Familial isolated primary pigmented nodular adrenocortical disease associated with a novel low penetrance PRKAR1A gene splice site mutation

Helen L Storr; Louise A Metherell; Renuka Dias; Martin O Savage; Åse Krogh Rasmussen; Adrian J L Clark; Katharina M Main

doi:10.1159/000277629

Familial isolated primary pigmented nodular adrenocortical disease associated with a novel low penetrance PRKAR1A gene splice site mutation

Helen L Storr, Louise A Metherell, Renuka Dias, Martin O Savage, Åse Krogh Rasmussen, Adrian J L Clark, Katharina M Main

Department of Growth and Reproduction

8 Citations (Scopus)

Abstract

Primary pigmented nodular adrenocortical disease (PPNAD) is associated with inactivating germline protein kinase A regulatory subunit type 1-alpha (PRKAR1A) mutations and loss of heterozygosity at the 17q22-24 locus in approximately 50% patients. PRKAR1A mutations are observed in both isolated PPNAD (iPPNAD) and Carney complex (CNC). Most mutations result in a functionally null-allele and exhibit high penetrance. We genotyped members of an extended family for a novel PRKAR1A mutation and undertook detailed phenotyping for CNC in the affected individuals.

Original language	English
Journal	Hormone research in paediatrics
Volume	73
Issue number	2
Pages (from-to)	115-9
Number of pages	5
DOIs	https://doi.org/10.1159/000277629
Publication status	Published - 1 Jan 2010

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title = "Familial isolated primary pigmented nodular adrenocortical disease associated with a novel low penetrance PRKAR1A gene splice site mutation",

abstract = "Primary pigmented nodular adrenocortical disease (PPNAD) is associated with inactivating germline protein kinase A regulatory subunit type 1-alpha (PRKAR1A) mutations and loss of heterozygosity at the 17q22-24 locus in approximately 50% patients. PRKAR1A mutations are observed in both isolated PPNAD (iPPNAD) and Carney complex (CNC). Most mutations result in a functionally null-allele and exhibit high penetrance. We genotyped members of an extended family for a novel PRKAR1A mutation and undertook detailed phenotyping for CNC in the affected individuals.",

author = "Storr, {Helen L} and Metherell, {Louise A} and Renuka Dias and Savage, {Martin O} and Rasmussen, {{\AA}se Krogh} and Clark, {Adrian J L} and Main, {Katharina M}",

year = "2010",

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doi = "10.1159/000277629",

language = "English",

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T1 - Familial isolated primary pigmented nodular adrenocortical disease associated with a novel low penetrance PRKAR1A gene splice site mutation

AU - Storr, Helen L

AU - Metherell, Louise A

AU - Dias, Renuka

AU - Savage, Martin O

AU - Rasmussen, Åse Krogh

AU - Clark, Adrian J L

AU - Main, Katharina M

PY - 2010/1/1

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N2 - Primary pigmented nodular adrenocortical disease (PPNAD) is associated with inactivating germline protein kinase A regulatory subunit type 1-alpha (PRKAR1A) mutations and loss of heterozygosity at the 17q22-24 locus in approximately 50% patients. PRKAR1A mutations are observed in both isolated PPNAD (iPPNAD) and Carney complex (CNC). Most mutations result in a functionally null-allele and exhibit high penetrance. We genotyped members of an extended family for a novel PRKAR1A mutation and undertook detailed phenotyping for CNC in the affected individuals.

AB - Primary pigmented nodular adrenocortical disease (PPNAD) is associated with inactivating germline protein kinase A regulatory subunit type 1-alpha (PRKAR1A) mutations and loss of heterozygosity at the 17q22-24 locus in approximately 50% patients. PRKAR1A mutations are observed in both isolated PPNAD (iPPNAD) and Carney complex (CNC). Most mutations result in a functionally null-allele and exhibit high penetrance. We genotyped members of an extended family for a novel PRKAR1A mutation and undertook detailed phenotyping for CNC in the affected individuals.

U2 - 10.1159/000277629

DO - 10.1159/000277629

M3 - Journal article

C2 - 20190548

SN - 1663-2826

VL - 73

SP - 115

EP - 119

JO - Hormone research in paediatrics

JF - Hormone research in paediatrics

IS - 2

ER -

Familial isolated primary pigmented nodular adrenocortical disease associated with a novel low penetrance PRKAR1A gene splice site mutation

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