RELATIONSHIPS AMONG PAIN THRESHOLD, SELF-REGULATION, EXECUTIVE FUNCTIONING, AND AUTONOMIC ACTIVITY: A GENERAL INHIBITORY SYSTEM PERSPECTIVE

Boggero, Ian Andres

01 January 2013

Chronic pain patients have poorer pain inhibition, self-regulatory ability, executive functioning and autonomic inhibition than those without pain, supporting the view that suppressing pain is mentally taxing. In the current study, an alternate explanation was proposed; namely, that pain inhibition, self-regulation, executive functions, and heart rate variability (HRV) are all controlled by the same general inhibitory system. To test this hypothesis, participants came into the laboratory for three sessions. At the first session, individual differences in pain thresholds, self-regulatory strength, executive functioning, and HRV were measured. At the second and third sessions, self-regulatory persistence and within-session changes in pain thresholds were measured under conditions of high and low self-regulatory fatigue. Results revealed that those low in inhibitory strength, operationalized as the aggregate of pain inhibition, self-regulation, executive functioning, and HRV, became more sensitive to pain under conditions of self-regulatory fatigue, whereas no significant changes in pain threshold were found for those high in inhibitory strength. Additional analyses revealed that high baseline pain threshold marginally protected against the effects of self-regulatory fatigue. The findings provide some support for a general inhibitory system and suggest that physiological inhibition of pain and autonomic activity may be influenced by phasic self-regulatory fatigue.

Pain threshold

Self-Regulation

Executive Functioning

Heart Rate Variability

Inhibition

Health Psychology

Subjective Vs. Objective Physical Pain in Individuals Who Report a History of Nonsuicidal Self-Injury: A Closer Look at What it Means to Experience Pain

Sturycz, Cassandra A.

01 August 2014

Non-Suicidal Self-Injury (NSSI) is the self-inflicted damage to one’s bodily tissues without the intent to die. Previous research has sought to discover the motivation of an individual to perform such behavior and differences in the experience of pain among those who self-injure. The goals for the current study were to reveal any relationships between the function of NSSI, the subjective experience of pain, and an objective measurement of pressure pain threshold. Participants completed the Inventory of Statements About Self- Injury (ISAS; Klonsky & Glenn, 2009), which measures the functions that NSSI serves, and a measure assessing subjective pain experience, specifically frequency and severity of pain. Pain thresholds were also induced and recorded using a pressure algometer. The findings suggest that pain frequency significantly predicted pain threshold, whereas subjective pain severity did not. Furthermore, marking distress, the function of NSSI which serves as creating a tangible representation of emotional distress, was significantly associated with pain frequency, such that as marking distress increases in relevance, the less often one would be expected to experience pain. Therefore, the current study has implications relevant to both future research and the clinical setting.

Non-suicidal Self-injury

Pain Threshold Affect

Pain Managment

Applied Behavior Analysis

Child Psychology

Pain Management

Psychology

A Combination of Eccentric Muscle Exercise and Repeated Cold Stress (RCS) Induced Prolonged Hyperalgesia : An Attempt to Develop an Animal Model of Chronic Muscle Pain

TAGUCHI, Toru, SATO, Jun, MIZUMURA, Kazue

12 1900

国立情報学研究所で電子化したコンテンツを使用している。

repeated cold stress

extensor digitorum longus muscle

delayed onset muscle soreness

eccentric contraction

mechanical pain threshold

Combined oral contraceptives - impact on the vulvar vestibular mucosa and pain mechanisms /

Johannesson, Ulrika,

January 2007

Diss. (sammanfattning) Stockholm : Karolinska institutet, 2007. / Härtill 5 uppsatser.

Identification of subgroups in experimental and chronic pain : sensory, emotional and evaluative aspects /

Raak, Ragnhild,

January 2002

Diss. (sammanfattning) Linköping : Univ., 2002. / Härtill 5 uppsatser.

Pain influences somatosensory perception : an experimental and clinical study /

Leffler, Ann-Sofie,

January 1900

Diss. (sammanfattning) Stockholm : Karol. inst., 2002. / Härtill 5 uppsatser.

Local and systemic inflammatory mediators and their relation to pressure-pain threshold and pain of the temporomandibular joint /

Fredriksson, Lars,

January 2006

Diss. (sammanfattning) Stockholm : Karolinska institutet, 2006. / Härtill 5 uppsatser.

Eficácia da melatonina no tratamento da dor miofascial crônica facial : ensaio clínico randomizado, duplo-cego, controlado com placebo

Vidor, Liliane Pinto

January 2010

Cenário clínico: A síndrome dolorosa miofascial (SDM), causa comum de dor musculoesquelética, pode ser incapacitante e desafiadora terapeuticamente, devido à ineficácia dos tratamentos convencionais para dor. Intervenções terapêuticas alternativas precisam ser pesquisadas para alcançar vias do processo de doença não contempladas com a terapêutica clássica. Dentre estas, o uso da melatonina, com efeitos cronobiótico, ansiolítico e analgésico, tem se apresentado como uma opção terapêutica atrativa no tratamento da SDM, que cursa com alterações de sono, dor, sintomas depressivos e de ansiedade. Objetivos: Avaliar a eficácia da melatonina exógena na redução da dor, no limiar de dor à pressão (LDP) e na qualidade de sono de pacientes com SDM facial. Métodos e Resultados: Um estudo randomizado, controlado foi realizado em 45 mulheres com dor miofascial, com idades entre 18 e 40 anos, segundo critérios Research Diagnostic Criteria for Temporomandibular Disorder (RDC/TMD). A eficácia da melatonina oral foi avaliada na redução da dor e melhora tanto do limiar de dor a pressão (LDP) como da qualidade do sono. Os participantes foram randomizados para receber 5 mg / dia de melatonina, 5 mg / dia ciclobenzaprina, ou placebo durante um período de quatro semanas. O efeito absoluto das intervenções, apresentado como ES (tamanho do efeito) sobre a dor: placebo versus melatonina foi de 2,08 (1,17-2,97) e de ciclobenzaprina vs placebo foi de -1,25 (0,45-2,06)]. O número de pacientes necessários para tratar (NNT) para evitar a dor moderada a intensa foi 3 (95% CI, 2-4) e 18 (95% IC, 9 a a) nos grupos de melatonina e de ciclobenzaprina, respectivamente, em relação ao placebo. O ES no LDP melatonina vs placebo e ciclobenzaprina vs placebo foi de 2,72 (1,69-3,75) e 1,01 (0,23-1,79), respectivamente. O ES na escala visual analógica de Qualidade de Sono (VASQS) utilizada para avaliar a forma como as pacientes se sentiram ao acordar, durante o período de tratamento, foi nos grupos melatonina versus placebo de 2,47 (1,49-3,45) e 1,01 (0,23-1,79), respectivamente. Conclusão: Melatonina foi mais eficaz do que placebo para melhorar a dor miofascial crônica facial e ambos os tratamentos foram mais eficazes do que placebo para melhorar o LDP e a qualidade de sono. / Background: The Myofascial Pain Syndrome (SDM), a common cause of musculoskeletal pain, can course with disability and can be a therapeutical challenge, due to the ineffectiveness of conventional treatments for pain. Alternative therapeutic interventions must be researched to achieve the process of the disease process that in not dealt with the classical therapy. Among these, the use of melatonin, which takes effect chronobiotic, anxiolytic and analgesic, has been presented as an attractive therapeutic option in the treatment of SDM, which leads to sleep disturbances, pain, anxiety and depressive symptoms. Objectives: Evaluate the efficacy of exogenous melatonin in reducing pain, pain pressure threshold (PPT) and the sleep quality of patients with chronic myofascial face pain. Methods and Results: A randomized, controlled trial was conducted with 45 females, aged 18 to 40 years who presented myofascial pain according to the Research Diagnostic Criteria for Temporomandibular Disorder (RDC/TMD) guidelines. The efficacy of oral melatonin was evaluated in reducing pain and improving both the pain pressure threshold (PPT) and sleep quality. Participants were randomized to receive 5 mg/day melatonin, 5 mg/day cyclobenzaprine, or a placebo during a four-week period. The absolute effect of interventions, presented as ES (effect size) on pain for melatonin vs. placebo was 2.08 (1.17 to 2.97) and for cyclobenzaprine vs. placebo -1.25 (0.45 to 2.06)], respectively. The Number of Patients Needed to be Treated (NNT) to prevent moderate to intense pain was 3 (95% CI, 2 to 4) and 18 (95% CI, 9 to ) in the melatonin and cyclobenzaprine groups, respectively compared to the placebo. The ES on the PPT for melatonin vs. placebo and cyclobenzaprine vs. placebo was 2.72 (1.69 to 3.75) and 1.01 (0.23 to 1.79), respectively. The ES on the Visual Analog Sleep Quality Scale (VASQS) scores used to assess how they felt when they woke up during the treatment period for the melatonin vs. placebo were 2.47 (1.49 to 3.45) and 1.01 (0.23 to 1.79), respectively. Conclusion: Melatonin was more effective than placebo for improving chronic myofascial face pain and both treatments were more effective than placebo for improving sleep quality and the PPT.

Síndromes da dor miofascial

Dor facial

Melatonina

Limiar da dor

Myofascial pain syndrome

Melatonin

Cyclobenzaprine

Pain threshold

Interação entre limiar de dor e função autonômica após restrição de sono em indivíduos saudáveis

Dall'Agnol, Letizzia

January 2011

Introdução: Embora a relação entre privação de sono e limiar de dor tenha sido estudada em condições patológicas de quadros álgicos agudos e crônicos, os mecanismos envolvidos neste processo ainda carecem de investigações. Nesse contexto, sabe-se que são crescentes as situações nas quais a restrição de sono aguda é induzida por atividades laborais cotidianas, e a compreensão desta relação demanda modelos que permitam observar o efeito em condições em que os estímulos sejam padronizados e controlados. Assim sendo, investigamos o efeito da restrição aguda de sono na função autonômica e sua relação com limiares de dor em indivíduos saudáveis. Objetivos: Avaliar a relação entre respostas autonômicas e percepção a estímulos nociceptivos térmicos e elétricos pós-restrição aguda de sono ocasionada por estresse laboral. Métodos: Foram avaliados 19 estudantes de Medicina saudáveis após noite de sono habitual (SN) e após plantão noturno de 12 horas (RS). Primeiramente examinamos características clínicas dos sujeitos utilizando escalas para avaliação de sono e sintomas psiquiátricos. Foram realizados também testes quantitativos de sensibilidade para sensações térmicas e elétricas e registradas respostas cutâneas simpáticas (RCS) induzidas por estímulo elétrico duplo com diferentes intervalos interestímulos (ISI). Resultados: A média de duração do sono durante as 12 horas de plantão noturno foi de 120+ 28 minutos. Os escores de ansiedade foram maiores na fase RS quando comparados com os da fase SN (p<0,01). Após restrição de sono, houve diminuição no limiar de dor, mas não nos limiares de calor e elétricos. Em relação às respostas autonômicas, foram evidenciadas maiores amplitudes da RCS bem como aumento do número de duplas respostas em ISI 2s na fase RS. Também foi observada moderada correlação inversa entre limiares de dor e amplitudes da RCS (r= -0,45; p<0,01). Não foi encontrada correlação entre escores de ansiedade e parâmetros RCS. No entanto, no modelo de regressão linear multivariada, a percepção do limiar de dor ao estímulo térmico foi significativamente correlacionada com a amplitude da resposta cutânea simpática (β = - 0.55; 95% CI, -0.65 to -0.07), mas não com escores de ansiedade (p>0.05). Conclusões: Os efeitos da restrição aguda de sono no limar de dor são específicos e parecem não estar relacionados com alterações na percepção sensorial geral. Hiperalgesia foi associada com respostas autonômicas anormais, mas não com aumento da ansiedade, sugerindo a existência de uma associação entre o sistema nociceptivo e o autonômico, independente do estado emocional. / Background: Although the relationship between sleep deprivation and pain threshold has been studied in pathological acute and chronic conditions, the mechanisms involved in this process still require investigation. In this context, it is known that there is an increasing of situations where acute sleep restriction is induced by daily working activities and to understand this relationship is necessary models that allow the observation of the effect in situations in which the stimuli are standardized and controlled. Therefore, we investigated the effect of the acute sleep restriction on autonomic function and its relation with pain thresholds in healthy subjects. Objectives: Evaluating the relationship between autonomic responses and perception of thermal and electrical nociceptive stimuli after acute sleep restriction caused by stressful work. Methods: We evaluated 19 healthy medical students after normal night of sleep (NS) and after 12-hour night shift (SR). First we examined clinical characteristics of the subjects using scales for assessment of sleep and psychiatric symptoms. Also, we performed quantitative tests of sensitivity to thermal and electrical sensations and recorded double-electric-induced sudomotor skin responses (SSR) at different inter-stimulus intervals (ISI). Results: The total mean duration of sleep was 120 ± 28 minutes out of 12 hours of night shift. The anxiety scores were higher in SR Phase in comparison with those from NS Phase (p<0.01). After SR, there was a decrease in heat pain, but not in warm neither electrical threshold. Regarding autonomic responses, SR subjects showed higher SSR amplitudes and increased number of double responses at ISI 2s. It was also observed a moderate inverse correlation between heat pain thresholds and SSR amplitude (r = -0.45; P<0.01). However, there was no correlation between anxiety scores and SSR parameters. Indeed, in the multivariate linear regression model, heat pain perception was significantly correlated with SSR amplitudes (β = - 0.55; 95% CI, -0.65 to -0.07), but not with anxiety scores (p>0.05). Conclusions: The effects of SR on pain are specific and seem to be not related to general changes in sensory perception. Hyperalgesia was associated with abnormal autonomic responses, but not with increased anxiety, suggesting an association between the nociceptive and autonomic systems, independent of the emotional state.

Sono

Estresse psicológico

Limiar da dor

Privação do sono

Sleep deprivation

Autonomic function

Stress

Pain threshold

Efeito da estimulação trancraniana de corrente contínua na hiperalgesia induzida pelo remifentanil : um ensaio clínico randomizado em homens saudáveis

Braulio, Gilberto

January 2017

Introdução: Os opioides são os analgésicos mais efetivos para tratamento da dor moderada a intensa. No entanto, evidências crescentes têm demonstrado que seu uso pode levar a mudanças na sensibilidade dolorosa. Nesse contexto, a hiperalgesia induzida pelo remifentanil (r-IH) envolve um desequilíbrio nos sistemas inibitórios e excitatórios. Postula-se que um dos mecanismos centrais seja a disfunção do sistema modulador descendente da dor. Então, neste estudo, testamos a hipótese de que a estimulação transcraniana de corrente contínua (ETCC), devido aos seus efeitos analgésicos, poderia prevenir a r-IH. Os desfechos primários incluíram a escala numérica de dor (END 0-10) durante o teste repetitivo ao frio (rCOLDT), e a alteração na END (0-10) durante o teste de modulação condicionada de dor (CPM-TASK). Os desfechos secundários foram os limiares de dor ao calor (HPT) e o tempo de reação durante o teste de dor à água gelada [zero graus oC, (IPT)]. Métodos: Ensaio clínico randomizado, fatorial, duplo cego, que incluiu 48 homens saudáveis, com idades entre 19 e 40 anos. Os sujeitos foram randomizados em quatro grupos (n=12): ativo (a) - ETCC / solução salina, Sham (s) - ETCC / solução salina, a-ETCC / remifentanil e s-ETCC / remifentanil. Foi aplicado o ETCC sobre o córtex motor primário, com uma sessão única de 20 min e 2 mA. Resultados: Durante o rCOLDT, houve um efeito significativo entre os grupos nos escores cumulativos da END (P = 0,01). O grupo s-ETCC / remifentanil apresentou maiores escores de dor durante rCOLDT, [media (SD) 5,49 (1,04)] e a-ETCC / remifentanil apresentaram escores relativamente menores [4,15 (1,62)]. Este achado mostra que o efeito da ETCC bloqueou a HI-R. Os grupos a-ETCC / solução salina e s-ETCC / salina apresentaram menor índice de dor durante rCOLDT, [3.11 (1.2)] e [3.15 (1.62)], respectivamente. A incidência de hiperalgesia definida como um aumento de 15% na END durante o rCOLDT foi de: 31% no grupo s-ETCC/remifentanil; 22% no grupo a-ETCC/remifentanil; 11% no grupo a-ETCC/salina; e 8.3% no grupo s-ETCC/salina. Os grupos com remifentanil apresentaram escore positivo na END (0-10) durante a tarefa CPM, ou seja, produziu um desengate do sistema modulador descendente de dor (DPMS). Além disso, s-ETCC / Remifentanil em comparação com a-ETCC/remifentanil apresentou menor HPT e maior tempo de reação durante o IPT. Conclusão: Esses achados sugerem que os efeitos da a-ETCC previne a disfunção da capacidade inibitória do sistema modulador descendente da dor induzido pelo remifentanil durante o rCOLDT. / Background: Opioids are the most effective analgesics to treat moderate to severe pain. However, growing evidence shows that opioids can elicit unexpected changes in pain sensitivity. In this sense, remifentanil-induced hyperalgesia (r-IH) involves an imbalance in the inhibitory and excitatory systems. It postulates that one of the central mechanisms is the dysfunction of the descending pain modulating system. We tested the hypothesis that transcranial Direct Current Stimulation (t-DCS), given its analgesics effects, could prevent r-IH. The primary outcomes included the Numerical Pain Score NPS (0-10) during the repetitive cold test (rCOLDT) and the change on the NPS (0-10) during the conditioned pain modulation (CPM)-task. The secondary outcomes were the heat pain threshold (HPT) and the reaction-time during the Ice-Water Pain Test (IPT). Methods: This double blinded, explanatory factorial randomized trial included 48 healthy males, ages ranging 19 to 40 years. They were randomized into four equal groups: active (a)-tDCS/saline, sham (s)-tDCS/saline, a-tDCS/remifentanil and s-tDCS/remifentanil. We applied tDCS over the primary motor-cortex, with a single session of 20 minutes and 2mA. Results: During the rCOLDT, there was a significant group effect on the cumulative NPS scores (P=0.01). The s-tDCS/remifentanil group presented larger pain scores during rCOLDT, [mean (SD) 5.49 (1.04)] and a-tDCS/remifentanil group had relative lower pain scores [4.15 (1.62)]; showing its blocking effect on r-IH. a-tDCS/saline and s-tDCS/saline groups showed lowest pain scores during rCOLDT, [3.11(1.2)] and [3.15(1.62)], respectively. The incidence of hyperalgesia defined as a 15% increase in NPS during rCOLDT was: 30.3% in the s-tDCS / remifentanil group; 22% in the a-tDCS / remifentanil group; 11% in the a- tDCS / saline group; 8.3% in the s-tDCS / saline group. Remifentanil groups showed positive scores in the NPS (0-10) during the CPM-task, that is, it produced a disengagement of the descending pain modulatory system (DPMS). Also, s- tDCS/Remifentanil compared to a-tDCS/Remifentanil showed lower HPT and larger reaction-time during the IPT. Conclusion: These findings suggest that the effects of a-tDCS prevents the dysfunction of the inhibitory capacity of the descending modulatory pain system induced by remifentanil during rCOLDT.

Hiperalgesia

Limiar da dor

Homens

TDCS

Remifentanil

Hyperalgesia

CPM

Pain threshold