Long-term observational study of sporadic inclusion body myositis

Benveniste, Olivier; Guiguet, Marguerite; Freebody, Jane; Dubourg, Odile; Squier, Waney; Maisonobe, Thierry; Stojkovic, Tanya; Leite, Maria Isabel; Allenbach, Yves; Herson, S.; Brady, Stefen; Eymard, B.; Hilton‐Jones, David

doi:10.1093/brain/awr213

Cited by 268 publications

(304 citation statements)

References 37 publications

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“…The clinical presentation is heterogenous and at times difficult to distinguish from other inflammatory myopathies (muscle weakness and atrophy), motor‐neuron disease (asymmetry), and muscular dystrophies (slowly progressive disease) 3. In two large observational studies, the mean age of onset has been reported to be 59 ± 9 and 61 years, respectively 9, 11. The cardinal symptom of this highly debilitating disease is the late‐onset steady acquisition of muscular weakness and atrophy over a long period of time whilst sensory function is completely preserved.…”

Section: Clinical Presentationmentioning

confidence: 99%

“…The cardinal symptom of this highly debilitating disease is the late‐onset steady acquisition of muscular weakness and atrophy over a long period of time whilst sensory function is completely preserved. The decline of muscle strength ranges between 3.5 and 5.5% per annum 9, 11. Unlike other myopathies, during which proximal muscles are initially affected, IBM shows early involvement of distal muscles.…”

Section: Clinical Presentationmentioning

confidence: 99%

“…The chronic disease progression of IBM makes it challenging to detect the condition at an early time point and on average there is a 5‐year delay in diagnosis 9, 39. Creatine kinase levels in serum can be normal to only mildly elevated and will not exceed 10‐fold increase above the upper limit of normal.…”

Section: Diagnosismentioning

confidence: 99%

“…The underlying interrelationship between the inflammatory component of the disease and the observed multi‐protein aggregation remains elusive and subject to vigorous debate 3, 6, 7, 8. Unlike other inflammatory myopathies, IBM presents mainly refractory toward immunosuppressive therapy and at present, there is no effective treatment available 5, 9, 10. In this review, we will focus on the current knowledge about the interrelationship of inflammatory and myodegenerative pathomechanisms in IBM.…”

Section: Introductionmentioning

confidence: 99%

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Immune and myodegenerative pathomechanisms in inclusion body myositis

Keller

Schmidt

Lünemann

2017

Ann Clin Transl Neurol

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Inclusion Body Myositis (IBM) is a relatively common acquired inflammatory myopathy in patients above 50 years of age. Pathological hallmarks of IBM are intramyofiber protein inclusions and endomysial inflammation, indicating that both myodegenerative and inflammatory mechanisms contribute to its pathogenesis. Impaired protein degradation by the autophagic machinery, which regulates innate and adaptive immune responses, in skeletal muscle fibers has recently been identified as a potential key pathomechanism in IBM. Immunotherapies, which are successfully used for treating other inflammatory myopathies lack efficacy in IBM and so far no effective treatment is available. Thus, a better understanding of the mechanistic pathways underlying progressive muscle weakness and atrophy in IBM is crucial in identifying novel promising targets for therapeutic intervention. Here, we discuss recent insights into the pathomechanistic network of mutually dependent inflammatory and degenerative events during IBM.

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Section: Clinical Presentationmentioning

confidence: 99%

Section: Clinical Presentationmentioning

confidence: 99%

Section: Diagnosismentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Immune and myodegenerative pathomechanisms in inclusion body myositis

Keller

Schmidt

Lünemann

2017

Ann Clin Transl Neurol

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“…In the UK-based IBM-Net Project to identify outcome measures for clinical trials, a 27.9% decline in strength was found with QMT at one-year follow-up in a group of 23 patients and a 13.8% annual decline in the 10-point IBM Functional Rating Scale (IBM-FRS) and it was concluded that QMT and the IBM-FRS are the best indicators of disease progression (Jackson et al, 2008, Cortese et al, 2013. A longitudinal study of 136 IBM patients from two European Centres used a composite clinical weakness index (ICWI) to assess progression in a subgroup of 71 patients, and found a good correlation with other measures of strength and walking handicap (Benveniste et al, 2011). This study also identified male gender and older age at onset as adverse prognostic indicators with respect to progression of disability and walking handicap.…”

Section: Natural Historymentioning

confidence: 99%

Sporadic inclusion body myositis: A review of recent clinical advances and current approaches to diagnosis and treatment

Needham

Mastaglia

2016

Clinical Neurophysiology

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Sporadic inclusion body myositis is the most frequent acquired myopathy of middle and later life and is distinguished from other inflammatory myopathies by its selective pattern of muscle involvement and slowly progressive course, and by the combination of inflammatory and degenerative muscle pathology and multi-protein deposits in muscle tissue. This review summarises the findings of recent studies that provide a more complete picture of the clinical phenotype and natural history of the disease and its global prevalence and genetic predisposition. Current diagnostic criteria, including the role of electrophysiological and muscle imaging studies and the recently identified anti-5'-nucleotidase (anti-cN1A) antibody in diagnosis are also discussed as well as current trends in the treatment of the disease.

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Development of a New Classification System for Idiopathic Inflammatory Myopathies Based on Clinical Manifestations and Myositis-Specific Autoantibodies

et al. 2018

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myopathies are heterogeneous in their pathophysiologic features and prognosis. The emergence of myositis-specific autoantibodies suggests that subgroups of patients exist.OBJECTIVE To develop a new classification scheme for idiopathic inflammatory myopathies based on phenotypic, biological, and immunologic criteria.DESIGN, SETTING, AND PARTICIPANTS An observational, retrospective cohort study was performed using a database of the French myositis network. Patients identified from referral centers for neuromuscular diseases were included from January 1, 2003, to February 1, 2016. Of 445 initial patients, 185 patients were excluded and 260 adult patients with myositis who had complete data and defined historical classifications for polymyositis, dermatomyositis, and inclusion body myositis were enrolled. All patients were tested for anti-histidyl-ARN-tsynthetase (Jo1), anti-threonine-ARN-t-synthetase (PL7), anti-alanine-ARN-t-synthetase (PL12), anti-complex nucleosome remodeling histone deacetylase (Mi2), anti-Ku, anti-polymyositis/systemic scleroderma (PMScl), anti-topoisomerase 1 (Scl70), and anti-signal recognition particle (SRP) antibodies. A total of 708 variables were collected per patient (eg, cancer, lung involvement, and myositis-specific antibodies). MAIN OUTCOMES AND MEASURESUnsupervised multiple correspondence analysis and hierarchical clustering analysis to aggregate patients in subgroups. RESULTS Among 260 participants (163 [62.7%] women; mean age, 59.7 years; median age [range], 61.5 years [48-71 years]), 4 clusters of patients emerged. Cluster 1 (n = 77) included patients who were male, white, and older than 60 years and had finger flexor and quadriceps weakness and findings of vacuolated fibers and mitochondrial abnormalities. Cluster 1 regrouped patients who had inclusion body myositis (72 of 77 patients [93.5%]; 95% CI, 85.5%-97.8%; P < .001). Cluster 2 (n = 91) regrouped patients who were women and had high creatine phosphokinase levels, necrosis without inflammation, and anti-SRP or anti-3-hydroxy-3-methylglutaryl-coenzyme A reductase (HMGCR) antibodies corresponding to immune-mediated necrotizing myopathy (53 of 91 [58.2%]; 95% CI, 47.4%-68.5%; P < .001). Cluster 3 (n = 52) regrouped patients who had dermatomyositis rash and anti-Mi2, anti-melanoma differentiation-associated protein 5 (MDA5), or anti-transcription intermediary factor-1γ (TIF1γ) antibodies, mainly corresponding with patients who had dermatomyositis (43 of 52 [82.7%]; 95% CI, 69.7%-91.8%; P < .001). Cluster 4 (n = 40) was defined by the presence of anti-Jo1 or anti-PL7 antibodies corresponding to antisynthetase syndrome (36 of 40 [90.0%]; 95% CI, 76.3%-97.2%; P < .001). The classification of an independent cohort (n = 50) confirmed the 4 clusters (Cohen κ light, 0.8; 95% CI, 0.6-0.9). CONCLUSIONS AND RELEVANCEThese findings suggest a classification of idiopathic inflammatory myopathies with 4 subgroups: dermatomyositis, inclusion body myositis, immune-mediated necrotizing myopathy, and antisynthetase syndrome. This classification...

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Long-term observational study of sporadic inclusion body myositis

Cited by 268 publications

References 37 publications

Immune and myodegenerative pathomechanisms in inclusion body myositis

Immune and myodegenerative pathomechanisms in inclusion body myositis

Sporadic inclusion body myositis: A review of recent clinical advances and current approaches to diagnosis and treatment

Development of a New Classification System for Idiopathic Inflammatory Myopathies Based on Clinical Manifestations and Myositis-Specific Autoantibodies

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