et al. 2010

American Journal of Physiology-Renal Physiology

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“…In the last decade, studies have demonstrated that the interactions between EphBRs and their ephrinB ligands modulate neural plasticity induction in the mammalian central nervous system, mainly, but not exclusively, via exhibiting effects on NMDAR (8,12). A recent study also demonstrated that, in association with thermal hyperalgesia, EphBR activation caused by immunoglobulin fusion protein of ephrinB2 (ephrinB2-Fc)-induced, Src kinase-dependent NR2B phosphorylation in the spinal cord (2), suggesting that ephrinB2-EphBR tyrosine kinase interactions could probably modulate pain signaling via spinal Src-dependent NMDAR phosphorylation (2).Although further proof is still needed for the physiological and/or pathophysiological relevance, the induction of pelvicurethra reflex potentiation (15, 16), a form of NR2B phosphorylation-dependent neural plasticity (5,25,31,41), has been linked to the development of visceral pain from pelvic organs (26,27,30,32,33). Studies have shown that the activation of nociceptive afferent fibers expressing transient receptor potential vanilloid/transient receptor potential ankyrin by the instillation of irritants into the uterus (32, 33) and the descending colon (29) facilitated pelvic-urethra reflex activity in a crossorgan manner.…”

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confidence: 99%

“…Although further proof is still needed for the physiological and/or pathophysiological relevance, the induction of pelvicurethra reflex potentiation (15, 16), a form of NR2B phosphorylation-dependent neural plasticity (5,25,31,41), has been linked to the development of visceral pain from pelvic organs (26,27,30,32,33). Studies have shown that the activation of nociceptive afferent fibers expressing transient receptor potential vanilloid/transient receptor potential ankyrin by the instillation of irritants into the uterus (32, 33) and the descending colon (29) facilitated pelvic-urethra reflex activity in a crossorgan manner.…”

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EphrinB2 induces pelvic-urethra reflex potentiation via Src kinase-dependent tyrosine phosphorylation of NR2B

Chang

Peng

et al. 2011

American Journal of Physiology-Renal Physiology

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Recently, the role of EphB receptor (EphBR) tyrosine kinase and their ephrinB ligands in painrelated neural plasticity at the spinal cord level have been identified. To test whether Src-family tyrosine kinase-dependent glutamatergic N-methyl-D-aspartate receptor NR2B subunit phosphorylation underlies lumbosacral spinal EphBR activation to mediate pelvic-urethra reflex potentiation, we recorded external urethra sphincter electromyogram reflex activity and analyzed protein expression in the lumbosacral (L6-S2) dorsal horn in response to intrathecal ephrinB2 injections. When compared with vehicle solution, exogenous ephrinB2 (5 g/rat it)-induced reflex potentiation, in associated with phosphorylation of EphB1/2, Src-family kinase, NR2B Y1336 and Y1472 tyrosine residues. Both intrathecal EphB1 and EphB2 immunoglobulin fusion protein (both 10 g/rat it) prevented ephrinB2-dependent reflex potentiation, as well as protein phosphorylation. Pretreatment with PP2 (50 M, 10 l it), an Src-family kinase antagonist, reversed the reflex potentiation, as well as Src kinase and NR2B phosphorylation. Together, these results suggest the ephrinB2-dependent EphBR activation, which subsequently provokes Src kinase-mediated N-methyl-D-aspartate receptor NR2B phosphorylation in the lumbosacral dorsal horn, is crucial for the induction of spinal reflex potentiation contributing to the development of visceral pain and/or hyperalgesia in the pelvic area. pelvic pain; urethra; Src-family kinase; N-methyl-D-aspartate IN THE LUMBOSACRAL DORSAL horn, neurotransmission mediated by glutamatergic N-methyl-D-aspartate receptors (NMDARs) has been implicated in processing nociceptive afferent inputs coming from the lower urinary tract (4, 10). Spinal administration of NMDAR agonists has dose-dependently facilitated the visceromotor reflex, together with pressor responses to pelvic noxious stimulation (14). Conversely, blockage of NMDAR using pharmacological antagonists has inhibited pain behavior caused by irritation of the pelvic viscera (24, 43). Among subunits of NMDAR, the role of the NR2B subunit in pain development has been intensively investigated, as electrophysiological studies have demonstrated that phosphorylation of specific NR2B tyrosine residues is an important determinant for NMDAR-mediated currents (22), which defines the role of NMDARs in pain-related neural plasticity (3,17,18,20). The signaling of Src kinases, a family of protooncogenic tyrosine kinases, has been shown to modulate NMDAR-mediated synaptic transmission and plasticity (1). In inflammatory animal models, the intrathecal administration of Src-family kinase inhibitors prevented spinal NR2B phosphorylation and behavior hyperalgesia, implying that Src-dependent phosphorylation of NMDAR NR2B subunits plays a crucial role in the development of postinflammatory pain and/or hyperalgesia (35).EphB receptors (EphBRs), transmembrane molecules, were initially identified as guidance cues during neural development (40). In the last decade, studies have demonstrated that the intera...

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“…Cross-sensitization between the bladder and other pelvic viscera is a clinical concern that makes diagnosing and treating the etiology difficult (Berkley, 2005, Baranowski et al, 2008, Theoharides et al, 2008, van de Merwe et al, 2008. In humans and in animals, the organs that seem to be most often involved in pelvic cross-sensitization besides bladder and colon, with respect to spinal afferents, appear to be the pelvic urethra and the uterus (Dmitrieva et al, 2001, Giamberardino et al, 2001, Dmitrieva and Berkley, 2002, Morrison et al, 2006, Peng et al, 2008a, Peng et al, 2008b, Peng et al, 2009). …”

Section: Electrophysiological Properties Of Ng Neuronsmentioning

confidence: 99%

The effect of spinal cord injury on vagal afferents.

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Colon mustard oil instillation induced cross-organ reflex sensitization on the pelvic–urethra reflex activity in rats

Cited by 44 publications

References 78 publications

Endogenous ephrinB2 mediates colon-urethra cross-organ sensitization via Src kinase-dependent tyrosine phosphorylation of NR2B

Endogenous ephrinB2 mediates colon-urethra cross-organ sensitization via Src kinase-dependent tyrosine phosphorylation of NR2B

EphrinB2 induces pelvic-urethra reflex potentiation via Src kinase-dependent tyrosine phosphorylation of NR2B

The effect of spinal cord injury on vagal afferents.

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