A summary of 20 CACNA1F mutations identified in 36 families with incomplete X-linked congenital stationary night blindness, and characterization of splice variants

Boycott, Kym M.; Maybaum, Tracy A.; Naylor, Margaret Jane; Weleber, Richard G.; Robitaille, Johane; Miyake, Yoichi; Bergen, Arthur A. B.; Pierpont, Mary Ella M; Pearce, W G; Bech-Hansen, N. Torben

doi:10.1007/s004390100461

Cited by 89 publications

(49 citation statements)

References 12 publications

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“…From eight mutations published recently, 9 the mutation 3133insC has been found in Mennonite families which have been emigrated since 1683 from Germany, Netherlands, Poland and Russia to North America. 11,30 No overlap is found between our mutation spectrum and the mutation pattern in five Japanese families carrying the incomplete type of CSNB. 12 In this study, one missense, one nonsense, one splice site mutation, a single nucleotide insertion and a del/ins combination could be detected.…”

Section: Discussionmentioning

confidence: 72%

“…Two stop mutations (R82X and R1288X) have also been identified in other populations 11 and might be caused by the frequent C-to-T transition 29 rather than by a founder mutation. From eight mutations published recently, 9 the mutation 3133insC has been found in Mennonite families which have been emigrated since 1683 from Germany, Netherlands, Poland and Russia to North America.…”

Section: Discussionmentioning

confidence: 96%

“…Its expression is restricted to the retina and initial mutation analyses revealed loss of function as well as missense mutations. 9 So far, mutation spectra have been published only for mixed populations 10,11 or few Japanese families. 12 In order to establish a mutation spectrum for the German population and to further support the strong association of the CACNA1F gene with CSNB2, we completed analysis in 10 families partially characterised previously 9 and included another 24 CSNB2 families to the study.…”

Section: Introductionmentioning

confidence: 99%

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Thirty distinct CACNA1F mutations in 33 families with incomplete type of XLCSNB and Cacna1f expression profiling in mouse retina

Wutz¹,

Sauer

Zrenner³

et al. 2002

Eur J Hum Genet

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X-linked CSNB patients may exhibit myopia, nystagmus, strabismus and ERG abnormalities of the Schubert-Bornschein type. We recently identified the retina-specific L-type calcium channel a1 subunit gene CACNA1F localised to the Xp11.23 region, which is mutated in families showing the incomplete type (CSNB2). Here, we report comprehensive mutation analyses in the 48 CACNA1F exons in 36 families, most of them from Germany. All families were initially diagnosed as having the incomplete type of CSNB, except for two which have been designated as Å land Island eye disease (Å IED)-like. Out of 33 families, a total of 30 different mutations were identified, of which 24 appear to be unique for the German population. The mutations, 20 of which are published here for the first time, were found to be equally distributed over the entire gene sequence. No mutation could be found in a classic Å IED family previously shown to map to the CSNB2 interval. Cacna1f expression in photoreceptor-negative mice strains indicate that the gene is expressed in the outer nuclear, the inner nuclear, and the ganglion cell layer. Such a distribution points to the central role of calcium regulation in the interaction of retinal cells that mediate signal transmission.

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Section: Discussionmentioning

confidence: 72%

Section: Discussionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Thirty distinct CACNA1F mutations in 33 families with incomplete type of XLCSNB and Cacna1f expression profiling in mouse retina

Wutz¹,

Sauer

Zrenner³

et al. 2002

Eur J Hum Genet

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“…The incomplete form, CSNB2, is caused by mutations in the Cacna1f gene, encoding the α 1F subunit of VDCCs (Bech-Hansen et al, 1998;Strom et al, 1998;Boycott et al, 2001;Wutz et al, 2002). In the outer retina, expression of the α 1F subunit has been localized to the OPL where it is concentrated on the presynaptic side in the terminals of the photoreceptors at their "active zones," which are specialized to mediate continuous calcium-dependent neurotransmitter release (Morgans et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

Thenob2mouse, a null mutation inCacna1f: Anatomical and functional abnormalities in the outer retina and their consequences on ganglion cell visual responses

et al. 2006

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Glutamate release from photoreceptor terminals is controlled by voltage-dependent calcium channels (VDCCs). In humans, mutations in the Cacna1f gene, encoding the α 1F subunit of VDCCs, underlie the incomplete form of X-linked congenital stationary night blindness (CSNB2). These mutations impair synaptic transmission from rod and cone photoreceptors to bipolar cells. Here, we report anatomical and functional characterizations of the retina in the nob2 (no b-wave 2) mouse, a naturally occurring mutant caused by a null mutation in Cacna1f. Not surprisingly, the b-waves of both the light-and dark-adapted electroretinogram are abnormal in nob2 mice. The outer plexiform layer (OPL) is disorganized, with extension of ectopic neurites through the outer nuclear layer that originate from rod bipolar and horizontal cells, but not from hyperpolarizing bipolar cells. These ectopic neurites continue to express mGluR6, which is frequently associated with profiles that label with the

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“…The single base deletion in exon 9 detected in family C3532 results in a frameshift at amino acid position 341 resulting in loss of domains and motifs downstream from domain I and predicted loss of function. This mutation was previously identified in one other family (Bech-Hansen et al, 1998, Boycott et al 2001. The third mutation (nonsense) identified in exon 24 (family A1397) was also previously identified in a single family (Strom et al, 1998) and occurs in domain III resulting in protein truncation.…”

Section: Resultsmentioning

confidence: 68%

Mutations in theCACNA1F andNYX genes in British CSNBX families

Zito¹,

Allen

Patel³

et al. 2003

Hum. Mutat.

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Communicated by Jean-Louis MandelX-linked congenital stationary night blindness (CSNBX) is a genetically and phenotypically heterogeneous non-progressive disorder, characterised by impaired night vision but grossly normal retinal appearance. Other more variable features include reduction in visual acuity, myopia, nystagmus and strabismus. Genetic mapping studies by other groups, and our own studies of British patients, identified key recombination events indicating the presence of at least 2 disease genes on Xp11. Two causative genes (CACNA1F and NYX) for CSNBX have now been identified through positional cloning strategies. In this report, we present the results of comprehensive mutation screening in 14 CSNBX families, three with mutations in the CACNA1F gene and 10 with mutations in the NYX gene. In one family we failed to identify the mutation after testing RP2, RPGR, NYX and CACNA1F. NYX gene mutations are a more frequent cause of CSNBX, although there is evidence for founder mutations. Our report of patient population mutation screening for both CSNBX genes, and our exclusion of RP2 and RGPR, indicates that mutations in CACNA1F and NYX are likely to account for all CSNBX.

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A summary of 20 CACNA1F mutations identified in 36 families with incomplete X-linked congenital stationary night blindness, and characterization of splice variants

Cited by 89 publications

References 12 publications

Thirty distinct CACNA1F mutations in 33 families with incomplete type of XLCSNB and Cacna1f expression profiling in mouse retina

Thirty distinct CACNA1F mutations in 33 families with incomplete type of XLCSNB and Cacna1f expression profiling in mouse retina

Thenob2mouse, a null mutation inCacna1f: Anatomical and functional abnormalities in the outer retina and their consequences on ganglion cell visual responses

Mutations in theCACNA1F andNYX genes in British CSNBX families

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