Turkish variant late infantile neuronal ceroid lipofuscinosis (CLN7) may be allelic to CLN8

One variant form of late infantile neuronal ceroid lipofuscinosis (LINCL) is found predominantly within the Turkishpopulation ( CLN7). Exclusion mapping showed that CLN7 was not an allelic variant of known NCL loci ( CLN1, CLN2, CLN3, CLN5 or CLN6). Using the method of homozygosity mapping, a genome...

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Published inEuropean journal of paediatric neurology Vol. 5; pp. 21 - 27
Main Authors Mitchell, Wayne A., Wheeler, Ruth B., Sharp, Julie D., Bate, S. Louise, Gardiner, R. Mark, Ranta, U. Susanna, Lonka, Liina, Williams, Ruth E., Lehesjoki, Anna-Elina, Mole, Sara E.
Format Journal Article
LanguageEnglish
Published England Elsevier Ltd 2001
Subjects
Alleles
Child
Child, Preschool
Chromosome Mapping
CLN7
CLN8
DNA Mutational Analysis
DNA Primers
Family Health
Genetic Linkage
Haplotypes
Homozygosity mapping
Homozygote
Humans
Infant
Microsatellite Repeats
NCL
Neuronal Ceroid-Lipofuscinoses - genetics
Turkey
Turkish variant
Turkey
Homozygosity mapping
CLN8
CLN7
Turkish variant
NCL
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Summary:One variant form of late infantile neuronal ceroid lipofuscinosis (LINCL) is found predominantly within the Turkishpopulation ( CLN7). Exclusion mapping showed that CLN7 was not an allelic variant of known NCL loci ( CLN1, CLN2, CLN3, CLN5 or CLN6). Using the method of homozygosity mapping, a genome-wide search was undertaken and a total of 358 microsatellite markers were typed at an average distance of about 10cM. A region of shared homozygosity was identified on chromosome 8p23. This telomeric region contained the recently identified CLN8 gene. A missense mutation in CLN8 causes progressive epilepsy with mental retardation (EPMR) or Northern epilepsy, which has so far been reported only from Finland and is now classified as an NCL. The mouse model mnd has been shown to carry a 1 by insertion in the orthologous CIn8 gene. Statistically significant evidence for linkage was obtained in this region, with LOD scores > 3, assuming either homogeneity or heterogeneity. Flanking recombinants defined a critical region of 14 cM between D8S504 and D8S1458 which encompasses CLN8. This suggests that Turkish variant LINCL, despite having an earlier onset and more severe phenotype, may be an allelic variant of Northern epilepsy. However mutation analysis has not so far identified a disease causing mutation within the coding or non-coding exons of CLN8 in the families. The Turkish variant LINCL disease-causing mutation remains to be delineated.
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ISSN:1090-3798
1532-2130
DOI:10.1053/ejpn.2000.0429