Abstract

EXCEED THE SPACE PROVIDED. It has been increasingly recognized that dysfunction in endogenous pain regulatory systems may play a role in chronic pain. An important component of the endogenous pain regulatory process is the functional interaction between the cardiovascular and pain regulatory systems, which results in an inverse relationship between resting blood pressure (BP) and acute pain sensitivity. This inverse BP/pain sensitivity relationship is believed to reflect an adaptive homeostatic feedback loop that helps restore arousal levels in the presence of painful stimuli. The inverse BP/acute pain sensitivity relationship appears to be significantly altered (i.e., reversed) in chronic pain patients. It is proposed that these alterations reflect chronic pain-related dysfunction in normal pain regulatory processes. The overall objective of the proposed project is to identify underlying mechanisms that may account for these alterations in the BPlpain sensitivity relationship in chronic pain sufferers. In pain-free normotensives, baroreceptor-mediated mechanisms and alpha-2 adrenergic descending pain inhibitory pathways appear likely to contribute to expression of the inverse blood pressure/acute pain sensitivity relationship. Chronic pain-related decreases in baroreceptor sensitivity and/or impairments in adrenergic pain inhibitory pathways are hypothesized to mediate the altered blood pressure/pain sensitivity relationship in chronic pain sufferers. Chronic pain-related activation of descending pain facilatory pathways (central sensitization) that may interact with blood pressure regulation could also contribute to this altered BP/pain sensitivity relationship. Identifying the mechanisms responsible for chronic pain-related alterations in the BP/pain sensitivity relationship will contribute to improved understanding of the role of dysfunctional pain regulatory processes in chronic pain. Sixty chronic low back pain patients and 60 pain-free controls will participate in two laboratory sessions, once under alpha-2 adrenergic blockade with yohimbine and once under placebo. During each session, resting blood pressure and spontaneous baroreceptor sensitivity will be determined, degree of central sensitization will be ascertained (reflected in temporal summation), and sensitivity to acute finger pressure, ischemic, and heat pain stimuli will be assessed. Data obtained from this protocol will be used to determine: 1) the extent to which alpha-2 adrenergic mechanisms contribute to the inverse BP/acute pain sensitivity relationship in pain-free normotensives, 2) whether chronic pain-related impairments in alpha-2 adrenergic inhibitory pathways contribute to alterations in the blood pressure/acute pain sensitivity relationship across chronic pain/pain-free groups, 3) whether changes in baroreceptor sensitivity contribute to chronic pain-related alterations in the BP/pain sensitivity relationship, and 4) whether chronic pain-related activation of pain facilatory pathways contributes to alterations in the BP/pain sensitivity relationship. PERFORMANCE SITE ========================================Section End===========================================

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
3R01NS046694-01A2S1
Application #
7093902
Study Section
Biobehavioral Mechanisms of Emotion, Stress and Health Study Section (MESH)
Program Officer
Porter, Linda L
Project Start
2004-09-15
Project End
2008-06-30
Budget Start
2004-09-15
Budget End
2005-06-30
Support Year
1
Fiscal Year
2005
Total Cost
$23,573
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Anesthesiology
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Bruehl, Stephen; Denton, Jerod S; Lonergan, Daniel et al. (2013) Associations between KCNJ6 (GIRK2) gene polymorphisms and pain-related phenotypes. Pain 154:2853-9
Bruehl, S; Burns, J W; Chung, O Y et al. (2012) What do plasma beta-endorphin levels reveal about endogenous opioid analgesic function? Eur J Pain 16:370-80
Dengler-Crish, Christine M; Bruehl, Stephen; Walker, Lynn S (2011) Increased wind-up to heat pain in women with a childhood history of functional abdominal pain. Pain 152:802-8
Bruehl, Stephen; Burns, John W; Chung, Ok Y et al. (2010) Hypoalgesia associated with elevated resting blood pressure: evidence for endogenous opioid involvement. J Behav Med 33:168-76
Bruehl, Stephen; Chung, Ok Y; Chont, Melissa (2010) Chronic pain-related changes in endogenous opioid analgesia: a case report. Pain 148:167-71
Bruehl, Stephen; Dengler-Crish, Christine M; Smith, Craig A et al. (2010) Hypoalgesia related to elevated resting blood pressure is absent in adolescents and young adults with a history of functional abdominal pain. Pain 149:57-63
Walker, Lynn S; Dengler-Crish, Christine M; Rippel, Sara et al. (2010) Functional abdominal pain in childhood and adolescence increases risk for chronic pain in adulthood. Pain 150:568-72
Bruehl, Stephen; Burns, John W; Chung, Ok Y et al. (2009) Pain-related effects of trait anger expression: neural substrates and the role of endogenous opioid mechanisms. Neurosci Biobehav Rev 33:475-91
Bruehl, Stephen; Chung, Ok Y; Burns, John W (2008) The mu opioid receptor A118G gene polymorphism moderates effects of trait anger-out on acute pain sensitivity. Pain 139:406-15
Burns, John W; Quartana, Phillip J; Bruehl, Stephen (2008) Anger inhibition and pain: conceptualizations, evidence and new directions. J Behav Med 31:259-79

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