Glycogen Storage Disease Type I (von Gierke’s Disease, Glucose-6-Phosphatase Deficiency [Type Ia], Glucose-6-Phosphatase Translocase Deficiency [Type 1b])

Clinical manifestations of type I glycogen storage disease are profound hypoglycaemia, associated with hyperlipidaemia, hyperuricaemia and lactic acidosis. It presents in childhood, primarily involving the liver, kidneys, and mucous layers of the small intestine. Pulmonary hypertension has been described in association with the type Ia variant. Postulated mechanisms include chronic stimulation of the smooth muscle of the pulmonary arterioles by the persistent hepatic metabolism of circulating catecholamines such as serotonin. Levels of serotonin have been shown to be elevated in patients with glycogen storage disease type I. Such elevation of the levels of serotonin in isolation do not appear to confer pulmonary vascular disease on these patients. Rather, it is hypothesised that other mediating factors working in concert with persistently elevated levels of serotonin increase the risk for pulmonary vascular changes. ^1–3

Glycogen Storage Disease Type II (Pompe’s Disease, α-1,4-Glucosidase Deficiency)

Pompe’s disease is a generalised glycogen storage disease in which glycogen of normal structure is accumulated in the myocardium, skeletal muscle, and liver. The disease is progressive, and is associated with deficiency of lysosomal α-1,4-glucosidase. There are four subtypes based upon age at onset of clinical symptoms. It is the form presenting in infancy that is recognised as classical Pompe’s disease, but patients can also present in childhood, adolescence (giving rise to the juvenile form), or adulthood. The age at onset correlates inversely with the measured activity of lysosomal α-1,4-glucosidase in myocytes or fibroblasts. In the infantile form, which is more severe in its cardiac involvement than those forms of later onset, there is generalised accumulation of glycogen in the heart, including the conduction tissues, in skeletal muscle, notably the tongue and diaphragm, and in the liver. Central and peripheral neurons and smooth muscle are also affected. The results are cardiomegaly, hepatomegaly, a thickened diaphragm, and macroglossia. In the heart, the glycogen is deposited mainly in ventricular muscle. There is gross thickening of the ventricular walls, with impairment of both diastolic and systolic performance. The infants typically appear normal at birth, though cases of severe neonatal ventricular hypertrophy have been reported. ⁴ The median age at onset of clinical symptoms is 1.6 months. Muscular weakness and hypotonia along with loss of motor milestones are noted during the first 6 months of life, and signs of congestive cardiac failure become evident. Although there is excess glycogen in the liver, hepatomegaly is not commonly present until cardiac failure is apparent. The disease is progressive, and most affected babies die before the age of 1 year. The clinical course may be complicated by arrhythmias. Since patients with Pompe’s disease appear very sensitive to digoxin, this drug must be used with extreme caution. Irritability and poor feeding often draw attention to the disease. The cardiac physical signs are not characteristic, variable murmurs being heard. Unexplained cardiomegaly and congestive cardiac failure in a generally floppy baby should suggest the diagnosis. ⁵

The chest radiograph may be normal at birth, but in all affected infants the heart becomes enlarged within a few weeks. There is no specific cardiac silhouette, but rather a generalised smooth enlargement of the contour. The characteristic electrocardiographic features are a short PR interval, wider than normal QRS complexes, and voltage evidence of left or biventricular hypertrophy, which can be severe ( Fig. 57-1 ). In addition, in the majority there are Q waves and inverted T waves in leads I and II and the left chest leads. ⁶ Electrophysiological studies have shown a short AH interval. ⁷ Both M-mode and cross sectional echocardiograms demonstrate gross increase in the thickness of the ventricular free walls and the ventricular septum ( Fig. 57-2 ). An impairment of ventricular filling in diastole has been noted, ⁸ together with reduction of the rate and extent of systolic shortening. Angiocardiography is rarely performed, as it adds little to the diagnosis or management.

The typical electrocardiogram of a patient with Pompe’s disease demonstrates striking biventricular hypertrophy.

Typical echocardiographic findings in glycogen storage disease type II. A shows a diastolic frame in long axis, revealing severe concentric left ventricular hypertrophy, while the systolic frame from the same child ( B ) shows the absence of subaortic obstruction.

The complete clinical picture, together with the characteristic electrocardiographic and echocardiographic findings, will lead immediately to the definitive diagnostic investigation. This is the demonstration of deficiency of lysosomal α-1,4-glucosidase in fibroblasts grown from a skin biopsy. Sometimes the skeletal muscular abnormalities are less evident. The presentation is then as a cardiomyopathy alone. Pompe’s disease should be considered in any such case, and skin biopsy performed. Until recently, there was no specific treatment available, and supportive and decongestive measures failed to improve outcomes. Recent studies using recombinant human lysosomal acid α-glucosidase show promise in improving survival. ⁹ Since the disease appears to be inherited in an autosomal recessive fashion, parents should be advised of the availability of prenatal diagnosis via culture of amniocytes obtained by amniocentesis.

We include Danon disease in this section because it was previously considered to be a variant of Pompe’s disease known as glycogen storage disease type IIb with normal acid maltase. The disease is due to a deficiency of lysosome-associated protein 2, and it manifests as a progressive hypertrophic cardiomyopathy with skeletal myopathy. Other similar diseases in this family of autophagic vacuolar myopathies are still being studied. Some demonstrate autosomal recessive inheritance while others are X-linked, and the degree of cardiac and skeletal involvement is variable. ¹⁰

Glycogen Storage Disease Type III (Cori’s Disease, Amylo-1,6-Glucosidase [Debrancher] Deficiency)

In Cori’s disease, an autosomal recessive condition, glycogen accumulates in skeletal muscle, in the liver, and in cardiac muscle. The disease is due to a deficiency of amylo-1,6-glucosidase, the enzyme necessary for breaking down branch points in glycogen chains. There are three subtypes dependent upon the primary site of abnormal glycogen storage. Type IIIa involves the liver and muscle, Type IIIb the liver, and Type IIIc the muscle. ^4,11 A fourth subtype, IIId, involves normal debrancher enzymic activity but a deficiency of debrancher enzyme transferase activity. Patients with types IIIa and IIIc have a tendency to develop weakness of the skeletal muscles and left ventricular hypertrophy, ¹² which is progressive. The clinical course appears to be less severe, with fewer symptoms as compared to hypertrophic obstructive cardiomyopathy. ^13,14

Glycogen Storage Disease Type Iv (Andersen’s Disease, α-1,4-Glucan-6-Glucosyltransferase [Brancher] Deficiency)

Andersen’s disease is a rare heterogeneous glycogen storage disease characterised by deposition of glycogen of abnormal structure in the liver, leading to cirrhosis. There may also be deposition of polysaccharide in the heart. While liver dysfunction is the most common clinical manifestation, the disease can rarely present with dilated cardiomyopathy, which is typically severe. ^15–17

Glycogen Storage Disease Type V (McArdle’s Disease, Muscle Phosphorylase Deficiency)

McArdle’s disease results from a deficiency of muscle phosphorylase. It is usually recognised in adolescence or adult life. Its main clinical features are muscular fatiguability, muscular cramps, and myoglobinuria. Rare lethal variants have been reported in infants, ¹⁸ but the heart is typically spared. This may be due to activity of a distinct cardiac phosphorylase isozyme, which retains activity in patients with deficiency of the skeletal isozyme. ¹⁹ No clinical cardiac manifestations have been reported, but on occasion the electrocardiogram has features similar to those seen in Pompe’s disease. ²⁰

Glycogen Storage Disease Type VI (Hers’ Disease, Phosphorylase B Kinase Deficiency, Liver Phosphorylase Deficiency)

Hers’ disease involves both X-linked and autosomal recessive modes of inheritance. It results from deficiency of liver phosphorylase. Both types involve the liver in childhood, whereas involvement of muscles occurs in young adults with the autosomal recessive form of the disease. Rare forms of phosphorylase b kinase deficiency have been described in which deposition of glycogen is limited to the heart. ²¹

Glycogen Storage Disease Type VII (Tarui’s Disease, Muscle Phosphofructokinase I Deficiency)

Tarui’s disease is a rare form of glycogen storage disease that presents in early childhood or adult life with fatiguability, muscular weakness that can be progressive, muscular cramps, and myoglobinuria. Typically, the heart is spared. An infantile form of the disease has also been described in the members of one family. Cardiomyopathy occurred in addition to the progressive muscular weakness, and abnormal deposition of glycogen was noted in the cardiac muscle at autopsy. ²² Progressive cardiomyopathy has also been reported in an adult. ²³

Mucopolysaccharidosis Type I (α- l -Iduronidase Deficiency)

The three major clinical forms of α- l -iduronidase deficiency are Hurler’s syndrome, Scheie’s syndrome, and a syndrome intermediate between the two, known unsurprisingly as Hurler-Scheie syndrome. These diseases are due to defects in the gene encoding α- l -iduronidase, and multiple defects have been elucidated. These include nonsense, missense, insertional, deletional, and splice-type gene defects. It is thought that the clinical severity of the disease is related to the level of new enzymic activity, which in turn is due to a specific genetic defect. ^25,26

Mucopolysaccharidosis Type II (Hunter’s Syndrome, Iduronate Sulfatase Deficiency)

Deficiency of iduronate sulfatase results in a block of degradation of dermatan sulphate. The difference in clinical profile between this and Hurler’s and Scheie’s syndromes, for example, the absence of corneal clouding in Hunter’s syndrome, may result from specific variability in the degree of blockage of degradation of the mucopolysaccharide. Furthermore, it may be that the block to degradation caused by the accumulation of iduronate sulfate may be bypassed by hyaluronidase. The severe and mild forms of Hunter’s syndrome both have total, or near total, deficiency of iduronate sulfatase. As with mucopolysaccharidosis type I, the clinical phenotype may be representative of the degree of residual enzymic activity specific to certain gene mutations, of which more than 300 have been found for Hunter’s syndrome. ³⁶

The condition can occur with a wide variety in severity. Apart from the extreme rarity of corneal clouding in Hunter’s syndrome, and the presence of loss of hearing, the clinical features are those of Hurler’s syndrome, although usually less severe. A positive distinguishing physical sign, pointed out by Hunter himself in 1916, is the occurrence of pebble-like ivory-coloured dermal lesions. These are seen over the scapulas and occasionally on the pectoral regions.

Cardiac involvement produces all the manifestations so far mentioned, namely, aortic and mitral regurgitation or stenosis, ischaemic changes, and evidence of myocardial dysfunction. Echocardiography is a useful method for evaluating cardiac involvement. The clinical course is extremely varied. Severely affected individuals die before the age of 15 years. At the opposite end of the spectrum, survival beyond the sixth decade has been reported. Death in younger patients is usually associated with progressive neurological deterioration. The disease is inherited as an X-linked recessive trait, though cases in females have been reported. ³⁷ Since the reproductive fitness of the Hunter gene is low, a large minority of cases must result from new mutations.

A new treatment for Hunter’s syndrome has recently emerged with the development of recombinant human iduronate-2-sulfatase. This was well tolerated, and demonstrated improvement in several parameters for outcome, including forced vital capacity, urinary excretion of glycosaminoglycans, the size of the liver and spleen, and 6-minute walk distance. ^38,39 The effect of enzymic therapy on the cardiac lesions, however, remains to be determined.

Mucopolysaccharidosis Type III (Sanfilippo’s Syndrome)

The degradation of heparan sulphate and N-sulphated or N-acetylated α-linked glucosamine requires four enzymes: heparan N-sulphatase, N-acetyl-α- d -glucosaminidase, acetyl-CoA:α-glucosaminide N-acetyltransferase, and N-acetyl-α- d -glucosamine-6-sulphate sulphatase. Deficiency of one of the four enzymes required for this degradation results in Sanfilippo’s syndrome. Consequently, there are four biochemically distinct types of the disease, designated A through D, although they all present the same clinical features.

The onset is usually evident in the first few years of life with behavioural problems. Mental and neurological deterioration are severe and lead to death in the first two decades. Bone, joint, and cardiac involvement are generally less severe than in Hurler’s syndrome. Corneal clouding is never seen. There is wide variation in the severity and age at death in all four forms, but type A is likely to be the most severe. Inheritance is in an autosomal recessive fashion. A number of patients with mitral valvar involvement have been reported. ^40,41 Cardiac involvement is similar to that of other mucopolysaccharidoses, with thickening of the valvar leaflets. While treatment is primarily supportive, animal studies have been undertaken to assess replacement of the enzymes in a mouse model with mucopolysaccharidosis type III-B. ⁴²

Mucopolysaccharidosis Type IV (Morquio’s Syndrome)

Morquio’s syndrome results from defective degradation of keratan sulphate. It occurs in two biochemically distinct forms. The so-called type A is due to a deficiency of N-acetylgalactosamine-6-sulfate sulfatase, while type B results from deficiency of β-galactosidase. The two types have similar clinical features, but type B is less severe, sometimes called the long-legged variant. Despite the generally increased severity of features in type A, more mild forms of type A can occur. Keratan sulphate is excreted in the urine in type A, but this is less evident in type B.

Keratan sulphate is found in cartilage, intervertebral discs, and the cornea. Thus, skeletal involvement with dwarfism, pectus deformities, and bow legs are the most obvious manifestations. Corneal clouding is common. In contrast to the mucopolysaccharidoses described above, the joints in patients with Morquio’s syndrome are hyperextensible. Absence or severe hypoplasia of the odontoid process, together with laxity of its associated ligaments, leads to atlanto-occipital subluxation, and consequent cervical myelopathy. The heart is clinically involved only in the severe type. Valves of the heart are primarily involved, with thickening of mitral and aortic leaflets. Concentric left ventricular hypertrophy and, rarely, asymmetrical septal hypertrophy have been described. ^40,43 Survival beyond the third or fourth decade is not unusual. The effects of the cervical myelopathy and respiratory problems are the usual cause of death. Experimentation with enzymic replacement therapy in animals has been undertaken and holds some promise. ⁴⁴

Mucopolysaccharidosis Type VI (Maroteaux-Lamy Syndrome)

Deficiency of arylsulfatase B results in an inability to hydrolyse the sulfate groups in dermatan sulfate. The clinical picture is similar to that of Hurler’s syndrome, but normal intelligence is usually maintained. Although severe in its classical form, milder variations exist. Affected infants can present with an acute cardiopathy. ⁴⁵ Thickened mitral and aortic valvar leaflets necessitating valvar replacement has been noted in young adults. ⁴⁶ A left ventricular aneurysm has also been reported. ⁴⁷ Death usually occurs in the third decade. The condition is inherited in autosomal recessive fashion, though some cases have been presumed to be X-linked. ⁴⁸ Enzymic replacement therapy with human recombinant arylsulfatase B has been studied, and found to be safe and beneficial in terms of exertional tolerance and urinary excretion of glycosaminoglycan. ⁴⁹

Mucopolysaccharidosis Type VII (Sly’s Syndrome)

Deficiency of β-glucuronidase results in a clinical syndrome of extremely variable severity. Included in the features are coarse facies, corneal clouding, abdominal and inguinal hernias, puffy hands and feet, hepatosplenomegaly, and a small thoracolumbar hump. Cardiovascular manifestations include hypertension, aortic aneurysm, aortic regurgitation, obstructive arterial disease, and cardiomyopathy. ^50,51 Fetal hydrops has also been reported. ⁵² This extremely rare condition is inherited in autosomal recessive fashion. Duration of survival varies widely, and depends on the severity of the disease. Death as early as 30 months has occurred in one child with severe disease. Animal studies involving enzymic replacement therapy have been performed and are encouraging in terms of improving the cardiovascular changes associated with this disease. ⁵³

Mucolipidosis Type II (Inclusion Cell Disease, I-Cell Disease)

I-cell disease results from a severe deficiency of the phosphotransferase enzyme due to specific genetic mutations which result in a marked reduction in enzymic activity. Various defects in the gene encoding this enzyme have been discovered in patients with this disorder. ⁵⁵ The patients with inclusion cell disease present with clinical features very similar to those with Hurler’s syndrome. Hepatosplenomegaly is not so obvious, while striking gingival hypertrophy is a feature not encountered in Hurler’s syndrome. Furthermore, the disease becomes evident earlier than does Hurler’s syndrome. Corneal clouding is the rule. The skeletal and joint abnormalities, together with myocardial infiltration, usually lead to death by the age of 5 years, either from respiratory causes or cardiac failure. Asymmetrical septal hypertrophy has been reported. ⁵⁶ Treatment of the cardiac manifestations is usually supportive, though surgical management of valvar involvement has been reported. ⁵⁷ Transplantation of allogeneic stem cells has stemmed the progression of disease in a small number of reported cases. ⁵⁸

Mucolipidosis Type III (Pseudo-Hurler Polydystrophy)

Mucolipidosis type III is less severe, and also less common, than type II, and is due to a deficiency of the same phosphotransferase enzyme. In type III, the enzymic activity is less severely reduced, and the manifestations are less severe. There is a fair amount of variability in clinical severity. ⁵⁹ This is likely due to various genetic defects leading to different levels of enzymic activity. Patients are usually spared the joint manifestations of I-cell disease early in life, and often present with joint stiffness at the age of 4 or 5 years. Growth is moderately retarded, and corneal clouding is present by the age of 7 or 8 years. The patients are disabled by carpal tunnel syndrome and destruction of the hip joints. Cardiac involvement, particularly aortic regurgitation, does occur but is usually not sufficiently severe to cause clinical problems. Patients with pseudo-Hurler polydystrophy survive into the fourth decade.

Mannosidosis

Deficiency of α-mannosidase results in the accumulation of oligosaccharides, as their degradation is dependent upon lysosomal activity of this enzyme. Oligosaccharides are excreted in the urine. Several defects in the gene encoding α-mannosidase have been discovered. The specific defect may result in decreased enzymic synthesis, decreased enzymic activity within the lysosomal environment, decreased localisation of the enzyme within the lysosome, or faulty post-translational modification of the enzyme. The patients present with features suggestive of mucopolysaccharidosis but have an increased susceptibility to infections. Progressive mental retardation is typical. Early onset of the disease shown as type I is associated with increased severity. Death occurs between 3 and 10 years of age. Late-onset, or type II, runs a more benign course. Cardiac manifestations are not frequently reported. A short PR interval has been reported in several patients, albeit that its mechanism is unknown. ⁶⁰ Treatment has been attempted with transplantation of bone marrow, and current strategies under investigation include various forms of enzymic replacement therapy. ⁶¹

Fucosidosis

Deficiency of α- l -fucosidase results in the accumulation of fucosylated oligosaccharides and glycolipids. Two clinical types are recognised. The first type presents in infancy with coarse facies, growth retardation, mental retardation, and neurological deterioration. Convulsions and respiratory infections often occur. The second type has a more benign course and a later onset. Cardiomegaly, probably as a part of a generalised visceromegaly, is the most common cardiac feature. These two types probably represent both ends of a continuum which is dictated by specific enzymic activity as determined by the specific genetic defect. Transplantation of bone marrow has been performed with good results, and further experimentation with enzymic replacement therapy is under way. ⁶²

Sialidosis

The basic defect in sialidosis is deficiency of α-neuraminidase, with accumulation of sialoglycoconjugates. There are two forms. The first is of late onset. Patients are of normal appearance, but develop the cherry red spot myoclonus syndrome. Decreased visual acuity is associated with a cherry red spot in the macular region. Neurological, and occasionally renal, manifestations dominate the clinical picture. The second type has an early onset, even upon occasion being obvious at birth. The patients have coarse features and enlargement of various organs, including the heart. Echocardiography has shown a thickened left ventricular wall along with thickening of the mitral valve. ⁶³ There is great variability in the spectrum of severity, even in the group with early onset. Survival beyond 20 years is rare, while, occasionally, affected subjects are stillborn. Fetal hydrops has been reported as a presenting feature. ⁶⁴ Sialidosis is inherited in autosomal recessive fashion. Enzymic replacement therapy and gene transfer are under investigation. ⁶⁵

Galactosialidosis

In galactosialidosis, patients have a defect in the production of lysosomal protective protein/cathepsin A, which helps form a stable and activated complex with β-galactosidase and α-neuraminidase. ⁶⁶ Thus, the symptoms are a combination of those seen in sialidosis and Morquio’s syndrome, the severity of which is likely determined by the specific genetic defect and its overall effect on production of functional levels of the protein. An infantile form has been described, ⁶⁷ though there appears to be clinical variation even in those diagnosed as infants. ⁶⁸ Complex congenital cardiac malformations have been reported in patients with galactosialidosis. ⁶⁹ The cardiac manifestations are similar to those seen in Morquio’s syndrome and sialidosis, with aortic and mitral valvar thickening which is progressive. ^70,71 Recently, the role of these enzymes and protective protein/cathepsin A in elastogenesis has begun to be unraveled, helping further to explain the phenotype associated with these genetic disorders. ⁷² Early work has begun on therapies involving enzymic replacement or gene transfer. ^65,73

Aspartylglycosaminuria

Aspartylglycosaminuria is a lysosomal storage disease produced by defective or deficient glycosylasparaginase. This enzyme is required for complete breakdown of asparagine-linked glycoproteins within the lysosome. ⁷⁴ Accumulation of these glycoprotein residues leads to severe and progressive neurologic impairment. It is associated with coarse features, joint laxity, early rapid somatic growth followed by a reduced adolescent growth spurt leading ultimately to short stature, and mental retardation. Animal models demonstrate accumulation of residues within the heart, but clinical cardiac involvement does not appear to predominate. Enzymic replacement is currently being studied in animal models. ⁷⁵

Sphingomyelin Lipidosis (Niemann-Pick Disease)

In Niemann-Pick disease, there is accumulation of sphingomyelin in the cells as a result of deficiency of sphingomyelinase. The primary cells affected are those of monocyte-macrophage lineage, as they are frequently employed in the metabolic turnover of these substances. At least four variants exist, but the most frequently encountered is the infantile acute neuronopathic form. Many of these patients are of Ashkenazi Jewish heritage. The disease is characterised by hepatosplenomegaly and the occurrence of foam storage cells in many tissues. The heart is not usually affected, but one infant with acute neuronopathic disease had endocardial fibroelastosis. ⁷⁹ Since there were no storage cells in the heart, however, this may have been a chance association. Abnormalities in the lipid profile have also been described in children with Niemann-Pick disease types A and B, possibly leading to premature atherosclerosis. ⁸⁰ Low levels of high density lipid cholesterol were the most consistent finding, while elevated levels of triglyceride and low density lipid cholesterol were seen in approximately two-thirds. These abnormalities were noted at an early age, and may reflect deranged cholesterol metabolism in these cells as a result of sphingomyelin accumulation. Niemann-Pick disease in most of its forms is inherited in an autosomal recessive fashion.

Glucosylceramidosis (Gaucher’s Disease)

Gaucher’s disease is the most common inherited disorder of glycolipid metabolism. In his original description, ⁸¹ Phillippe Gaucher ascribed the changes to a primary epithelioma of the spleen. There is excessive accumulation of glucosylceramide in cells of the reticuloendothelial system in organs throughout the body, resulting from deficiency of the enzyme glucocerebrosidase, which cleaves glucose from glucocerebroside. While over 150 different mutations of the gene encoding glucocerebrosidase have been described, the disease occurs in three varieties based upon the presence or absence of, and rate of progression of, neurologic manifestations. Type I, or the chronic non-neuronopathic form, can be diagnosed at any age. It is the most common form, being characterised by hypersplenism, hepatomegaly with evidence of abnormal hepatic function, and skeletal lesions, including aseptic necrosis of the femoral head. Other long bones and vertebras may also be eroded. In patients with this type of disease, cardiac involvement may be seen with myocardial infiltration or restrictive pericardial disease. ⁸² The most frequently encountered cardiac problem, however, is cor pulmonale secondary to pulmonary involvement. Mitral and aortic stenosis and insufficiency can also be seen, ⁸³ and severe valvar and aortic arch calcification has been reported. ⁸⁴ The course is variable. Death may occur in early childhood or, particularly when onset is late, there may be a normal life expectancy. Further variability is apparently the consequence of the non-neuronopathic form at onset changing to one of the other forms with a poorer prognosis.

The acute neuronopathic form, or type II, is usually recognised within the second half of the first year of life. Neurological involvement is evident early, afflicting particularly the cranial nerves and extrapyramidal tracts. The mechanism of death is usually a respiratory infection, since aspiration is common owing to incoordination of the nasopharynx. The subacute neuronopathic form, or type III, falls between the acute and chronic forms. The neurological involvement renders it less benign than the chronic variant, but its course usually stretches over many years.

While describing Gaucher’s disease in terms of three distinct phenotypes is convenient, the observed characteristics of this disease are much less well defined. Patients with the same genotype can have widely differing phenotypes, and patients even within a particular type can have markedly differing clinical courses. Thus, while the genetic defects leading to Gaucher’s disease are being elucidated, and include over 150 specific mutations already identified, the link between genotype and phenotype is still unclear.

The diagnosis of Gaucher’s disease is confirmed by the finding of typical storage cells in the bone marrow, or by liver biopsy. The Gaucher cell is large and lipid laden. The cytoplasm is described as having an appearance of wrinkled tissue paper or crumpled silk. The nucleus is eccentric. These cells have to be differentiated from cells found in multiple myeloma, leucaemia, thalassaemia, and congenital dyserythropoietic anaemia. Demonstration of the enzymic deficiency in cultured skin fibroblasts, or in leucocytes, confirms the diagnosis. Approaches to treatment have included transplantation of organs and enzymic replacement. Improvement in the visceral involvement is common, but neurologic damage is generally not responsive to exogenous enzymic therapy. All three variants are inherited as autosomal recessive traits. Intra-uterine diagnosis is available, and heterozygotes can be identified at least for the acute and chronic types.

α-Galactosidase A Deficiency (Fabry’s Disease)

Deficiency of α-galactosidase, a lysosomal enzyme, results in accumulation of phosphosphingolipids in the lysosomes of many tissues and also in the body fluids. The most frequently affected tissue is the vascular endothelium. The disease is of X-linked inheritance, but heterozygous women can show severe manifestations of the disease. ⁸⁵ The gene locus for the enzyme is on the long arm of the X chromosome.

The disease usually presents in childhood in the male homozygote, often with periodic crises of severe pain of burning character, which usually start in the hands and feet. Crises occur most usually in the afternoon. Development of crises, which become less frequent and severe with time, may be followed by eruption of skin lesions, by angiokeratomas, and by typical opacities of the cornea and the lens. The angiokeratomas are clusters of dark red to purple punctate lesions which are usually flat or slightly raised. They occur most frequently between the umbilicus and the knees. They do not blanch on pressure. Hyperkeratosis and hypohidrosis usually accompany the angiokeratomas. Ocular lesions include typical creamy whorl-like opacities in the cornea. They are frequently found in the female heterozygote as well as the male homozygote. Cardiac disease is manifest with increasing age. Myocardial ischaemia and infarction are common and are secondary to the vascular lesions. Mitral regurgitation and aortic stenosis are the most frequently encountered valvar lesions. ⁸⁶ Infiltration of the conduction tissues occurs. This results in progressive shortening of the PR interval as in other storage diseases that affect the specialised atrioventricular conduction axis. ⁸⁷ Myocardial deposition can be detected echocardiographically by demonstration of septal and left ventricular wall thickening. ⁸⁸ Progressive deposition of glycosphingolipid means that the cardiac problems themselves are also progressive. Since there is concomitant renal involvement, the cardiac effects are exacerbated by, for example, renal hypertension. The clinical course in the male homozygote is one of steady deterioration during early adult life, death being from cardiac or renal disease. The heterozygote female experiences little limitation of style and length of life. The diagnosis can be confirmed, and heterozygotes identified, by demonstrating the enzymic deficiency in leucocytes, and by finding an abnormally high content of accumulated substrates in tears or urinary sediment. Prenatal diagnosis is available. Enzymic replacement was reported in 2002, ⁸⁹ and positive effects on cardiac involvement are evident. ⁹⁰

GM ₁ Gangliosidosis

There are many enzymatic and clinical subdivisions of GM ₁ gangliosidosis. The gene locus is on the short arm of chromosome 3. Mutation at this locus results in absence of enzymic activity for acid β-galactosidase, leading to accumulation of GM ₁ ganglioside in the brain and organs. The wide variation in clinical picture has resulted in a broad classification of infant, juvenile, and adult forms. All forms of GM ₁ gangliosidosis are inherited as autosomal recessive traits.

When seen in infancy, the disease is rapidly progressive, characterised by hypotonia, poor feeding, and failure to make motor or intellectual progress. Progressive neurological deterioration results in spastic quadriplegia or decerebrate rigidity. Rarified bones and beaked vertebrae are some of the skeletal lesions encountered. As in Tay-Sachs disease, to be discussed below, a cherry red spot is seen in the macular region of the retina. Death usually occurs by the age of 3 years, frequently from bronchopneumonia. The heart is frequently involved. The spectrum from congestive cardiac failure with systolic dysfunction to isolated valvar thickening has been observed. ^91,92 Neonatal ascites has also been reported. ⁹³ Cardiac involvement usually includes cardiomegaly on chest radiography, left ventricular hypertrophy on the echocardiogram, and congestive cardiac failure. ⁹⁴ Patients with GM ₁ gangliosidosis have a defect in the same enzyme which is involved in patients with Morquio’s syndrome type B. The clinical heterogeneity among patients with this enzymatic defect is unclear, but probably is related to residual activity of the enzyme, post-processing of the enzyme, and other proteins involved, such as saposin B. ⁹⁵ A novel therapeutic strategy is under investigation, and involves molecular chaperones, substances which stabilise the configuration of defective enzymes and enable them to remain enzymatically active. ⁹⁶ Treatment in a mouse model demonstrated improved enzymic activity, ⁹⁷ and reduced the quantity of substrate in neuronal tissues. ⁹⁸

GM ₂ Gangliosidoses

The GM ₂ gangliosidoses result in variable deficiency of hexosaminidase, the locus for which has been mapped to the q arm of chromosome 5. This enzyme, which is composed of alpha and beta subunits, comes in two forms. Hexosaminidase A, found in the central nervous system, is composed of an alpha and beta subunit, while hexosaminidase B, found in peripheral tissues, is composed of two beta subunits. Thus, the GM ₂ gangliosidoses result from a defect in either the alpha subunit, producing Tay-Sachs disease and severe deficiency of hexosaminidase A, or the beta subunit, which produces Sandhoff’s disease, with severe deficiency of both types A and B of the enzyme. The juvenile and adult chronic GM ₂ gangliosidoses result from less severe deficiencies of hexosaminidase A. Treatment for these disorders is still under investigation and has included gene therapy, substrate reduction, and transplantation of bone marrow. ^99–101

Hypothyroidism

Hyperthyroidism

Infantile Marfan Syndrome

An infantile variant of Marfan syndrome is seen on rare occasions. The skeletal and ocular manifestations are similar to the adult forms, but the cardiovascular features are distinct. ¹⁸⁶ There is marked myxomatous thickening and redundancy of the leaflets of the mitral and tricuspid valves, with elongation of the tendinous cords leading to severe valvar insufficiency. Morbidity and mortality are primarily related to mitral and tricuspid valvar disease, as opposed to aortic dissection and rupture as seen in the adult form. ¹⁸⁷ Additionally, patients with the infantile syndrome frequently exhibit pulmonary emphysematous changes. Because the infantile syndrome carries a poor prognosis, it is important to differentiate it from the classic syndrome, which can occasionally be evident in a neonate. Neonates with the infantile syndrome present in congestive cardiac failure that responds poorly to conventional therapy. Death often occurs within the first 2 years of life, though surgical repair of mitral valvar disease at this age is feasible. A family history of Marfan syndrome is much less common in infants who present with severe cardiovascular symptoms early in life. ¹⁸⁸ Most mutations resulting in the infantile syndrome occur between exons 24 and 32 in the fibrillin gene.

Duchenne’s Muscular Dystrophy

Duchenne’s muscular dystrophy is an X-linked recessive disease. Because of this, it almost always afflicts males. Its incidence in male children is calculated at between 13 and 33 cases for each 100,000 live births. Since females with Turner syndrome have only one X chromosome, they too can inherit the disease, and it is seen rarely in this setting. The disease is due to a defect in the gene encoding dystrophin. Dystrophin helps to form a complex which stabilises the sarcolemmal membrane during contraction. While the exact mechanism for muscle degeneration has not been elucidated, abnormal nitric oxide regulation, abnormal sarcolemmal fragility, and increased susceptibility to oxidative stress are felt to play important roles. ¹⁹²

The earliest symptoms are clumsiness in walking, a tendency to fall, and an inability to run. Those with the disease also have difficulty in climbing stairs and getting up from the floor. Clinical onset is usually manifested before 4 years of age, and the diagnosis is usually made around 6 years of age. Deterioration is continuous. Most are unable to walk by the age of 10 years. Life expectancy is increasing owing to improved medical therapies, including nocturnal ventilation, early and aggressive management of cardiomyopathy, and perhaps the use of corticosteroids. ¹⁹³ Muscular weakness and atrophy initially affect the proximal muscle groups of the upper limbs. Involvement of the legs extends from the quadriceps and gluteal muscles to the anterior tibial muscles. Weakness later affects other muscle groups. More power is generally retained in the distal muscles. Slight facial weakness occurs in the late stages. Scapular winging is also a later phenomenon. Muscular hypertrophy of the calves, masticatory muscles, and deltoids is followed by a pseudohypertrophic phase of fatty replacement. Tendon reflexes are lost in the weak muscles. Contractures of the calves and flexor muscles of the hip develop around the age of 8 years. Contractures appear in the hips, knees, elbows, and wrist when the patients are confined to wheelchairs. Severe spinal and thoracic deformities are seen late in the disease. Kyphoscoliosis is common. These result from disuse and abnormal posture. Generalised decalcification of the bones leads to frequent pathological fractures.

Myocardial involvement is common. It is uncertain at what stage it begins, since the physical incapacity limits its manifestation. The heart can be involved from an early age, and in ambulatory patients, subclinical disease may become symptomatic with exercise. In non-ambulatory patients, a resting tachycardia, ¹⁹⁴ decreased heart rate variability, ¹⁹⁵ echocardiographic evidence of diastolic dysfunction, ¹⁹⁶ and myocardial strain changes on magnetic resonance imaging ¹⁹⁷ may help to alert the clinician to subclinical myocardial involvement so that medical therapy can be initiated. The roles of cardiac troponins and brain natriuretic peptide are also being evaluated in the assessment of these patients. ¹⁹⁸ The cardiac dysfunction is progressive, ultimately resulting in a dilated cardiomyopathy, and the benefits of early medical therapy are controversial. Some advocate early use of afterload reduction therapy, ^199,200 but others have shown a benefit only when afterload reduction is combined with β-blockade. ²⁰¹

There is a distinctive electrocardiographic pattern in from half to nine-tenths of patients. This includes tall R waves over the right precordial leads with increased R:S amplitude ratios, together with narrow and deep Q waves in the limb and left precordial leads. Female carriers may also have the abnormal electrocardiogram. ²⁰² These findings correspond to pathological observations. There is fatty and fibrous tissue replacement of the myocardium, with selective scarring of the posterolateral wall of the left ventricle and, sometimes, involvement of the posterolateral papillary muscle. Conduction abnormalities are also frequently seen. Among these are prolonged intra-atrial conduction, right bundle branch block, a superior QRS axis, and a short PR interval. Histological studies of the conduction system show multifocal areas of fibrosis, vacuolisation and fatty infiltration. ²⁰³ The echocardiogram reveals impairment of both systolic and diastolic function. The thickness of the left ventricular wall is decreased, and this is not related to physical inactivity. The end-diastolic and end-systolic dimensions of the left ventricle increase as systolic function deteriorates.

The diagnosis is made from the clinical characteristics, the high levels of activity of creatine kinase, and biopsy of the skeletal muscles. Creatine kinase activity is from 100 to 300 times the normal when the patients are aged from 1 to 5 years. Other muscle enzymes, like aldolase, glutamic oxalic transaminase, lactic dehydrogenase, and pyruvate kinase are also grossly elevated. The levels of creatine kinase diminish later in the disease, but still remain well above normal limits. Muscle biopsy shows scattered hyaline fibres with active muscular necrosis and regeneration. There is splitting of the muscle fibres, with fatty replacement. The nucleuses are of varied size. The muscle fascicles also become surrounded by perimysial and endomysial connective tissue. Electromyography reveals a decrease in the mean action potential voltage and its duration. An increase in the number of polyphasic potentials is also seen.

Careful general medical management is critical. Since bedrest is harmful, regular physical activity and exercise are to be encouraged. Avoidance of obesity is an important general measure, along with prevention of muscular contractures by passive stretching. Because of the risks of anaesthesia and immobilisation, the benefit from major orthopaedic procedures must be carefully considered. Prevention of scoliosis and thoracic deformities in the wheelchair phase help to avoid respiratory impairment and slow the deterioration of respiratory function. Death is usually from respiratory infections and insufficiency, and cardiac failure or arrhythmias. Detection of carriers is important for appropriate genetic counselling. More than half the carriers can be identified by their elevated levels of creatine kinase, by electromyography and by muscle biopsy. The analysis of the pedigree is particularly useful. Novel treatments for this myopathy are actively being investigated. They include gene therapy, ²⁰⁴ use of inhibitors of proteases, ²⁰⁵ membrane stabilisers, ²⁰⁶ and transplantation of the muscle precursor cells. ²⁰⁷

Childhood Limb-girdle Muscular Dystrophy

The childhood limb-girdle muscular dystrophies are a heterogeneous group of genetic muscular disorders. At least 17 different types have been described. They can be inherited in either an autosomal dominant or recessive fashion, with 7 genetic defects now identified in the dominant forms, and 11 in the recessive forms. The age at onset is variable, but symptoms generally appear between 5 and 10 years of age. Weakness of the pelvic and shoulder muscles predominates. The disease is slowly progressive, the patients often becoming unable to walk by their twenties. The disease is first suspected when weakness of the limb girdles becomes apparent, although Duchenne’s and Becker’s muscular dystrophy must be ruled out. An elevated level of creatine kinase will not differentiate between this entity and the dystrophinopathies. This can be done through analysis of the dystrophin gene, and by examination of a muscle biopsy. Various forms of the disease affect the heart. Those with the so-called 1B variant, produced by a mutation in the lamin A/C gene, frequently develop arrhythmias which can be lethal and which may require placement of an implantable defibrillator. Atrioventricular block can also occur, necessitating placement of a pacemaker. ²⁰⁸ This disorder can also result in a dilated cardiomyopathy.

Those with the 2I variant, caused by a defect in the gene encoding the fukutin-related protein, may develop a dilated cardiomyopathy by the third decade. Evidence of arrhythmias is not seen. ²⁰⁹ The precise role of the fukutin-related protein is unknown, but it may play a role in the glycosylation of muscle membrane proteins.

Myotonic Muscular Dystrophy (Steinert Disease)

The involvement of systemic tissues, together with the presence of myotonia and muscular atrophy, separates myotonic muscular dystrophy from the other muscular dystrophies. It has a high incidence, calculated at 13.5 per 100,000 live births. Onset is usually between 20 and 50 years of age, but many cases are clinically apparent during childhood. It is due to an expansion of a CTG trinucleotide repeat on the q arm of chromosome 19. ²¹⁰ It is transmitted in an autosomal dominant fashion and demonstrates genetic anticipation. Myotonia is the presenting clinical feature in one-third of cases. Others present with weakness of the hands, foot drop, or a tendency to fall. The heart may occasionally become involved prior to diagnosis of the neuromuscular disorder. The facial, masticatory, sternomastoid, forearm, anterior tibial and peroneal muscles are those first affected by weakness. Later it extends to neighbouring muscle groups. The typical facies are characterised by lack of facial expression, and difficulty in closing the eyes and moving the mouth. Ptosis and dysarthria are frequent. Myotonia is often limited to the tongue, forearms and hands, but it may be generalised. The tendon reflexes in the affected muscle groups are reduced.

Cataracts are present in almost all those affected. Impaired pulmonary vital capacity and maximum breathing capacity are common. Abnormal contractions of the oesophagus are thought to be the cause of dysphagia and pulmonary aspiration. Testicular atrophy, diabetes mellitus, increased metabolism of immunoglobulin G with low levels in the serum, progressive dementia, and subnormal intelligence are frequent associations. Cardiac involvement is common and manifests with conduction defects and arrhythmias. First-degree atrioventricular block is commonly seen, and this may progress to complete heart block requiring implantation of a pacemaker. ²¹¹ No relationship exists between the degree of involvement of the cardiac and the skeletal muscles. Chest radiography will show the associated deformities of the bony thorax, together with elevated hemidiaphragms. The cardiac silhouette is normal. Death from cardiac involvement is almost always caused by complete atrioventricular block or ventricular tachycardia. It is very rarely caused by myocardial failure.

The most common abnormalities in the electrocardiogram are low amplitudes of the P wave, atrioventricular block of any degree, right and left bundle branch block, abnormal Q waves, and changes in the ST segment and T wave. It is believed that regional myocardial dystrophy is responsible for the abnormal Q waves. ²¹² Rhythm disturbances include sinus brachycardia, premature atrial beats, atrial fibrillation, atrial flutter, ventricular premature beats and ventricular tachycardia. Four-fifths of the patients have electrophysiological evidence of disease of the atrioventricular conduction axis. A further one-fifth have evidence of intra-atrial conduction disturbances. ²¹³ Disease of the atrioventricular conduction axis progresses with time. A correlative study revealed fibrosis of the right and left bundle branches and fatty infiltration and degeneration around the atrioventricular node, which corresponded accurately with the electrocardiographic and electrophysiological evaluation performed during life. ¹⁸⁶

Mitral valvar prolapse is frequently associated with myotonic muscular dystrophy and is diagnosed echocardiographically. It is present in approximately one-third of patients. There is no relationship, however, between mitral valvar prolapse and the arrhythmias. Systolic and diastolic function are normal. Normal ejection fractions at rest are recorded with radionuclide angiography. Some patients fail to show an increase with exercise. Apical hypokinesia may be present but is of doubtful significance. Careful clinical examination and a high degree of suspicion are required for an early diagnosis. Electromyography and muscle biopsy are useful techniques, as is examination for cataracts using a slit lamp. Cardiological evaluation is required in all patients because of the frequent association of cardiac disease. The disease shows progressive deterioration, with physical incapacity usually occurring 15 to 20 years after the onset of muscular symptoms. Death is usually from respiratory infections, aspiration, cardiac arrhythmias, or anaesthetic complications. There is no specific treatment for the condition. Active exercise and control of weight are important general therapeutic measures. Systemic complications are treated as they arise. Myotonia is relieved by the use of procainamide or phenytoin. Caution must be exerted, however, since procainamide exacerbates pre-existing disturbances of conduction. Electrophysiological studies are warranted in symptomatic patients presenting with syncope or presyncope. A ventricular pacemaker is needed when there are significant abnormalities in the formation or conduction of the cardiac impulse. Myotonic muscular dystrophy appears and progresses during early adult life in the majority of those affected. In a proportion, however, the disease is present at birth. Such congenital cases are often treated as a separate entity. Indeed, as will be seen, they have a totally different presentation and clinical picture. In the fullness of time, they come to resemble the adult form.

The congenital form is characterised by bilateral facial weakness, hypotonia, and mental retardation with delayed motor and speech development. Neonatal respiratory distress is very frequent. Such infants have a high incidence of feeding difficulties owing to muscle weakness. Talipes are a common association. Clinical myotonia is absent but can be demonstrated electromyographically. The adult features of the disease appear during late childhood and adolescence. Cardiac involvement takes the form of a dilated cardiomyopathy. Non-specific electrocardiographic abnormalities appear with progression of the disease. Mortality occurs in the neonatal period as a result of respiratory distress. Beyond this time, there is a tendency to improve, only for the patients to deteriorate as the adult characteristics of the disease appear. The condition is transmitted by the mother. Her clinical involvement has often failed previously to be noted.

Autosomal Dominant Scapuloperoneal Myopathy

Scapuloperoneal myopathy is a very rare form of muscular dystrophy. It is possible to recognise two distinct groups according to the age of onset. They share an autosomal dominant form of inheritance, and involve the same muscle groups. Weakness and atrophy affect the neck, shoulder girdle, and upper arm muscles, together with the tibial and peroneal muscles in the legs. Foot drop and an awkward gait are frequent early symptoms. Deep tendon reflexes are commonly absent. Levels of creatine kinase are slightly elevated in the serum. Electromyography and muscle biopsy show the changes common to muscular dystrophies.

The group of patients with early onset generally present under the age of 10 years. In these, the disease takes a rapid course. Patients develop early contractures and are severely incapacitated by their late teens. They frequently have clinical and electrocardiographic signs of a dilated cardiomyopathy with congestive cardiac failure. ²¹⁴ Those patients having a late onset present over the age of 40 years, and their clinical course is slow. They seldom develop contractures. Cardiac involvement, usually late, could well be a result of ischaemic heart disease. ²¹⁵

Becker’s Muscular Dystrophy

Becker’s muscular dystrophy is one of the most frequent types of muscular dystrophy. It is inherited in X-linked recessive fashion. The incidence is of the order of 3 to 6 per 100,000 male births. The muscular groups involved are very similar to those in Duchenne’s muscular dystrophy. The peroneal and anterior tibial muscles are also affected in the Becker variant. The facial muscles are not involved. Calf hypertrophy and muscle cramps are frequent early symptoms. Club feet are often seen. Contractures appear in the final stages, and scoliosis is rare. Developmental delay is uncommon. The onset of the symptoms is between 5 and 15 years of age, with inability to walk being present by the third decade, and death occurring in the fifth. The individual range, however, is very wide. The diagnosis is primarily clinical. Activity of creatine kinase in the serum is 25 to 200 times the normal. The electromyogram and the muscle biopsy are nonspecific but help to rule out other conditions.

Cardiac abnormalities are infrequent in childhood but are almost always present in some form by the onset of the fourth decade. ²¹⁶ Electrocardiographic abnormalities are common and include resting tachycardia, interventricular conduction delay, and Q waves in leads II, III, and aVF, suggesting damage to the lateral wall of the left ventricle. ²¹⁷ Heart rate variability is also decreased and may indicate a risk for sudden death. ²¹⁸ Dilated cardiomyopathy is seen, and the risk of ventricular dysfunction increases with age, though many patients are asymptomatic from a cardiac standpoint, exhibiting abnormalities only on the electrocardiogram or echocardiogram. ²¹⁹ Transplantation of the heart for severe left ventricular systolic dysfunction is a well-established palliative option. ²²⁰

Facioscapulohumeral Muscular Dystrophy (Landouzy-Dejerine Syndrome)

Fascioscapulohumeral muscular dystrophy is inherited in an autosomal dominant fashion. It has an incidence of approximately 5 per 100,000 live births. Facial and shoulder weakness generally develop in the second or third decade and progress very slowly. Patients with severe forms of this disease will occasionally present early in life, and progression is then rapid. Characteristically, there are no facial lines and the eyelids are very weak. Winging of the scapulas is seen when the arms are abducted, and there is a marked thoracolumbar lordosis. Affected muscles include the neck flexors, the serrate and pectoral muscles, biceps and triceps in the upper limbs, the hip flexors, and the anterior tibial muscles. In the later stages, the quadriceps and sartorius in the lower limbs are also affected. Retinal vasculopathy is also seen frequently. The levels of creatine kinase in the serum are normal or else only mildly elevated. The precise molecular mechanism for expression has not been elucidated, but patients are known to have a large deletion involving the q arm of chromosome 4. No gene has been identified within this region, and so various hypotheses have been presented to explain the mechanism whereby this deletion induces clinical disease. ²²¹

Ventricular function is not affected. Supraventricular tachycardia has been reported with a frequency higher than that of the general population. ²²² Sinus nodal dysfunction, abnormal atrioventricular nodal or infranodal conduction, and easily inducible atrial fibrillation or flutter have also been reported in around one-quarter of patients studied. ²²³

Emery-Dreifuss Muscular Dystrophy

Emery-Dreifuss muscular dystrophy typically presents between 5 and 15 years of age. It can be inherited in an X-linked recessive fashion, or in autosomal dominant or autosomal recessive forms. The biceps and triceps are more severely affected than the deltoid muscle. The peroneals are more involved than the proximal musculature of the legs. Contractures generally develop at the elbows, posterior cervical muscles, and Achilles tendon. Pseudohypertrophy is absent. Levels of creatine kinase are from 3 to 10 times above normal. Progression is very slow, and the physical limitations are minimal. There is normal intellectual function.

The X-linked form is due to a defect in the gene encoding emerin, a nuclear envelope protein which plays a role in the regulation of many cellular and nucleolar processes. Its role in the pathogenesis of muscle damage remains to be elucidated. The autosomal dominant form is due to defects in the lamin A/C gene, similar to variant 1B of limb-girdle muscular dystrophy. Again, the role of lamin A/C mutations in the development of the myopathy is not clear. The recessive form is also due to defects in the gene encoding lamins A and C. ²²⁴ How and why defects in the same gene can cause dominant and recessive forms of the disease remains to be discerned.

Cardiac involvement is often manifested by atrial arrhythmias and atrioventricular block. Any degree of atrioventricular block can be present, and a slow junctional escape rhythm is common. Severe sinus bradycardia or sinus arrest is seen and may require implantation of a pacemaker because of the increased risk of sudden death. ²²⁵ Atrial paralysis, with the absence of P waves and an inability to electrically pace the atrium, is seen. Ventricular function is often normal, but progressive left ventricular dysfunction occurs due to fibrous infiltration of the myocardium. ²²⁶ Cardiac transplantation has been employed for end-stage disease. ²²⁷ Those with bradycardia may have hypertrophied and dilated left ventricles, probably as a compensatory physiological response. Electrophysiological studies show prolonged HV intervals and, on some occasions, a complete absence of the His potential. This finding, together with the very slow junctional escape rhythms, suggests that the myopathic process extends into the atrioventricular conduction axis. The high risk of sudden death in this variety of muscular dystrophy makes early recognition important, since insertion of a ventricular pacemaker in patients with bradycardia will improve survival.