Advertising Disclaimer »

Discover Pediatric Collections on COVID-19 and Racism and Its Effects on Pediatric Health

A statement of reaffirmation for this policy was published at

AMERICAN ACADEMY OF PEDIATRICS

Cardiovascular Health Supervision for Individuals Affected by Duchenne or Becker Muscular Dystrophy

; Section on Cardiology and Cardiac Surgery
Pediatrics December 2005, 116 (6) 1569-1573; DOI: https://doi.org/10.1542/peds.2005-2448
Download PDF

Abstract

Duchenne muscular dystrophy is the most common and severe form of the childhood muscular dystrophies. The disease is typically diagnosed between 3 and 7 years of age and follows a predictable clinical course marked by progressive skeletal muscle weakness with loss of ambulation by 12 years of age. Death occurs in early adulthood secondary to respiratory or cardiac failure. Becker muscular dystrophy is less common and has a milder clinical course but also results in respiratory and cardiac failure. The natural history of the cardiomyopathy in these diseases has not been well established. As a result, patients traditionally present for cardiac evaluation only after clinical symptoms become evident. The purpose of this policy statement is to provide recommendations for optimal cardiovascular evaluation to health care specialists caring for individuals in whom the diagnosis of Duchenne or Becker muscular dystrophy has been confirmed.

INTRODUCTION

Duchenne muscular dystrophy (DMD) is a common genetic disease that affects approximately 1 in 3000 males. Becker muscular dystrophy (BMD) is less common, affecting approximately 1 in 30000 males.1 Both diseases result from a mutation in the gene located at Xp21,2,3 which encodes dystrophin, a sarcolemmal protein abundant in skeletal and cardiac muscle cells.4 Dystrophin is typically absent in DMD and reduced or abnormal in size in BMD.5

DMD typically is diagnosed between the ages of 3 and 7 years and is characterized by progressive skeletal muscle weakness with loss of ambulation between the ages of 7 and 13 years. The BMD phenotype is clinically more heterogeneous with initial presentation in the teenage years. Death secondary to cardiac or respiratory failure typically occurs in the second or third decade in DMD and in the fourth or fifth decade in BMD. Cardiac disease in both DMD and BMD manifests as a dilated cardiomyopathy and/or cardiac arrhythmia.6,7 End-stage cardiac disease is characterized by alternating areas of myocyte hypertrophy, atrophy, and fibrosis.8

Over the last 20 years, respiratory care of this group of patients has improved as a result of the development of supportive equipment and techniques.9 Consequently, dilated cardiomyopathy is increasing as the major cause of death.1012 The time course for the development of cardiomyopathy has not been well characterized; however, clinical studies demonstrate that the disease process in the heart is underway long before symptoms appear.1315 Early manifestations of heart failure often go unrecognized secondary to physical inactivity and a lack of classic signs and symptoms.16 Signs of cardiac dysfunction may be vague and nonspecific, such as fatigue, weight loss, vomiting, or sleep disturbance. Currently at many medical centers, affected individuals do not come to the attention of the cardiac specialist until late in the disease process when the clinical manifestations of cardiac dysfunction become evident. This reactive, rather than proactive, approach must change if progress is to be made in the treatment of dilated cardiomyopathy in this patient population.17 Sensitive and specific diagnostic tests to detect early and subtle manifestations of cardiac dysfunction are not available currently and need to be developed. Echocardiography, which remains the standard noninvasive diagnostic modality for cardiomyopathy, is often limited in patients with DMD and BMD by scoliosis and poor echocardiographic acoustic windows.

Cardiac rhythm abnormalities are frequent and play a significant role in morbidity and mortality in both DMD and BMD.18 Electrocardiographic abnormalities can be seen early in the disease, with an incidence of 26% by 6 years of age.16 Autonomic dysfunction with increased mean baseline heart rate and decreased rate variability has been well described.1921 However, the significance of these findings relative to the course of the cardiomyopathy has not been well established.

Treatment paradigms to date have been individually based and rely on evidence acquired from other patient populations. Cardiac dysfunction is treated by using standard heart-failure strategies that remain suboptimal. Unfortunately, there is minimal evidence-based literature regarding the use and effect of angiotensin-converting enzyme inhibitors or β-blockers on morbidity and mortality in this patient population.2224 Prospective clinical trials are required to evaluate the effectiveness of these treatments in this group of patients. Strategies that target the unique molecular etiology of heart failure in dystrophin-deficient individuals need to be developed if the cardiovascular care of patients with DMD and BMD is to improve.

The cardiovascular system must also be considered when addressing the diverse medical and surgical issues faced by patients with DMD and BMD. The administration of systemic glucocorticoids is becoming standard treatment for the skeletal muscle disease.2527 In addition to the potential to improve or stabilize cardiac function, there is the potential to increase long-term cardiovascular risk28,29 including but not limited to the development of obesity and systemic arterial hypertension. Glucocorticoid treatment also may result in the development of left ventricular hypertrophy, with the potential of altering cardiac function.30 At present, there is no uniformly accepted or standardized treatment protocol for glucocorticoid use.31,32 Research is required to determine the cardiovascular effects of long-term glucocorticoid use in patients with DMD.

To manage the musculoskeletal complications in DMD and BMD, orthopedic surgical procedures are frequently recommended.33,34 The patient with DMD or BMD faces unique risks not only in the operating room but also in the postoperative period.35,36 Potential complications include respiratory failure, pulmonary aspiration, atelectasis or collapse of major lung segments, postoperative pneumonia, congestive heart failure, and cardiac arrhythmias. The patient with DMD or BMD often has a limited ability to increase cardiac output in response to stress and thus is at risk of inadequate oxygen delivery. Blood loss and fluid shifts during surgical procedures further compromise cardiac output and adequate oxygen delivery.37 As a result, it is essential that baseline cardiac and pulmonary function be evaluated before any major surgical procedure. Patients with DMD or BMD have additional operative risks. Succinylcholine chloride should be avoided because of its predilection to cause a hyperkalemic response, which is different from malignant hyperthermia but is potentially as life threatening. Prolonged exposure to inhaled anesthetic agents should also be avoided, because they may provoke a life-threatening hypermetabolic state similar to malignant hyperthermia. All patients with DMD or BMD should be monitored during surgery by measuring expired carbon dioxide concentration and body temperature.3840

The patient with DMD or BMD continues to be at risk during the postoperative period. Pain may worsen already compromised pulmonary mechanics, leading to additional increases in oxygen consumption. Treatment with narcotics may result in hypoventilation, which affects airway clearance. In addition, anemia or inadequate volume replacement can impair oxygen delivery. After major surgical procedures such as scoliosis surgery, the patient is likely to experience significant, prolonged fluid shifts, which markedly affect ventricular preload. Postoperative maintenance of fluid balance and cardiopulmonary monitoring is critical for this patient population.

Nutrition is also critical in the care and management of patients with DMD, because they require regular monitoring to maintain ideal body weight. Obesity and undernutrition are known to occur in this group of patients.41,42 Both have been shown to be detrimental to cardiac health in other populations,43 although there is a paucity of literature regarding the effect of nutrition on cardiovascular health in patients with DMD. Glucocorticoid-induced obesity and osteoporosis will further nutritionally affect the patient with DMD.

Patients with DMD and BMD may also be at increased risk of thromboembolic events secondary to the prothrombotic consequences of muscle degeneration.4448 This risk is amplified in the presence of cardiac dysfunction. As a result, anticoagulation therapy should be considered in this subgroup of patients. However, there is minimal evidence-based literature regarding the use and effect of anticoagulation therapy in these patients.

Optimal cardiac care cannot be accomplished without maximizing pulmonary function.49 Hypoventilation and respiratory muscle weakness are known to increase wall stress.50 Aggressive pulmonary care not only affects morbidity and mortality as a result of reducing respiratory complications but also functions to decrease afterload and left ventricular wall stress, resulting in improved cardiac output. In 2004, the American Thoracic Society released a consensus statement regarding the respiratory care of patients with DMD.9 These recommendations should be considered carefully.

Female carriers of DMD or BMD are also at risk of developing cardiomyopathy. The age of onset of clinically significant disease is unclear but is thought to be in the adult years.51 Cardiac involvement in the carrier can be variable, ranging from asymptomatic to severe heart failure necessitating cardiac transplantation.52,53 Carriers, therefore, require periodic cardiovascular screening.54,55 In addition, there is a critical need to research the natural history and outcome of therapies in female carriers.

Mutations in dystrophin clearly place affected individuals at risk of developing cardiac disease irrespective of skeletal muscle disease. The dystrophin gene has been shown to be the cause of X-linked dilated cardiomyopathy and some cases of sporadic dilated cardiomyopathy.5660

Ultimately, investigation of cardiomyopathy in patients with DMD and BMD, as well as carriers, will benefit affected individuals, and new knowledge may lead to the elucidation of novel treatment strategies for dilated cardiomyopathy. Given the number of affected children and limited financial resources available for investigation, medical information must be pooled and shared for maximal effectiveness.

RECOMMENDATIONS FOR CARDIAC CARE IN PATIENTS WITH DMD OR BMD

  1. Cardiac care of the patient with DMD or BMD should begin after confirmation of the diagnosis. The patient should be referred for evaluation to a cardiac specialist with an interest in the management of cardiac dysfunction and/or neuromuscular disorders.

  2. A complete cardiac evaluation should include (but not be limited to) a history and physical examination, electrocardiogram, and transthoracic echocardiogram. Consideration should be given to a multigated acquisition study (MUGA) or cardiac MRI in patients with limited echocardiographic acoustic windows.

  3. Clinicians should be aware that the typical signs and symptoms of cardiac dysfunction may not be present secondary to the patient's musculoskeletal limitations. Weight loss, cough, nausea and vomiting, orthopnea, and increased fatigue with a decreased ability to tolerate the daily regimen may represent cardiac impairment and should be investigated. However, the development of dilated cardiomyopathy usually precedes the development of heart-failure symptoms by years and must be identified at its earliest onset.

  4. Signs and symptoms of cardiac dysfunction should be treated. Consideration should be given to the use of diuretics, angiotensin-converting enzyme inhibitors, and/or β-blockers.

  5. Abnormalities of cardiac rhythm should be promptly investigated and treated. Periodic Holter monitoring should be considered for patients with demonstrated cardiac dysfunction.

  6. Respiratory abnormalities contribute to the cardiovascular morbidity and mortality of the disease. Concurrent evaluation and treatment of respiratory abnormalities are recommended.

  7. Individuals undergoing treatment with glucocorticoids warrant increased cardiac surveillance with specific monitoring for weight gain and hypertension.

  8. Complete cardiac evaluation should be undertaken before scoliosis surgery or other major surgical procedures. Consideration should be given to cardiac stress testing (such as a dobutamine stress echocardiogram) if abnormalities of cardiac function are present during resting evaluation. Medical therapy should be optimized before surgery, and the risks and benefits of the procedure should be discussed in detail with the patient and the family.

  9. Intraoperative cardiac monitoring should be undertaken in individuals with DMD or BMD during major surgical procedures. Specific anesthetic techniques and decisions about intraoperative ventilation will depend on the patient and the procedure. Agents known to trigger hyperkalemia (eg, succinylcholine chloride) or a hypermetabolic state (eg, inhaled anesthetic agents) should be avoided. Cardiac monitoring should continue in the postoperative period.

  10. Anticoagulation therapy should be considered in patients with severe cardiac dysfunction to prevent systemic thromboembolic events.

  11. Clinicians who are experienced in the care of patients with DMD or BMD and are knowledgeable about the pathogenesis of the disease should be actively involved when patients are treated in an intensive care setting.

  12. Nutritional status should be optimized to the special needs of patients with DMD or BMD.

RECOMMENDATIONS SPECIFIC FOR CARDIAC CARE IN PATIENTS WITH DMD

  1. Patients should be routinely managed in early childhood with a complete cardiac evaluation at least biannually.

  2. Yearly complete cardiac evaluations should begin at approximately 10 years of age or at the onset of cardiac signs and symptoms. However, individuals demonstrating these signs and symptoms are relatively late in their course.

RECOMMENDATIONS SPECIFIC FOR CARDIAC CARE IN PATIENTS WITH BMD

  1. Complete cardiac evaluations should begin at approximately 10 years of age or at the onset of signs and symptoms. Evaluations should continue at least biannually.

RECOMMENDATIONS FOR CARDIAC CARE IN CARRIERS OF DMD OR BMD

  1. Carriers of DMD or BMD should be made aware of the risk of developing cardiomyopathy and educated about the signs and symptoms of heart failure.

  2. Carriers of DMD or BMD should be referred for evaluation by a cardiac specialist with experience in the treatment of heart failure and/or neuromuscular disorders. Patients should undergo initial complete cardiac evaluation in late adolescence or early adulthood or at the onset of cardiac signs and symptoms, if these signs or symptoms appear earlier.

  3. Carriers should be screened with a complete cardiac evaluation at a minimum of every 5 years starting at 25 to 30 years of age.

  4. Treatment of cardiac disease is similar to that outlined for boys with DMD or BMD.

Section on Cardiology and Cardiac Surgery, 2004–2005

Thomas S. Klitzner, MD, PhD, Chairperson

Robert H. Beekman, III, MD

Frank M. Galioto, Jr, MD

Thomas K. Jones, MD

Peter B. Manning, MD

W. Robert Morrow, MD

Jane Newburger, MD, MPH

John W. M. Moore, MD, MPH, Immediate Past Chairperson

Invited Contributor

*

Staff

Lynn Colegrove, MBA

Footnotes

  • All clinical reports from the American Academy of Pediatrics automatically expire 5 years after publication unless reaffirmed, revised, or retired at or before that time.

  • * Lead author

    Linda H. Cripe, MD

  • * Lead author

DMD, Duchenne muscular dystrophyBMD, Becker muscular dystrophy

REFERENCES

  1. Emery AE. Population frequencies of inherited neuromuscular diseases: a world survey. Neuromuscul Disord.1991;1 :19– 29
    OpenUrlCrossRefPubMed
  2. Kunkel LM, Monaco AP, Middlesworth W, Ochs HD, Latt SA. Specific cloning of DNA fragments absent from the DNA of a male patient with an X chromosome deletion. Proc Natl Acad Sci USA.1985;82 :4778– 4782
    OpenUrlAbstract/FREE Full Text
  3. Ray PN, Belfall B, Duff C, et al. Cloning of the breakpoint of an X;21 translocation associated with Duchenne muscular dystrophy. Nature.1985;318 :672– 675
    OpenUrlCrossRefPubMed
  4. Hoffman EP, Brown RH, Kunkel LM. Dystrophin: the protein product of the Duchene muscular dystrophy locus. 1987. Biotechnology.1992;24 :457– 466
    OpenUrlPubMed
  5. Monaco AP, Bertelson CJ, Liechti-Gallati S, Moser H, Kunkel LM. An explanation for the phenotypic differences between patients bearing partial deletions of the DMD locus. Genomics.1988;2 :90– 95
    OpenUrlCrossRefPubMed
  6. de Kermadec JM, Becane HM, Chenard A, Tertrain F, Weiss Y. Prevalence of left ventricular systolic dysfunction in Duchenne muscular dystrophy: an echocardiographic study. Am Heart J.1994;127 :618– 623
    OpenUrlCrossRefPubMed
  7. Chenard AA, Becane HM, Tertrain F, de Kermadec JM, Weiss YA. Ventricular arrhythmia in Duchenne muscular dystrophy: prevalence, significance and prognosis. Neuromuscul Disord.1993;3 :201– 206
    OpenUrlCrossRefPubMed
  8. Moriuchi T, Kagawa N, Mukoyama M, Hizawa K. Autopsy analyses of the muscular dystrophies. Tokushima J Exp Med.1993;40 :83– 93
    OpenUrlPubMed
  9. Finder JD, Birnkrant D, Carl J, et al. Respiratory care of the patient with Duchenne muscular dystrophy: ATS consensus statement. Am J Respir Crit Care Med.2004;170 :456– 465
    OpenUrlCrossRefPubMed
  10. Eagle M, Baudouin SV, Chandler C, Giddings DR, Bullock R, Bushby K. Survival in Duchenne muscular dystrophy: improvements in life expectancy since 1967 and the impact of home nocturnal ventilation. Neuromuscul Disord.2002;12 :926– 929
    OpenUrlCrossRefPubMed
  11. Simonds AK, Muntoni F, Heather S, Fielding S. Impact of nasal ventilation on survival in hypercapnic Duchenne muscular dystrophy. Thorax.1998;53 :949– 952
    OpenUrlAbstract/FREE Full Text
  12. Clinical indications for noninvasive positive pressure ventilation in chronic respiratory failure due to restrictive lung disease, COPD, and nocturnal hypoventilation: a consensus conference report. Chest.1999;116 :521– 534
    OpenUrlCrossRefPubMed
  13. Giglio V, Pasceri V, Messano L, et al. Ultrasound tissue characterization detects preclinical myocardial structural changes in children affected by Duchenne muscular dystrophy. J Am Coll Cardiol.2003;42 :309– 316
    OpenUrlCrossRefPubMed
  14. Sasaki K, Sakata K, Kachi E, Hirata S, Ishihara T, Ishikawa K. Sequential changes in cardiac structure and function in patients with Duchenne type muscular dystrophy: a two-dimensional echocardiographic study. Am Heart J.1998;135 :937– 944
    OpenUrlCrossRefPubMed
  15. Takenaka A, Yokota M, Iwase M, Miyaguchi K, Hayashi H, Saito H. Discrepancy between systolic and diastolic dysfunction of the left ventricle in patients with Duchenne muscular dystrophy. Eur Heart J.1993;14 :669– 676
    OpenUrlAbstract/FREE Full Text
  16. Nigro G, Comi LI, Politano L, Bain RJ. The incidence and evolution of cardiomyopathy in Duchenne muscular dystrophy. Int J Cardiol.1990;26 :271– 277
    OpenUrlCrossRefPubMed
  17. Bushby K, Muntoni F, Bourke JP. 107th ENMC International Workshop: the management of cardiac involvement in muscular dystrophy and myotonic dystrophy—7th–9th June 2002. Naarden, the Netherlands. Neuromuscul Disord.2003;13 :166– 172
    OpenUrlCrossRefPubMed
  18. Corrado G, Lissoni A, Beretta S, et al. Prognostic value of electrocardiograms, ventricular late potentials, ventricular arrhythmias, and left ventricular systolic dysfunction in patients with Duchenne muscular dystrophy. Am J Cardiol.2002;89 :838– 841
    OpenUrlCrossRefPubMed
  19. Yotsukura M, Fujii K, Katayama A, et al. Nine-year follow-up study of heart rate variability in patients with Duchenne-type progressive muscular dystrophy. Am Heart J.1998;136 :289– 296
    OpenUrlCrossRefPubMed
  20. Yotsukura M, Sasaki K, Kachi E, Sasaki A, Ishihara T, Ishikawa K. Circadian rhythm and variability of heart rate in Duchenne-type progressive muscular dystrophy. Am J Cardiol.1995;76 :947– 951
    OpenUrlCrossRefPubMed
  21. Lanza GA, Dello Russo A, Giglio V, et al. Impairment of cardiac autonomic function in patients with Duchenne muscular dystrophy: relationship to myocardial and respiratory function. Am Heart J.2001;141 :808– 812
    OpenUrlCrossRefPubMed
  22. Saito T, Matsumura T, Miyai I, Nozaki S, Shinno S. Carvedilol effectiveness for left ventricular-insufficient patients with Duchenne muscular dystrophy. [in Japanese] Rinsho Shinkeigaku.2001;41 :691– 694
    OpenUrlPubMed
  23. Ishikawa Y, Bach JR, Minami R. Cardioprotection for Duchenne's muscular dystrophy. Am Heart J.1999;137 :895– 902
    OpenUrlCrossRefPubMed
  24. Shaddy RE, Tani LY, Gidding SS, et al. Beta-blocker treatment of dilated cardiomyopathy with congestive heart failure in children: a multi-institutional experience. J Heart Lung Transplant.1999;18 :269– 274
    OpenUrlCrossRefPubMed
  25. Drachman DB, Toyka KV, Myer E. Prednisone in Duchenne muscular dystrophy. Lancet.1974;2 (7894):1409–1412
  26. Mesa LE, Dubrovsky AL, Corderi J, Marco P, Flores D. Steroids in Duchenne muscular dystrophy: deflazacort trial. Neuromuscul Disord.1991;1 :261– 266
    OpenUrlCrossRefPubMed
  27. Dubrovsky AL, Angelini C, Bonifati MD, Pegoraro E, Mesa L. Steroids in muscular dystrophy: where do we stand? Neuromuscul Disord.1998;8 :380– 384
    OpenUrlCrossRefPubMed
  28. Biggar WD, Gingras M, Fehlings DL, Harris VA, Steele CA. Deflazacort treatment of Duchenne muscular dystrophy. J Pediatr.2001;138 :45– 50
    OpenUrlCrossRefPubMed
  29. Silversides CK, Webb GD, Harris VA, Biggar DW. Effects of deflazacort on left ventricular function in patients with Duchenne muscular dystrophy. Am J Cardiol.2003;91 :769– 772
    OpenUrlCrossRefPubMed
  30. Bulkley BH, Roberts WC. The heart in systemic lupus erythematosus and the changes induced in it by corticosteroid therapy: a study of 36 necropsy patients. Am J Med.1975;58 :243– 264
    OpenUrlCrossRefPubMed
  31. Dubowitz V. 75th European Neuromuscular Centre International Workshop: 2nd workshop on the treatment of muscular dystrophy 10–12 December, 1999, Naarden, the Netherlands. Neuromuscul Disord.2000;10 :313– 320
    OpenUrlCrossRefPubMed
  32. Wong BL, Christopher C. Corticosteroids in Duchenne muscular dystrophy: a reappraisal. J Child Neurol.2002;17 :183– 190
    OpenUrlAbstract/FREE Full Text
  33. Shapiro F, Sethna N, Colan S, Wohl ME, Specht L. Spinal fusion in Duchenne muscular dystrophy: a multidisciplinary approach. Muscle Nerve.1992;15 :604– 614
    OpenUrlCrossRefPubMed
  34. Granata C, Merlini L, Cervellati S, et al. Long-term results of spine surgery in Duchenne muscular dystrophy. Neuromuscul Disord.1996;6 :61– 68
    OpenUrlCrossRefPubMed
  35. Kerr TP, Duward A, Hodgson SV, Hughes E, Robb SA. Hyperkalaemic cardiac arrest in a manifesting carrier of Duchenne muscular dystrophy following general anaesthesia. Eur J Pediatr.2001;160 :579– 580
    OpenUrlCrossRefPubMed
  36. Schmidt GN, Burmeister MA, Lilje C, Wappler F, Bischoff P. Acute heart failure during spinal surgery in a boy with Duchenne muscular dystrophy. Br J Anaesth.2003;90 :800– 804
    OpenUrlAbstract/FREE Full Text
  37. Noordeen MH, Haddad FS, Muntoni F, Gobbi P, Hollyer JS, Bentley G. Blood loss in Duchenne muscular dystrophy: vascular smooth muscle dysfunction? J Pediatr Orthop B.1999;8 :212– 215
    OpenUrlCrossRefPubMed
  38. Wedel DJ. Malignant hyperthermia and neuromuscular disease. Neuromuscul Disord.1992;2 :157– 164
    OpenUrlCrossRefPubMed
  39. Larach MG, Rosenberg H, Gronert GA, Allen GC. Hyperkalemic cardiac arrest during anesthesia in infants and children with occult myopathies. Clin Pediatr (Phila).1997;36 :9– 16
    OpenUrlAbstract/FREE Full Text
  40. Breucking E, Reimnitz P, Schara U, Mortier W. Anesthetic complications: the incidence of severe anesthetic complications in patients and families with progressive muscular dystrophy of the Duchenne and Becker types [in German]. Anaesthesist.2000;49 :187– 195
    OpenUrlCrossRefPubMed
  41. Willig TN, Carlier L, Legrand M, Riviere H, Navarro J. Nutritional assessment in Duchenne muscular dystrophy. Dev Med Child Neurol.1993;35 :1074– 1082
    OpenUrlPubMed
  42. Willig TN, Bach JR, Venance V, Navarro J. Nutritional rehabilitation in neuromuscular disorders. Semin Neurol.1995;15 :18– 23
    OpenUrlPubMed
  43. Balaguru D, Artman M, Auslender M. Management of heart failure in children. Curr Probl Pediatr.2000;30 :1– 35
    OpenUrlPubMed
  44. Porreca E, Guglielmi MD, Uncini A, et al. Haemostatic abnormalities, cardiac involvement and serum tumor necrosis factor levels in X-linked dystrophic patients. Thromb Haemost.1999;81 :543– 546
    OpenUrlPubMed
  45. Gaffney JF, Kingston WJ, Metlay LA, Gramiak R. Left ventricular thrombus and systemic emboli complicating the cardiomyopathy of Duchenne's muscular dystrophy. Arch Neurol.1989;46 :1249– 1252
    OpenUrlCrossRefPubMed
  46. Nakayama T, Saito Y, Uchiyama T, Yatabe K, Kawai M. Pathogenesis of pulmonary thrombosis in Duchenne muscular dystrophy; a consideration from changes in serum CK and LDH levels [in Japanese]. Rinsho Shinkeigaku.2000;40 :55– 58
    OpenUrlPubMed
  47. Saito T, Matsumura T, Nozaki S, Shinno S. A case of Duchenne muscular dystrophy showing coagulation cascade activation induced by muscle destruction due to convulsion [in Japanese]. Rinsho Shinkeigaku.2003;43 :274– 276
    OpenUrlPubMed
  48. Saito T, Takenaka M, Miyai I, et al. Coagulation and fibrinolysis disorder in muscular dystrophy. Muscle Nerve.2001;24 :399– 402
    OpenUrlCrossRefPubMed
  49. Padman R, Lawless S, Von Nessen S. Use of BiPAP by nasal mask in the treatment of respiratory insufficiency in pediatric patients: preliminary investigation. Pediatr Pulmonol.1994;17 :119– 123
    OpenUrlCrossRefPubMed
  50. Ugalde V, Walsh S, Abresch RT, Bonekat HW, Breslin E. Respiratory abdominal muscle recruitment and chest wall motion in myotonic dystrophy. J Appl Physiol.2001;91 :395– 407
    OpenUrlAbstract/FREE Full Text
  51. Politano L, Nigro V, Nigro G, et al. Development of cardiomyopathy in female carriers of Duchenne and Becker muscular dystrophies. JAMA.1996;275 :1335– 1338
    OpenUrlCrossRefPubMed
  52. Hoogerwaard EM, van der Wouw PA, Wilde AA, et al. Cardiac involvement in carriers of Duchenne and Becker muscular dystrophy. Neuromuscul Disord.1999;9 :347– 351
    OpenUrlCrossRefPubMed
  53. Melacini P, Fanin M, Angelini A, et al. Cardiac transplantation in a Duchenne muscular dystrophy carrier. Neuromuscul Disord.1998;8 :585– 590
    OpenUrlCrossRefPubMed
  54. Grain L, Cortina-Borja M, Forfar C, Hilton-Jones D, Hopkin J, Burch M. Cardiac abnormalities and skeletal muscle weakness in carriers of Duchenne and Becker muscular dystrophies and controls. Neuromuscul Disord.2001;11 :186– 191
    OpenUrlCrossRefPubMed
  55. Nolan MA, Jones OD, Pedersen RL, Johnston HM. Cardiac assessment in childhood carriers of Duchenne and Becker muscular dystrophies. Neuromuscul Disord.2003;13 :129– 132
    OpenUrlCrossRefPubMed
  56. Towbin JA, Hejtmancik JK, Brink P, et al. X-linked dilated cardiomyopathy: molecular genetic evidence of linkage to the Duchenne muscular dystrophy (dystrophin) gene at the Xp21 locus. Circulation.1993;87 :1854– 1865
    OpenUrlAbstract/FREE Full Text
  57. Muntoni F, Cau M, Ganau A, et al. Brief report: deletion of the dystrophin muscle-promoter region associated with X-linked dilated cardiomyopathy. N Engl J Med.1993;329 :921– 925
    OpenUrlCrossRefPubMed
  58. Milasin J, Muntoni F, Severini GM, et al. A point mutation in the 5′ splice site of the dystrophin gene first intron responsible for X-linked dilated cardiomyopathy. Hum Mol Genet.1996;5 :73– 79
    OpenUrlAbstract/FREE Full Text
  59. Feng J, Yan J, Buzin CH, Towbin JA, Sommer SS. Mutations in the dystrophin gene are associated with sporadic dilated cardiomyopathy. Mol Genet Metab.2002;77 :119– 126
    OpenUrlCrossRefPubMed
  60. Feng J, Yan JY, Buzin CH, Sommer SS, Towbin JA. Comprehensive mutation scanning of the dystrophin gene in patients with nonsyndromic X-linked dilated cardiomyopathy. J Am Coll Cardiol.2002;40 :1120– 1124
    OpenUrlCrossRefPubMed
Back to top

In this issue

Pediatrics
Vol. 116, Issue 6
December 2005
View this article with LENS
Email Article
Request Permissions
Article Alerts
Citation Tools
Cardiovascular Health Supervision for Individuals Affected by Duchenne or Becker Muscular Dystrophy
Pediatrics Dec 2005, 116 (6) 1569-1573; DOI: 10.1542/peds.2005-2448
del.icio.us logo Digg logo Reddit logo Twitter logo CiteULike logo Facebook logo Google logo Mendeley logo
Print
Download PDF
Insight Alerts

Jump to section

Related Articles

  • No related articles found.

Cited By...

More in this TOC Section

Similar Articles

Subjects