Further evidence for dominant inheritance at the chromosome 15q11-13 locus in familial angelman syndrome

J Clayton-Smith; T. Webb; S.A. Robb; I. Dijkstra; P. Willems; X.J. Cheng; M.E. Pembrey; S. Malcolm

doi:10.1002/ajmg.1320440236

Further evidence for dominant inheritance at the chromosome 15q11-13 locus in familial angelman syndrome

J Clayton-Smith
, T. Webb
, S.A. Robb
, I. Dijkstra
, P. Willems
, X.J. Cheng
, M.E. Pembrey
, S. Malcolm

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

28 Citations (Scopus)

Abstract

Eleven patients with Angelman syndrome (AS) and their parents from 5 families have been studied with high resolution chromosome analysis and molecular probes from region 15q11-13 in an attempt to elucidate the mode of inheritance in familial AS. No deletions were detected. All families were informative with a combination of different short arm cytogenetic markers. All sets of sibs inherited the same maternal chromosome 15, but in 3 families sibs inherited different paternal 15s. Analysis of 6 polymorphic DNA markers supported the conclusion that AS sibs inherit the same maternal 15, but often different paternal 15s. These data make autosomal recessive inheritance at a 15q11-13 locus very unlikely and support the hypothesis that familial AS is due to maternal transmission of a mutation within 15q11-13.

Original language	English
Pages (from-to)	256-260
Number of pages	5
Journal	American Journal of Medical Genetics
Volume	44
Issue number	2
DOIs	https://doi.org/10.1002/ajmg.1320440236
Publication status	Published - 15-Sept-1992

Keywords

FAMILIAL
ANGELMAN SYNDROME
SIBLINGS
CHROMOSOME-15
IMPRINTING
HAPPY PUPPET SYNDROME
PRADER-WILLI SYNDROME
PARENTAL ORIGIN
RECURRENCE RISK
DELETIONS
POLYMORPHISM
15Q11-13
DISOMY

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title = "Further evidence for dominant inheritance at the chromosome 15q11-13 locus in familial angelman syndrome",

abstract = "Eleven patients with Angelman syndrome (AS) and their parents from 5 families have been studied with high resolution chromosome analysis and molecular probes from region 15q11-13 in an attempt to elucidate the mode of inheritance in familial AS. No deletions were detected. All families were informative with a combination of different short arm cytogenetic markers. All sets of sibs inherited the same maternal chromosome 15, but in 3 families sibs inherited different paternal 15s. Analysis of 6 polymorphic DNA markers supported the conclusion that AS sibs inherit the same maternal 15, but often different paternal 15s. These data make autosomal recessive inheritance at a 15q11-13 locus very unlikely and support the hypothesis that familial AS is due to maternal transmission of a mutation within 15q11-13.",

keywords = "FAMILIAL, ANGELMAN SYNDROME, SIBLINGS, CHROMOSOME-15, IMPRINTING, HAPPY PUPPET SYNDROME, PRADER-WILLI SYNDROME, PARENTAL ORIGIN, RECURRENCE RISK, DELETIONS, POLYMORPHISM, 15Q11-13, DISOMY",

author = "J Clayton-Smith and T. Webb and S.A. Robb and I. Dijkstra and P. Willems and X.J. Cheng and M.E. Pembrey and S. Malcolm",

year = "1992",

month = sep,

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doi = "10.1002/ajmg.1320440236",

language = "English",

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T1 - Further evidence for dominant inheritance at the chromosome 15q11-13 locus in familial angelman syndrome

AU - Clayton-Smith, J

AU - Webb, T.

AU - Robb, S.A.

AU - Dijkstra, I.

AU - Willems, P.

AU - Cheng, X.J.

AU - Pembrey, M.E.

AU - Malcolm, S.

PY - 1992/9/15

Y1 - 1992/9/15

N2 - Eleven patients with Angelman syndrome (AS) and their parents from 5 families have been studied with high resolution chromosome analysis and molecular probes from region 15q11-13 in an attempt to elucidate the mode of inheritance in familial AS. No deletions were detected. All families were informative with a combination of different short arm cytogenetic markers. All sets of sibs inherited the same maternal chromosome 15, but in 3 families sibs inherited different paternal 15s. Analysis of 6 polymorphic DNA markers supported the conclusion that AS sibs inherit the same maternal 15, but often different paternal 15s. These data make autosomal recessive inheritance at a 15q11-13 locus very unlikely and support the hypothesis that familial AS is due to maternal transmission of a mutation within 15q11-13.

AB - Eleven patients with Angelman syndrome (AS) and their parents from 5 families have been studied with high resolution chromosome analysis and molecular probes from region 15q11-13 in an attempt to elucidate the mode of inheritance in familial AS. No deletions were detected. All families were informative with a combination of different short arm cytogenetic markers. All sets of sibs inherited the same maternal chromosome 15, but in 3 families sibs inherited different paternal 15s. Analysis of 6 polymorphic DNA markers supported the conclusion that AS sibs inherit the same maternal 15, but often different paternal 15s. These data make autosomal recessive inheritance at a 15q11-13 locus very unlikely and support the hypothesis that familial AS is due to maternal transmission of a mutation within 15q11-13.

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KW - ANGELMAN SYNDROME

KW - SIBLINGS

KW - CHROMOSOME-15

KW - IMPRINTING

KW - HAPPY PUPPET SYNDROME

KW - PRADER-WILLI SYNDROME

KW - PARENTAL ORIGIN

KW - RECURRENCE RISK

KW - DELETIONS

KW - POLYMORPHISM

KW - 15Q11-13

KW - DISOMY

U2 - 10.1002/ajmg.1320440236

DO - 10.1002/ajmg.1320440236

M3 - Article

SN - 0148-7299

VL - 44

SP - 256

EP - 260

JO - American Journal of Medical Genetics

JF - American Journal of Medical Genetics

IS - 2

ER -

Further evidence for dominant inheritance at the chromosome 15q11-13 locus in familial angelman syndrome

Abstract

Keywords

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