VPS13B
vacuolar protein sorting 13 homolog B
Normal Function
Health Conditions Related to Genetic Changes
Cohen syndrome
More than 150 different mutations in the VPS13B gene have been found in individuals with Cohen syndrome. Individuals with this condition typically have intellectual disability, eye problems, and distinctive facial features. Another common feature of the condition is obesity, particularly around the torso but not the arms and legs (truncal obesity). Most of the mutations that cause Cohen syndrome result in a premature stop signal in the instructions for making the VPS13B protein. Researchers believe that this genetic change leads to the production of an abnormally short, nonfunctional version of the protein. Studies suggest that a loss of this protein's function disrupts the organization of the Golgi apparatus and impairs normal glycosylation. However, it is not known how the absence of functional VPS13B protein or these cellular changes lead to the signs and symptoms of Cohen syndrome. Researchers speculate that problems with neuron development underlie intellectual disability, eye problems and other features of Cohen syndrome. Abnormal fat storage may cause truncal obesity in people with the condition.
In the Finnish population, 75 percent of individuals with Cohen syndrome have a mutation in both copies of the VPS13B gene that deletes two DNA building blocks (base pairs). This mutation is sometimes written as 3348_3349delCT. The deletion causes a premature stop signal in the instructions for making the VPS13B protein.
Two common mutations occur in the Old Order Amish population. The first mutation adds one base pair and is sometimes written as 9258_9259insT. This mutation creates a premature stop signal in the instructions for making the VPS13B protein. The second mutation changes a single protein building block (amino acid) in the VPS13B protein. Specifically, this mutation replaces the amino acid isoleucine with the amino acid threonine at position 2820 (written as Ile2820Thr or I2820T). Outside the Finnish and Amish populations, nearly all mutations in the VPS13B gene occur in only one or a small number of families.
More About This Health ConditionRelated Conditions
Cohen syndrome
Health Conditions Related to Genetic Changes
More than 150 different mutations in the VPS13B gene have been found in individuals with Cohen syndrome. Individuals with this condition typically have intellectual disability, eye problems, and distinctive facial features. Another common feature of the condition is obesity, particularly around the torso but not the arms and legs (truncal obesity). Most of the mutations that cause Cohen syndrome result in a premature stop signal in the instructions for making the VPS13B protein. Researchers believe that this genetic change leads to the production of an abnormally short, nonfunctional version of the protein. Studies suggest that a loss of this protein's function disrupts the organization of the Golgi apparatus and impairs normal glycosylation. However, it is not known how the absence of functional VPS13B protein or these cellular changes lead to the signs and symptoms of Cohen syndrome. Researchers speculate that problems with neuron development underlie intellectual disability, eye problems and other features of Cohen syndrome. Abnormal fat storage may cause truncal obesity in people with the condition.
In the Finnish population, 75 percent of individuals with Cohen syndrome have a mutation in both copies of the VPS13B gene that deletes two DNA building blocks (base pairs). This mutation is sometimes written as 3348_3349delCT. The deletion causes a premature stop signal in the instructions for making the VPS13B protein.
Two common mutations occur in the Old Order Amish population. The first mutation adds one base pair and is sometimes written as 9258_9259insT. This mutation creates a premature stop signal in the instructions for making the VPS13B protein. The second mutation changes a single protein building block (amino acid) in the VPS13B protein. Specifically, this mutation replaces the amino acid isoleucine with the amino acid threonine at position 2820 (written as Ile2820Thr or I2820T). Outside the Finnish and Amish populations, nearly all mutations in the VPS13B gene occur in only one or a small number of families.