Glucocorticoids are the sole drugs of clinical interest for DMD patients.
The mechanism for their beneficial action is not completely understood yet and may involve multiple effects, beside the classical anti-inflammatory and immunosuppressive ones. These include an improvement of regeneration and an increased expression of utrophin, the homologue-surrogate for dystrophin [20–22]. However, the clinical use of glucocorticoids in DMD children is limited by severe side effects over long-term use; this compels the search of safer drugs or of strategies to limit their side selleck chemicals toxicity [23]. As for other complex disorders, one feasible strategy is to find compounds with relevant synergistic interactions: thus glucocorticoids in combination with a synergistic drug, may exert greater effects and/or have less side effects as a result of dose lowering. This rationale is reinforced by the anecdotal report that DMD patients often take various food and drink supplements or herbal remedies along with the classical glucocorticoids and it is important
to develop a more systematic preclinical evaluation of the outcome of drug combinations, both in vitro and in vivo[23,24]. For instance, the combination of deflazacort with the food supplement L-arginine has been reported to produce an improved functional benefit in dystrophic mdx ABT-888 purchase mice [25]. We therefore aimed to investigate the effects of a combined treatment of α-methyl-prednisolone (PDN), a clinically used glucocorticoid, with taurine. Taurine is a sulphonic amino acid normally present in skeletal muscle, able to modulate sarcolemmal excitability and calcium homeostasis [26]. It is used as a soft-drink supplement for its claimed ability to stimulate metabolism and provide energy. Little, if any, toxicity has been reported for taurine
at the generally assumed quantities [27]. Complex PFKL fluctuations in tissue taurine content occur in mdx mouse in the different phases of muscle degeneration/regeneration, suggesting that the amino acid levels may be influenced by myofibre state and may in turn contribute to cellular and tissue dysfunction and/or repair; taurine increases seem to be generally associated with muscle regeneration and membrane stabilization [28–30]. In addition, taurine exerts anti-inflammatory and antioxidant actions [31], with potential beneficial outcomes on the pathology progression. We have previously found that taurine either applied in vitro or administered in vivo exerts beneficial effects on the altered excitation-contraction coupling mechanism of mdx myofibres [8,29]. Also the amino acid administration enhances mdx mouse strength impaired by a chronic exercise on treadmill, a protocol that is able to exacerbate in vivo and ex vivo markers of the murine pathology [2,8]. We have performed a chronic (4–8 weeks treatment) in vivo treatment with α-methyl-prednisolone (1 mg/kg i.p.