Tay-Sachs Disease and Sandhoff Disease

Deficiency of hexosaminidase A results in accumulation of GM2 in the brain. Inheritance is autosomal recessive; the most common mutations are carried by 1/27 unaffected adults of Eastern European (Ashkenazi) Jewish origin, although other mutations cluster in some French-Canadian and Cajun populations. The disease develops in 25% of the children when both parents are carriers.

Children with Tay-Sachs disease start missing developmental milestones after age 6 months and develop progressive cognitive and motor deterioration resulting in seizures, intellectual disability, paralysis, and death by age 5 years.

A cherry-red macular spot is common.

Cherry-Red Macular Spot

Image

RALPH C. EAGLE, JR./SCIENCE PHOTO LIBRARY

Diagnosis of Tay-Sachs disease is clinical and can be confirmed by DNA analysis and/or enzyme assay. (See also testing for suspected inherited disorders of metabolism.)

In the absence of effective treatment, management is focused on screening adults of childbearing age in high-risk populations to identify carriers (by way of enzyme activity and mutation testing) combined with genetic counseling.

There is a combined hexosaminidase A and B deficiency. Clinical manifestations include progressive cerebral degeneration beginning at 6 months, accompanied by blindness, cherry-red macular spot, and hyperacusis.

Sandhoff disease is almost indistinguishable from Tay-Sachs disease in course, diagnosis, and management, except that there is visceral involvement (hepatomegaly and bone change) and no ethnic association.

The following English-language resource may be useful. Please note that THE MANUAL is not responsible for the content of this resource.

1. Online Mendelian Inheritance in Man (OMIM) database: Complete gene, molecular, and chromosomal location information