Allelic imbalance at the beta-catenin gene (CTNNB1 at 3p22-21.3) in various human tumor types

F Nollet; A Vandenberg; A Kersemaekers; A Cletonjansen; G Berx; A Vanderveen; C Eichperger; I Wieland; J Degreve; G Liefers; W Xiao; C Buys; C Cornelisse; F Vanroy

Allelic imbalance at the beta-catenin gene (CTNNB1 at 3p22-21.3) in various human tumor types

F Nollet, A Vandenberg, A Kersemaekers, A Cletonjansen, G Berx, A Vanderveen, C Eichperger, I Wieland, J Degreve, G Liefers, W Xiao, C Buys, C Cornelisse, F Vanroy

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

Abstract

beta-catenin is a multifunctional protein: it plays a central role in the cell-cell adhesive junctions, and participates in transduction of the morphogenic Wingless/Wnt-signal. Upon detailed analysis of the human beta-catenin gene, an intragenic polymorphic microsatellite marker could be identified. This marker shows 62% heterozygosity and was used in a study of eleven different tumor types. A high level of beta-catenin allelic imbalance was observed for small cell lung carcinoma, squamous cell lung carcinoma and cervix carcinoma. Other microsatellite markers on 3p24-21 could demonstrate frequent but not invariable codeletion of flanking chromosomal loci. This intragenic polymorphic marker will allow selection of tumor types and tumor samples possibly bearing recessive mutations in the remaining allele of the beta-catenin gene.

Original language	English
Pages (from-to)	311-8
Number of pages	8
Journal	International journal of oncology
Volume	11
Issue number	2
Publication status	Published - Aug 1997
Externally published	Yes

Cite this

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title = "Allelic imbalance at the beta-catenin gene (CTNNB1 at 3p22-21.3) in various human tumor types",

abstract = "beta-catenin is a multifunctional protein: it plays a central role in the cell-cell adhesive junctions, and participates in transduction of the morphogenic Wingless/Wnt-signal. Upon detailed analysis of the human beta-catenin gene, an intragenic polymorphic microsatellite marker could be identified. This marker shows 62% heterozygosity and was used in a study of eleven different tumor types. A high level of beta-catenin allelic imbalance was observed for small cell lung carcinoma, squamous cell lung carcinoma and cervix carcinoma. Other microsatellite markers on 3p24-21 could demonstrate frequent but not invariable codeletion of flanking chromosomal loci. This intragenic polymorphic marker will allow selection of tumor types and tumor samples possibly bearing recessive mutations in the remaining allele of the beta-catenin gene.",

author = "F Nollet and A Vandenberg and A Kersemaekers and A Cletonjansen and G Berx and A Vanderveen and C Eichperger and I Wieland and J Degreve and G Liefers and W Xiao and C Buys and C Cornelisse and F Vanroy",

year = "1997",

month = aug,

language = "English",

volume = "11",

pages = "311--8",

journal = "International journal of oncology",

issn = "1019-6439",

publisher = "Spandidos Publications",

number = "2",

}

TY - JOUR

T1 - Allelic imbalance at the beta-catenin gene (CTNNB1 at 3p22-21.3) in various human tumor types

AU - Nollet, F

AU - Vandenberg, A

AU - Kersemaekers, A

AU - Cletonjansen, A

AU - Berx, G

AU - Vanderveen, A

AU - Eichperger, C

AU - Wieland, I

AU - Degreve, J

AU - Liefers, G

AU - Xiao, W

AU - Buys, C

AU - Cornelisse, C

AU - Vanroy, F

PY - 1997/8

Y1 - 1997/8

N2 - beta-catenin is a multifunctional protein: it plays a central role in the cell-cell adhesive junctions, and participates in transduction of the morphogenic Wingless/Wnt-signal. Upon detailed analysis of the human beta-catenin gene, an intragenic polymorphic microsatellite marker could be identified. This marker shows 62% heterozygosity and was used in a study of eleven different tumor types. A high level of beta-catenin allelic imbalance was observed for small cell lung carcinoma, squamous cell lung carcinoma and cervix carcinoma. Other microsatellite markers on 3p24-21 could demonstrate frequent but not invariable codeletion of flanking chromosomal loci. This intragenic polymorphic marker will allow selection of tumor types and tumor samples possibly bearing recessive mutations in the remaining allele of the beta-catenin gene.

AB - beta-catenin is a multifunctional protein: it plays a central role in the cell-cell adhesive junctions, and participates in transduction of the morphogenic Wingless/Wnt-signal. Upon detailed analysis of the human beta-catenin gene, an intragenic polymorphic microsatellite marker could be identified. This marker shows 62% heterozygosity and was used in a study of eleven different tumor types. A high level of beta-catenin allelic imbalance was observed for small cell lung carcinoma, squamous cell lung carcinoma and cervix carcinoma. Other microsatellite markers on 3p24-21 could demonstrate frequent but not invariable codeletion of flanking chromosomal loci. This intragenic polymorphic marker will allow selection of tumor types and tumor samples possibly bearing recessive mutations in the remaining allele of the beta-catenin gene.

M3 - Article

C2 - 21528216

SN - 1019-6439

VL - 11

SP - 311

EP - 318

JO - International journal of oncology

JF - International journal of oncology

IS - 2

ER -