Characterization of germline TP53 splicing mutations and their genetic and functional analysis

J. M. Varley; C. Attwooll; G. White; G. McGown; M. Thorncroft; A. M. Kelsey; M. Greaves; J. Boyle; J. M. Birch

doi:10.1038/sj.onc.1204369

Characterization of germline TP53 splicing mutations and their genetic and functional analysis

J. M. Varley, C. Attwooll, G. White, G. McGown, M. Thorncroft, A. M. Kelsey, M. Greaves, J. Boyle, J. M. Birch

Cancer Research UK Manchester Institute

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

Abstract

Germline TP53 splicing mutations have been described infrequently (>2%) in the literature, however in a series of 40 patients and families identified by our group in which there are germline TP53 mutations, seven affect splicing (18%). The low figure reported in the literature might reflect the method of mutation detection, which in many studies does not include all splice junctions. These data indicate that a significant proportion of TP53 germline mutations are currently unrecognized. We have carried out detailed studies of the effects of the different mutations on splicing, and see distinct variations in the effects of the same mutation in different patients. Furthermore we have identified the usage of a nonconsensus splice donor site in four families with an intron 4 splice donor mutation.

Original language	English
Pages (from-to)	2647-2654
Number of pages	7
Journal	Oncogene
Volume	20
Issue number	21
DOIs	https://doi.org/10.1038/sj.onc.1204369
Publication status	Published - 10 May 2001

Keywords

Li-Fraumeni
Splicing
TP53

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10.1038/sj.onc.1204369

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title = "Characterization of germline TP53 splicing mutations and their genetic and functional analysis",

abstract = "Germline TP53 splicing mutations have been described infrequently (>2\%) in the literature, however in a series of 40 patients and families identified by our group in which there are germline TP53 mutations, seven affect splicing (18\%). The low figure reported in the literature might reflect the method of mutation detection, which in many studies does not include all splice junctions. These data indicate that a significant proportion of TP53 germline mutations are currently unrecognized. We have carried out detailed studies of the effects of the different mutations on splicing, and see distinct variations in the effects of the same mutation in different patients. Furthermore we have identified the usage of a nonconsensus splice donor site in four families with an intron 4 splice donor mutation.",

keywords = "Li-Fraumeni, Splicing, TP53",

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year = "2001",

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doi = "10.1038/sj.onc.1204369",

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T1 - Characterization of germline TP53 splicing mutations and their genetic and functional analysis

AU - Varley, J. M.

AU - Attwooll, C.

AU - White, G.

AU - McGown, G.

AU - Thorncroft, M.

AU - Kelsey, A. M.

AU - Greaves, M.

AU - Boyle, J.

AU - Birch, J. M.

PY - 2001/5/10

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N2 - Germline TP53 splicing mutations have been described infrequently (>2%) in the literature, however in a series of 40 patients and families identified by our group in which there are germline TP53 mutations, seven affect splicing (18%). The low figure reported in the literature might reflect the method of mutation detection, which in many studies does not include all splice junctions. These data indicate that a significant proportion of TP53 germline mutations are currently unrecognized. We have carried out detailed studies of the effects of the different mutations on splicing, and see distinct variations in the effects of the same mutation in different patients. Furthermore we have identified the usage of a nonconsensus splice donor site in four families with an intron 4 splice donor mutation.

AB - Germline TP53 splicing mutations have been described infrequently (>2%) in the literature, however in a series of 40 patients and families identified by our group in which there are germline TP53 mutations, seven affect splicing (18%). The low figure reported in the literature might reflect the method of mutation detection, which in many studies does not include all splice junctions. These data indicate that a significant proportion of TP53 germline mutations are currently unrecognized. We have carried out detailed studies of the effects of the different mutations on splicing, and see distinct variations in the effects of the same mutation in different patients. Furthermore we have identified the usage of a nonconsensus splice donor site in four families with an intron 4 splice donor mutation.

KW - Li-Fraumeni

KW - Splicing

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U2 - 10.1038/sj.onc.1204369

DO - 10.1038/sj.onc.1204369

M3 - Article

SN - 0950-9232

VL - 20

SP - 2647

EP - 2654

JO - Oncogene

JF - Oncogene

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ER -

Characterization of germline TP53 splicing mutations and their genetic and functional analysis

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Keywords

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