Abstract

While many pain syndromes are thought to have a vascular component, the underlying mechanisms remain elusive. Previous studies have provided strong evidence for a role of mediators that can be released by endothelial cells which line the lumen of blood vessels, but mechanisms by which endothelial cells themselves could dynamically participate in pain generation have not been described. We recently discovered a novel mechanism which drives an active contribution of vascular endothelial cells to peripheral hyperalgesia. This phenomenon, referred to as stimulus-dependent hyperalgesia (SDH) can be elicited by two vasoactive compounds, endothelin-1 (ET-1) and epinephrine, acting at their cognate receptors on the endothelial cell to produce a state in which mechanical stimulation now produces release of ATP that, in turn, acts on P2X3 receptors on sensory neurons. This discovery was made possible by our innovative adaptation of two independent methods from the cardiovascular and renal vascular literature to attenuate endothelial cell function at the site of nociceptive testing: treatment with octoxynol-9 and methionine-induced hyperhomocysteinemia. This grant application outlines experiments to investigate the cellular mechanisms of SDH and to explore the potential role of this or other endothelial cell mechanisms in vascular pain syndromes. In the first Specific Aim, we will investigate mechanisms of SDH including: 1) the role of the endothelial cell in SDH, 2) endothelial cell mediators involved in SDH and mechanisms by which they are released from the endothelial cell, 3) second messenger pathways in endothelial cells involved in SDH, and 4) which nociceptors mediate SDH. In contrast to Specific Aim 1 which probes cellular mechanisms by which vascular endothelial cells actively participate in particular mechanism of SDH, the second Specific Aim will more generally examine the role of the endothelial cell in models of clinical pai syndromes with a vascular component, not limited to the SDH mechanism.
This aim will also evaluate the endothelial cell as a possible target of existing treatments for vascular pain syndromes (e.g., triptans and ?-blockers) the mechanisms of which are not fully understood. Furthermore, since stress is a major factor in clinical pain conditions in which blood vessels are thought to play a role, we will study the impact of neuroendocrine stress axis mediators on endothelialdependent pain in such syndromes. By elucidating the endothelial cell contribution to pain, these studies have the potential to identify novel targets for the development of pharmacological treatments of vascular pain syndromes.

Public Health Relevance

Pain syndromes associated with vascular dysfunction, such as migraine headache, Raynaud's, angina and work-related pain, are common and difficult to treat, greatly impacting an individual's health and wellbeing. We have recently shown that the vascular endothelial cell, which provides an interface between circulating inflammatory cells and sensory nerve fibers that signal pain, plays a key role in peripheral pain mechanisms, and that the potent vasoactive peptide, endothelin, produces pain by acting both on pain nerve fibers and on endothelial cells. Knowledge of the role of endothelin and endothelial cells in preclinical models of vascular pain syndromes and underlying mechanisms will provide a better understanding of the role of blood vessels in vascular pain syndromes, and a rationale for approaches to the treatment of patients with these conditions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS085831-03
Application #
9096900
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Oshinsky, Michael L
Project Start
2014-08-01
Project End
2019-07-31
Budget Start
2016-08-01
Budget End
2017-07-31
Support Year
3
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Dentistry
Type
Schools of Dentistry/Oral Hygn
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94118

  Publications

Araldi, Dionéia; Ferrari, Luiz F; Levine, Jon D (2018) Mu-opioid Receptor (MOR) Biased Agonists Induce Biphasic Dose-dependent Hyperalgesia and Analgesia, and Hyperalgesic Priming in the Rat. Neuroscience 394:60-71
Araldi, Dionéia; Ferrari, Luiz F; Levine, Jon D (2018) Role of GPCR (mu-opioid)-receptor tyrosine kinase (epidermal growth factor) crosstalk in opioid-induced hyperalgesic priming (type II). Pain 159:864-875
Ferrari, Luiz F; Khomula, Eugen V; Araldi, Dioneia et al. (2018) CD44 Signaling Mediates High Molecular Weight Hyaluronan-Induced Antihyperalgesia. J Neurosci 38:308-321
Araldi, Dioneia; Ferrari, Luiz F; Green, Paul et al. (2017) Marked sexual dimorphism in 5-HT1 receptors mediating pronociceptive effects of sumatriptan. Neuroscience 344:394-405
Ferrari, L F; Levine, J D; Green, P G (2016) Mechanisms mediating nitroglycerin-induced delayed-onset hyperalgesia in the rat. Neuroscience 317:121-9
Ferrari, L F; Araldi, D; Bogen, O et al. (2016) Extracellular matrix hyaluronan signals via its CD44 receptor in the increased responsiveness to mechanical stimulation. Neuroscience 324:390-8
Araldi, Dioneia; Ferrari, Luiz F; Levine, Jon D (2016) Gi-protein-coupled 5-HT1B/D receptor agonist sumatriptan induces type I hyperalgesic priming. Pain 157:1773-82
Bogen, Oliver; Bender, Olaf; Löwe, Jana et al. (2015) Neuronally produced versican V2 renders C-fiber nociceptors IB4 -positive. J Neurochem 134:147-55
Ferrari, Luiz F; Levine, Jon D (2015) Plasma membrane mechanisms in a preclinical rat model of chronic pain. J Pain 16:60-6
Green, Paul G; Alvarez, Pedro; Levine, Jon D (2015) Topical Tetrodotoxin Attenuates Photophobia Induced by Corneal Injury in the Rat. J Pain 16:881-6

Showing the most recent 10 out of 19 publications