Abstract

BackgroundDepressive symptoms and reduced quality of life (QOL) are parts of the chronic stress syndrome and predictive of adverse outcome in patients with ischemic heart disease (IHD). Chronic stress is associated with increased sensitivity for pain, which can be measured by algometry as Pressure Pain Sensitivity (PPS) on the sternum.AimTo evaluate if stress focus by self-measurement of PPS, followed by stress reducing actions including acupressure, can decrease depressive symptoms and increase psychological well-being in people with stable IHD.DesignObserver blinded randomized clinical trial over 3 months of either intervention or treatment as usual (TAU). Statistical analysis: Intention to treat.MethodsTwo hundred and thirteen participants with IHD were included: 106 to active treatment and 107 to TAU. Drop-out: 20 and 12, respectively. The active intervention included self-measurement of PPS twice daily followed by acupressure as mandatory action, aiming at a reduction in PPS. Primary endpoint: change in depressive symptoms as measured by Major depression inventory (MDI). Other endpoints: changes in PPS, Well-being (WHO-5) and mental and physical QOL (SF-36).ResultsAt 3 months PPS decreased 28%, to 58, in active and 11%, to 72, in TAU, p<0.001. MDI decreased 22%, to 6.5, in active group vs. 12%, to 8.3 in TAU, p = 0.040. WHO-5 increased to 71.0 and 64.8, active group and TAU, p = 0.015. SF-36 mental score sum increased to 55.3 and 53.3, active and TAU, p = 0.08.ConclusionsPPS measurements followed by acupressure reduce PPS, depressive symptoms and increase QOL in patients with stable IHD.Trial RegistrationClinicalTrials.gov NCT01513824

Highlights

  • The bidirectional interaction between depression and ischemic heart disease (IHD) has been documented numerous times and is generally accepted [1]

  • Pressure Pain Sensitivity (PPS) measurements followed by acupressure reduce PPS, depressive symptoms and increase quality of life (QOL) in patients with stable IHD

  • Twenty dropouts (19%) were reported in the active group and 12 (11%) in the treatment as usual (TAU) group, p = 0.18. (Fig. 1) Drop outs were similar to those who completed with regard to sex, age, Major depression inventory (MDI) and WHO-5 scores

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Summary

Introduction

The bidirectional interaction between depression and ischemic heart disease (IHD) has been documented numerous times and is generally accepted [1]. After an acute myocardial infarction (MI) the risk of being depressed is approximately 3 times increased as compared with the general population [2]. In out-patients the 12month odds ratio of major depression has been found to be 2.3 times higher in individuals with cardiac disease as compared with those with no medical illness [3]. Depression, quality of life and general well-being is all part of the chronic stress concept [6]. Depressive symptoms and reduced quality of life (QOL) are parts of the chronic stress syndrome and predictive of adverse outcome in patients with ischemic heart disease (IHD). Chronic stress is associated with increased sensitivity for pain, which can be measured by algometry as Pressure Pain Sensitivity (PPS) on the sternum

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