Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24

H. A. Phillips; I. E. Scheffer; K. M. Crossland; K. P. Bhatia; D. R. Fish; C. D. Marsden; S. J L Howell; J. B P Stephenson; J. Tolmie; G. Plazzi; O. Eeg-Olofsson; R. Singh; I. Lopes-Cendes; E. Andermann; F. Andermann; S. F. Berkovic; J. C. Mulley

doi:10.1086/302047

Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24

H. A. Phillips, I. E. Scheffer, K. M. Crossland, K. P. Bhatia, D. R. Fish, C. D. Marsden, S. J L Howell, J. B P Stephenson, J. Tolmie, G. Plazzi, O. Eeg-Olofsson, R. Singh, I. Lopes-Cendes, E. Andermann, F. Andermann, S. F. Berkovic, J. C. Mulley

Istituto Scienze Neurologiche

Research output: Contribution to journal › Article › peer-review

Abstract

Autosomal dominant nocturnal frontal-lobe epilepsy (ADNFLE) is a recently identified partial epilepsy in which two different mutations have been described in the α4 subunit of the neuronal nicotinic acetylcholine receptor (CHRNA4). An additional seven families are presented in which ADNFLE is unlinked to the CHRNA4 region on chromosome 20q13.2. Seven additional sporadic cases showed no evidence of defective CHRNA4. One of the families showed evidence of linkage to 15q24, close to the CHRNA3/CHRNA5/CHRNB4 cluster (maximum LOD score of 3.01 with D15S152). Recombination between ADNFLE and CHRNA4, linkage to 15q24 in one family, and exclusion from 15q24 and 20q13.2 in others demonstrate genetic heterogeneity with at least three different genes for ADNFLE. The CHRNA4 gene and the two known CHRNA4 mutations are responsible for only a minority of ADNFLE. Although the ADNFLE phenotype is clinically homogeneous, there appear to be a variety of molecular defects responsible for this disorder, which will provide a challenge to the understanding of the basic mechanism of epileptogenesis.

Original language	English
Pages (from-to)	1108-1116
Number of pages	9
Journal	American Journal of Human Genetics
Volume	63
Issue number	4
DOIs	https://doi.org/10.1086/302047
Publication status	Published - 1998

ASJC Scopus subject areas

Genetics

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Phillips, H. A., Scheffer, I. E., Crossland, K. M., Bhatia, K. P., Fish, D. R., Marsden, C. D., Howell, S. J. L., Stephenson, J. B. P., Tolmie, J., Plazzi, G., Eeg-Olofsson, O., Singh, R., Lopes-Cendes, I., Andermann, E., Andermann, F., Berkovic, S. F., & Mulley, J. C. (1998). Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24. American Journal of Human Genetics, 63(4), 1108-1116. https://doi.org/10.1086/302047

Phillips, HA, Scheffer, IE, Crossland, KM, Bhatia, KP, Fish, DR, Marsden, CD, Howell, SJL, Stephenson, JBP, Tolmie, J, Plazzi, G, Eeg-Olofsson, O, Singh, R, Lopes-Cendes, I, Andermann, E, Andermann, F, Berkovic, SF & Mulley, JC 1998, 'Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24', American Journal of Human Genetics, vol. 63, no. 4, pp. 1108-1116. https://doi.org/10.1086/302047

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title = "Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24",

abstract = "Autosomal dominant nocturnal frontal-lobe epilepsy (ADNFLE) is a recently identified partial epilepsy in which two different mutations have been described in the α4 subunit of the neuronal nicotinic acetylcholine receptor (CHRNA4). An additional seven families are presented in which ADNFLE is unlinked to the CHRNA4 region on chromosome 20q13.2. Seven additional sporadic cases showed no evidence of defective CHRNA4. One of the families showed evidence of linkage to 15q24, close to the CHRNA3/CHRNA5/CHRNB4 cluster (maximum LOD score of 3.01 with D15S152). Recombination between ADNFLE and CHRNA4, linkage to 15q24 in one family, and exclusion from 15q24 and 20q13.2 in others demonstrate genetic heterogeneity with at least three different genes for ADNFLE. The CHRNA4 gene and the two known CHRNA4 mutations are responsible for only a minority of ADNFLE. Although the ADNFLE phenotype is clinically homogeneous, there appear to be a variety of molecular defects responsible for this disorder, which will provide a challenge to the understanding of the basic mechanism of epileptogenesis.",

author = "Phillips, {H. A.} and Scheffer, {I. E.} and Crossland, {K. M.} and Bhatia, {K. P.} and Fish, {D. R.} and Marsden, {C. D.} and Howell, {S. J L} and Stephenson, {J. B P} and J. Tolmie and G. Plazzi and O. Eeg-Olofsson and R. Singh and I. Lopes-Cendes and E. Andermann and F. Andermann and Berkovic, {S. F.} and Mulley, {J. C.}",

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AU - Phillips, H. A.

AU - Scheffer, I. E.

AU - Crossland, K. M.

AU - Bhatia, K. P.

AU - Fish, D. R.

AU - Marsden, C. D.

AU - Howell, S. J L

AU - Stephenson, J. B P

AU - Tolmie, J.

AU - Plazzi, G.

AU - Eeg-Olofsson, O.

AU - Singh, R.

AU - Lopes-Cendes, I.

AU - Andermann, E.

AU - Andermann, F.

AU - Berkovic, S. F.

AU - Mulley, J. C.

PY - 1998

Y1 - 1998

N2 - Autosomal dominant nocturnal frontal-lobe epilepsy (ADNFLE) is a recently identified partial epilepsy in which two different mutations have been described in the α4 subunit of the neuronal nicotinic acetylcholine receptor (CHRNA4). An additional seven families are presented in which ADNFLE is unlinked to the CHRNA4 region on chromosome 20q13.2. Seven additional sporadic cases showed no evidence of defective CHRNA4. One of the families showed evidence of linkage to 15q24, close to the CHRNA3/CHRNA5/CHRNB4 cluster (maximum LOD score of 3.01 with D15S152). Recombination between ADNFLE and CHRNA4, linkage to 15q24 in one family, and exclusion from 15q24 and 20q13.2 in others demonstrate genetic heterogeneity with at least three different genes for ADNFLE. The CHRNA4 gene and the two known CHRNA4 mutations are responsible for only a minority of ADNFLE. Although the ADNFLE phenotype is clinically homogeneous, there appear to be a variety of molecular defects responsible for this disorder, which will provide a challenge to the understanding of the basic mechanism of epileptogenesis.

AB - Autosomal dominant nocturnal frontal-lobe epilepsy (ADNFLE) is a recently identified partial epilepsy in which two different mutations have been described in the α4 subunit of the neuronal nicotinic acetylcholine receptor (CHRNA4). An additional seven families are presented in which ADNFLE is unlinked to the CHRNA4 region on chromosome 20q13.2. Seven additional sporadic cases showed no evidence of defective CHRNA4. One of the families showed evidence of linkage to 15q24, close to the CHRNA3/CHRNA5/CHRNB4 cluster (maximum LOD score of 3.01 with D15S152). Recombination between ADNFLE and CHRNA4, linkage to 15q24 in one family, and exclusion from 15q24 and 20q13.2 in others demonstrate genetic heterogeneity with at least three different genes for ADNFLE. The CHRNA4 gene and the two known CHRNA4 mutations are responsible for only a minority of ADNFLE. Although the ADNFLE phenotype is clinically homogeneous, there appear to be a variety of molecular defects responsible for this disorder, which will provide a challenge to the understanding of the basic mechanism of epileptogenesis.

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Autosomal dominant nocturnal frontal-lobe epilepsy: Genetic heterogeneity and evidence for a second locus at 15q24

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