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Michael D. Nelson Ryan Rosenberry Rita Barresi Evgeny I. Tsimerinov Florian Rader Xiu Tang O'Neil Mason Avery Schwartz Thomas Stabler Sarah Shidban Neigena Mobaligh Shomari Hogan Robert Elashoff Jason D. Allen Ronald G. Victor 《The Journal of physiology》2015,593(23):5183-5200
AbstractBecker muscular dystrophy (BMD) is a progressive X‐linked muscle wasting disease for which there is no treatment. BMD is caused by in‐frame mutations in the gene encoding dystrophin, a structural cytoskeletal protein that also targets other proteins to the sarcolemma. Among these is neuronal nitric oxide synthase mu (nNOSμ), which requires specific spectrin‐like repeats (SR16/17) in dystrophin''s rod domain and the adaptor protein α‐syntrophin for sarcolemmal targeting. When healthy skeletal muscle is exercised, sarcolemmal nNOSμ‐derived nitric oxide (NO) attenuates α‐adrenergic vasoconstriction, thus optimizing perfusion. In the mdx mouse model of dystrophinopathy, this protective mechanism (functional sympatholysis) is defective, resulting in functional muscle ischaemia. Treatment with a NO‐donating non‐steroidal anti‐inflammatory drug (NSAID) alleviates this ischaemia and improves the murine dystrophic phenotype. In the present study, we report that, in 13 men with BMD, sympatholysis is defective mainly in patients whose mutations disrupt sarcolemmal targeting of nNOSμ, with the vasoconstrictor response measured as a decrease in muscle oxygenation (near infrared spectroscopy) to reflex sympathetic activation. Then, in a single‐arm, open‐label trial in 11 BMD patients and a double‐blind, placebo‐controlled cross‐over trial in six patients, we show that acute treatment with oral sodium nitrate, an inorganic NO donor without a NSIAD moiety, restores sympatholysis and improves post‐exercise hyperaemia (Doppler ultrasound). By contrast, sodium nitrate improves neither sympatholysis, nor hyperaemia in healthy controls. Thus, a simple NO donor recapitulates the vasoregulatory actions of sarcolemmal nNOS in BMD patients, and constitutes a putative novel therapy for this disease.
Abbreviations
- BMD
- Becker muscular dystrophy
- deoxyHb
- deoxyhaemoglobin
- deoxyMb
- deoxymyoglobin
- DMD
- Duchenne muscular dystrophy
- LBNP
- lower body negative pressure
- MVC
- maximal voluntary contraction
- NIRS
- near infrared spectroscopy
- NO
- nitric oxide
- NO2−
- nitrite
- NO3−
- nitrate
- nNOSμ
- neuronal nitric oxide synthase mu
- NSAID
- non‐steroidal anti‐inflammatory drug
- PDE5
- phosphodiesterase 5
- TLS
- total labile signal
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