Vascular abnormalities in reflex sympathetic dystrophy (CRPS I): mechanisms and diagnostic value

doi:10.1093/brain/124.3.587

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Brain, Vol. 124, No. 3, 587-599, March 2001
© 2001 Oxford University Press

Vascular abnormalities in reflex sympathetic dystrophy (CRPS I): mechanisms and diagnostic value

Gunnar Wasner, Jörn Schattschneider, Klaus Heckmann, Christoph Maier and Ralf Baron

Klinik für Neurologie, Christian-Albrechts-Universität, Kiel, Germany

Correspondence to: Professor Dr med. Ralf Baron, Klinik für Neurologie, Christian-Albrechts-Universität Kiel, Niemannsweg 147, 24105 Kiel, Germany E-mail: r.baron@neurologie.uni-kiel.de

Complex regional pain syndrome type I (CRPS I, formerly knownas reflex sympathetic dystrophy) is a painful neuropathic disorderthat develops after trauma affecting the limbs without overtnerve injury. Clinical features are spontaneous pain, hyperalgesia,impairment of motor function, swelling, changes in sweating,and vascular abnormalities. In this study, the pathophysiologicalmechanisms of vascular abnormalities were investigated. Furthermore,the incidence, sensitivity and specificity of side differencesin skin temperature were defined in order to distinguish patientswith definite CRPS I from patients with extremity pain of otherorigin. In 25 CRPS I patients and two control groups (20 healthysubjects and 15 patients with other types of extremity pain),cutaneous sympathetic vasoconstrictor activity was altered tonicallyby the use of controlled thermoregulation. Whole-body temperaturechanges were induced with a thermal suit in which cold or hotwater circulated. The vascular reflex response (skin blood flow,laser Doppler flowmetry, skin temperature, infrared thermometry)was analysed to quantify sympathetic outflow. Measurements wereperformed during a complete thermoregulatory cycle, i.e. duringthe entire spectrum of sympathetic vasoconstrictor activityfrom high (whole-body cooling) to low sympathetic activity (whole-bodywarming). Venous noradrenalin levels were determined bilaterallyin five CRPS patients. (i) Three distinct vascular regulationpatterns were identified related to the duration of the disorder.In the `warm' (acute) type of regulation, the affected limbwas warmer and perfusion values were higher than in the contralaterallimb during the entire spectrum of sympathetic activity. Inthe `intermediate' type of regulation the limb was either warmeror colder. In the `cold' (chronic) type of regulation, skintemperature and perfusion values were lower on the affectedside during the entire spectrum of sympathetic vasoconstrictoractivity. (ii) Noradrenalin levels were lower on the affectedside, even in chronic patients with considerable cutaneous vasoconstriction.(iii) Temperature and blood flow differences between the twosides were dynamic and most prominent at a high to medium levelof vasoconstrictor activity. (iv) In both control groups, therewere only minor side differences in flow and temperature. Inconclusion, it is suggested that, in CRPS I, unilateral inhibitionof sympathetic vasoconstrictor neurones leads to a warmer affectedlimb in the acute stage. Secondary changes in neurovasculartransmission may lead to vasoconstriction and cold skin in chronicCRPS I, whereas sympathetic activity is still depressed. Vascularabnormalities are dynamic. The maximal skin temperature differencethat occurs during the thermoregulatory cycle distinguishesCRPS I from other extremity pain syndromes with high sensitivityand specificity.

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