AI Article Synopsis

  • A longitudinal study examined changes in the neuromuscular junction of SOD1-G93A mice, focusing on histological and biochemical markers of muscle function and the effects of the heat shock protein inducer, arimoclomol.
  • Findings revealed that denervation and nerve sprouting began as symptoms appeared, with a decline in cholinergic enzyme activities and alterations in muscle fiber characteristics, particularly in fast muscles.
  • Treatment with arimoclomol not only delayed these harmful changes but also improved muscle innervation and enzyme activities, along with increased Hsp70 expression, suggesting a potential therapeutic strategy for ALS.

Article Abstract

We undertook a longitudinal study of the histological and biochemical changes at the neuromuscular junction (NMJ) in muscles of SOD1-G93A mice. We also assessed these functions in mice treated with a known heat shock protein inducer, arimoclomol. Tissue samples of treated and untreated mSOD mice were analysed for AChE and ChAT enzyme activities as markers of neuromuscular function. Sections of hindlimb muscles (TA, EDL and soleus) were also stained for succinate dehydrogenase and silver cholinesterase activities as well as for immunohistochemistry. Hsp70 levels were also measured from muscle samples using ELISA. Results showed that denervation and nerve sprouting were present at symptom onset in fast muscles, although slow muscles remained fully innervated. Cholinergic enzyme activities were reduced prior to denervation and declined further with disease progression. Reduction of endplate size, a slow to fast shift in muscle phenotype was also observed. Treatment with arimoclomol delayed the appearance of these changes, increased innervation, cholinergic enzyme activities and endplate size and reversed muscle fibre transformation. These beneficial effects of arimoclomol in muscles were accompanied by an increase in Hsp70 expression. In conclusion, our results indicate that pharmacological targeting of muscles at early stages of disease may be a successful strategy to ameliorate disease progression in ALS.

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Source
http://dx.doi.org/10.3109/17482968.2012.660953DOI Listing

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