Effects of a health education program on cytokines and cortisol levels in fibromyalgia patients: a randomized controlled trial

Pernambuco, Andrei Pereira; Carvalho, Lucina de Souza Cota; Schetino, Luana Pereira Leite; Polese, Janaíne Cunha; Viana, Renato de Souza; Reis, Débora d’ Ávila

doi:10.1186/s42358-018-0022-z

Abstract

Background:

Fibromyalgia (FM) is a syndrome characterized by widespread chronic pain associated to other symptoms, such as: fatigue, anxiety, depression and sleep disorders. Health education programs (HEP) have emerged as good non-pharmacological strategies to treat it. However, it is still not clear if the benefits are only subjective, or it has also objective impacts on immune and or neuroendocrine systems.

Methods:

Fifty-eight fibromyalgia women were randomly allocated in experimental group (n = 27) or control group (n = 31). The experimental group was submitted to HEP treatment for 11 weeks, while control group did not receive intervention at the same period. All data were collected at zero and 11th week by a blinded researcher. The statistical analysis were made in GraphPad Prism software (version 5.0) with significant level adjusted for α = 0.05.

Results:

Forty-four patients concluded the full study, 21 in the experimental group and 23 in the control group. Intragroup and intergroup analysis revealed that treatment induced significant increases of IL-4 plasma levels, antiinflammatory cytokine/inflammatory cytokine ratio (AC/IC ratio), salivary cortisol levels, in addition to significant decreases on FIQ scores. Intergroup variation analyses revealed also significant increases of IL-10 plasma levels.

Conclusion:

The results presented suggest that this kind of HEP could induce subjective and objective changes (immune and neuroendocrine), that could explain, at least in part the improvement of fibromyalgia patient's health status. (Clinical Trial Registration Number - ReBEC - RBR-5tdnbr).

Keywords:
Fibromyalgia; Health education program; Treatment; Cortisol; Cytokines

Background

Fibromyalgia (FM) is a syndrome characterized by chronic widespread pain associated to others symptoms such as fatigue, anxiety, depression and sleep disturbances [¹1. Wolfe F, Hauser W. Fibromyalgia diagnosis and diagnostic criteria. Ann Med. 2011;43(7):495-502. Epub 2011/07/21]. Some studies have provided evidence of the neuroendocrine and immune systems involvement in FM, [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18–⁵5. Pernambuco AP, Schetino LP, Viana RS, Carvalho LS, d’Avila Reis D. The involvement of melatonin in the clinical status of patients with fibromyalgia syndrome. Clin Exp Rheumatol. 2015;33(1 Suppl 88):S14-9. Epub 2014/02/26] but its pathophysiology remain unclear despite all studies in the area [⁶6. Sarzi-Puttini P, Atzeni F, Di Franco M, Buskila D, Alciati A, Giacomelli C, et al. Dysfunctional syndromes and fibromyalgia: a 2012 critical digest. Clin Exp Rheumatol. 2012;30(6 Suppl 74):143-51. Epub 2013/02/27].

FM has been considered a clinical condition derived from disturbances in the stress system, with abnormalities in the hypothalamic-pituitary-adrenal (HPA) axis and in the serotoninergic system [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29, ⁷7. Mease P, Arnold LM, Bennett R, Boonen A, Buskila D, Carville S, et al. Fibromyalgia syndrome. J Rheumatol. 2007;34(6):1415-25. Epub 2007/06/07, ⁸8. Cordero MD, Alcocer-Gomez E, Cano-Garcia FJ, de Miguel M, Sanchez- Alcazar JA, Moreno Fernandez AM. Low levels of serotonin in serum correlates with severity of fibromyalgia. Medicina clinica. 2010;135(14):644-6. Epub 2010/07/02. Bajos valores de serotonina en suero se correlacionan con la gravedad de los sintomas de la fibromialgia]. Patients bearing this syndrome present significant abnormalities in the levels of some hormones such as melatonin [⁵5. Pernambuco AP, Schetino LP, Viana RS, Carvalho LS, d’Avila Reis D. The involvement of melatonin in the clinical status of patients with fibromyalgia syndrome. Clin Exp Rheumatol. 2015;33(1 Suppl 88):S14-9. Epub 2014/02/26] and cortisol, [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29] and of inflammatory cytokines [⁴4. Pernambuco AP, Schetino LP, Alvim CC, Murad CM, Viana RS, Carvalho LS, et al. Increased levels of IL-17A in patients with fibromyalgia. Clin Exp Rheumatol. 2013; Epub 2013/09/12]. For the treatment of this chronic condition, a range of pharmacological and non-pharmacological treatments have been used, however, its multifactorial etiology, associated with patients’ clinical heterogeneity has turned out extremely difficult to establish efficient therapeutic practices [⁶6. Sarzi-Puttini P, Atzeni F, Di Franco M, Buskila D, Alciati A, Giacomelli C, et al. Dysfunctional syndromes and fibromyalgia: a 2012 critical digest. Clin Exp Rheumatol. 2012;30(6 Suppl 74):143-51. Epub 2013/02/27].

Regarding the non-pharmacological treatments, health education programs (HEP) have been successfully adopted in some cases. They can induce healthy habits, coping strategies and empowerment, and their benefits have been demonstrated through clinical progress evaluations, that consider subjective variables such as pain level, fatigue, sleep quality, anxiety and depression [⁹9. Lemstra M, Olszynski WP. The effectiveness of multidisciplinary rehabilitation in the treatment of fibromyalgia: a randomized controlled trial. Clin J Pain. 2005;21(2):166-74. Epub 2005/02/22–¹¹11. Mannerkorpi K, Nyberg B, Ahlmen M, Ekdahl C. Pool exercise combined with an education program for patients with fibromyalgia syndrome. A prospective, randomized study. J Rheumatol. 2000;27(10):2473-81. Epub 2000/10/19].

In the current study we aimed to evaluate if HEP could impact on objective immune and neuroendocrine parameters, besides subjective variables. For this purpose, after 11 week of intervention, we evaluated plasma levels of cytokines: IL-2, IL-4, IL-6, IL-10, TNF, and IL-17A, salivary cortisol levels, and general health status of FM patients evaluated through the self-administered Fibromyalgia Impact Questionnaire (FIQ).

Methods

Ethical aspects

The research protocol was approved by Human Research Committee of XXXXX and by the XXXXX (protocol numbers: 0224.0.203.000-10 and 141/2010). All participants were volunteers and provided written informed consent before inclusion in this study.

Sample size calculation

Based on previous studies that has used the similar intervention [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.] and outcomes^2,12,13 which included sample sizes varying between 15 and 30 participants per group, it was estimate a minimum of 21 participants for each group. In order to verify the statistical power of the results achieved with that sample size, a posteriori calculation was performed, using the G*Power software (Version 3.1.9.2), [¹²12. Faul F, Erdfelder E, Lang AG, Buchner A. G*power 3: a flexible statistical power analysis program for the social, behavioral, and biomedical sciences. Behav Res Methods. 2007;39:175-91.] considering a 0.05 significance level (α = 0.05) and a power of 80% (|3 = 0.20). The variable AC/IC ratio values were used for calculation.

Participants

Patient recruitment was done through advertisements in local radio, print newspapers and posters displayed in health facilities of Formiga, Minas Gerais, Brasil. All potential patients were submitted to clinical evaluation for the research physician to confirm the FM diagnosis according to the 1990's American College of Rheumatology (ACR) criteria [¹³13. Wolfe F, Smythe HA, Yunus MB, Bennett RM, Bombardier C, Goldenberg DL, et al. The American College of Rheumatology 1990 criteria for the classification of fibromyalgia. Report of the multicenter criteria committee. Arthritis Rheum. 1990;33(2):160-72. Epub 1990/02/01]. The new diagnosis criteria [¹1. Wolfe F, Hauser W. Fibromyalgia diagnosis and diagnostic criteria. Ann Med. 2011;43(7):495-502. Epub 2011/07/21] was not used because they were published after submission of the research project to the Ethics Committee. It was included every women with: confirmed FM diagnosis, those aged between 18 and 60 years old, fluent in Portuguese and who that gave written informed consent. It was excluded every woman that: were not literate, have not confirmed the FM diagnosis, those aged under 18 and over 60 years old, who had past or present of chronic inflammatory disease (such as spondyloarthritis and ankylosing spondylitis) or autoimmune diseases (such as systemic lupus erythematosus or rheumatoid arthritis), who had past or present of psychiatric diseases (such as major depression, schizophrenia, bipolar disorder), who presented acute infectious disease at the time of data collect, who had used anti-allergic, antibiotics or anti-inflammatory drugs in the last three months, those who got pregnant or breast-feeding and those who had no pharmacological stability for a period of at least three months before the beginning of the intervention or who changed medicines during the intervention period [⁴4. Pernambuco AP, Schetino LP, Alvim CC, Murad CM, Viana RS, Carvalho LS, et al. Increased levels of IL-17A in patients with fibromyalgia. Clin Exp Rheumatol. 2013; Epub 2013/09/12, ⁵5. Pernambuco AP, Schetino LP, Viana RS, Carvalho LS, d’Avila Reis D. The involvement of melatonin in the clinical status of patients with fibromyalgia syndrome. Clin Exp Rheumatol. 2015;33(1 Suppl 88):S14-9. Epub 2014/02/26]. No man was selected for the study because fibromyalgia affects up to nine women for each affected man, [⁶6. Sarzi-Puttini P, Atzeni F, Di Franco M, Buskila D, Alciati A, Giacomelli C, et al. Dysfunctional syndromes and fibromyalgia: a 2012 critical digest. Clin Exp Rheumatol. 2012;30(6 Suppl 74):143-51. Epub 2013/02/27] in addition the inclusion of men in a sample composed mostly of women could generate interpretation bias.

Study design

It is a randomized clinical trial with parallel group approved by Brazilian Register of Clinical Trials ReBEC-RBR-5tdnbr (full protocol available in http://www.ensaiosclinicos.gov.br/rg/RBR-5tdnbr/). Seventy-five women were enrolled to the study, but only fifty-eight had confirmed FM diagnosis. Those 58 women were randomly allocated by envelope at experimental or control group. The experimental group was submitted to treatment by Inter-relational School of fibromyalgia, while the control group did not receive intervention at the same period. Both groups had collected blood and saliva samples and filled the FIQ questionnaire at zero and 11th week. All data were collected by a blinded researcher regarding the study objectives and groups (Fig. 1).

Fig. 1
CONSORT flow diagram for individual randomized, controlled trials of non-pharmacological treatment

Intervention

The experimental group was submitted to the HEP based on the “Inter-relational School of Fibromyalgia (ISF), [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.] with some modifications. The intervention started in June 2012. The description of the activities is shown at Table 1. The original ISF use predominantly vertical lectures, but we opted for more patient-oriented and interactive approaches. In each meeting day, the monitors briefly presented the general issue to be addressed, and soon after started up a casual conversation that was based on personal questions raised by the attendees. The duration of the intervention was eleven weeks with a face-to-face meeting once a week and a pause of fifteen days between the sixth and seventh week. This pause was considering important to allow the incorporation of the activities to the daily routine of the participants [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.]. Each meeting had two health professionals whose formation varied according to the discussed topic [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.]. The duration of the intervention, the number of meetings, the break and the topics covered in each meeting were based on the original study by Souza et al. [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.].

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Table 1
Description of activities

During the first eleven weeks, the control group was not submitted to any intervention. Patients were kept in hold and they submitted to the HEP treatment only after the completion of the research.

Data collection

A trained professional unknowing the study objectives and groups performed all data collection. All data of interest were collected in both groups at the same time and in two moments: a) baseline - before intervention b) after eleven weeks of intervention (Fig. 1).

Cytokines levels

Blood sample was collected in the morning using tubes coated with ethylenediamine tetraacetic acid (EDTA) as the anticoagulant and it was immediately centrifuged for 10 min, at 4 °C and 2000 rpm and the plasma was collected and stored at -80 °C. To measure the cytokine levels it was used the BD™ Cytometric Bead Array kit (CBA) T_h1/T_h2/T_H17 according to the manufactory instructions (BD Bioscience, San Jose, CA, USA). The flow cytometer data acquisition was performed using the FACSCalibur (BD Bioscience, San Jose, CA, USA) and the data analyses were done by BD CellQuest Software (BD Bioscience, San Jose, CA, USA). The cytokines levels were calculated by FlowJo 7.6.1 Software (Tree StarTM, Inc., Ashland, OR) and were expressed as pg/ml. The AC/IC ratio was calculated by sum of anti-inflammatory cytokines (IL-4 + IL-10) and the resulted was divided by the sum of inflammatory cytokines (IL-2 + IL-6 + TNF + IL-17A).

Salivary cortisol levels

Salivary cortisol levels were used as an objective marker of HPA axis activity. Saliva samples from patients of experimental and control group were collected using cotton rolls at 8 a.m. at the day before blood sample collected. Subjects were instructed not to intake food nor brush their teeth 30 min before sample collection to avoid contamination of saliva samples, and to store saliva samples at their freezers until completing the experimental protocol and then return the samples to the laboratory. Samples were centrifuged and frozen at -20 °C until the analysis. Free cortisol in saliva was determined using a time-resolved immunoassay according manufactory instructions (DSL-10 67,100 Diagnostic Systems Laboratories, Webster, TX, USA). The sensitivity of this test was 0.071 ng/ml. The intra- and inter-assay coefficients of variation were 5.4 and 9.3% respectively.

Fibromyalgia impact questionnaire - FIQ

It is a self-administered questionnaire designed specifically to analyses the current health status of FM patients [¹⁴14. Burckhardt CS, Clark SR, Bennett RM. The fibromyalgia impact questionnaire: development and validation. J Rheumatol. 1991;18(5):728-33. Epub 1991/05/01]. It is compound by 19 questions that evaluated the physical functioning, work status (missed days of work and job difficulty) depression, anxiety, morning tiredness, pain, stiffness, fatigue and well-being over the past week. The questions are scored from 0 to 10 wherein the final score could vary from 0 to 100. Higher scores are related to more severe impact in the quality of life [¹⁴14. Burckhardt CS, Clark SR, Bennett RM. The fibromyalgia impact questionnaire: development and validation. J Rheumatol. 1991;18(5):728-33. Epub 1991/05/01]. The Brazilian version of the FIQ was used [¹⁵15. Marques AP, Santos AMB, Assumpção A, Matsutani LA, Lage LV, Pereira CAB. Validação da versão brasileira do Fibromyalgia Impact Questionnaire (FIQ). Rev Bras Reumatol. 2006;46:24-31.].

Statistical analysis

The management of the database and statistical analyzes were performed by an independent researcher, blinded regarding the groups. Professionals responsible for intervention carried out the adherence to the treatment. Descriptive statistics were performed for all outcome measures. The effect of the intervention was analyzed considering only the patients who started and completed the study. The Kolmogorov-Smirnov (with Dallal-Wilkinson Lilliefor p-value) was used to evaluate the distribution of the data. Paired t test was used for comparison between pretreatment and post treatment in both groups. Student's T test or Mann-Whitney test was used to investigate intergroup results. The post treatment data in the experimental group were also used to perform a linear regression test using the AC/ IC as dependent variable. All data were analyzed with GraphPad Prism software (version 5.0) with significance set at 5% level (α = 0.05). The results were presented as mean ± standard deviation, and intra-group and inter-group differences were also presented as mean ± standard deviation and 95% confidence interval (95% CI).

Results

Adherence to treatment

Fifth-eight patients were initially enrolled in the study, and forty-four remained until the end o of the research. In the experimental group, three women dropped out during the intervention period (two women claimed they did not have time to participate in activities due to domestic chores and one claimed that she needed to discontinue treatment to travel with her family). Moreover, three patients were excluded close to the end, two of them because of the change in pharmacological treatment, and one because of pregnancy. In the control group, six women dropped out (three of them gave up because of the waiting time, two changed their mind and one moved out). In this group, two patients were excluded because they changed pharmacological treatment (Fig. 1).

Studied groups

The mean age of the 44 women that concluded the study was 49.77 ± 11.13 years old and the body mass index (BMI) was 26.65 ± 4.70 kg/m². The mean time of diagnosis was 6.14 ± 5.55 years and mean tender point count was 16.28 ± 1.76. There were no statistical differences between groups considering age, BMI, time of diagnosis and tender point count (Table 2).

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Table 2
Studied groups

Baseline

Table 3 demonstrates that there was not significant difference between groups at the beginning of the study considering the following variables: serum levels of IL-2, IL-4, IL-6, IL-10, TNF, IL-17A, AC/IC ratio, salivary cortisol levels, and FIQ score.

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Table 3
Baseline data

Intervention effects

For intragroup analysis, differences between baseline data and 11th week data were calculated. The group that was submitted to intervention presented increasing of the following parameters analyzed: IL-4 plasma levels (MD = 0.76; 95%CI = 0.14 to 1.39; p =0.02), AC/IC ratio (MD = 0.07; 95%CI = 0.01 to 0.13; p = 0.02), and salivary cortisol levels (MD = 0.98; 95%CI = 0.18 to 1.78; p = 0,02) and significant reduced in the mean FIQ score (MD = - 30.36; 95%CI = - 39.16 to - 21.56, p < 0.01). The other data did not evidence any significant difference during the study period (Fig. 2).

Fig. 2
Intragroup analysis of FM patients from experimental group. Plasma levels of IL2 (a), IL-4 (b), IL-6 (c),IL-10 (d), TNF (e) andIL-17A (f), AC/IC ratio (g), salivary cortisol levels (h) and mean FIQ score (i) in FM patients from experimental group. Baseline data are represented in white bars while the data from eleventh week are represented in the black bars. Data were expressed as mean ± standard deviation and 95% confidence interval(95% CI). MD means mean difference. The asterisks demonstrate significant difference (p < 0.05)

The analysis of difference in the baseline data and at the end of the study in the control group did not show significant differences (Fig. 3).

Fig. 3
Intragroup analysis of FM patients from control group. Plasma levels of IL-2 (a), IL-4 (b), IL-6 (c), IL-10 (d), TNF (e) and IL-17A (f), AC/IC ratio (g), salivary cortisol levels (h) and mean FIQ score (i) in FM patients from control group. Baseline data are represented in white bars while the data from eleventh week are represented in the black bars. Data were expressed as mean ± standard deviation and 95% confidence interval(95% CI). MD means mean difference

To evaluate the intergroup analysis, it was calculated the difference between the value of each variable at the 11th week and week zero to every participant to determine the individual variation and followed the means variation of each data. This analysis showed that FM patients from experimental group had significant increased plasma levels of IL-4 (MD = 1.48; 95%CI = 0.40 to 2.56; p< 0,01) and IL-10 (MD = 0.39; 95%CI = 0.01 to 0.76; p = 0,04), such as significant increase in AC/IC ratio 0.01 to 0.19; p = 0,03) and in the salivary cortisol levels (MD = 1.35; 95%CI = 0.11 to 2.60; p = 0,03), in the other hand, it was noticed significant reduced in mean FIQ score (MD = - 31.42; 95%CI = - 42.96 to - 19.88; p < 0.01). No other data presented any significant difference between groups (Table 4).

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Table 4
Intergroup analysis at the eleventh week

The regression analysis in the experimental group showed that IL-4 levels at the end of the study explained 51% of the variance on AC/IC ratio (β = 0.06; 95%CI 0.01 to 0.11; p = 0.02).

Discussion

One of the hypotheses that try to explain the pathophysiology of FM is the central sensitization of pain transmission pathways with concomitant increase of neurotransmitters and inflammatory cytokines in the cerebrospinal fluid [¹⁶16. Meeus M, Nijs J. Central sensitization: a biopsychosocial explanation for chronic widespread pain in patients with fibromyalgia and chronic fatigue syndrome. Clin Rheumatol. 2007;26(4):465-73. Epub 2006/11/23]. Such changes appear to be related to HPA axis dysfunctions, such as decreased release of cortisol, which in turn may influence the metabolic and immune activity of the individual [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29]. We believe that the hypocortisolism presented by fibromyalgia patients is responsible for an inflammatory state with increased of inflammatory cytokines [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18, ³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29, ¹⁷17. Riva R, Mork PJ, Westgaard RH, Lundberg U. Comparison of the cortisol awakening response in women with shoulder and neck pain and women with fibromyalgia. Psychoneuroendocrinology. 2012;37(2):299-306. Epub 2011/07/19, ¹⁸18. Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis Rheum. 2006;54(8):2656-64. Epub 2006/07/28] that could affected the nociceptors [¹⁹19. Pernambuco AP, Schetino LPL, Carvalho LSC, Reis DA. Involvement of oxidative stress and nitric oxide in fibromyalgia pathophysiology: a relationship to be elucidated. Fibromyalgia: Open Access. 2016;1(1):105., ²⁰20. Albrecht PJ, Hou Q, Argoff CE, Storey JR, Wymer JP, Rice FL. Excessive Peptidergic sensory innervation of cutaneous arteriole-Venule shunts (AVS) in the palmar glabrous skin of fibromyalgia patients: implications for widespread deep tissue pain and fatigue. Pain Med. 2013;14(6):895-915. Epub 2013/05/23].

In this study, we chose to use an RCT for the study of biomarkers in FM patients because most of the research using non-pharmacological treatments for FM uses only subjective variables collected through questionnaires and or interviews [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25., ²¹21. Dobkin PL, Da Costa D, Abrahamowicz M, Dritsa M, Du Berger R, Fitzcharles MA, et al. Adherence during an individualized home based 12-week exercise program in women with fibromyalgia. J Rheumatol. 2006;33(2):333—41. Epub 2006/02/09]. However, here we would like to know if the subjective changes presented by such studies are accompanied by objective changes in biomarkers of immune and neuroendocrine activity. The biomarkers used in this study were selected because they are frequently described as altered in patients with FM [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18, ³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29, ¹⁷17. Riva R, Mork PJ, Westgaard RH, Lundberg U. Comparison of the cortisol awakening response in women with shoulder and neck pain and women with fibromyalgia. Psychoneuroendocrinology. 2012;37(2):299-306. Epub 2011/07/19, ¹⁸18. Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis Rheum. 2006;54(8):2656-64. Epub 2006/07/28]. In this sense, the HEP adopted in this study was able to promote reducing of FIQ scores, and, interestingly, it also induces objective changes revealed by changes in salivary cortisol levels, plasma cytokine levels (IL-4 and IL-10) and AC/IC ratio.

Both cytokines, IL-4 and IL-10, are very important in the modulation of immune response [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18]. IL-4 induces the phosphorylation of the transcription factor STAT6, and thus inhibits the production of some inflammatory cytokines and chemokines such as IL-1|3, IL-6, IL-8 and TNF- a by macrophages and monocytes [²²22. Albanesi C, Fairchild HR, Madonna S, Scarponi C, De Pita O, Leung DY, et al. IL-4 and IL-13 negatively regulate TNF-alpha- and IFN-gamma-induced beta-defensin expression through STAT-6, suppressor of cytokine signaling (SOCS)-1, and SOCS-3. J Immunol. 2007;179(2):984-92. Epub 2007/07/10, ²³23. Klementiev B, Enevoldsen MN, Li S, Carlsson R, Liu Y, Issazadeh-Navikas S, et al. Antiinflammatory properties of a peptide derived from interleukin-4. Cytokine. 2013;64(1):112-21. Epub 2013/08/27]. IL-10 has been considered one of the most powerful anti-inflammatory cytokines, since it blocks NFkB pathway and module JAK-STAT pathway decreasing the synthesis of IL-1, IL-6, TNF and IFNγ by macrophages and Th1 cells [²⁴24. Saraiva M, O’Garra A. The regulation of IL-10 production by immune cells. Nat Rev Immunol. 2010;10(3):170-81., ²⁵25. Mosser DM, Zhang X. Interleukin-10: new perspectives on an old cytokine. Immunol Rev. 2008;226:205-18.]. In FM patients, decreased levels of IL- 4 and IL-10 have been described [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18, ²⁶26. Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis & Rheumatism. 2006;54(8):2656-64.]. In this context, the observed HEP induced increasing in both, IL-4 and IL-10 levels, point to the success of such intervention, by inducing a more modulatory immune response. Indeed, IL-4 and IL-10 have been tested in therapeutic interventions in some autoimmune diseases such as psoriasis and rheumatoid arthritis with satisfactory results [²⁷27. Ren X, Li J, Zhou X, Luo X, Huang N, Wang Y, et al. Recombinant murine interleukin 4 protein therapy for psoriasis in a transgenic VEGF mouse model. Dermatology. 2009;219(3):232-8. Epub 2009/09/05–²⁹29. Henningsson L, Eneljung T, Jirholt P, Tengvall S, Lidberg U, van den Berg WB, et al. Disease-dependent local IL-10 production ameliorates collagen induced arthritis in mice. PLoS One. 2012;7(11):16.]. It is also important to mention that if the inflammatory changes observed in FM are really associated with dysregulation of the HPA axis, [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29] it is likely that other health conditions related to psychoemotional stress may benefit from this type of intervention [³⁰30. Cohen M, Granger S, Fuller-Thomson E. The association between bereavement and biomarkers of inflammation. Behav Med. 2013;22:22.–³²32. Hartwell KJ, Moran-Santa Maria MM, Twal WO, Shaftman S, DeSantis SM, McRae-Clark AL, et al. Association of elevated cytokines with childhood adversity in a sample of healthy adults. J Psychiatr Res. 2013;47(5):604-10.]. To confirm this hypothesis, further studies should be conducted.

Another important finding in this study was the increased AC/IC ratio presented by HEP treated group that was mainly influenced by the increased levels of IL-4. According to the literature, the imbalance between anti-inflammatory and inflammatory cytokines is one of the responsible for the occurrence and perpetuation of FM symptoms [²2. Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18, ⁴4. Pernambuco AP, Schetino LP, Alvim CC, Murad CM, Viana RS, Carvalho LS, et al. Increased levels of IL-17A in patients with fibromyalgia. Clin Exp Rheumatol. 2013; Epub 2013/09/12, ³³33. Bazzichi L, Rossi A, Massimetti G, Giannaccini G, Giuliano T, De Feo F, et al. Cytokine patterns in fibromyalgia and their correlation with clinical manifestations. Clin Exp Rheumatol. 2007;25(2):225-30. Epub 2007/06/05–³⁵35. Rodriguez-Pinto I, Agmon-Levin N, Howard A, Shoenfeld Y. Fibromyalgia and cytokines. Immunol Lett. 2014;161(2):200-3. Epub 2014/01/28]. Low levels of IL - 4 and IL-10 have been related to depressive behavior and pain (IL-4), [³¹31. Holtzman S, Abbey SE, Chan C, Bargman JM, Stewart DE. A genetic predisposition to produce low levels of IL-10 is related to depressive symptoms: a pilot study of patients with end stage renal disease. Psychosomatics. 2012;53(2):155-61.] chronic fatigue (IL-10) [³⁶36. Korenromp IHE, Grutters JC, van den Bosch JMM, Zanen P, Kavelaars A, Heijnen CJ. Reduced Th2 cytokine production by sarcoidosis patients in clinical remission with chronic fatigue. Brain Behav Immun. 2011;25(7):1498-502.] and hyperalgesia (IL-10) [²⁶26. Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis & Rheumatism. 2006;54(8):2656-64.]. In the current study, HEP induced increased levels of IL-4 and IL-10 associated with decreased in FIQ score, which in turn is an indicative of an improved clinical status and quality of life [¹⁴14. Burckhardt CS, Clark SR, Bennett RM. The fibromyalgia impact questionnaire: development and validation. J Rheumatol. 1991;18(5):728-33. Epub 1991/05/01, ¹⁵15. Marques AP, Santos AMB, Assumpção A, Matsutani LA, Lage LV, Pereira CAB. Validação da versão brasileira do Fibromyalgia Impact Questionnaire (FIQ). Rev Bras Reumatol. 2006;46:24-31.]. It is likely that the reduction in FIQ scores is related, at least in part, to the Hawthorne effect. This effect, known as the expectation effect of the individual, consists of positive changes in the behavior of subjects or groups simply because they are receiving attention or interest from others [³⁷37. Paradis E, Sutkin G. Beyond a good story: from Hawthorne effect to reactivity in health professions education research. Med Educ. 2017;51(1): 31-9. Epub 2016/09/02, ³⁸38. Leurent B, Reyburn H, Muro F, Mbakilwa H, Schellenberg D. Monitoring patient care through health facility exit interviews: an assessment of the Hawthorne effect in a trial of adherence to malaria treatment guidelines in Tanzania. BMC Infect Dis. 2016;16:59. Epub 2016/02/05]. However, some strategies used in HEP, such as stress management activities and physical activities are able to ameliorate the inflammatory process and improve the health [³⁹39. Golzari Z, Shabkhiz F, Soudi S, Kordi MR, Hashemi SM. Combined exercise training reduces IFN-gamma and IL-17 levels in the plasma and the supernatant of peripheral blood mononuclear cells in women with multiple sclerosis. Int Immunopharmacol. 2010;10(11):1415-9. Epub 2010/08/28–⁴¹41. Rosenkranz MA, Davidson RJ, MacCoon DG, Sheridan JF, Kalin NH, Lutz A. A comparison of mindfulness-based stress reduction and an active control in modulation of neurogenic inflammation. Brain Behav Immun. 2013;27C:174-84.].

The HEP treatment also induced an enhanced in the salivary morning cortisol levels, which is a clinically important finding. Hypocortisolism in FM, mainly in the morning, has been demonstrated by some studies, [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29, ⁴²42. Kadetoff D, Kosek E. Evidence of reduced sympatho-adrenal and hypothalamic-pituitary activity during static muscular work in patients with fibromyalgia. J rehab med offic j UEMS Europ Board Physic Rehab Med. 2010;42(8):765-72. Epub 2010/09/03] and it has been considered to be responsible in part by the claimed pain, fatigue and depression by FM patients [¹⁷17. Riva R, Mork PJ, Westgaard RH, Lundberg U. Comparison of the cortisol awakening response in women with shoulder and neck pain and women with fibromyalgia. Psychoneuroendocrinology. 2012;37(2):299-306. Epub 2011/07/19, ⁴³43. Wingenfeld K, Nutzinger D, Kauth J, Hellhammer DH, Lautenbacher S. Salivary cortisol release and hypothalamic pituitary adrenal axis feedback sensitivity in fibromyalgia is associated with depression but not with pain. j pain offic j Am Pain Soc. 2010;11(11):1195-202. Epub 2010/07/16]. It is important to note that the hypocortisolism presented by FM patients are related to HPA axis dysfunction, also named stress response axis [³3. Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29]. According to this theory, individuals expose to stress agents (physical or psychoemotional) for long periods could experience a phenomenon called burnout syndrome, characterized by lower cortisol production in response to stress agent [³⁰30. Cohen M, Granger S, Fuller-Thomson E. The association between bereavement and biomarkers of inflammation. Behav Med. 2013;22:22.]. We believe that the increasing of cortisol levels in the experimental group could indicate that the coping strategies taught in the ISF contributed in a positive way to these patients, helping them to live or face more adequately the different types of adversity.

In this study, 78% of those enrolled to treatment remained until the end of the 11th week (the researchers excluded 11% and the other 11% dropped out the study). If we consider only the participants who voluntarily withdrew from the study, the adherence to treatment was 89%. It has been considered that adhesion to treatment is one of the main negative points in the HEP [¹⁰10. Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25., ²¹21. Dobkin PL, Da Costa D, Abrahamowicz M, Dritsa M, Du Berger R, Fitzcharles MA, et al. Adherence during an individualized home based 12-week exercise program in women with fibromyalgia. J Rheumatol. 2006;33(2):333—41. Epub 2006/02/09]. In this study the HEP adherence level could be considered satisfactory, and we think that it could be explained mainly by the use of a patient-centered methodology, instead of using traditional models of HEP, with hierarchical relationships.

Finally, the results from the present study, in conjunction with data from the literature, reinforces the hypothesis that HEP might satisfactorily contribute to FM patients treatment. After all, in this group of FM patients, the HEP like ISF, not only promoted the subjective perception of improvement in the FM patients, but, above all, they were able to promote objective changes in biomarkers of neuroendocrine and immunological activity. Because of the sample size and clinical variability presented by people with FM, [⁶6. Sarzi-Puttini P, Atzeni F, Di Franco M, Buskila D, Alciati A, Giacomelli C, et al. Dysfunctional syndromes and fibromyalgia: a 2012 critical digest. Clin Exp Rheumatol. 2012;30(6 Suppl 74):143-51. Epub 2013/02/27] it is not possible to state that this type of intervention will promote the same benefits for all other FM patients. Thus, the use of HEP for FM should be a choice of the health professional in agreement with the patient. We encourage further studies with larger sample size and that seek to analyze other important biomarkers for fibromyalgia.

Conclusion

The HEP like ISF program significantly improved the health status of the participants underwent intervention. This was evidenced by increased plasma levels of IL-4 and IL-10, increase AC/ IC ratio, and the salivary cortisol levels of the participants underwent the intervention in addition to reduced FIQ score. Despite the limited sample size, we recommend the use of HEP like ISF to treat FM patients and we expect that this study may serve as a starting point for further investigations to clarify issues that were not addressed here.

Funding

The Fundação de Amparo à Pesquisa do Estado de Minas Gerais (FAPEMIG) financed the PhD scholarship of the APP researcher and the purchase of the reagents for laboratory analysis. The funding agency did not participate in the project's elaboration and did not participate in any stage of project execution or writing of the manuscript.
Availability of data and materials

We declare that the data collected during this research is found in databases of Excel, GraphPad Prism and SPSS software. They are currently in the possession of responsible researchers who undertake to make them available to third parties, if requested. To do so, we kindly ask you to send the request email to: pernambucoap@ymail.com

More details about the methodology can be accessed at the following link: http://www.ensaiosclinicos.gov.br/rg/RBR-5tdnbr/
Declaration

We declare that this research protocol was submitted to the Ethic Committee of Universidade Federal de Minas Gerais and to the Ethic Committee of Centro Universitário de Formiga and that the protocol was approved by both committees according to their respective decisions: ETIC n° 0224.0.203.00-10 and N° 141/210.

We also stated that all participants in the research signed a two-way informed consent form. These and other procedures were based on CNS Resolution 196/ 96 and the Helsinki Declaration.

Finally, we declare that this randomized clinical trial was protocolized and approved in the Brazilian Registry of Clinical Trials and received the Clinical Trial Registration Number (ReBEC - RBR- 5tdnbr).
Consent for publication

Not applicable.
Competing interests

We declare that there is no competing interest related to this manuscript, be it financial or otherwise.
Publisher's Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Acknowledgments

We thank the Fundação de Amparo à Pesquisa do Estado de Minas Gerais (FAPEMIG) for the financial support of the Fundação Oswaldo Cruz Foundation (FIOCRUZ) - Instituto René Rachou for laboratory analysis and the Centro Universitário de Formiga - MG (UNIFOR-MG) for logistical support to the project.

References

¹
Wolfe F, Hauser W. Fibromyalgia diagnosis and diagnostic criteria. Ann Med. 2011;43(7):495-502. Epub 2011/07/21
²
Sturgill J, McGee E, Menzies V. Unique cytokine signature in the plasma of patients with fibromyalgia. J Immunol Res. 2014;2014:938576. Epub 2014/ 04/18
³
Carvalho LS, Correa H, Silva GC, Campos FS, Baiao FR, Ribeiro LS, et al. May genetic factors in fibromyalgia help to identify patients with differentially altered frequencies of immune cells? Clin Exp Immunol. 2008;154(3):346-52. Epub 2008/11/29
⁴
Pernambuco AP, Schetino LP, Alvim CC, Murad CM, Viana RS, Carvalho LS, et al. Increased levels of IL-17A in patients with fibromyalgia. Clin Exp Rheumatol. 2013; Epub 2013/09/12
⁵
Pernambuco AP, Schetino LP, Viana RS, Carvalho LS, d’Avila Reis D. The involvement of melatonin in the clinical status of patients with fibromyalgia syndrome. Clin Exp Rheumatol. 2015;33(1 Suppl 88):S14-9. Epub 2014/02/26
⁶
Sarzi-Puttini P, Atzeni F, Di Franco M, Buskila D, Alciati A, Giacomelli C, et al. Dysfunctional syndromes and fibromyalgia: a 2012 critical digest. Clin Exp Rheumatol. 2012;30(6 Suppl 74):143-51. Epub 2013/02/27
⁷
Mease P, Arnold LM, Bennett R, Boonen A, Buskila D, Carville S, et al. Fibromyalgia syndrome. J Rheumatol. 2007;34(6):1415-25. Epub 2007/06/07
⁸
Cordero MD, Alcocer-Gomez E, Cano-Garcia FJ, de Miguel M, Sanchez- Alcazar JA, Moreno Fernandez AM. Low levels of serotonin in serum correlates with severity of fibromyalgia. Medicina clinica. 2010;135(14):644-6. Epub 2010/07/02. Bajos valores de serotonina en suero se correlacionan con la gravedad de los sintomas de la fibromialgia
⁹
Lemstra M, Olszynski WP. The effectiveness of multidisciplinary rehabilitation in the treatment of fibromyalgia: a randomized controlled trial. Clin J Pain. 2005;21(2):166-74. Epub 2005/02/22
¹⁰
Souza JB, Bourgault P, Charest J, Marchand S. Escola inter-relacional de fibromialgia: aprendendo a lidar com a dor - estudo clínico randomizado. Rev Bras Reumatol. 2008;48:218-25.
¹¹
Mannerkorpi K, Nyberg B, Ahlmen M, Ekdahl C. Pool exercise combined with an education program for patients with fibromyalgia syndrome. A prospective, randomized study. J Rheumatol. 2000;27(10):2473-81. Epub 2000/10/19
¹²
Faul F, Erdfelder E, Lang AG, Buchner A. G*power 3: a flexible statistical power analysis program for the social, behavioral, and biomedical sciences. Behav Res Methods. 2007;39:175-91.
¹³
Wolfe F, Smythe HA, Yunus MB, Bennett RM, Bombardier C, Goldenberg DL, et al. The American College of Rheumatology 1990 criteria for the classification of fibromyalgia. Report of the multicenter criteria committee. Arthritis Rheum. 1990;33(2):160-72. Epub 1990/02/01
¹⁴
Burckhardt CS, Clark SR, Bennett RM. The fibromyalgia impact questionnaire: development and validation. J Rheumatol. 1991;18(5):728-33. Epub 1991/05/01
¹⁵
Marques AP, Santos AMB, Assumpção A, Matsutani LA, Lage LV, Pereira CAB. Validação da versão brasileira do Fibromyalgia Impact Questionnaire (FIQ). Rev Bras Reumatol. 2006;46:24-31.
¹⁶
Meeus M, Nijs J. Central sensitization: a biopsychosocial explanation for chronic widespread pain in patients with fibromyalgia and chronic fatigue syndrome. Clin Rheumatol. 2007;26(4):465-73. Epub 2006/11/23
¹⁷
Riva R, Mork PJ, Westgaard RH, Lundberg U. Comparison of the cortisol awakening response in women with shoulder and neck pain and women with fibromyalgia. Psychoneuroendocrinology. 2012;37(2):299-306. Epub 2011/07/19
¹⁸
Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis Rheum. 2006;54(8):2656-64. Epub 2006/07/28
¹⁹
Pernambuco AP, Schetino LPL, Carvalho LSC, Reis DA. Involvement of oxidative stress and nitric oxide in fibromyalgia pathophysiology: a relationship to be elucidated. Fibromyalgia: Open Access. 2016;1(1):105.
²⁰
Albrecht PJ, Hou Q, Argoff CE, Storey JR, Wymer JP, Rice FL. Excessive Peptidergic sensory innervation of cutaneous arteriole-Venule shunts (AVS) in the palmar glabrous skin of fibromyalgia patients: implications for widespread deep tissue pain and fatigue. Pain Med. 2013;14(6):895-915. Epub 2013/05/23
²¹
Dobkin PL, Da Costa D, Abrahamowicz M, Dritsa M, Du Berger R, Fitzcharles MA, et al. Adherence during an individualized home based 12-week exercise program in women with fibromyalgia. J Rheumatol. 2006;33(2):333—41. Epub 2006/02/09
²²
Albanesi C, Fairchild HR, Madonna S, Scarponi C, De Pita O, Leung DY, et al. IL-4 and IL-13 negatively regulate TNF-alpha- and IFN-gamma-induced beta-defensin expression through STAT-6, suppressor of cytokine signaling (SOCS)-1, and SOCS-3. J Immunol. 2007;179(2):984-92. Epub 2007/07/10
²³
Klementiev B, Enevoldsen MN, Li S, Carlsson R, Liu Y, Issazadeh-Navikas S, et al. Antiinflammatory properties of a peptide derived from interleukin-4. Cytokine. 2013;64(1):112-21. Epub 2013/08/27
²⁴
Saraiva M, O’Garra A. The regulation of IL-10 production by immune cells. Nat Rev Immunol. 2010;10(3):170-81.
²⁵
Mosser DM, Zhang X. Interleukin-10: new perspectives on an old cytokine. Immunol Rev. 2008;226:205-18.
²⁶
Uceyler N, Valenza R, Stock M, Schedel R, Sprotte G, Sommer C. Reduced levels of antiinflammatory cytokines in patients with chronic widespread pain. Arthritis & Rheumatism. 2006;54(8):2656-64.
²⁷
Ren X, Li J, Zhou X, Luo X, Huang N, Wang Y, et al. Recombinant murine interleukin 4 protein therapy for psoriasis in a transgenic VEGF mouse model. Dermatology. 2009;219(3):232-8. Epub 2009/09/05
²⁸
Docke WD, Asadullah K, Belbe G, Ebeling M, Hoflich C, Friedrich M, et al. Comprehensive biomarker monitoring in cytokine therapy: heterogeneous, time-dependent, and persisting immune effects of interleukin-10 application in psoriasis. J Leukoc Biol. 2009;85(3):582-93. Epub 2008/11/29
²⁹
Henningsson L, Eneljung T, Jirholt P, Tengvall S, Lidberg U, van den Berg WB, et al. Disease-dependent local IL-10 production ameliorates collagen induced arthritis in mice. PLoS One. 2012;7(11):16.
³⁰
Cohen M, Granger S, Fuller-Thomson E. The association between bereavement and biomarkers of inflammation. Behav Med. 2013;22:22.
³¹
Holtzman S, Abbey SE, Chan C, Bargman JM, Stewart DE. A genetic predisposition to produce low levels of IL-10 is related to depressive symptoms: a pilot study of patients with end stage renal disease. Psychosomatics. 2012;53(2):155-61.
³²
Hartwell KJ, Moran-Santa Maria MM, Twal WO, Shaftman S, DeSantis SM, McRae-Clark AL, et al. Association of elevated cytokines with childhood adversity in a sample of healthy adults. J Psychiatr Res. 2013;47(5):604-10.
³³
Bazzichi L, Rossi A, Massimetti G, Giannaccini G, Giuliano T, De Feo F, et al. Cytokine patterns in fibromyalgia and their correlation with clinical manifestations. Clin Exp Rheumatol. 2007;25(2):225-30. Epub 2007/06/05
³⁴
Iannuccelli C, Di Franco M, Alessandri C, Guzzo MP, Croia C, Di Sabato F, et al. Pathophysiology of fibromyalgia: a comparison with the tension-type headache, a localized pain syndrome. Ann N Y Acad Sci. 2010;1193:78-83. Epub 2010/04/20
³⁵
Rodriguez-Pinto I, Agmon-Levin N, Howard A, Shoenfeld Y. Fibromyalgia and cytokines. Immunol Lett. 2014;161(2):200-3. Epub 2014/01/28
³⁶
Korenromp IHE, Grutters JC, van den Bosch JMM, Zanen P, Kavelaars A, Heijnen CJ. Reduced Th2 cytokine production by sarcoidosis patients in clinical remission with chronic fatigue. Brain Behav Immun. 2011;25(7):1498-502.
³⁷
Paradis E, Sutkin G. Beyond a good story: from Hawthorne effect to reactivity in health professions education research. Med Educ. 2017;51(1): 31-9. Epub 2016/09/02
³⁸
Leurent B, Reyburn H, Muro F, Mbakilwa H, Schellenberg D. Monitoring patient care through health facility exit interviews: an assessment of the Hawthorne effect in a trial of adherence to malaria treatment guidelines in Tanzania. BMC Infect Dis. 2016;16:59. Epub 2016/02/05
³⁹
Golzari Z, Shabkhiz F, Soudi S, Kordi MR, Hashemi SM. Combined exercise training reduces IFN-gamma and IL-17 levels in the plasma and the supernatant of peripheral blood mononuclear cells in women with multiple sclerosis. Int Immunopharmacol. 2010;10(11):1415-9. Epub 2010/08/28
⁴⁰
Bote ME, Garcia JJ, Hinchado MD, Ortega E. Fibromyalgia: anti-inflammatory and stress responses after acute moderate exercise. PLoS One. 2013;8(9): e74524. Epub 2013/09/12
⁴¹
Rosenkranz MA, Davidson RJ, MacCoon DG, Sheridan JF, Kalin NH, Lutz A. A comparison of mindfulness-based stress reduction and an active control in modulation of neurogenic inflammation. Brain Behav Immun. 2013;27C:174-84.
⁴²
Kadetoff D, Kosek E. Evidence of reduced sympatho-adrenal and hypothalamic-pituitary activity during static muscular work in patients with fibromyalgia. J rehab med offic j UEMS Europ Board Physic Rehab Med. 2010;42(8):765-72. Epub 2010/09/03
⁴³
Wingenfeld K, Nutzinger D, Kauth J, Hellhammer DH, Lautenbacher S. Salivary cortisol release and hypothalamic pituitary adrenal axis feedback sensitivity in fibromyalgia is associated with depression but not with pain. j pain offic j Am Pain Soc. 2010;11(11):1195-202. Epub 2010/07/16

Publication Dates

Publication in this collection
29 July 2019
Date of issue
2018

History

Received
29 June 2018
Accepted
13 July 2018
Published
03 Aug 2018

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] Funding

The Fundação de Amparo à Pesquisa do Estado de Minas Gerais (FAPEMIG) financed the PhD scholarship of the APP researcher and the purchase of the reagents for laboratory analysis. The funding agency did not participate in the project's elaboration and did not participate in any stage of project execution or writing of the manuscript.

[2] Availability of data and materials

We declare that the data collected during this research is found in databases of Excel, GraphPad Prism and SPSS software. They are currently in the possession of responsible researchers who undertake to make them available to third parties, if requested. To do so, we kindly ask you to send the request email to: pernambucoap@ymail.com

More details about the methodology can be accessed at the following link: http://www.ensaiosclinicos.gov.br/rg/RBR-5tdnbr/

[3] Declaration

We declare that this research protocol was submitted to the Ethic Committee of Universidade Federal de Minas Gerais and to the Ethic Committee of Centro Universitário de Formiga and that the protocol was approved by both committees according to their respective decisions: ETIC n° 0224.0.203.00-10 and N° 141/210.

We also stated that all participants in the research signed a two-way informed consent form. These and other procedures were based on CNS Resolution 196/ 96 and the Helsinki Declaration.

Finally, we declare that this randomized clinical trial was protocolized and approved in the Brazilian Registry of Clinical Trials and received the Clinical Trial Registration Number (ReBEC - RBR- 5tdnbr).

[4] Consent for publication

Not applicable.

[5] Competing interests

We declare that there is no competing interest related to this manuscript, be it financial or otherwise.

[6] Publisher's Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Meeting topic	Objective
1a - Therapeutic Contract / 1b-Workshop of the senses	Briefly introducing the nine steps of the program and negotiate the therapeutic contract. This contract has an objective to modulate the expectations of patients and consists of: a) define three realistic and measurable personal objectives; b) determine the lowest percentage of improvement in the clinical picture, acceptable (between 5 and 20%). According to the contract, participants also agree to devote 45 min/day, 6 days/week to practice the activities prescribed by the ISF such as relaxation techniques, diaphragmatic breathing, stretching, strengthening and aerobic exercise. Promoting experimentation of sensory organs. Discuss the ways in which people feel and perceive the world and the reality around them. Demonstrating deep diaphragmatic breathing.
2 -Mental Preparation	Demonstrating that the environment perceptions are related to previous experience and so then perception of pain, as well as other symptoms may also be influenced by prior experience. Demonstrate some techniques of mental preparation and coping strategies to deal with the pain. Practice yoga class with emphasis on meditation. The participant will choose a relaxation technique and practice it 3 times a week for 15 to 20 min.
3 - Physical preparation	Discussing the effects of a sedentary lifestyle and physical activity. Demonstrate warm-up, stretching, strengthening and aerobic exercises. Perform calculations to identify heart rate (HR) max. Practice session of Pilates on the ground. Prescribe an exercise program to be held at home: a) exercise routine: 6 times/week, 15 min, with stretching and strengthening; b) walk, moderate 40 to 60% HR max; 3 times/week; 30 min.
4 - Stress and individuality	Studying the hypothalamic-pituitary-adrenal axis, its importance in the homeostatic systems and stress. Discussing coping strategies that contribute to the understanding and improvement of individual levels of energy / disposition (learn to say no when necessary, defer or delegate tasks at moments of suffering, be seen and be valued)
5 - Symptoms	Studying the mechanisms involved in pain, fatigue, muscle stiffness, in sleep disorders, anxiety and depression.
6 - Nutrition	Discussing the basic components of a healthy balanced diet, the benefits of hydration and the dangers provided by foods rich in sugars, fats and or sodium.
PAUSE	2 weeks of self-employment: integration of strategies individually (without meeting with therapists).
7 - Consequence of chronicity	Discussing the influence of chronic pain on the emotional, interpersonal relationships, daily activities and sexuality. Discuss aspects related to suicidal thoughts.
8 - Treatment	Presenting and discuss scientific evidence based on the main types of pharmacological and non-pharmacological treatments currently used to treat fibromyalgia.
9 - Retrospective	Motivate patients to continue the prescribed activities. Presenting a retrospective of the issues addressed.

	Experimental (n = 21)	Control (n = 23)	Mean Difference (MD)		P value
Age (years)	51.43 ±11.26	48.26 ±11.03	3.17 ± 3.36	-3.62 a 9.96	0.35
BMI(Kg/cm²)	26.51 ± 5.18	26.82 ± 4.22	- 0.31 ± 1.53	-3.41 a 2.79	0.84
Time of diagnostic (years)	5.47 ± 5.05	6.74 ± 6.02	- 1.26 ± 1.68	-4.66 a 2.14	0.46
Tender points (number)	16.05 ± 1.79	16.48 ± 1.75	- 0.43 ± 0.54	-1.52 a 0.66	0.43

	Experimental (n = 21)	Control (n = 23)	Mean of difference (MD)	95% CI	P value
IL-2	2.79 ± 1.50	2.59 ± 1.28	0.21 ± 0.43	- 0.66 to 1.07	0.84
IL-4	1.67 ± 1.17	1.93 ± 0.93	- 0.25 ± 0.33	- 0.92 to 0.41	0.25
IL-6	4.13 ±4.08	4.83 ± 6.40	- 0.70 ± 1.73	-4.21 to 2.81	0.91
IL-10	1.13 ± 0.47	1.14 ±0.44	- 0.004 ± 0.14	-0.29 to 0.29	0.86
TNF	0.86 ± 0.92	1.11 ± 1.09	-0.25 ± 0.31	-0.87 to 0.37	0.35
IL-17A	11.45 ± 7.26	13.14 ± 8.56	-1.70 ± 2.52	-6.81 to 3.42	0.44
AC/IC ratio	0.13 ± 0.04	0.18 ± 0.11	- 0.04 ± 0.03	-0.10 to 0.01	0.13
Cortisol	5.28 ± 1.67	4.63 ± 1.35	0.64 ± 0.46	- 0.29 to 1.58	0.17
FIQ	72.65 ± 15.10	77.54 ± 8.53	- 4.89 ± 3.83	- 12.65 to 2.87	0.21

	VariationEG (EGV)	Variation CG (CGV)	MD (EGV minus CGV)	95%CI	p value
IL2	-0.56	- 0.58	0.47 ± 0.77	- 1.09 to 2.03	0.54
IL4	0.76	-0.64	**1.48 ± 0.53** ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.40 to 2.56* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*<0.01* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic
IL6	1.28	- 1.10	4.98 ± 2.69	-0.46 to 10.42	0.07
IL10	0.17	-0.23	**0.39 ± 0.18** ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.01 to 0.76* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.04* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic
TNF	0.04	-0.31	0.12 ± 0.32	- 0.53 to 0.78	0.70
IL17	0.42	1.04	-2.66 ± 4.09	-10.95 to 5.62	0.51
AC/IC ratio	0.05	-0.04	*0.10 ± 0.04* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.01 to 0.19* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.03* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic
Cortisol	0,98	-0.32	**1.35 ± 0.61** ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*1.11 to 2.60* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*0.03* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic
FIQ	-30.36	2.62	**-31.42 ± 5.70** ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	− 42.96 to − 19.88 ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic	*< 0.01* ^* * Statistically significant results were marked with an asterisk and have been shown in boldface and italic