Cardiac disease among Gemcitabine solubility dmso children ranges from unaffected to moderate cardiac hypertrophy and cardiac dysfunction while adult patients usually have no clinically identifiable heart disease. A less frequent complication of late onset Pompe disease is vascular involvement of intracranial blood vessels; glycogen accumulation in vasculare
smooth muscle, results in aneyeurysm and rupture of basilar artery, internal carotid artery and medial cerebral arteries Inhibitors,research,lifescience,medical (1). In a review of 225 published cases of late onset Pompe disease the median age at the onset was 24 years (0-68), at the start of ventilation 34 years, at the start of wheelchair use 16 years, at the death 24.5 years. Patients with a later onset of symptoms have a better prognosis (2). Emerging clinical features Natural history Inhibitors,research,lifescience,medical of infantile Pompe disease reflects the predominant involvement of cardiac and respiratory systems. However glycogen storage is autoptically present also in the brain, brainstem and anterior horns (8). It is expected that enzyme replacement therapy will have a tremendous beneficial impact upon systemic manifestations of Pompe disease, but enzyme does Inhibitors,research,lifescience,medical not cross blood brain barrier and cannot cure central nerve system disease. Therefore neurological manifestations may be uncovered during long-term enzyme replacement therapy. The hearing loss was discovered in patients with infantile Pompe disease treated by enzyme replacement therapy.
It was not reported before because the medical attention was drawn to the cardiopulmonary Inhibitors,research,lifescience,medical complications that lead to death in the first year of life. Hearing deficits are due to conductive apparatus and cochlea involvement and seem not to be present in patients with late onset form (9). Furthermore in some patients with infantile onset form delay myelination was shown by brain MRI (10). Finally some children experienced fever of central origin, causing death despite Inhibitors,research,lifescience,medical having had a good cardiac and muscular response to enzyme replacement therapy (11). Diagnostic tests In the first evaluation
of a patient suspected of having Pompe disease laboratory testing should include serum creatine kinase, AST, ALT, LDH and tetrasaccharides in blood and urine. However, adult patients are reported to have normal creatine kinase (2). Due to variability of glycogen accumulation between different muscles and muscle fiber types within muscle, lack of muscle glycogen storage demonstration does not PAK6 exclude Pompe disease: actually 20% of late onset patients have a normal glycogen muscle content (2). GAA assay on skin fibroblasts or muscle biopsy is the diagnostic gold standard for diagnosis (12). White cells are unreliable tissue for measurement of enzyme activity because of interfering alternate isoenzyme activities: GAA assay in leukocyte can give false negative results in 10% of the patients (13), except for using inhibitors of interfering maltase, like acarbose.