Refined exercise testing can aid dna‐based diagnosis in muscle channelopathies

Tan, S. Veronica; Matthews, Emma; Barber, Marcus; Burge, J.; Rajakulendran, Sanjeev; Fialho, Doreen; Sud, Richa; Haworth, Andrea; Koltzenburg, M; Hanna, Michael G.

doi:10.1002/ana.22238

Cited by 89 publications

(130 citation statements)

References 17 publications

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“…Hundred percent of the recessive and 71% of the dominant MC patients displayed pattern II after combination of tests performed at room temperature and cold [7]. Moreover, the area decrement was 27% in the first case and 57.9% in the second case which, according to Tan et al [9], is specific to the type II pattern. In patient 3, the provocative tests showed a type III pattern, in this case the mixed clinical presentation led us to perform CLCN1 sequencing.…”

Section: Discussionmentioning

confidence: 86%

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Heterozygous CLCN1 mutations can modulate phenotype in sodium channel myotonia

Furby

Vicart

Camdessanché

et al. 2014

Neuromuscular Disorders

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Section: Discussionmentioning

confidence: 86%

“…It comprised short and long exercise tests and needle examination. Short exercise test (SET) has been shown to be a reliable biomarker to distinguish between SCN4A and CLCN1 mutations [6][7][8][9]. Molecular testing was performed after informed consent of the patients or their parents, accordingly to bioethics laws.…”

Section: Methodsmentioning

confidence: 99%

Heterozygous CLCN1 mutations can modulate phenotype in sodium channel myotonia

Furby

Vicart

Camdessanché

et al. 2014

Neuromuscular Disorders

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“…In addition to myotonic discharges, low-amplitude (100-600 mV), high-frequency (150-250 Hz) discharges resembling neuromyotonic discharges have recently been observed in some NDM patients. 16 Occasionally, repetitive firing of muscle fibers following a single stimulus termed "postexercise myotonic potentials" can be observed as delayed lower amplitude motor responses following the compound motor action potential (CMAP) during performance of routine nerve conduction studies. 14 Postexercise myotonic potentials are described in both SCN4A and CLCN1 mutations.…”

Section: Sodium Channel Myotonias (Group 2 Scm)mentioning

confidence: 99%

“…10,13 SCM can also be distinguished from PC and chloride channelopathies based on electrodiagnostic testing(see later discussion). [14][15][16] Electrodiagnosis of NDM Commercial genetic testing is available for some of the causative mutations in NDM, but there is a false-negative rate in these conditions as high as 20%. 17 Electrodiagnostic studies are extremely helpful in directing genetic testing and also making the diagnosis of NDM in patients with negative genetic testing.…”

Section: Sodium Channel Myotonias (Group 2 Scm)mentioning

confidence: 99%

“…12,14,15 Repeating the protocol with limb cooling (to 20-25 C) improves the sensitivity in MC (70%-100%) and exaggerates the abnormality observed in PC. 15,16 Three patterns are observed in patients with NDM, Fournier I, II, and III. 10,14,15 Patients with PC exhibit Fournier pattern I with a decrement in CMAP amplitude (19%-40% less than preexercise baseline CMAP), which persists for 60 seconds and which increases with subsequent trials and with cooling ( Fig.…”

Section: Short-exercise Protocolmentioning

confidence: 99%

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Electrodiagnosis of Myotonic Disorders

Hehir

Logigian

2013

Physical Medicine and Rehabilitation Clinics of North America

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Mexiletine for Symptoms and Signs of Myotonia in Nondystrophic Myotonia

Statland

Bundy

Rayan

et al. 2012

JAMA

156

164

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Context Non-dystrophic myotonias (NDM) are rare diseases caused by mutations in skeletal muscle ion channels. Patients experience delayed muscle relaxation causing functionally-limiting stiffness and pain. Mexiletine-induced sodium channel blockade reduced myotonia in case studies and one single blind trial. As is common in rare diseases, larger studies of safety and efficacy have not previously been considered feasible. Objective To determine the effects of mexiletine for symptoms and signs of myotonia in NDM. Design, Setting, and Participation Fifty-nine patients with NDM participated in a randomized, double-blind, placebo-controlled two-period crossover study conducted between December 23, 2008 and March 30, 2011 at 7 neuromuscular referral centers in 4 countries, as part of the NIH-funded Rare Disease Clinical Research Network. Intervention Oral 200 mg mexiletine or placebo capsules three times daily for 4 weeks, followed by the opposite intervention for 4 weeks, with 1 week wash-out between periods. Main Outcome Measures Patient-reported stiffness recorded on an interactive voice response diary (IVR) was the primary endpoint (1 ‘minimal’ to 9 ‘worst ever experienced’). Secondary endpoints included IVR-reported changes in pain, weakness, and tiredness, clinical myotonia assessment, quantitative grip myotonia, Individualized Neuromuscular Quality of Life (INQoL, percent of maximal detrimental impact), SF-36, electrophysiological exercise testing, and needle EMG. Results Mexiletine significantly improved patient-reported stiffness on the IVR. Because of a statistically significant interaction between treatment and period for this outcome, primary endpoint is presented by period (period 1 means were mexiletine 2.53 versus placebo 4.21, difference −1.68, 95% Confidence Interval [CI] −2.66, −0.706, P<0.001; period 2 means were mexiletine 1.60 versus placebo 5.27, difference −3.68, 95% CI −3.85, −0.139, P=0.04). Mexiletine improved the INQoL QOL score (mexiletine 14.0, placebo 16.7, difference −2.69, 95% CI −4.07, −1.30, P<0.001) and decreased handgrip myotonia on clinical exam (seconds: mexiletine 0.164, placebo 0.494, difference −0.330, 95% CI −0.633, −0.142, P<0.001). The most common adverse effect was gastrointestinal (9 mexiletine, 1 placebo). Two participants experienced transient cardiac effects that did not require stopping the study (1 placebo, 1 mexiletine). One serious adverse event was determined to be not study-related. Conclusion In this preliminary study of patients with NDM, the use of mexiletine compared with placebo resulted in improved patient-reported stiffness over 4 weeks of treatment, despite some concern about the maintenance of blinding. Trial Registration Clinicaltrials.gov identifier: NCT 00832000

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Refined exercise testing can aid dna‐based diagnosis in muscle channelopathies

Cited by 89 publications

References 17 publications

Heterozygous CLCN1 mutations can modulate phenotype in sodium channel myotonia

Heterozygous CLCN1 mutations can modulate phenotype in sodium channel myotonia

Electrodiagnosis of Myotonic Disorders

Mexiletine for Symptoms and Signs of Myotonia in Nondystrophic Myotonia

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