A splicing mutation in RB1 in low penetrance retinoblastoma

Elizabeth L. Schubert; Louise C. Strong; Marc F. Hansen

doi:10.1007/s004390050551

A splicing mutation in RB1 in low penetrance retinoblastoma

Elizabeth L. Schubert, Louise C. Strong, Marc F. Hansen

Genetics

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

44 Scopus citations

Abstract

The pediatric eye-tumor retinoblastoma is widely held as a paradigm of human cancer genetics and has been a model system for both the two-hit hypothesis of dominantly inherited cancer as well as for the concept of tumor-specific loss of constitutional heterozygosity to achieve expression of the tumorigenic phenotype. Familial retinoblastoma is usually inherited as an autosomal dominant disease with high penetrance and expressivity. In a small but significant number of families, however, retinoblastoma is inherited with greatly reduced penetrance and expressivity. In these families, retinoblastoma tumors occur relatively late, are often unilateral, and unaffected carriers may exist. We have identified a mutation in such a family that exhibited extremely low penetrance and expressivity. This mutation appeared to affect splicing of the mutant allele such that both a normal length RB1 mRNA and a truncated RB1 mRNA were expressed from the same allele.

Original language	English (US)
Pages (from-to)	557-563
Number of pages	7
Journal	Human genetics
Volume	100
Issue number	5-6
DOIs	https://doi.org/10.1007/s004390050551
State	Published - 1997

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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@article{f235f5e7af5c4a33b400ab8c6bf6907d,

title = "A splicing mutation in RB1 in low penetrance retinoblastoma",

abstract = "The pediatric eye-tumor retinoblastoma is widely held as a paradigm of human cancer genetics and has been a model system for both the two-hit hypothesis of dominantly inherited cancer as well as for the concept of tumor-specific loss of constitutional heterozygosity to achieve expression of the tumorigenic phenotype. Familial retinoblastoma is usually inherited as an autosomal dominant disease with high penetrance and expressivity. In a small but significant number of families, however, retinoblastoma is inherited with greatly reduced penetrance and expressivity. In these families, retinoblastoma tumors occur relatively late, are often unilateral, and unaffected carriers may exist. We have identified a mutation in such a family that exhibited extremely low penetrance and expressivity. This mutation appeared to affect splicing of the mutant allele such that both a normal length RB1 mRNA and a truncated RB1 mRNA were expressed from the same allele.",

author = "Schubert, {Elizabeth L.} and Strong, {Louise C.} and Hansen, {Marc F.}",

note = "Funding Information: Acknowledgements The authors would like to thank the family for their participation in this study. We also thank Janet Gruhn, Phillis Begin, and Joanne Cook for their assistance in sample collection as well as Karen Peterson and Carmen Sapienza for their assistance in linkage analysis. We appreciate the technical sugges- tions of Laura L. Whitaker and Carl C. Ton on this work. Beppino Giovanelli kindly established the lymphoblastoid cell line used in this study. The computer program for statistical analysis was provided by Barry W. Brown. This work was funded by the National Cancer Institute Grant CA50331 (to MFH) as well as grants from the Retina Research Foundation of Houston (to LCS) and the American Legion Auxiliary of Texas (to ELS).",

year = "1997",

doi = "10.1007/s004390050551",

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T1 - A splicing mutation in RB1 in low penetrance retinoblastoma

AU - Schubert, Elizabeth L.

AU - Strong, Louise C.

AU - Hansen, Marc F.

N1 - Funding Information: Acknowledgements The authors would like to thank the family for their participation in this study. We also thank Janet Gruhn, Phillis Begin, and Joanne Cook for their assistance in sample collection as well as Karen Peterson and Carmen Sapienza for their assistance in linkage analysis. We appreciate the technical sugges- tions of Laura L. Whitaker and Carl C. Ton on this work. Beppino Giovanelli kindly established the lymphoblastoid cell line used in this study. The computer program for statistical analysis was provided by Barry W. Brown. This work was funded by the National Cancer Institute Grant CA50331 (to MFH) as well as grants from the Retina Research Foundation of Houston (to LCS) and the American Legion Auxiliary of Texas (to ELS).

PY - 1997

Y1 - 1997

N2 - The pediatric eye-tumor retinoblastoma is widely held as a paradigm of human cancer genetics and has been a model system for both the two-hit hypothesis of dominantly inherited cancer as well as for the concept of tumor-specific loss of constitutional heterozygosity to achieve expression of the tumorigenic phenotype. Familial retinoblastoma is usually inherited as an autosomal dominant disease with high penetrance and expressivity. In a small but significant number of families, however, retinoblastoma is inherited with greatly reduced penetrance and expressivity. In these families, retinoblastoma tumors occur relatively late, are often unilateral, and unaffected carriers may exist. We have identified a mutation in such a family that exhibited extremely low penetrance and expressivity. This mutation appeared to affect splicing of the mutant allele such that both a normal length RB1 mRNA and a truncated RB1 mRNA were expressed from the same allele.

AB - The pediatric eye-tumor retinoblastoma is widely held as a paradigm of human cancer genetics and has been a model system for both the two-hit hypothesis of dominantly inherited cancer as well as for the concept of tumor-specific loss of constitutional heterozygosity to achieve expression of the tumorigenic phenotype. Familial retinoblastoma is usually inherited as an autosomal dominant disease with high penetrance and expressivity. In a small but significant number of families, however, retinoblastoma is inherited with greatly reduced penetrance and expressivity. In these families, retinoblastoma tumors occur relatively late, are often unilateral, and unaffected carriers may exist. We have identified a mutation in such a family that exhibited extremely low penetrance and expressivity. This mutation appeared to affect splicing of the mutant allele such that both a normal length RB1 mRNA and a truncated RB1 mRNA were expressed from the same allele.

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A splicing mutation in RB1 in low penetrance retinoblastoma

Abstract

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