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Literature DB >> 27436359

Facilitation of TRPV4 by TRPV1 is required for itch transmission in some sensory neuron populations.

Seungil Kim¹, Devin M Barry¹, Xian-Yu Liu¹, Shijin Yin¹, Admire Munanairi¹, Qing-Tao Meng², Wei Cheng³, Ping Mo⁴, Li Wan⁵, Shen-Bin Liu¹, Kasun Ratnayake⁶, Zhong-Qiu Zhao¹, Narasimhan Gautam⁷, Jie Zheng⁸, W K Ajith Karunarathne⁶, Zhou-Feng Chen⁹.

Abstract

The transient receptor potential channels (TRPs) respond to chemical irritants and temperature. TRPV1 responds to the itch-inducing endogenous signal histamine, and TRPA1 responds to the itch-inducing chemical chloroquine. We showed that, in sensory neurons, TRPV4 is important for both chloroquine- and histamine-induced itch and that TRPV1 has a role in chloroquine-induced itch. Chloroquine-induced scratching was reduced in mice in which TRPV1 was knocked down or pharmacologically inhibited. Both TRPV4 and TRPV1 were present in some sensory neurons. Pharmacological blockade of either TRPV4 or TRPV1 significantly attenuated the Ca(2+) response of sensory neurons exposed to histamine or chloroquine. Knockout of Trpv1 impaired Ca(2+) responses and reduced scratching behavior evoked by a TRPV4 agonist, whereas knockout of Trpv4 did not alter TRPV1-mediated capsaicin responses. Electrophysiological analysis of human embryonic kidney (HEK) 293 cells coexpressing TRPV4 and TRPV1 revealed that the presence of both channels enhanced the activation kinetics of TRPV4 but not of TRPV1. Biochemical and biophysical studies suggested a close proximity between TRPV4 and TRPV1 in dorsal root ganglion neurons and in cultured cells. Thus, our studies identified TRPV4 as a channel that contributes to both histamine- and chloroquine-induced itch and indicated that the function of TRPV4 in itch signaling involves TRPV1-mediated facilitation. TRP facilitation through the formation of heteromeric complexes could be a prevalent mechanism by which the vast array of somatosensory information is encoded in sensory neurons.

Entities: Chemical

Mesh：

Substances：

Year: 2016 PMID： 27436359 PMCID： PMC5310287 DOI： 10.1126/scisignal.aaf1047

Source DB: PubMed Journal: Sci Signal ISSN： 1945-0877 Impact factor: 9.517

58 in total

1. An N-terminal variant of Trpv1 channel is required for osmosensory transduction.

Authors: Reza Sharif Naeini; Marie-France Witty; Philippe Séguéla; Charles W Bourque
Journal: Nat Neurosci Date: 2005-12-04 Impact factor: 24.884

2. Differential regulation of TRPV1, TRPV3, and TRPV4 sensitivity through a conserved binding site on the ankyrin repeat domain.

Authors: Christopher B Phelps; Ruiqi R Wang; Shelly S Choo; Rachelle Gaudet
Journal: J Biol Chem Date: 2009-10-28 Impact factor: 5.157

Review 3. Intracellular signaling and the origins of the sensations of itch and pain.

Authors: Sang-Kyou Han; Melvin I Simon
Journal: Sci Signal Date: 2011-08-02 Impact factor: 8.192

4. Atomic force microscopy reveals the alternating subunit arrangement of the TRPP2-TRPV4 heterotetramer.

Authors: Andrew P Stewart; Graham D Smith; Richard N Sandford; J Michael Edwardson
Journal: Biophys J Date: 2010-08-04 Impact factor: 4.033

5. TRPV1 in GABAergic interneurons mediates neuropathic mechanical allodynia and disinhibition of the nociceptive circuitry in the spinal cord.

Authors: Yong Ho Kim; Seung Keun Back; Alexander J Davies; Heejin Jeong; Hyun Jung Jo; Geehoon Chung; Heung Sik Na; Yong Chul Bae; Sang Jeong Kim; Joong Soo Kim; Sung Jun Jung; Seog Bae Oh
Journal: Neuron Date: 2012-05-24 Impact factor: 17.173

6. Protease-activated receptor 2 (PAR2) protein and transient receptor potential vanilloid 4 (TRPV4) protein coupling is required for sustained inflammatory signaling.

Authors: Daniel P Poole; Silvia Amadesi; Nicholas A Veldhuis; Fe C Abogadie; TinaMarie Lieu; William Darby; Wolfgang Liedtke; Michael J Lew; Peter McIntyre; Nigel W Bunnett
Journal: J Biol Chem Date: 2013-01-03 Impact factor: 5.157

Review 7. Why we scratch an itch: the molecules, cells and circuits of itch.

Authors: Diana M Bautista; Sarah R Wilson; Mark A Hoon
Journal: Nat Neurosci Date: 2014-01-28 Impact factor: 24.884

8. Cross-inhibition of NMBR and GRPR signaling maintains normal histaminergic itch transmission.

Authors: Zhong-Qiu Zhao; Li Wan; Xian-Yu Liu; Fu-Quan Huo; Hui Li; Devin M Barry; Stephanie Krieger; Seungil Kim; Zhong-Chun Liu; Jinbin Xu; Buck E Rogers; Yun-Qing Li; Zhou-Feng Chen
Journal: J Neurosci Date: 2014-09-10 Impact factor: 6.167

9. Structural basis for toxin resistance of beta4-associated calcium-activated potassium (BK) channels.

Authors: Geliang Gan; Hong Yi; Maorong Chen; Liang Sun; Wenxin Li; Yingliang Wu; Jiuping Ding
Journal: J Biol Chem Date: 2008-06-16 Impact factor: 5.157

10. Activity-dependent silencing reveals functionally distinct itch-generating sensory neurons.

Authors: David P Roberson; Sagi Gudes; Jared M Sprague; Haley A W Patoski; Victoria K Robson; Felix Blasl; Bo Duan; Seog Bae Oh; Bruce P Bean; Qiufu Ma; Alexander M Binshtok; Clifford J Woolf
Journal: Nat Neurosci Date: 2013-05-19 Impact factor: 24.884

31 in total

Facilitation of TRPV4 by TRPV1 is required for itch transmission in some sensory neuron populations.

1. An N-terminal variant of Trpv1 channel is required for osmosensory transduction.

2. Differential regulation of TRPV1, TRPV3, and TRPV4 sensitivity through a conserved binding site on the ankyrin repeat domain.

Review 3. Intracellular signaling and the origins of the sensations of itch and pain.

4. Atomic force microscopy reveals the alternating subunit arrangement of the TRPP2-TRPV4 heterotetramer.

5. TRPV1 in GABAergic interneurons mediates neuropathic mechanical allodynia and disinhibition of the nociceptive circuitry in the spinal cord.

6. Protease-activated receptor 2 (PAR2) protein and transient receptor potential vanilloid 4 (TRPV4) protein coupling is required for sustained inflammatory signaling.

Review 7. Why we scratch an itch: the molecules, cells and circuits of itch.

8. Cross-inhibition of NMBR and GRPR signaling maintains normal histaminergic itch transmission.

9. Structural basis for toxin resistance of beta4-associated calcium-activated potassium (BK) channels.

10. Activity-dependent silencing reveals functionally distinct itch-generating sensory neurons.

1. A disease mutation reveals a role for NaV1.9 in acute itch.

2. Transient receptor potential vanilloid 4 (TRPV4) channel as a target of crotamiton and its bimodal effects.

3. TRPV4 Moves toward Center-Fold in Rosacea Pathogenesis.

4. PAR2 Mediates Itch via TRPV3 Signaling in Keratinocytes.

Review 5. Regulation of Pain and Itch by TRP Channels.

6. Modulation of Itch by Localized Skin Warming and Cooling.

Review 7. Peripheral and Central Mechanisms of Itch.

Review 8. Physiology and Pathophysiology of Itch.

Review 9. Common and discrete mechanisms underlying chronic pain and itch: peripheral and central sensitization.

10. Expression and function of the ectopic olfactory receptor OR10G7 in patients with atopic dermatitis.