Progressive muscular dystrophy
Duchenne type. Controversies of the kinesitherapy treatment
Keywords:
Neuromuscular disease, Duchenne muscular dystrophyAbstract
The authors carried out a study of children with progressive muscular dystrophy of Duchenne type (DMD), giving special attention to physiatrical follow-up, having in mind that the practice of exercises has been debated very much in the specialized literature. The goal of this study is to try to settle the limits for the utilization of kinesitherapy which should be applied only in specific situations, such as: after skeletal muscular trauma or when the respiratory system is at risk. In this situation the physiatrical procedure would be to restrict physical activity, with early use of wheelchairs and the exclusion of the use of orthoses for orthostatism. DMD, at present, has been considered a result of duplication (60%), deletion (5 to 6%) or point mutations at gen Xp21 (Zatz, 1994), that codifies a protein called Dystrophin ( Hoffman et al., 1987). Dystrophin is a cytoskeletal sarcolemmic protein that constitutes about .002% of the total protein of the muscle, present in skeletal fibers concentrated in muscle tendinous joints, which supplies mechanical reinforcement to the surface of the membrane during stretching and shortening physical activity. This protein is absent in DMD cases, wherefore, the sarcolemma undergoes a segmentary necrosis losing its contractile property during eccentric and concentric physical activity. The importance of physiatrical follow-up for DMD patients is to avoid deformities and tendon shortening, to ameliorate the patient's quality of life, to provide respiratory assistance and general couseling to members of the patient's family. The objective of this study is to try to clarify the risks and possibilities of kinesitherapy applied to DMD cases.
Downloads
References
ARCHIBALD, K. C. ET VIGNOS JR., P. (1959) - The Clinical Management of Muscle Disease apud Siegel, I . M., London, William Heinemann Medical Books, 1977, pp. 89-91.
BERTORINI, T. E.; PALMIERI, G. M. A.; BROWN, R.; NUTTING, D. E; KARAS, J. G. - Effect of chronic treatment with the calcium antagonist diltiazem in Duchenne muscular dystrophy. J of Neurol 38: 609-613, 1988.
BYRNE, E. - Dystrophin input of a neurologist. in: B. A. Kakulas et F. Mastaglia: Pathogenesis and Therapy of Duchenne and Becker Muscular Distrophies Raven Press, New York, 1990, pp. 137-138.
BULLER, A. J.; GOODFELLOW, J. et NEWSOM-DAVIES, J. M. - Management of children: Pharmacological and Physical. British Medical Bulletin 45(3): 788-801, 1989.
ELDER, G. et SOLA, O. M. - Past Therapeutic Trials and Current Corrective Procedures, in: B. A. Kakulas et F Mastaglia: Pathogenesis and Therapy of Duchenne and Becker Muscular Distrophies Raven Press, New York, pp. 217, 1990.
HILLER, L. B.; WADE, C. K. - Upper extremities functional assessment scales in children with Duchenne Muscular Dystrophy: a comparison. Archives of Phys Med & Rehab, 73(6): 527- 534, 1992.
HOFFMAN, E. P.; BROWN, E. P. et KUNKEL, L. M. - Dystrophin: the protein product of the Duchenne Muscular Dystrophy locus. Cell 51: 919-928, 1987.
DUBOWITZ,V. - Physical therapy in neuromuscular disorders. Journal of the Neurological Sciences 98 (Supp): 29-30, 1990.
KAKULAS, B. A. et MASTAGLIA, F. L. - Pathogenesis and Therapy of Duchenne and Becker Muscular Distrophies Raven Press, New York, 1990.
LAW, P. K. - Summary: Past Therapeutic Trials, in: Pathogenesis and Therapy of Duchenne and Becker Muscular Distrophies Raven Press, New York, 1990, pp. 216-217.
SIEGEL, I. M. - The Clinical Management of Muscle Disease William Heinemann Books LTD, London, 1977, pp. 89-91.
WELLER, B.; KARPATI, G.; CARPENTER, S. - Dystrophin deficient MDX muscle fibers area preferentially vulnerable to necrosis induced by experimental lenghthening contraction. J. of Neurologic Sciences 100: 9-13, 1990.
WERNECK, L. C. - Perspectivas em doenças neuromusculares: 1. Distrofia muscular de Duchenne. Rev Bras Neurol 30(2): 33-35, 1994.
ZATZ, M. et al. - O impacto da biologia molecular na compreensão e prevenção das miopatias hereditárias. Rev Bras Neurol 30(2): 41-44,1994.
