Acid alpha-glucosidase

Acid Alpha-Glucosidase

Acid alpha-glucosidase, also known as acid maltase, is an enzyme that plays a crucial role in the breakdown of glycogen into glucose within the lysosomes. This enzyme is encoded by the GAA gene located on chromosome 17 in humans. Deficiency in acid alpha-glucosidase activity leads to the accumulation of glycogen in the lysosomes, resulting in a condition known as Glycogen storage disease type II, or Pompe disease.

Function[edit | edit source]

Acid alpha-glucosidase is responsible for catalyzing the hydrolysis of alpha-1,4 and alpha-1,6 glycosidic linkages in glycogen, maltose, and isomaltose. This enzymatic activity is essential for the proper degradation of glycogen into glucose, which is then utilized by the body for energy production. The enzyme functions optimally at an acidic pH, which is characteristic of the lysosomal environment.

Genetic Basis[edit | edit source]

The GAA gene provides instructions for synthesizing acid alpha-glucosidase. Mutations in the GAA gene can lead to reduced or absent enzyme activity, causing the accumulation of glycogen in the lysosomes. Over 300 mutations in the GAA gene have been identified, which can result in varying degrees of enzyme deficiency and clinical severity of Pompe disease.

Clinical Significance[edit | edit source]

Deficiency of acid alpha-glucosidase results in Pompe disease, a rare autosomal recessive disorder. The disease manifests in various forms, ranging from the severe infantile-onset form to the milder late-onset form. Symptoms of Pompe disease include muscle weakness, respiratory difficulties, and cardiomyopathy. Early diagnosis and treatment are crucial for managing the disease and improving patient outcomes.

Diagnosis and Treatment[edit | edit source]

Diagnosis of Pompe disease involves measuring the activity of acid alpha-glucosidase in blood, skin fibroblasts, or muscle tissue. Genetic testing can confirm the diagnosis by identifying mutations in the GAA gene. Treatment options include enzyme replacement therapy (ERT) with recombinant human acid alpha-glucosidase, which can help reduce glycogen accumulation and alleviate symptoms.

Research and Future Directions[edit | edit source]

Ongoing research aims to improve the understanding of acid alpha-glucosidase function and the pathophysiology of Pompe disease. Advances in gene therapy and novel therapeutic approaches hold promise for more effective treatments in the future.

Also see[edit | edit source]

• Glycogen storage disease
• Lysosomal storage disease
• Enzyme replacement therapy
• Genetic testing

Template:Glycogen storage diseases Template:Lysosomal storage disorders