Mutational Analysis of the Defective Protease in Classic Late-Infantile Neuronal Ceroid Lipofuscinosis, a Neurodegenerative Lysosomal Storage Disorder

The late-infantile form of neuronal ceroid lipofuscinosis (LINCL) is a progressive and ultimately fatal neurodegenerative disease of childhood. The defective gene in this hereditary disorder, CLN2, encodes a recently identified lysosomal pepstatin-insensitive acid protease. To better understand the...

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Bibliographic Details
Published in:American journal of human genetics 1999-06, Vol.64 (6), p.1511-1523
Main Authors: Sleat, David E., Gin, Rosalie M., Sohar, Istvan, Wisniewski, Krystyna, Sklower-Brooks, Susan, Pullarkat, Raju K., Palmer, David N., Lerner, Terry J., Boustany, Rose-Mary, Uldall, Peter, Siakotos, Aristotle N., Donnelly, Robert J., Lobel, Peter
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Aminopeptidases
Biological and medical sciences
Biomarkers
CLN2 protease
Dipeptidyl-Peptidases and Tripeptidyl-Peptidases
Endopeptidases
Errors of metabolism
Genotype
Humans
Infant
Late-infantile neuronal ceroid lipofuscinosis
Lipids (lysosomal enzyme disorders, storage diseases)
Medical sciences
Metabolic diseases
Molecular Sequence Data
Mutation
Mutations
Neuronal Ceroid-Lipofuscinoses - enzymology
Neuronal Ceroid-Lipofuscinoses - genetics
Peptide Hydrolases - genetics
Polymorphism, Genetic
Sequence Homology, Amino Acid
Serine Proteases
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Summary:The late-infantile form of neuronal ceroid lipofuscinosis (LINCL) is a progressive and ultimately fatal neurodegenerative disease of childhood. The defective gene in this hereditary disorder, CLN2, encodes a recently identified lysosomal pepstatin-insensitive acid protease. To better understand the molecular pathology of LINCL, we conducted a genetic survey of CLN2 in 74 LINCL families. In 14 patients, CLN2 protease activities were normal and no mutations were identified, suggesting other forms of NCL. Both pathogenic alleles were identified in 57 of the other 60 LINCL families studied. In total, 24 mutations were associated with LINCL, comprising six splice-junction mutations, 11 missense mutations, 3 nonsense mutations, 3 small deletions, and 1 single-nucleotide insertion. Two mutations were particularly common: an intronic G→C transversion in the invariant AG of a 3′ splice junction, found in 38 of 115 alleles, and a C→T transition in 32 of 115 alleles, which prematurely terminates translation at amino acid 208 of 563. An Arg→His substitution was identified, which was associated with a late age at onset and protracted clinical phenotype, in a number of other patients originally diagnosed with juvenile NCL.
ISSN:0002-9297
1537-6605
DOI:10.1086/302427