Efeitos do treinamento de força acompanhado de oclusão vascular em pacientes com polimiosite e dermatomiosite / Efficacy and safety of low-intensity resistance training combined with partial blood flow restriction in polymyositis and dermatomyositis

Ordones, Melina Andrade Mattar

22 August 2016

INTRODUÇÃO: Polimiosite (PM) e Dermatomiosite (DM) são miopatias inflamatórias que se caracterizam por fraqueza, atrofia e disfunção muscular, levando a perda de capacidade funcional e de qualidade de vida. Assim, o objetivo do estudo foi avaliar se um treino de força com oclusão vascular (TF-OV) de baixa intensidade é seguro e efetivo em melhorar a força, a massa e a função muscular, além da qualidade de vida destes pacientes. MÉTODOS: Treze pacientes com PM ou DM estáveis foram submetidos a um TF-OV parcial e baixa intensidade (30% de 1RM) duas vezes por semana, por 12 semanas. Foram avaliados então as enzimas musculares, a força, a massa e a função muscular, além da qualidade de vida e as limitações para atividades diárias antes e após o protocolo de treinamento. RESULTADOS: Os pacientes apresentaram um aumento da força muscular do leg-press (19,6%, p < 0,001) e do leg-extension (25,2% p < 0,001), além de aumento da massa muscular avaliada pela área de secção transversa do quadríceps (4,57%, p =0,01). Nos testes funcionais, houve melhora do desempenho nos testes timed-stands (15,1%, p < 0,001) e timed-up-and-go (-4,5%, p=0,002). Foi observado melhora dos escores do HAQ e de todos os componentes do SF-36, além de queda significativa do VAS do médico e do paciente (p < 0,05), enquanto que as enzimas musculares permaneceram estáveis (p > 0,05). Por fim, nenhum evento adverso foi relatado. CONCLUSÃO: O TF-OV de baixa intensidade foi seguro e efetivo em melhorar a força, a massa e a função muscular, além da qualidade de vida dos pacientes com PM e DM estáveis / INTRODUCTION: Our aim was to evaluate the safety and efficacy of a low-intensity resistance training program combined with partial blood flow restriction (BFR training) in a cohort of patients with polymyositis (PM) and dermatomyositis (DM). METHODS: In total, 13 patients with PM and DM completed a 12-week twice a week low-intensity (that is, 30% onerepetition-maximum (1RM)) resistance exercise training program combined with partial blood flow restriction (BFR). Assessments of muscle strength, physical function, quadriceps cross sectional (CSA) area, health-related quality of life, and clinical and laboratory parameters were assessed at baseline and after the intervention. RESULTS: The BFR training program was effective in increasing the maximal dynamic strength in both the leg-press (19.6%, p < 0.001) and leg-extension exercises (25.2% p < 0.001), as well as in the timed-stands (15.1%, p < 0.001) and timed-up-and-go test (-4.5%, P =0.002). Quadriceps CSA was also significantly increased after the intervention (4.57%, p =0.01). Similarly, all of the components of the Short Form-36 Health Survey, the Health Assessment Questionnaire scores, and the patient- and physician reported Visual Analogue Scale were significantly improved after training (p < 0.05). Importantly, no clinical evidence or any other self-reported adverse event were found. Laboratory parameters (creatine kinase and aldolase) were also unchanged (p > 0.05) after the intervention. CONCLUSIONS: We demonstrated that a 12-week supervised low-intensity resistance training program associated with partial blood flow restriction may be safe and effective in improving muscle strength and function as well as muscle mass and health-related quality of life in patients with PM and DM

Dermatomiosite

Dermatomyositis

Exercício

Exercise

Hipóxia

Hypoxia

Miosite

Myositis

Polimiosite

Polymyositis

Qualidade de vida

Quality of life

Avaliação da função gonadal em pacientes do sexo masculino com dermatomiosite e polimiosite / Gonadal function evaluation in male patients with dermatomyositis and polymyositis

Ana Julia Pantoja de Moraes

20 January 2009

Objetivo: Avaliar a função gonadal de homens com miopatias inflamatórias idiopáticas (MII). Métodos: Vinte e cinco pacientes com MII foram avaliados e comparados com 25 homens saudáveis. Os pacientes foram subdivididos em dois sub-grupos de acordo com as alterações dos espermatozóides: grupo A (n=10, duas ou mais das seguintes alterações: terato/oligo/astenozoospermia ou azoospermia) e grupo B (n=15, teratozoospermia). Foram realizados: exame urológico, ultra-sonografia testicular, análise dos espermatozóides (critérios da OMS e Kruger), pesquisa dos anticorpos anti-espermatozóides e dosagens hormonais Nos subgrupos foram também avaliados: Disease Activity Score (DAS), Visual Analogue Scale (VAS), Manual Muscle Testing (MMT), myositis disease activity assessment visual analogue scales (MYOACT), myositis intention to treat activity index (MITAX), Myositis damage index [MDI], enzimas musculares e tratamento. Resultados: Pacientes apresentaram alterações nos espermatozóides comparados com controles com freqüência maior de nível elevado de FSH (20% versus 0%, p=0,05). O sub-grupo A apresentou freqüência e mediana maior do nível de CK (p=0,001 e p=0,001) assim como DAS (p=0,01), VAS (p=0,051), MMT (p=0,003). As medianas dos volumes testiculares foram menores no grupo A (direito, p=0,015 e esquerdo, p=0,025). As medianas dos parâmetros espermáticos foram reduzidas no grupo A [contagem total (p=0,0001); motilidade (p=0,0001); morfologia pela OMS (p=0,0001) e por Kruger (p=0,0001). A mediana de FSH foi elevada (p=0,035) e de androstenediona foi reduzida (p=0,02) no sub-grupo A. Afrequência de ciclofosfamida foi similar nos grupos (30% versus 6%, p=0,26). Conclusões: Atividade da doença foi o principal fator contribuinte para disfunção gonadal. Hipogonadismo hipergonadotrófico pode explicar as alterações anatômicas e funcionais observadas / Objective: To perform a global gonad evaluation in male idiopathic inflammatory myopathies (IIM) patients. Methods: Twentyfive consecutive IIM were compared to 25 age-matched healthy subjects. Patients were subdivided in two groups according to the severity of sperm abnormalities: group A (at least two of the following terato/oligo/asthenozoospermia or azoospermia) and group B (teratozoospermia). Patients and controls underwent a systematic assessment consisting of: urologic examination, testicular ultrasound, semen analysis and hormones. Patients´ serum CK levels, visual analogue scale (VAS), disease activity score (DAS), manual muscle testing (MMT), myositis disease activity assessment visual analogue scales (MYOACT), myositis intention to treat activity index (MITAX), and Myositis damage index (MDI) were evaluated. Results: Several sperm variables were significantly altered compared to controls (p<0.05). The subgroup analysis according to the severity of sperm alterations revealed that the frequency of elevated CK and its median level was significantly higher in group A (p=0.001 and p=0.001), as also was DAS, VAS and MMT (p=0.01; p=0.051 and p=0.03). The median of testicular volumes were lower in group A (right p=0.015 and left p=0.025). All median sperm parameters were lower in group A (total sperm count, p=0.0001; total motile sperm count, p=0.0001; and sperm morphology by Kruger p=0.0001 and WHO p=0.0001). Higher median FSH (p=0.035) and lower median androstenedione levels (p=0.02) were observed in group A. The frequency of cyclophosphamide was similar in both groups (30% vs. 6%, p=0.26). Conclusions: Active disease was the major contributing factor for severe gonad dysfunction. The hypergonadotrophic hypogonadism may explain the anatomical and dysfunctional alterations observed

Dermatomiosite

Espermatozóides

Gônadas

Hormônios

Masculino

Polimiosite

Ultra-sonografia

Dermatomyositis

Gonads

Hormones

Male

Polymyositis

Spermatozoa

Ultrasonography

Efeitos do treinamento de força acompanhado de oclusão vascular em pacientes com polimiosite e dermatomiosite / Efficacy and safety of low-intensity resistance training combined with partial blood flow restriction in polymyositis and dermatomyositis

Melina Andrade Mattar Ordones

22 August 2016

INTRODUÇÃO: Polimiosite (PM) e Dermatomiosite (DM) são miopatias inflamatórias que se caracterizam por fraqueza, atrofia e disfunção muscular, levando a perda de capacidade funcional e de qualidade de vida. Assim, o objetivo do estudo foi avaliar se um treino de força com oclusão vascular (TF-OV) de baixa intensidade é seguro e efetivo em melhorar a força, a massa e a função muscular, além da qualidade de vida destes pacientes. MÉTODOS: Treze pacientes com PM ou DM estáveis foram submetidos a um TF-OV parcial e baixa intensidade (30% de 1RM) duas vezes por semana, por 12 semanas. Foram avaliados então as enzimas musculares, a força, a massa e a função muscular, além da qualidade de vida e as limitações para atividades diárias antes e após o protocolo de treinamento. RESULTADOS: Os pacientes apresentaram um aumento da força muscular do leg-press (19,6%, p < 0,001) e do leg-extension (25,2% p < 0,001), além de aumento da massa muscular avaliada pela área de secção transversa do quadríceps (4,57%, p =0,01). Nos testes funcionais, houve melhora do desempenho nos testes timed-stands (15,1%, p < 0,001) e timed-up-and-go (-4,5%, p=0,002). Foi observado melhora dos escores do HAQ e de todos os componentes do SF-36, além de queda significativa do VAS do médico e do paciente (p < 0,05), enquanto que as enzimas musculares permaneceram estáveis (p > 0,05). Por fim, nenhum evento adverso foi relatado. CONCLUSÃO: O TF-OV de baixa intensidade foi seguro e efetivo em melhorar a força, a massa e a função muscular, além da qualidade de vida dos pacientes com PM e DM estáveis / INTRODUCTION: Our aim was to evaluate the safety and efficacy of a low-intensity resistance training program combined with partial blood flow restriction (BFR training) in a cohort of patients with polymyositis (PM) and dermatomyositis (DM). METHODS: In total, 13 patients with PM and DM completed a 12-week twice a week low-intensity (that is, 30% onerepetition-maximum (1RM)) resistance exercise training program combined with partial blood flow restriction (BFR). Assessments of muscle strength, physical function, quadriceps cross sectional (CSA) area, health-related quality of life, and clinical and laboratory parameters were assessed at baseline and after the intervention. RESULTS: The BFR training program was effective in increasing the maximal dynamic strength in both the leg-press (19.6%, p < 0.001) and leg-extension exercises (25.2% p < 0.001), as well as in the timed-stands (15.1%, p < 0.001) and timed-up-and-go test (-4.5%, P =0.002). Quadriceps CSA was also significantly increased after the intervention (4.57%, p =0.01). Similarly, all of the components of the Short Form-36 Health Survey, the Health Assessment Questionnaire scores, and the patient- and physician reported Visual Analogue Scale were significantly improved after training (p < 0.05). Importantly, no clinical evidence or any other self-reported adverse event were found. Laboratory parameters (creatine kinase and aldolase) were also unchanged (p > 0.05) after the intervention. CONCLUSIONS: We demonstrated that a 12-week supervised low-intensity resistance training program associated with partial blood flow restriction may be safe and effective in improving muscle strength and function as well as muscle mass and health-related quality of life in patients with PM and DM

Dermatomiosite

Exercício

Hipóxia

Miosite

Polimiosite

Qualidade de vida

Dermatomyositis

Exercise

Hypoxia

Myositis

Polymyositis

Quality of life

Vaskuläres Regenerationspotential im Muskel und endotheliale Vorläuferzellen im Blut bei Patienten mit Myositis / Vascular Regeneration Potential in Muscle and Endothelial Progenitor Cells in Blood of Patients with Myositis

Lemmer, Dana

06 June 2018

No description available.

610

myositis

endothelial progenitor cells

EPCs

idiopathic inflammatory myopathy

dermatomyositis

polymyositis

necrotizing myopathy

Rheumatologie (PPN619875887)

Intramuscular dissociation of echogenicity in the triceps surae characterizes sporadic inclusion body myositis / 下腿三頭筋での筋エコー輝度の解離は孤発性封入体筋炎に特徴的である

Nodera, Hiroyuki

23 May 2016

京都大学 / 0048 / 新制・論文博士 / 博士(医学) / 乙第13030号 / 論医博第2112号 / 新制||医||1016(附属図書館) / 32988 / (主査)教授 三森 経世, 教授 松田 秀一, 教授 戸口田 淳也 / 学位規則第4条第2項該当 / Doctor of Medical Science / Kyoto University / DFAM

inclusion body myositis

polymyositis

dermatomyositis

ultrasound

echo intensity

triceps surae

490

Vliv pohybové intervence na průběh a aktivitu vybraných revmatických onemocnění / The effect of physical activity interventions on the course and activity of selected rheumatic diseases

Špiritović, Maja

January 2020

Introduction: This work focused on two rare rheumatic diseases systemic sclerosis (SSc) and idiopathic inflammatory myopathies (IIM). Skin and musculoskeletal involvement in patients with SSc leads to disability and loss of functional abilities of an individual. Chronic inflammation of the muscles, subsequent muscle atrophy and permanent muscle damage in patients with IIM are the cause of a decrease in muscle strength and endurance. Moreover, both diseases also affect internal organs and manifest often with impaired lung and heart function. All of these involvements in both diseases lead to a decrease in the quality of life of patients. The data on efficacy of non-pharmacological care in SSc and IIM are very limited due to the heterogeneity of the studied interventions and/or outcomes. However, due to limitations in pharmacological therapy, non-pharmacological interventions could help bring patients back into their everyday life and improve their quality of life. Objectives: The main objective of this project was to evaluate the impact of physical intervention on disease course and activity in a substantial number of SSc and IIM patients, with the aim of minimizing the limitations of available studies, thereby improving the quality and reliability of the obtained results. Methods: This is a...

BAFF (B-cell activating factor of the TNF family) u nemocných s idiopatickými zánětlivými myopatiemi se zřetelem na autoprotilátkový profil. / BAFF (B-cell Activating Factor of the TNF Family) in patients with idiopathic inflammatory myopathieswith respect to autoantibody profile.

Kryštůfková, Olga

January 2018

The idiopathic inflammatory myopathies (IIMs) are a heterogeneous group of chronic muscle diseases with frequent extramuscular organ involvement that contributes to serious prognosis. The presence of autoantibodies and composition of muscle infiltrates both support autoimmune nature of the disease and pathogenic role of B lymphocytes. Besides the traditional diagnostic subgroups, autoantibody characterised phenotype subsets have been identified with presumed similar pathogenic mechanisms. The best known is the antisynthetase syndrome which is characterised by presence of myositis, antisynthetase autoantibodies (with anti-Jo-1 being the most frequent), interstitial lung disease and other extramuscular manifestations. BAFF (B cell-Activating Factor of the TNF Family) is a key factor in B cell homeostasis modulation. In high levels, it allows survival of autoreactive B cell clones and thus participates in the pathogenesis of autoimmune diseases. Its expression is induced by type I interferons (IFN-1). The aim of the PhD thesis was to explore the role of BAFF in pathogenesis of IIMs by analysis of its serum levels, the receptors for BAFF in muscle tissue, their associations to IFN-1 and expression of BAFF gene mRNA transcription variants in peripheral blood cells. Further aspect was to study a possible...

Immunité innée, balance th1/th17 et précurseurs musculaires dans les myopathies inflammatoires / Innate immune system, Th1/Th17 balance and immature myoblast precursors in inflammatory myopathies

Tournadre, Anne

19 November 2010

Cette thèse, consacrée aux myopathies inflammatoires, démontre le rôle dans les maladies auto-immunes des Toll-like récepteurs (TLRs), véritable passerelle entre immunité innée et adaptative, et plus spécifiquement dans le muscle, le rôle fondamental de la cellule musculaire elle-même. Après une présentation globale des myopathies inflammatoires et des différents aspects immunopathologiques, la réponse immunitaire adaptative est abordée en rapportant notamment dans le muscle des myopathies inflammatoires une accumulation de cellules dendritiques matures, et la présence des lymphocytes Th1 et Th17, avec un profil prépondérant Th1. L’implication de l’immunité innée est démontrée in vivo par l’expression musculaire des TLR3 et 7, et des C-type lectin récepteurs, spécifique des myopathies inflammatoires. In vitro, l’activation de la voie TLR3 induit la production par les cellules musculaires d’IL6, de la βchémokine CCL20, contribuant au recrutement et à la différentiation des cellules dendritiques et lymphocytes T, et de l’IFNβ qui participe à la surexpression des antigènes HLA de classe I. Les mécanismes de régulation impliquent une balance cytokinique Th1 et Th17. Finalement, l’importance des précurseurs musculaires immatures est soulignée. Contrairement au tissu musculaire normal, une surexpression des antigènes HLA de classe I, des TLRs, des auto-antigènes et de l’IFNβ, par les précurseurs musculaires immatures, est caractéristique des myopathies inflammatoires. Le rôle central de ces cellules musculaires immatures à potentiel de régénération pourrait expliquer un défaut de réparation associé au processus auto-immun de destruction musculaire. / This thesis, devoted to the inflammatory myopathies, is demonstrating the potential role in autoimmune disorders of Toll-like receptors (TLRs), gateway between innate and adaptive immune system, and more specifically in muscular diseases the fundamental role of muscle cell it-self. After the presentation of the general clinical features and the immunopathology of inflammatory myopathies, the adaptive immune response is the subject of the second part,demonstrating the abnormal accumulation of mature dendritic cells in myositis muscle, and the presence of Th1 and Th17 cells with a predominant Th1 profile. Innate immune system is next investigated, demonstrating the overexpression of TLR3 and 7 and of C-type lectin receptors characteristic of inflammatory myopathies. In vitro, stimulation of the TLR3 pathway in human myoblasts induces the production of IL6 and of the βchemokine CCL20, which in turn participate to the differentiation and the migration of T cells and dendritic cells, and of IFNβ which contributes to HLA class I up-regulation. The expression of TLR3 is differentially regulated by Th1 and Th17 cytokines. Finally, this work strongly implicates immature myoblast precursors in the pathogenesis of inflammatory myopathies. In contrast to normal muscle tissue, myositis tissue is characterized by the overexpression of HLA class I antigens, TLR3 and TLR7, myositis autoantigens, and IFNβ, all observed in immature myoblast precursors. By focusing damage onto those cells accomplishing repair, a feedforward loop of tissue damage is induced and could explain the defective repair in muscle in addition to the autoimmune attack.

Myopathie inflammatoire

Polymyosite

Dermatomyosite

Précurseurs musculaires

Immunité innée

Toll-like récepteurs

Interféron type I

Cytokines

Inflammatory myopathy

Polymyositis

Dermatomyositis

Immature myoblast precursors

Innate immunity

Toll-like receptors

Type I interferon

Cytokines

571.96

Imunogenetické a hormonální predispoziční markery systémových revmatických onemocnění,zejména systémového lupus erythematodu / Immunogenetic and hormonal markers of predisposition to systemic rheumatic diseases particularly systemic lupus erythematosus

Fojtíková, Markéta

January 2011

Fojtikova 2011 INTRODUCTION: Several factors like genetic susceptibility is required for systemic rheumatic diseases development. Immunomodulatory PRL effect supports autoimmunity. AIMS: 1. To detect the immunogenetic background (alleles HLA class I, II and microsatellite polymorphism of the transmembrane part exon 5 of MIC-A gene) of SLE and PsA. 2. To detect PRL serum and synovial fluid with regard to clinical and laboratory RA activity. 3. To find the role of the functional polymorphism -1149G/T SNP PRL of extrapituitary promoter of PRL gene in SLE, RA, PsA, SSc and inflammatory myopathies development. METHODS: Genetic analyses of pateints with SLE (n=156), RA (n=173), PsA (n=100), SSc (n=75), PM (n=47) a DM (n=68) and 123 healthy individuals: PCR-SSP (HLA clase I and II), PCR-fragment analysis (MIC-A) a PCR-RFLP (-1149 G/T SNP PRL). In 29 RA a 26 OA PRL serum and synovial fluid concentrations were detected using immunoradiometric assay. RESULTS: 1. The allele HLA-DRB1*03 (pc=0.008; OR 2.5) and haplotype HLA-DRB1*03-DQB1*0201 (pc <0.001; OR 4.54) were determined as risk immunogenetic markers for SLE in Czech population. In SLE versus controls allele MIC-A5.1 was increased (pc =0.005; OR 1.88). MIC-A5.1 together with HLA-DRB1*03 increases the risk for SLE development, pc <0.000001; OR 9.71....

Imunogenetické a hormonální predispoziční markery systémových revmatických onemocnění,zejména systémového lupus erythematodu / Immunogenetic and hormonal markers of predisposition to systemic rheumatic diseases particularly systemic lupus erythematosus

Fojtíková, Markéta

January 2011

Fojtikova 2011 INTRODUCTION: Several factors like genetic susceptibility is required for systemic rheumatic diseases development. Immunomodulatory PRL effect supports autoimmunity. AIMS: 1. To detect the immunogenetic background (alleles HLA class I, II and microsatellite polymorphism of the transmembrane part exon 5 of MIC-A gene) of SLE and PsA. 2. To detect PRL serum and synovial fluid with regard to clinical and laboratory RA activity. 3. To find the role of the functional polymorphism -1149G/T SNP PRL of extrapituitary promoter of PRL gene in SLE, RA, PsA, SSc and inflammatory myopathies development. METHODS: Genetic analyses of pateints with SLE (n=156), RA (n=173), PsA (n=100), SSc (n=75), PM (n=47) a DM (n=68) and 123 healthy individuals: PCR-SSP (HLA clase I and II), PCR-fragment analysis (MIC-A) a PCR-RFLP (-1149 G/T SNP PRL). In 29 RA a 26 OA PRL serum and synovial fluid concentrations were detected using immunoradiometric assay. RESULTS: 1. The allele HLA-DRB1*03 (pc=0.008; OR 2.5) and haplotype HLA-DRB1*03-DQB1*0201 (pc <0.001; OR 4.54) were determined as risk immunogenetic markers for SLE in Czech population. In SLE versus controls allele MIC-A5.1 was increased (pc =0.005; OR 1.88). MIC-A5.1 together with HLA-DRB1*03 increases the risk for SLE development, pc <0.000001; OR 9.71....