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1. Pruritogenic mechanisms and gut sensation: putting the "irritant" into irritable bowel syndrome.

2. Activation of pruritogenic TGR5, MrgprA3, and MrgprC11 on colon-innervating afferents induces visceral hypersensitivity.

3. Colonic afferent input and dorsal horn neuron activation differs between the thoracolumbar and lumbosacral spinal cord.

4. Co-expression of μ and δ opioid receptors by mouse colonic nociceptors.

5. NaV1.1 inhibition can reduce visceral hypersensitivity.

6. Cyclic analogues of α-conotoxin Vc1.1 inhibit colonic nociceptors and provide analgesia in a mouse model of chronic abdominal pain.

7. α-Conotoxin Vc1.1 inhibits human dorsal root ganglion neuroexcitability and mouse colonic nociception via GABA B receptors.

8. Linaclotide inhibits colonic nociceptors and relieves abdominal pain via guanylate cyclase-C and extracellular cyclic guanosine 3',5'-monophosphate.

9. Sprouting of colonic afferent central terminals and increased spinal mitogen-activated protein kinase expression in a mouse model of chronic visceral hypersensitivity.

10. Olorinab (APD371), a peripherally acting, highly selective, full agonist of the cannabinoid receptor 2, reduces colitis-induced acute and chronic visceral hypersensitivity in rodents.

11. NaV1.1 inhibition can reduce visceral hypersensitivity

12. NaV1.6 regulates excitability of mechanosensitive sensory neurons.

13. Voltage‐gated sodium channels: (NaV)igating the field to determine their contribution to visceral nociception.

14. Contribution of membrane receptor signalling to chronic visceral pain.

15. Olorinab (APD371), a peripherally acting, highly selective, full agonist of the cannabinoid receptor 2, reduces colitis-induced acute and chronic visceral hypersensitivity in rodents

16. Activation of pruritogenic TGR5, MrgprA3, and MrgprC11 on colon-innervating afferents induces visceral hypersensitivity

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