Saying NO to muscular dystrophy

نویسنده

  • Alan W. Dove
چکیده

In This Issue In This Issue Saying NO to muscular dystrophy ccording to the prevailing model for Duchenne muscular dystrophy (DMD) pathogenesis, a lack of dystrophin protein makes muscle cells susceptible to mechanical damage, leading to muscle breakdown. On page 123, Wehling et al. suggest that the major damage in DMD may actually be caused by a secondary consequence of dystrophin loss: destruction of muscle tissue by a patient's own macrophages. Dystrophin forms a complex with several other proteins, including nitric oxide synthase (NOS). In dystrophin-deficient muscles, such as those of the mdx mouse, a model for DMD, NOS expression is decreased. Reasoning that the loss of nitric oxide's anti-inflammatory activity might exacerbate muscle breakdown, the authors introduced a transgene to A Muscle cells experience a nuclear buildup n response to stimulation, muscle fibers can switch between two types: fast-twitch, used for quick movement; and slow-twitch, which are more resistant to fatigue. On page 27, Liu et al. find that the nuclear localization of a transcription factor may be the key to this switch. I Liu et al. applied electrical pulses to isolated adult murine muscle fibers, thus simulating fast-twitch and slow-twitch muscle stimulation in vitro. They then looked at the localization of the transcription factor NFATc, which has been implicated in muscle-and T-cell transcriptional regulation. NFATc is cytoplasmic in unstimulated fast-twitch muscle fibers, but Slow stimulation sends NFATc into the nucleus. translocates to distinct nuclear foci when the fibers are exposed to kinase inhibitors or trains of electrical pulses at 10 Hz, simulating slow-twitch stimulation. Two conditions do not cause NFATc nuclear-translocation: simulated fast-twitch stimulation, and continuous 1 Hz stimulation, which provides the same number of electrical jolts per minute as the 10 Hz pulses without mimicking any natural stimulation pattern. The nuclear NFATc localizes to distinct intranuclear foci. Liu et al. report that the foci are similar in size and shape to the Cajal bodies that are believed to be involved in splicing in certain cells, but the two structures may not be the same. The authors are now trying to identify additional components of the NFATc-containing foci, and hope to use their in vitro system to determine whether NFATc translocation alone is sufficient to initiate the conversion of fast-twitch muscle fibers into slow-twitch fibers. ᭿ produce normal levels of NOS in the muscles of mdx mice. The transgene reduced the concentrations of macrophages in the muscles and …

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عنوان ژورنال:
  • The Journal of Cell Biology

دوره 155  شماره 

صفحات  -

تاریخ انتشار 2001