Description:
CEROID LIPOFUSCINOSIS, NEURONAL 3, JUVENILE; CLN3
CLN3 GENE; CLN3
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Repository
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NIGMS Human Genetic Cell Repository
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| Subcollection |
Heritable Diseases
Lysosomal Storage Diseases |
| Class |
Disorders of the Nervous System |
| Quantity |
25 µg |
| Quantitation Method |
Please see our FAQ |
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Biopsy Source
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Peripheral vein
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Cell Type
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B-Lymphocyte
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Tissue Type
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Blood
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Transformant
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Epstein-Barr Virus
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Sample Source
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DNA from LCL
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Relation to Proband
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proband
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Confirmation
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Molecular characterization before cell line submission to CCR
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Species
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Homo sapiens
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Common Name
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Human
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Remarks
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| IDENTIFICATION OF SPECIES OF ORIGIN |
Species of Origin confirmed by LINE assay |
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| Gene |
CLN3 |
| Chromosomal Location |
16p12.1 |
| Allelic Variant 1 |
204200.0001; BATTEN DISEASE |
| Identified Mutation |
1-KB DEL, NT598; The International Batten Disease Consortium (1995) demonstrated that the mutation responsible for 73% of Batten disease chromosomes as identified by the 56 haplotype is a genomic deletion of 1.02 kb, including 217 bp of the open reading frame (nucleotides 598-814), corresponding to 2 exons. Deletion of these 217 bp of coding sequence produces a frameshift, generating a TAA termination codon 84 bp downstream of the deletion junction. The predicted translation product is a truncated protein of 181 amino acids consisting of the first 153 residues of the protein, followed by 28 novel amino acids before the stop codon.
Even more of the patients in Finland carry the 1.02-kb deletion, namely 90%. Jarvela et al. (1996) developed a rapid diagnostic solid-phase minisequencing test to detect this deletion. |
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| Gene |
CLN3 |
| Chromosomal Location |
16p12.1 |
| Allelic Variant 2 |
204200.0005; BATTEN DISEASE, PROTRACTED |
| Identified Mutation |
GLU295LYS; Wisniewski et al. (1998) described compound heterozygosity for CLN3 mutations in 2 sibs with the rare, protracted form of juvenile neuronal ceroid lipofuscinosis (JNCL), or Batten disease. Both carried the 1.02-kb CLN3 deletion (204200.0001) on 1 CLN3 allele and had a G-to-A missense mutation at nucleotide 1020 on the other allele, which predicted a glu295-to-lys amino acid substitution. The sister died at age 51 of aspiration pneumonia; the brother was living at age 39. The sister had progressive visual loss, beginning at 5 years of age, and became totally blind at age 13. From 45 years of age, she had progressive impairment of coordination, memory loss, problems with naming and calculation, and episodes of confusion. A general examination at age 48 was normal. Neurologic examination showed disorientation for time and space, impairment of short- and long-term memory, dysarthria, oromandibular dystonia, and naming deficit. A pendular nystagmus was present. The optic fundi showed optic nerve atrophy, pigmentary retinal degeneration, and spicules. The brother began to lose vision at age 5 years, leading to blindness at the age of 12. The main finding on examination was blindness secondary to optic atrophy and pigmentary retinal degeneration.
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| Remarks |
Clinically affected; vision loss at age 5 years; seizures at age 11 years; movement and intelligence declined at age 12 years; EM showed fingerprint profile; donor subject is a compound heterozygote: one allele has a 1.02 kb deletion including 217 bp of the open reading frame (nucleotides 598-814), corresponding to 2 exons resulting in a frameshift that generates a termination codon 84 bp downstream of the deletion junction [1-KB DEL, NT598] and a second allele has a G>A transition at nucleotide 1020 in exon 11 of the CLN3 gene [1020G>A] resulting in a substitution of lysine for glutamic acid at codon 295 [Glu295Lys (E295K)]. |
| Zhong N, Wisniewski KE, Kaczmarski AL, Ju W, Xu WM, Xu WW, Mclendon L, Liu B, Kaczmarski W, Sklower Brooks SS, Brown WT, Molecular screening of Batten disease: identification of a missense mutation (E295K) in the CLN3 gene. Hum Genet102(1):57-62 1998 |
| PubMed ID: 9490299 |
| Gene Cards |
CLN3 |
| Gene Ontology |
GO:0005739 mitochondrion |
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GO:0005764 lysosome |
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GO:0006457 protein folding |
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GO:0016020 membrane |
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GO:0016021 integral to membrane |
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GO:0051082 unfolded protein binding |
| NCBI Gene |
Gene ID:1201 |
| NCBI GTR |
204200 CEROID LIPOFUSCINOSIS, NEURONAL, 3; CLN3 |
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607042 CLN3 LYSOSOMAL/ENDOSOMAL TRANSMEMBRANE PROTEIN, BATTENIN; CLN3 |
| OMIM |
204200 CEROID LIPOFUSCINOSIS, NEURONAL, 3; CLN3 |
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607042 CLN3 LYSOSOMAL/ENDOSOMAL TRANSMEMBRANE PROTEIN, BATTENIN; CLN3 |
| Omim Description |
AMAUROTIC FAMILY IDIOCY, JUVENILE TYPE |
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BATTEN DISEASE; BTS |
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CEROID LIPOFUSCINOSIS, NEURONAL 3, JUVENILE; CLN3 |
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NEURONAL CEROID LIPOFUSCINOSIS, JUVENILE TYPE; JNCL |
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VOGT-SPIELMEYER DISEASE |
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