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Publication : Calcium channel beta 4 (CACNB4): human ortholog of the mouse epilepsy gene lethargic.

First Author  Escayg A Year  1998
Journal  Genomics Volume  50
Issue  1 Pages  14-22
PubMed ID  9628818 Mgi Jnum  J:48152
Mgi Id  MGI:1266887 Doi  10.1006/geno.1998.5311
Citation  Escayg A, et al. (1998) Calcium channel beta4 (CACNB4): human ortholog of the mouse epilepsy gene lethargic. Genomics 50(1):14-22
abstractText  The mouse neurological mutant lethargic (lh) is characterized by ataxia, focal myoclonus, and absence epilepsy due to a loss-of-function mutation in the beta4 subunit of the voltage-gated calcium channel. To evaluate the role of this channel subunit in human neurological disease, we determined the chromosomal location and intron/exon structure of the human CACNB4 gene. The 1560-bp open reading frame of the CACNB4 cDNA predicts a 58-kDa protein with an amino acid sequence that is 99% identical to the rat protein. The 13 coding exons of CACNB4 span >55 kb of genomic DNA. Human cerebellar RNA contains one major CACNB4 transcript that is 9 kb in length. Expression of CACNB4 was detected in cerebellum, kidney, testis, retina, lymphoblasts, and circulating lympho-cytes. Retinal transcripts were localized by in situ hybridization to ganglion cells and the inner nuclear layer. Analysis of the GeneBridge 4 radiation hybrid mapping panel localized CACNB4 to position 791 cR on human chromosome 2, in a conserved linkage group on human 2q22-q31 and mouse chromosome 2. We localized CACNB4 to the 1.3-Mb YAC clone 952F10 in Whitehead contig WC861, along with the polymorphic markers D2S2236 and D2S2299. The chromosomal linkage of three of the four beta subunit genes to homeobox gene clusters associates the evolutionary origin of the beta gene family with the events that generated the four HOX clusters early in vertebrate evolution. Copyright 1998 Academic Press.
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