BDNF e efeito dose-resposta da melatonina no limiar de dor em individuos saudáveis

Stefani, Luciana Paula Cadore

January 2012

Introdução: A mensuracão da dor através de testes psicofísicos, entre eles o teste de quantificação sensitiva, definido como a determinação de limiares a estímulos álgicos controlados, possibilita o estudo de inúmeras variáveis que influenciam a percepção final da dor. Entre essas variáveis encontram-se o BDNF (Brain Derived Neurotrophic Factor), o gênero e sistemas modulatórios não classicamente descritos como o melatonérgico. Objetivos: Validar um equipamento para realização do teste de quantificação sensitiva usando amostra de voluntários brasileiros saudáveis e estudar fatores e sistemas neurobiológicos que alteram os limiares nociceptivos como sexo, BDNF e melatonina. Métodos: O novo equipamento (Heat Pain Stimulator-1.1.10; Brazil) foi utilizado em 20 voluntários saudáveis e em pacientes com neuropatia periférica, em duas sessões separadas, para acessar a reprodutibilidade dos limiares e a concordância com os equipamentos clássicos. Em etapa posterior, os limiares de dor foram medidos em voluntários e correlacionados com o gênero e os níveis de BDNF. Em estudo sucessivo 61 sujeitos foram randomizados em 1 dos 4 grupos: placebo, 0,05 mg/kg de melatonina sublingual (SL), 0,15 mg/kg de melatonina SL ou 0,25 mg/kg de melatonina e foram testados quanto aos limiares e tolerância à dor aos estímulos térmico e de pressão no tempo basal e 30 min após a intervenção. A sedação foi quantificada através de escala análogo-visual e pela análise do índice bispectral. Resultados: Os resultados iniciais mostraram concordância com a literatura e adequada reprodutibilidade dos limiares de dor térmica em indivíduos saudáveis (44.5±2.5°C ) e em indivíduos com neuropatias de fibras finas (49.9±3°C) em sessões separadas. Quando analisados em modelo de regressão linear multivariada, os limiares de dor térmica e de pressão mostraram um efeito significativo do gênero (p=0,01 para ambos os modelos), BDNF (p<0,04 para ambos os modelos) e interação entre BDNF e gênero (<0,001 para ambos os modelos). Altos níveis de BDNF foram correlacionados com alto limiar de dor em mulheres e essa relação foi inversa em homens. No estudo com a melatonina, os níveis plasmáticos foram proporcionais à dose administrada, e o modelo de regressão linear mostrou uma relação entre a concentração sérica de melatonina e as modificações nos limiares (R2=0,56 para o limiar de dor ao estímulo térmico e R2=0,518 para o limiar de dor na algometria de pressão). Uma dose única de melatonina igual ou acima de 0,15 mg/kg propiciou um delta médio dos limiares de dor ao estímulo térmico e à pressão maiores que placebo (MANOVA, p<0,05 para todas as análises). Além disso, dose igual ou acima que 0,15 mg/kg produziu maior escore de sedação. Conclusões: O equipamento desenvolvido produz resultados confiáveis para avaliação das vias nociceptivas em voluntários saudáveis e em pacientes com alterações sensitivas. O BDNF está associado a maiores limiares de dor nas mulheres (menos dor), mas tem efeito oposto nos homens, suportando a ideia de que ele modifica o efeito que o gênero exerce sobre os limiares de dor. A melatonina possui efeito analgésico dose-dependente no modelo de dor experimental desenvolvido, havendo correlação entre a concentração plasmática e as alterações nos limiares avaliados. O adequado perfil farmacocinético, e a ausência de efeitos colaterais significativos reforçam a sua consolidação como um fármaco modulador da dor. / Background: The measurement of pain through psychophysical tests, including quantitative sensory testing, allow for the study of many variables that influence the final perception of pain. Among these variables are BDNF (Brain Derived Neurotrophic Factor), in addition to gender and modulatory systems not classically described as melatonergic. Objectives: To validate a device to perform the quantitative sensory testing in a cohort of Brazilian healthy volunteers in order to study factors and neurobiological systems that alter the nociceptive thresholds including gender, BDNF, and melatonin. Methods: The new equipment (Heat Pain Stimulator, 01/01/10, Brazil) was tested on 20 healthy volunteers and patients with peripheral neuropathy in two separate sessions to access the reproducibility of thresholds with the classic features. In later stage, the pain thresholds were measured in volunteers and correlated with gender and levels of BDNF. 61 successive study subjects were randomized into one of four treatment groups: placebo, 0.05 mg / kg of melatonin sublingual (SL), 0.15 mg / kg of melatonin SL or 0.25 mg / kg of melatonin SL, and were tested for thresholds and pain tolerance to thermal and pressure stimuli at baseline and 30 min post intervention. Sedation was quantified by visual analog scale and the bispectral index analysis. Results: Initial results showed agreement with the literature and adequate reproducibility of thermal pain thresholds in healthy subjects (44.5 ± 2.5 ° C) and in patients with neuropathies of fine fibers (49.9 ± 3 ° C) in separate sessions. When analyzed in a multivariate linear regression model, the thermal and pressure pain thresholds showed a significant effect of gender (p = 0.01 for both models), BDNF (p <0.04 for both models) and correlation between BDNF and gender (<0.001 for both models). High levels of BDNF were correlated with high pain threshold in women and this relationship was reversed in men. In the study with melatonin, plasma levels were proportional to dose, and linear regression model showed a relationship between serum melatonin and changes in thresholds (R2 = 0.56 for pain threshold to thermal stimulation and R2 = 0.518 for the threshold of pain on pressure algometry). A single dose of melatonin at or above 0.15 mg / kg led to a delta average pain thresholds to thermal stimulation and a pressure greater than placebo (MANOVA, p <0.05 for all analyzes). Furthermore, a dose equal to or greater than 0.15 mg / kg produced the highest score of sedation. Conclusion: The heat pain stimulator produces reliable results for assessment of nociceptive pathways in healthy volunteers and in patients with sensory changes. BDNF has a facilitatory effect on pain thresholds in women, but has the opposite effect in men, supporting the idea that it modifies the effect gender has on the threshold of pain. Melatonin has a dose-dependent analgesic effect in the experimental pain model developed, there was no correlation between plasma concentration and changes in the thresholds evaluated. The appropriate pharmacokinetic profile, and the absence of significant side effects reinforce its consideration as a pain modulator drug.

Limiar da dor

Gênero

Melatonina

Pain threshold

Pain pathway

Gender

BDNF

Melatonin

Pain modulation

Doseresponse curve

Exploring pain & movement relationships: is greater physical activity associated with reduced pain sensitivity & does endogenous muscle pain alter protective reflexes in the upper extremity?

Merkle, Shannon L. M.

01 December 2016

Pain and movement are intimately connected and nearly universal human experiences. However, our understanding of the extent, significance, and mechanisms of pain-movement relationships is limited. While pain is a normal, protective response to injury and potentially harmful stimuli, prolonged or dysfunctional neuromuscular adaptions in response to pain can contribute to a variety of pain conditions. Alternatively, movement (in the form of global physical activity, individual exercise programs, and/or specific motor learning/functional tasks) is often prescribed to help decrease pain and improve function. While attempts have been made to show an effect of movement on pain or to better understand altered movement strategies in response to pain, much of the research has been limited to animal models or to those with specific persistent or chronic pain conditions limiting generalizability and interpretability. Therefore, this research sought to advance current understanding of the relationships between physical activity and normal variability in centrally- and peripherally-mediated pain in healthy adults. Additionally, we sought to characterize changes in reflexive motor responses in the upper extremity to an endogenous, naturally-occurring, long-lasting acute muscle pain. The results of these investigations indicate that greater, self-reported intense (i.e. vigorous) and leisure activity are more strongly associated with decreased pain sensitivity than is pain modulation or measured activity (via accelerometry). Future research is needed to determine directionality of these relationships. Further, reflexive motor responses to endogenous, acute muscle pain in the upper extremity were not significantly altered indicating that changes in pain-related, movement strategies may be more strongly influenced by supraspinal adaptations. These results may have value in improving understanding of pain-related, movement sequelae and directing future research in this area.

nociceptive withdrawal reflex

pain modulation

physical activity measurement

pressure pain threshold

quantitative sensory testing

referred pain

Rehabilitation and Therapy

The impact of acute stress and childhood traumatic events on pain sensitivity among adults with chronic low back pain

Comptdaer, Gabriela

31 January 2023

BACKGROUND AND AIMS: Globally, chronic low back pain (CLBP) affects 70-80% of adults at some point in their lives and current treatments are widely unsuccessful in relieving pain. Understanding the underlying neurophysiological (e.g., descending pain inhibition) and biobehavioral (e.g., stress) processes contributing to chronic pain in patients with CLBP is needed for the development of novel treatments. Previous studies have shown that acute stress can impact pain sensitivity and that childhood trauma may predispose a person to CLBP, but the mechanisms underlying this impact are unknown. Conditioned Pain Modulation (CPM) is a psychophysical paradigm used in research to assess descending pain modulatory pathways, which are thought to be impaired in patients with CLBP as well as in those with childhood trauma. The overlap of conditions has not been explored. The current study explored the impact of childhood trauma on the CPM response within a sample of patients with CLBP being treated at a tertiary pain clinic. CLBP patients exposed to an acute stress paradigm were expected to shower higher pain sensitivity, with acute stress significantly interacting with a history of childhood trauma as a factor leading to the higher pain sensitivity. METHODS: 46 Participants with CLBP (n=46, mean age=49 years, 55.3% female) recruited from a pain treatment service completed a Quantitative Sensory Testing (QST) and CPM before and after an acute psychological stressor. Participants were randomized to a control (n=25) or an acute-stress (n=21) condition. The acute-stress condition included the Stroop Color Word Task (SCWT) and a mental arithmetic task prior to completing the QST protocol a second time. The control participants did not undergo any additional stressors and completed the QST protocol a second time after a 20-minute break. Participants’ CPM response was measured by the average change in pressure pain threshold (PPT) from baseline to the conditioning stimulus (non-dominant hand in ice-water bath). A “Good CPM response” was defined as a CPM effect above 100, indicating that the pain threshold increased when exposed to the conditioning stimulus. To examine the impact of childhood trauma on pain sensitivity, participants completed a Childhood Traumatic Events Scale (CTES) to assess the presence and severity of six types of trauma (death, parental upheaval, sexual, violence, illness or injury, other upheaval) during childhood. The CTES was scored as a continuous variable by calculating the sum the trauma severity for all six trauma types. RESULTS: A large majority of the sample (94% of participants) showed an increase in pain threshold during hand immersion in ice water, which was contrary to our hypothesis based on prior research done on other chronic pain conditions and CLBP. Participants exposed to an acute stressor had an impaired CPM effect compared to those that were not exposed to an acute stressor, however there was no difference between groups (p=0.277). A history of childhood traumatic events did not correlate significantly with an impaired baseline CPM or a change in CPM effect when exposed to an acute stressor. CONCLUSION: The current study used novel QST modalities, including CPM, to analyze the interaction between acute and chronic stress on pain sensitivity. Ultimately, this study found that exposure to an acute stressor had a negative effect on CPM, indicating that when under experimental stress participants were more sensitive to pain compared to when they were not under stress, although the findings were not statistically significant. These findings should be further investigated to expand the understanding of the neurophysiological mechanisms underlying CLBP and to potentially provide novel treatment modalities for patients with CLBP.

Clinical psychology

Acute stress

Childhood traumatic events

Chronic low back pain

Conditioned pain modulation

Experimental pain

Quantitative sensory testing

Efficacité analgésique de la neurostimulation périphérique (TENS) chez les aînés / Analgesic efficacy of transcutaneous electrical nerve stimulation (TENS) in the elderly

Bergeron-Vézina, Kayla

January 2015

La neurostimulation périphérique (en anglais transcutaneous electrical nerve stimulation ou TENS) est une modalité thérapeutique fréquemment utilisée en réadaptation pour diminuer la douleur. À ce jour, cependant, l’efficacité analgésique du TENS chez les aînés demeure peu documentée. La majorité des études effectuées jusqu’à présent ont été réalisées chez les jeunes adultes ou chez des populations d’âge hétérogènes. La présente étude, un essai croisé randomisé à double insu, avait pour objectif de documenter l’efficacité analgésique du TENS conventionnel et du TENS acupuncture chez les aînés et d’observer si la réponse analgésique de ces deux modalités de TENS entre les aînés et les jeunes adultes est différente. Quinze aînés et quinze jeunes adultes ont participé à l’étude. Les participants étaient évalués à trois occasions distinctes pour recevoir en alternance un TENS conventionnel, un TENS acupuncture et un TENS placebo. Une douleur expérimentale était créée à l’aide d’une thermode de type Peltier, appliquée au niveau de la colonne lombaire pendant deux minutes, période durant laquelle les participants devaient évaluer l’intensité de leur douleur avec une échelle visuelle analogue reliée à un ordinateur (CoVAS). Les mesures de douleur ont été prises avant, pendant et après l’application de chaque type de TENS. Chez les jeunes adultes, lorsque comparée au niveau de douleur initiale, une diminution significative de la douleur a été observée pendant et après l’application du TENS conventionnel et acupuncture. Le TENS conventionnel et acupuncture étaient supérieurs au traitement placebo (toutes les valeurs de p < 0,05). Cependant, chez les aînés, le TENS conventionnel et acupuncture n’ont pas permis de diminuer significativement la douleur. De plus, aucune modalité TENS ne se démarquait du traitement placebo (toutes les valeurs de p > 0,05). Bien que le TENS conventionnel et le TENS acupuncture soient efficaces chez les jeunes adultes, les présents résultats suggèrent que le TENS n’est pas la meilleure option de traitement pour diminuer la douleur chez les aînés, du moins lorsqu’il est utilisé seul (monothérapie). Des études futures, visant à déterminer des façons de bonifier l’effet du TENS chez les aînés, sont nécessaires.

Neurostimulation périphérique (TENS)

Douleur

Analgésie

Vieillissement

Aînés

Réadaptation

Mécanismes inhibiteurs descendants

Analgésie segmentaire

Pain

Analgesia

Aging

Elderly

Rehabilitation

Conditioned pain modulation

Segmental analgesia

Modulation of nociception and pain by attention and stress

Cardinal-Aucoin, Natalie

11 1900

Les facteurs psychologiques tels que l'hypnose, l'émotion, le stress et l’attention exercent un effet modulant puissant sur la nociception et la douleur. Toutefois, l’influence de l'attention sur la nociception et la douleur, ainsi que les mécanismes neuronaux sous-jacents, ne sont pas clairs. La littérature actuelle sur la modulation attentionnelle des réponses spinales nociceptives, telles que mesurées par le réflexe RIII, et de la perception de l’intensité de la douleur est discordante et souvent contradictoire. Ce mémoire fournit un nouveau cadre pour examiner la modulation du réflexe RIII et de la douleur par l’attention. Une tâche de discrimination sensorielle a été décomposée en trois composantes attentionnelles : la vigilance, l’orientation, et le contrôle exécutif. Auparavant, la nature multidimensionnelle de l’attention fut largement ignorée dans la littérature. Nous démontrons que les composantes attentionnelles ont des effets modulatoires distincts sur la nociception et la douleur et suggérons que ceci représente une partie de la confusion présente dans la littérature. En prenant compte du stress indépendamment, nous démontrons, pour la première fois, que le stress inhibe la modulation attentionnelle du réflexe RIII ce qui indique une interaction et dissociation de la modulation des réponses nociceptives par l’attention et le stress. Ces résultats importants clarifient, en grande partie, les contradictions dans la littérature, puisque les tâches cognitives produisent souvent des augmentations du stress ce qui confond l’interprétation des résultats. De plus, la tâche de discrimination inclut des stimuli visuels et somatosensoriels et révèle que l’influence de l'attention sur la douleur est spatialement spécifique tandis que la modulation attentionnelle de la nociception est spécifique à la modalité des stimuli, au moins en ce qui concerne les modalités examinées. A partir de ces résultats, un nouveau modèle de la modulation attentionnelle des processus de la douleur, basée sur les composantes attentionnelles, a été proposé. Celui-ci est appuyé par la littérature et fournit une explication systématique et intégratrice des résultats antérieurement contradictoires. De plus, à partir de ce modèle, plusieurs mécanismes neuronaux ont été proposés pour sous-tendre la modulation attentionnelle de la nociception et de la douleur. / Psychological factors such as hypnosis, emotion, stress, and attention produce powerful modulatory effects on nociception and pain. However, the influence of attention on nociception and pain and the underlying neural mechanism responsible are unclear. The current literature on attentional modulation of spinal nociceptive responses, as measured by the RIII reflex, and pain perception (pain intensity) is inconsistent and often contradictory. The present thesis provides a new component-based framework for the examination of attentional modulation of the RIII reflex and pain. A delayed-discrimination task was decomposed into the three components of attention – namely alerting, orienting, and executive control (sensory working memory). Previously, the multidimensional nature of attention was largely ignored in the pain literature. We show that each component of attention exerts a distinct modulatory effect on nociception and pain and suggest that this accounts for some of the confusion in the literature. By considering stress separately, we demonstrate for the first time that stress blocks attentional modulation of the RIII reflex, indicating an interaction and dissociation of attention- and stress-mediated modulation of spinal nociceptive responses. This important finding clarifies much of the disagreement in the literature, since cognitive tasks often induce increases in stress that consequently confound interpretation. Additionally, both visual and somatosensory stimuli were included in the discrimination task, revealing that the influence of attention on pain intensity is spatially-specific whereas attentional modulation of nociception is modality-specific, at least for the modalities investigated. From these findings a component-based model for the attentional modulation of pain processes is proposed. This model is substantially supported by the literature and provides a meaningful and cohesive explanation of the seemingly contradictory results across studies. Moreover, this model suggests potential neural mechanisms underlying the attentional modulation of pain.

Pain

Nociception

RIII reflex

Attention

Stress

Pain modulation

Attentional components

Douleur

Réflexe RIII

Modulation de la douleur

Composants attentionnels

Mécanismes centraux de la perception et de la modulation de la douleur dans le vieillissement / Central mechanisms of pain perception and modulation in aging

Zhou, Shu

23 October 2015

De nombreuses études ont montré une modification de la perception de la douleur au cours du vieillissement. Cette modification s’exprime principalement par une diminution du seuil de la douleur aiguë et une augmentation de la prévalence de douleurs chroniques. Parallèlement, le vieillissement provoque des altérations cérébrales importantes, notamment dans les réseaux frontaux. Dans ce travail de thèse, nous avons étudié les mécanismes centraux, notamment les fonctions des réseaux frontaux sur la perception et la modulation de la douleur chez la personne âgée. Les résultats des expériences 1 à 3 suggèrent une forte corrélation positive entre l’altération des fonctions exécutives et le déclin de la modulation cognitive de la douleur et de la résistance à la douleur tonique. Dans l’expérience 4, nos résultats montrent que les scores aux tests mesurant les fonctions émotionnelles (e.g. la reconnaissance des émotions) sont corrélés au ressenti de la douleur. Cela pourrait indiquer un déficit chez les personnes âgées de la composante émotionnelle qui entre en jeu dans la perception de la douleur. / Age-related changes in pain perception have been widely reported in the literature, showing a reduced acute pain perception and an increased prevalence of chronic pain. Ageing also results in considerable alterations in brain structures and functions, particularly in frontal networks. In this thesis, we explored the underlying central mechanisms, especially the role of frontal functions in the age-related alterations in pain perception. Results of experiments 1-3 demonstrated a strong positive correlation between the age-related alterations in executive function and the decline in pain tolerance and cognitive pain modulation. In experiment 4 we observed that the emotional function measured by a test of emotions recognition was correlated to the verbal expression of perceived pain, indicating that the reduced pain expression in the elderly may result from the deficient responses to emotion.

Vieillissement non-pathologique

Douleur tonique

Modulation de la douleur

Cortex préfrontal

Fonctions exécutives

Fonctions émotionnelles

Non-pathological ageing

Tonic pain

Pain modulation

Prefrontal cortex

Executive functions

Emotional functions

616.047

Pain modulation in patients with chronic lumbar myalgia : An experimental study

Nygren, Karin, Glimstedt, Charlotte

January 2013

Syfte: Syftet med denna studie var att undersöka hur statisk muskelkontraktion och cold pressor test påverkar kroppsegna smärtreglerande system (”Exercise induced analgesia” (EIA) och ”Conditioned pain modulation” (CPM)) hos patienter med kronisk ländryggssmärta kännetecknad av lumbal myalgi (LM) jämfört med friska kontroller. Försökspersoner och metod: Tjugosex friska köns- och åldersmatchade personer och tjugosex LM-patienter deltog. De utförde standardiserad statisk muskelkontraktion med m. Erector spinae (ME) i form av rygglyft och kontraktion av m. Quadriceps femoris (MQ) i form av knäledsextension. För att bedöma CPM användes sk cold pressor test. Smärttrösklar för tryck (PPTs) mättes över m. Deltoideus (MD), m. Erector spinae (ME) samt över m. Quadriceps (MQ) i vila och under resp. efter kontraktionen/cold pressor test. Under kontraktion mättes PPTs över den arbetande muskeln respektive över de två vilande musklerna. Dessutom undersöktes PPTs och känsligheten för övertrösklig trycksmärta (P7) i vila på 8 olika punkter på kroppen. Resultat: Kvinnliga LM-patienter hade ökad känslighet för trycksmärta (PPT) och övertrösklig trycksmärta (P7) jämfört med köns- och åldermatchade friska kontroller, medan manliga LM-patienter paradoxalt nog hade minskad känslighet för övertrösklig trycksmärta. Beträffande EIA fann vi att LM-patienter och kontroller kunde aktivera lokal EIA under kontraktion med ME. Vi fann dessutom en minskad förmåga hos LM-patienter att rekrytera generaliserad EIA under kontraktion med MQ. Slutligen hade LM-patienterna en normal funktion av CPM. Slutsats: LM-patienter kunde aktivera lokal EIA under kontraktion av ME, men hade mindre effektiv generaliserad EIA jämfört med kontrollerna, trots normal funktion av CPM. Våra resultat tyder på att muskelarbete med smärtande ryggmuskler skulle kunna användas för att minska smärtkänslighet i det drabbade området.

Chronic low back pain

myalgia

presure pain thresholds

static contraction

endogenous pain modulation

exercise

Kronisk ländryggssmärta

myalgi

smärttröskel för tryck

statisk kontraktion

kroppsegen smärtmodulering

träning

Modulation of nociception and pain by attention and stress

Cardinal-Aucoin, Natalie

11 1900

Les facteurs psychologiques tels que l'hypnose, l'émotion, le stress et l’attention exercent un effet modulant puissant sur la nociception et la douleur. Toutefois, l’influence de l'attention sur la nociception et la douleur, ainsi que les mécanismes neuronaux sous-jacents, ne sont pas clairs. La littérature actuelle sur la modulation attentionnelle des réponses spinales nociceptives, telles que mesurées par le réflexe RIII, et de la perception de l’intensité de la douleur est discordante et souvent contradictoire. Ce mémoire fournit un nouveau cadre pour examiner la modulation du réflexe RIII et de la douleur par l’attention. Une tâche de discrimination sensorielle a été décomposée en trois composantes attentionnelles : la vigilance, l’orientation, et le contrôle exécutif. Auparavant, la nature multidimensionnelle de l’attention fut largement ignorée dans la littérature. Nous démontrons que les composantes attentionnelles ont des effets modulatoires distincts sur la nociception et la douleur et suggérons que ceci représente une partie de la confusion présente dans la littérature. En prenant compte du stress indépendamment, nous démontrons, pour la première fois, que le stress inhibe la modulation attentionnelle du réflexe RIII ce qui indique une interaction et dissociation de la modulation des réponses nociceptives par l’attention et le stress. Ces résultats importants clarifient, en grande partie, les contradictions dans la littérature, puisque les tâches cognitives produisent souvent des augmentations du stress ce qui confond l’interprétation des résultats. De plus, la tâche de discrimination inclut des stimuli visuels et somatosensoriels et révèle que l’influence de l'attention sur la douleur est spatialement spécifique tandis que la modulation attentionnelle de la nociception est spécifique à la modalité des stimuli, au moins en ce qui concerne les modalités examinées. A partir de ces résultats, un nouveau modèle de la modulation attentionnelle des processus de la douleur, basée sur les composantes attentionnelles, a été proposé. Celui-ci est appuyé par la littérature et fournit une explication systématique et intégratrice des résultats antérieurement contradictoires. De plus, à partir de ce modèle, plusieurs mécanismes neuronaux ont été proposés pour sous-tendre la modulation attentionnelle de la nociception et de la douleur. / Psychological factors such as hypnosis, emotion, stress, and attention produce powerful modulatory effects on nociception and pain. However, the influence of attention on nociception and pain and the underlying neural mechanism responsible are unclear. The current literature on attentional modulation of spinal nociceptive responses, as measured by the RIII reflex, and pain perception (pain intensity) is inconsistent and often contradictory. The present thesis provides a new component-based framework for the examination of attentional modulation of the RIII reflex and pain. A delayed-discrimination task was decomposed into the three components of attention – namely alerting, orienting, and executive control (sensory working memory). Previously, the multidimensional nature of attention was largely ignored in the pain literature. We show that each component of attention exerts a distinct modulatory effect on nociception and pain and suggest that this accounts for some of the confusion in the literature. By considering stress separately, we demonstrate for the first time that stress blocks attentional modulation of the RIII reflex, indicating an interaction and dissociation of attention- and stress-mediated modulation of spinal nociceptive responses. This important finding clarifies much of the disagreement in the literature, since cognitive tasks often induce increases in stress that consequently confound interpretation. Additionally, both visual and somatosensory stimuli were included in the discrimination task, revealing that the influence of attention on pain intensity is spatially-specific whereas attentional modulation of nociception is modality-specific, at least for the modalities investigated. From these findings a component-based model for the attentional modulation of pain processes is proposed. This model is substantially supported by the literature and provides a meaningful and cohesive explanation of the seemingly contradictory results across studies. Moreover, this model suggests potential neural mechanisms underlying the attentional modulation of pain.

Pain

Nociception

RIII reflex

Attention

Stress

Pain modulation

Attentional components

Douleur

Réflexe RIII

Modulation de la douleur

Composants attentionnels

Eficácia da estimulação transcraniana com corrente contínua de longo prazo em nível domiciliar sobre o córtex pré-frontal dorsolateral esquerdo na fibromialgia : um ensaio clínico randomizado

Brietzke, Aline Patrícia

January 2018

Introdução: Estimulação transcraniana com corrente contínua (ETCC) é um método não invasivo de estimulação cerebral que modifica o potencial de repouso da membrana neuronal através de uma corrente elétrica de baixa intensidade. Trata-se de uma técnica neuromodulatória aplicável ao contexto terapêutico de disfunções do sistema nervoso implicados na fisiopatologia da dor e transtornos neuropsiquiátricos, com baixo custo, mínimos efeitos adversos e fácil aplicação. A ETCC tem se mostrado eficaz no tratamento de dores crônicas incluindo a fibromialgia (FM) em curto prazo. Seu uso se sustenta na melhor compreensão dos mecanismos fisiopatológicos dessa síndrome, os quais incluem processos de desinibição em nível cortical e infracortical, demonstrado por medidas neurofisiológicas como facilitação e desinibição, assim como redução da potência dos sistemas modulatórios descendentes da dor, além de alterações nas vias nociceptivas periféricas, como as fibras nervosas finas. No entanto, essa alteração isolada não foi previamente associada à disfunção no sistema de modulação descendente da dor (SMDD), observado na FM. As áreas de aplicação da ETCC dependem do objetivo terapêutico. O córtex motor primário (M1) é o alvo mais estudado e com maior contingente de evidências para o tratamento da dor e reabilitação motora, enquanto o córtex pré-frontal dorsolateral esquerdo (DLPFC) tem sido eficaz na depressão e melhora dos componentes psicoafetivos dos pacientes com dor crônica. Seu principal limitador prático é a necessidade de ir ao centro de atendimento durante dias consecutivos, pois o efeito terapêutico sustentado da ETCC necessita repetição das sessões Objetivos: Esta tese está constituída por dois estudos. O primeiro objetiva examinar se a disfunção de fibras finas que ocorre em pacientes com FM está ligada a um mau funcionamento do sistema modulador descendente da dor. No segundo, o objetivo é avaliar a eficácia do uso em longo prazo da ETCC em nível domiciliar na FM, com o objetivo de facilitar o uso e permitir a disponibilização desta técnica a pacientes do Sistema Único de Saúde. Estudo I: No primeiro estudo avaliamos se a disfunção de fibras nervosas finas periféricas está ligada a um mau funcionamento do sistema modulador descendente da dor (SMD) na FM. Métodos: Foi realizado um estudo exploratório no qual 41 mulheres com FM e 28 voluntárias saudáveis foram submetidas a testes psicofísicos que avaliaram a função de fibras sensitivas envolvidas na nocicepção. O teste quantitativo sensorial (QST) foi utilizado para medir o limiar perceptivo térmico (HTT), o limiar de dor térmica (HPT) e o limiar de tolerância à dor térmica (HPTo), bem como avaliar a mudança na Escala Numérica de Dor (NPS0-10) durante uma tarefa de modulação da dor condicionada (CPM-task). A algometria foi utilizada para determinar o limiar de pressão de dor (PPT). Escalas para avaliação de catastrofização, ansiedade, depressão e distúrbios do sono também foram aplicadas. O fator neurotrófico derivado do cérebro (BDNF) foi medido como um marcador de neuroplasticidade. Realizamos modelos de regressão linear multivariada por grupo (saudáveis e FM) para estudar a relação entre a função do SMD e sua relação com as medidas psicofísicas. Resultados: As amostras diferiram em seu perfil psicológico, e nas medidas psicofísicas, o grupo e pacientes com FM apresentou menor sensibilidade e limiares de dor. Na FM, mas não nos saudáveis, os modelos de regressão revelaram que o HTT estava relacionado ao BDNF e ao CPM-Task (Hotelling's Trace = 1,80, P<0,001, poder=0,94, R2=0,64). HTT foi correlacionado positivamente com a CPM-task (B = 0,98, P= 0,004, Partial-ƞ2=0,25), e ao HPT (B=1,61, P=0,008, parcial -ƞ2= 0,21). No entanto PPT não foi correlacionado com o HTT. Na FM a relação do BDNF com CPM-Task teve uma relação negativa (B=-0,04, P=0,043, parcial-ƞ2=0,12) e a HPT foi diretamente proporcional (B= - 0,08, P=0,03, parcial-ƞ2 = 0,14). O BDNF não influenciou no modelo. E os efeitos adversos relatados foram maiores no grupo ativo (17,8%) em comparação com o grupo sham (6,6%). Conclusão: A disfunção sensorial periférica está associada positivamente à disfunção do sistema modulatório descendente da dor e aos níveis séricos de BDNF na FM, o que não ocorre em indivíduos saudáveis. Estudo II: O segundo estudo teve como objetivo avaliar a eficácia do uso domiciliar de 60 sessões da ETCC-ativa e ETCC-simulada aplicadas sobre a área DLPFC esquerda, nas pacientes com diagnóstico de FM. Métodos: Foi realizado um ensaio clínico randomizado, duplo cego, em paralelo, controlado com ETCC-simulada em 20 mulheres com diagnóstico de fibromialgia. A estimulação foi realizada durante cinco dias consecutivos na semana, durante 30 min, com a intensidade de 2 mA, por 12 semanas, totalizando 60 sessões. As pacientes receberam treinamento para uso do equipamento especialmente desenvolvido para uso domiciliar e mantinham contato com o pesquisador responsável por meio de mensagem de texto diariamente. Os efeitos foram medidos por meio da escala visual de dor (EAV) durante o curso de 12 semanas de tratamento, bem como o uso de analgésicos e possíveis eventos adversos, diariamente. Foram avaliados os níveis de depressão, catastrofismo e capacidade funcional para tarefas diárias, QST para verificar limiar de dor e tolerância ao calor, PPT e dosagem dos níveis séricos de BDNF no início, após 30 sessões e no final do tratamento. Um modelo linear misto com efeitos fixos foi usado para comparar mudanças nos escores de dor na EAV ao longo do tratamento. Resultados: A ETCC ativa domiciliar reduziu os escores de dor pela EAV (p<0.001) quando comparado ao sham, com uma redução média de dor de 64% (p<0.001). Além disso, ETCC ativa reduziu significativamente a incapacidade relacionada a dor [B-PCP:S escore total (p=0.023);-ƞ2=0.61]. Também reduziu os escores nas medidas clínicas de depressão, catastrofismo e qualidade do sono [BDI-II, PCS e PSQI (p<0.05)]. No entanto, ETCC ativa aumentou os escores na algometria (PPT) e tolerância térmica (HPTo) (p<0.01). O BDNF não influenciou no modelo. Os efeitos adversos relatados foram maiores no grupo ativo (17,8%) em comparação com o grupo sham (6,6%). Conclusão: A ETCC para uso domiciliar mostrou-se segura e eficaz na redução da dor, incapacidade relacionada a dor, sintomas depressivos e catastróficos e redução do uso de analgésicos. O conjunto de dados desta tese sugere que em pacientes fibromiálgicas, o nível de disfunção do sistema modulador descendente da dor está relacionado ao nível de disfunção de fibras nervosas finas periféricas envolvidas na nocicepção. Além disso, a ETCC de longo prazo em fibromiálgicas foi eficaz na melhora dos sintomas disfuncionais relacionados à dor crônica e se mostrou adequada para uso domiciliar. / Introduction: Transcranial direct current stimulation (tDCS) is a noninvasive method of brain stimulation that modifies the resting potential of the neuronal membrane through a low intensity electrical current. It is a neuromodulatory technique to the therapeutic context of dysfunctions of the nervous system implicit in physiotherapy and neuropsychological disorders, with low cost, adverse effects and easy application. tDCS has been effective without a chronic fight process, including fibromyalgia (FM), in which the processes of disinhibition are cortical and infracortical, demonstrated by neurophysiological as intracortical facilitation and desinhibition, as well as reduction of the power of the systems descending pain modulators. In addition, studies have shown a severity of inhibition of central positive correlation with BDNF (Brain Derived Neurotrophic Factor) levels and seems to have some relation to the peripheral nociceptive pathways, as the areas of application of the stimulation depend on the primary motor cortex (M1) is the most studied target and the largest contingent of selection for the treatment of pain and motor reaction, while the dorsolateral prefrontal cortex (DLPFC) was effective in the treatment of depression and psychoaffective components in cases of patients with the chronic condition. Although tDCS has been successful in treating FM, its main limiter is a need for the service center for consecutive days as it has cumulative effect. In fact, the erasure of the sessions guaranteed the therapeutic effect of the ETCC. The application of measures on consecutive days motivated the study of its value when applied at the household level, in order to allow the large-scale treatment technique to be adopted in the Unified Health System. This is proved by two studies. The first objective is to examine whether a fine-fiber dysfunction that occurs in patients with FM is linked to an operation of the pain-modulating system. Neuropathy of long nerve fibers has been implicated by a descriptor of pain, neurophysiological and psychophysiological neurophysiology, as well as skin biopsy studies. However, this comparison was not associated with dysfunction in the descending pain system (DPMS) not on FM. Objective did the study explore the association of dysfunction of small fibers with the DPMS and other substitutes for nociceptive changes in FM. In the second, the term is a measure of long-term use of ETCC at household level in FM Study I: In this first study evaluating the presence of nerve and peripheral fiber failure, it is linked to the functioning of the descending pain modulator system (DPMS) in FM Methods: It was performed an exploratory study with 41 FM women and 28 healthy volunteers whose were evaluated in psychophysical tests that evaluated a function of sensory fibers involved in nociception. The quantitative sensory test (QST) was used to measure the Heat thermal threshold (HTT), the heat pain threshold (HPT) and the thermal pain tolerance (HPTo), as well as the numerical scale of pain (NPS0 -10 ) over a task of modulation of conditioned pain (CPM-task). Algometry was used to determine the pain pressure threshold (PPT). Scales for evaluation of catastrophic, anxiety, depression and sleep disorders were also applied. Brain-derived neurotrophic factor (BDNF) was measured as a marker of neuroplasticity. Multivariate linear regression models by group (health and FM) for a relationship between a descending modulatory system function and its relationship with psychophysical measures. Results: The samples differed in their psychological profile, and in the psychophysical measures, the group and the patients with FM had lower sensitivity and pain thresholds. At FM, regression models revealed that HTT was related to BDNF and CPM-Task (Hotelling's Trace = 1.80, P <0.001, power = 0.94, R2 = 0.64). HTT was positively correlated with a CPM task (B = 0.98, P = 0.004, partial-ƞ2 = 0.25), and HPT (B = 1.61, P = 0.008, partial -ƞ2 = 0.21) . However PPT was not correlated with HTT. In FM, the relationship of BDNF with CPM, a negative relation was found (B = -0.04, P = 0.043, partial- = 2 = 0.12) and HPT was proportionally (B = -0.08, P = 0.03, partial-ƞ2 = 0.14). BDNF did not influence the model. And the adverse effects reported were higher in the active group (17.8%) compared to the sham group (6.6%). Conclusion: Peripheral sensory dysfunction is positively associated with the modulating dysfunction of BDNF levels in FM, which does not occur in isolated individuals. Study II: The second study had the purpose of evaluating the home use of 60 sessions of atDCS and s-tDCS on a left DLPFC area in patients with FM. Methods: A randomized, double-blind, parallel-sham controlled study in 20 women with FM. Stimulation was performed for five consecutive days in the week for 30 min at the intensity of 2 mA for 12 weeks, totaling 60 sessions. Patients were trained to use equipment specially designed for home use and maintained contact with the researcher responsible through daily text message. The effects were measured through visual pain scale (VAS) daily during the course of 12 weeks of treatment, as well as the use of analgesics and possible adverse events daily. The levels of depression, catastrophism and disability for daily tasks were assessed. The QST was used to check pain threshold and tolerance to heat, an algometry was used to check pressure pain threshold (PPT) and blood collection was performed to evaluate serum BDNF levels at baseline, after 30 sessions and at the end of treatment. A Mixed Linear Model with fixed effects was used to compare changes in pain scores in VAS throughout the treatment. Results: Home-based tDCS reduced dairy pain VAS scores (p<0.001), with cumulative mean pain drop of 64% (p<0.001). Furthermore, active home-based tDCS reduced significantly disability due to pain [B-PCP:S total scores (p=0.023; partial-ƞ2=0.61]. And also reduced scores in clinical measures like depression scores, catastrophizing pain scores and sleep quality scores [BDI-II and PCS (p<0.05), PSQI (p<0.05)]. However, active homebased tDCS enhance scores in algometry (PPT) and heat pain tolerance (HPTo) (p<0.01). Conclusion: Home-based anodal tDCS applied over the DLPFC in FM had a baseline neuroplasticity-dependent reduction effect on pain. In addition, it improved the disability due to pain, depressive symptoms and pain catastrophizing. It reduced the analgesic use and increased pressure and heat pain tolerance.

Fibromialgia

Dor

Plasticidade neuronal

BDNF

Conditioned pain modulation (CPM)

Fibromyalgia

Neuroplasticity

Eficácia da estimulação transcraniana com corrente contínua de longo prazo em nível domiciliar sobre o córtex pré-frontal dorsolateral esquerdo na fibromialgia : um ensaio clínico randomizado

Brietzke, Aline Patrícia

January 2018

Introdução: Estimulação transcraniana com corrente contínua (ETCC) é um método não invasivo de estimulação cerebral que modifica o potencial de repouso da membrana neuronal através de uma corrente elétrica de baixa intensidade. Trata-se de uma técnica neuromodulatória aplicável ao contexto terapêutico de disfunções do sistema nervoso implicados na fisiopatologia da dor e transtornos neuropsiquiátricos, com baixo custo, mínimos efeitos adversos e fácil aplicação. A ETCC tem se mostrado eficaz no tratamento de dores crônicas incluindo a fibromialgia (FM) em curto prazo. Seu uso se sustenta na melhor compreensão dos mecanismos fisiopatológicos dessa síndrome, os quais incluem processos de desinibição em nível cortical e infracortical, demonstrado por medidas neurofisiológicas como facilitação e desinibição, assim como redução da potência dos sistemas modulatórios descendentes da dor, além de alterações nas vias nociceptivas periféricas, como as fibras nervosas finas. No entanto, essa alteração isolada não foi previamente associada à disfunção no sistema de modulação descendente da dor (SMDD), observado na FM. As áreas de aplicação da ETCC dependem do objetivo terapêutico. O córtex motor primário (M1) é o alvo mais estudado e com maior contingente de evidências para o tratamento da dor e reabilitação motora, enquanto o córtex pré-frontal dorsolateral esquerdo (DLPFC) tem sido eficaz na depressão e melhora dos componentes psicoafetivos dos pacientes com dor crônica. Seu principal limitador prático é a necessidade de ir ao centro de atendimento durante dias consecutivos, pois o efeito terapêutico sustentado da ETCC necessita repetição das sessões Objetivos: Esta tese está constituída por dois estudos. O primeiro objetiva examinar se a disfunção de fibras finas que ocorre em pacientes com FM está ligada a um mau funcionamento do sistema modulador descendente da dor. No segundo, o objetivo é avaliar a eficácia do uso em longo prazo da ETCC em nível domiciliar na FM, com o objetivo de facilitar o uso e permitir a disponibilização desta técnica a pacientes do Sistema Único de Saúde. Estudo I: No primeiro estudo avaliamos se a disfunção de fibras nervosas finas periféricas está ligada a um mau funcionamento do sistema modulador descendente da dor (SMD) na FM. Métodos: Foi realizado um estudo exploratório no qual 41 mulheres com FM e 28 voluntárias saudáveis foram submetidas a testes psicofísicos que avaliaram a função de fibras sensitivas envolvidas na nocicepção. O teste quantitativo sensorial (QST) foi utilizado para medir o limiar perceptivo térmico (HTT), o limiar de dor térmica (HPT) e o limiar de tolerância à dor térmica (HPTo), bem como avaliar a mudança na Escala Numérica de Dor (NPS0-10) durante uma tarefa de modulação da dor condicionada (CPM-task). A algometria foi utilizada para determinar o limiar de pressão de dor (PPT). Escalas para avaliação de catastrofização, ansiedade, depressão e distúrbios do sono também foram aplicadas. O fator neurotrófico derivado do cérebro (BDNF) foi medido como um marcador de neuroplasticidade. Realizamos modelos de regressão linear multivariada por grupo (saudáveis e FM) para estudar a relação entre a função do SMD e sua relação com as medidas psicofísicas. Resultados: As amostras diferiram em seu perfil psicológico, e nas medidas psicofísicas, o grupo e pacientes com FM apresentou menor sensibilidade e limiares de dor. Na FM, mas não nos saudáveis, os modelos de regressão revelaram que o HTT estava relacionado ao BDNF e ao CPM-Task (Hotelling's Trace = 1,80, P<0,001, poder=0,94, R2=0,64). HTT foi correlacionado positivamente com a CPM-task (B = 0,98, P= 0,004, Partial-ƞ2=0,25), e ao HPT (B=1,61, P=0,008, parcial -ƞ2= 0,21). No entanto PPT não foi correlacionado com o HTT. Na FM a relação do BDNF com CPM-Task teve uma relação negativa (B=-0,04, P=0,043, parcial-ƞ2=0,12) e a HPT foi diretamente proporcional (B= - 0,08, P=0,03, parcial-ƞ2 = 0,14). O BDNF não influenciou no modelo. E os efeitos adversos relatados foram maiores no grupo ativo (17,8%) em comparação com o grupo sham (6,6%). Conclusão: A disfunção sensorial periférica está associada positivamente à disfunção do sistema modulatório descendente da dor e aos níveis séricos de BDNF na FM, o que não ocorre em indivíduos saudáveis. Estudo II: O segundo estudo teve como objetivo avaliar a eficácia do uso domiciliar de 60 sessões da ETCC-ativa e ETCC-simulada aplicadas sobre a área DLPFC esquerda, nas pacientes com diagnóstico de FM. Métodos: Foi realizado um ensaio clínico randomizado, duplo cego, em paralelo, controlado com ETCC-simulada em 20 mulheres com diagnóstico de fibromialgia. A estimulação foi realizada durante cinco dias consecutivos na semana, durante 30 min, com a intensidade de 2 mA, por 12 semanas, totalizando 60 sessões. As pacientes receberam treinamento para uso do equipamento especialmente desenvolvido para uso domiciliar e mantinham contato com o pesquisador responsável por meio de mensagem de texto diariamente. Os efeitos foram medidos por meio da escala visual de dor (EAV) durante o curso de 12 semanas de tratamento, bem como o uso de analgésicos e possíveis eventos adversos, diariamente. Foram avaliados os níveis de depressão, catastrofismo e capacidade funcional para tarefas diárias, QST para verificar limiar de dor e tolerância ao calor, PPT e dosagem dos níveis séricos de BDNF no início, após 30 sessões e no final do tratamento. Um modelo linear misto com efeitos fixos foi usado para comparar mudanças nos escores de dor na EAV ao longo do tratamento. Resultados: A ETCC ativa domiciliar reduziu os escores de dor pela EAV (p<0.001) quando comparado ao sham, com uma redução média de dor de 64% (p<0.001). Além disso, ETCC ativa reduziu significativamente a incapacidade relacionada a dor [B-PCP:S escore total (p=0.023);-ƞ2=0.61]. Também reduziu os escores nas medidas clínicas de depressão, catastrofismo e qualidade do sono [BDI-II, PCS e PSQI (p<0.05)]. No entanto, ETCC ativa aumentou os escores na algometria (PPT) e tolerância térmica (HPTo) (p<0.01). O BDNF não influenciou no modelo. Os efeitos adversos relatados foram maiores no grupo ativo (17,8%) em comparação com o grupo sham (6,6%). Conclusão: A ETCC para uso domiciliar mostrou-se segura e eficaz na redução da dor, incapacidade relacionada a dor, sintomas depressivos e catastróficos e redução do uso de analgésicos. O conjunto de dados desta tese sugere que em pacientes fibromiálgicas, o nível de disfunção do sistema modulador descendente da dor está relacionado ao nível de disfunção de fibras nervosas finas periféricas envolvidas na nocicepção. Além disso, a ETCC de longo prazo em fibromiálgicas foi eficaz na melhora dos sintomas disfuncionais relacionados à dor crônica e se mostrou adequada para uso domiciliar. / Introduction: Transcranial direct current stimulation (tDCS) is a noninvasive method of brain stimulation that modifies the resting potential of the neuronal membrane through a low intensity electrical current. It is a neuromodulatory technique to the therapeutic context of dysfunctions of the nervous system implicit in physiotherapy and neuropsychological disorders, with low cost, adverse effects and easy application. tDCS has been effective without a chronic fight process, including fibromyalgia (FM), in which the processes of disinhibition are cortical and infracortical, demonstrated by neurophysiological as intracortical facilitation and desinhibition, as well as reduction of the power of the systems descending pain modulators. In addition, studies have shown a severity of inhibition of central positive correlation with BDNF (Brain Derived Neurotrophic Factor) levels and seems to have some relation to the peripheral nociceptive pathways, as the areas of application of the stimulation depend on the primary motor cortex (M1) is the most studied target and the largest contingent of selection for the treatment of pain and motor reaction, while the dorsolateral prefrontal cortex (DLPFC) was effective in the treatment of depression and psychoaffective components in cases of patients with the chronic condition. Although tDCS has been successful in treating FM, its main limiter is a need for the service center for consecutive days as it has cumulative effect. In fact, the erasure of the sessions guaranteed the therapeutic effect of the ETCC. The application of measures on consecutive days motivated the study of its value when applied at the household level, in order to allow the large-scale treatment technique to be adopted in the Unified Health System. This is proved by two studies. The first objective is to examine whether a fine-fiber dysfunction that occurs in patients with FM is linked to an operation of the pain-modulating system. Neuropathy of long nerve fibers has been implicated by a descriptor of pain, neurophysiological and psychophysiological neurophysiology, as well as skin biopsy studies. However, this comparison was not associated with dysfunction in the descending pain system (DPMS) not on FM. Objective did the study explore the association of dysfunction of small fibers with the DPMS and other substitutes for nociceptive changes in FM. In the second, the term is a measure of long-term use of ETCC at household level in FM Study I: In this first study evaluating the presence of nerve and peripheral fiber failure, it is linked to the functioning of the descending pain modulator system (DPMS) in FM Methods: It was performed an exploratory study with 41 FM women and 28 healthy volunteers whose were evaluated in psychophysical tests that evaluated a function of sensory fibers involved in nociception. The quantitative sensory test (QST) was used to measure the Heat thermal threshold (HTT), the heat pain threshold (HPT) and the thermal pain tolerance (HPTo), as well as the numerical scale of pain (NPS0 -10 ) over a task of modulation of conditioned pain (CPM-task). Algometry was used to determine the pain pressure threshold (PPT). Scales for evaluation of catastrophic, anxiety, depression and sleep disorders were also applied. Brain-derived neurotrophic factor (BDNF) was measured as a marker of neuroplasticity. Multivariate linear regression models by group (health and FM) for a relationship between a descending modulatory system function and its relationship with psychophysical measures. Results: The samples differed in their psychological profile, and in the psychophysical measures, the group and the patients with FM had lower sensitivity and pain thresholds. At FM, regression models revealed that HTT was related to BDNF and CPM-Task (Hotelling's Trace = 1.80, P <0.001, power = 0.94, R2 = 0.64). HTT was positively correlated with a CPM task (B = 0.98, P = 0.004, partial-ƞ2 = 0.25), and HPT (B = 1.61, P = 0.008, partial -ƞ2 = 0.21) . However PPT was not correlated with HTT. In FM, the relationship of BDNF with CPM, a negative relation was found (B = -0.04, P = 0.043, partial- = 2 = 0.12) and HPT was proportionally (B = -0.08, P = 0.03, partial-ƞ2 = 0.14). BDNF did not influence the model. And the adverse effects reported were higher in the active group (17.8%) compared to the sham group (6.6%). Conclusion: Peripheral sensory dysfunction is positively associated with the modulating dysfunction of BDNF levels in FM, which does not occur in isolated individuals. Study II: The second study had the purpose of evaluating the home use of 60 sessions of atDCS and s-tDCS on a left DLPFC area in patients with FM. Methods: A randomized, double-blind, parallel-sham controlled study in 20 women with FM. Stimulation was performed for five consecutive days in the week for 30 min at the intensity of 2 mA for 12 weeks, totaling 60 sessions. Patients were trained to use equipment specially designed for home use and maintained contact with the researcher responsible through daily text message. The effects were measured through visual pain scale (VAS) daily during the course of 12 weeks of treatment, as well as the use of analgesics and possible adverse events daily. The levels of depression, catastrophism and disability for daily tasks were assessed. The QST was used to check pain threshold and tolerance to heat, an algometry was used to check pressure pain threshold (PPT) and blood collection was performed to evaluate serum BDNF levels at baseline, after 30 sessions and at the end of treatment. A Mixed Linear Model with fixed effects was used to compare changes in pain scores in VAS throughout the treatment. Results: Home-based tDCS reduced dairy pain VAS scores (p<0.001), with cumulative mean pain drop of 64% (p<0.001). Furthermore, active home-based tDCS reduced significantly disability due to pain [B-PCP:S total scores (p=0.023; partial-ƞ2=0.61]. And also reduced scores in clinical measures like depression scores, catastrophizing pain scores and sleep quality scores [BDI-II and PCS (p<0.05), PSQI (p<0.05)]. However, active homebased tDCS enhance scores in algometry (PPT) and heat pain tolerance (HPTo) (p<0.01). Conclusion: Home-based anodal tDCS applied over the DLPFC in FM had a baseline neuroplasticity-dependent reduction effect on pain. In addition, it improved the disability due to pain, depressive symptoms and pain catastrophizing. It reduced the analgesic use and increased pressure and heat pain tolerance.

Fibromialgia

Dor

Plasticidade neuronal

BDNF

Conditioned pain modulation (CPM)

Fibromyalgia

Neuroplasticity