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University Medical Center Groningen
Department of Genetics -
L1CAM Mutation Database
Introduction
Database
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Mutations
Protein domains
References
Mutation Details
DNA change
Protein change
Exon/intron
Type
Reported classification
Bateman
SIFT
PolyPhen
Conserved
Protein domain
Remarks
LOVD ID
c.1277C>A
p.Ala426Asp
Exon 11
Missense
Disease-causing
Surface site
Not tolerated
Benign
Moderately
Ig 5
The mutation severely reduces homophilic and heterophilic binding (De Angelis). Neurite outgrowth is comparable to wild type (Cheng).
Patients
Family
# Affected relatives
Clinical features
Remarks
Reference
1
1
Adducted thumbs, Mental retardation
Age: > 1yr
De Angelis et al. (1999), Fransen et al. (1997)
References
Year
Author
Title
Journal
Volume
Pages
Weblink
2004
Cheng and Lemmon
Pathological missense mutations of neural cell adhesion molecule L1 affect neurite outgrowth and branching on an L1 substrate
Mol. Cell. Neurosci.
27
522-530
15555929
1999
De Angelis et al.
Pathological missense mutations of neural cell adhesion molecule L1 affect homophilic and heterophilic binding activities.
EMBO J.
18 No. 17
4744-4453
10469653
2002
De Angelis et al.
Disease-associated mutations in L1 CAM interfere with ligand interactions and cell-surface expression
Hum. Mol. Genet.
11
1-12
11772994
1997
Fransen et al.
L1-associated diseases: clinical geneticists divide, molecular geneticists unite
Hum. Mol. Genet.
6
1625-1632
9300653
2000
Kenwrick et al.
Neural cell recognition molecule L1: relating biological complexity to human disease mutations
Hum. Mol. Genet.
9
879-886
10767310