Evidence implicating at least two genes on chromosome 17p in breast carcinogenesis

C. Coles; A. M. Thompson; P. A. Elder; B. B. Cohen; I. M. Mackenzie; G. Cranston; J. Mackay; M. Macdonald; C. M. Steel; A. M. Thompson; U. Chetty; J. Mackay; Y. Nakamura; B. Hoyheim

doi:10.1016/0140-6736(90)93236-I

Evidence implicating at least two genes on chromosome 17p in breast carcinogenesis

C. Coles, A. M. Thompson, P. A. Elder, B. B. Cohen, I. M. Mackenzie, G. Cranston, J. Mackay, M. Macdonald, C. M. Steel, A. M. Thompson, U. Chetty, J. Mackay, Y. Nakamura, B. Hoyheim

Surgical Oncology

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Abstract

The DNA of paired tumour and blood leucocyte samples from a large series of breast cancer patients was analysed to map regions of loss of heterozygosity on chromosome 17. The high frequency of loss of heterozygosity on 17p was confirmed, and a third of informative tumours had also lost an allele at the long arm locus THH59. On the short arm two distinct regions of loss of heterozygosity were identified, in bands p13-3 and p13-1. The latter probably involves the structural gene p53, which has been implicated as an oncogene or as a tumour suppressor in various human cancers. 17p 13-3, however, showed a significantly higher frequency of loss of heterozygosity, and there was no correlation between allele losses at the two sites. Nevertheless, loss of heterozygosity at 17p 13-3 is associated with overexpression of p53 mRNA, suggesting the existence of a gene some 20 megabases telomeric of p53 that regulates its expression. Lesions of this regulatory gene seem to be involved in the majority of breast cancers.

Original language	English (US)
Pages (from-to)	761-763
Number of pages	3
Journal	The Lancet
Volume	336
Issue number	8718
DOIs	https://doi.org/10.1016/0140-6736(90)93236-I
State	Published - Sep 29 1990

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General Medicine

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10.1016/0140-6736(90)93236-I

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@article{df0c410a2ecb4042bdae6f4ef0da5148,

title = "Evidence implicating at least two genes on chromosome 17p in breast carcinogenesis",

abstract = "The DNA of paired tumour and blood leucocyte samples from a large series of breast cancer patients was analysed to map regions of loss of heterozygosity on chromosome 17. The high frequency of loss of heterozygosity on 17p was confirmed, and a third of informative tumours had also lost an allele at the long arm locus THH59. On the short arm two distinct regions of loss of heterozygosity were identified, in bands p13-3 and p13-1. The latter probably involves the structural gene p53, which has been implicated as an oncogene or as a tumour suppressor in various human cancers. 17p 13-3, however, showed a significantly higher frequency of loss of heterozygosity, and there was no correlation between allele losses at the two sites. Nevertheless, loss of heterozygosity at 17p 13-3 is associated with overexpression of p53 mRNA, suggesting the existence of a gene some 20 megabases telomeric of p53 that regulates its expression. Lesions of this regulatory gene seem to be involved in the majority of breast cancers.",

author = "C. Coles and Thompson, {A. M.} and Elder, {P. A.} and Cohen, {B. B.} and Mackenzie, {I. M.} and G. Cranston and J. Mackay and M. Macdonald and Steel, {C. M.} and Thompson, {A. M.} and U. Chetty and J. Mackay and Y. Nakamura and B. Hoyheim",

note = "Funding Information: This study was supported by grants from the UK Breast Cancer Research Trust (C. C.). the Scottish Hospitals Endownment Research Trust (A. M. T., G. C.) and by Edinburgh University Faculty of Medicine Graduate Research Fellowships (A. M. T., J. M.). We thank Prof H. J. Evans, Professor Sir Patrick Forrest and Prof D. C. Carter for their active encouragement of this work; Dr Tom Anderson for histology of the tumours ; the medical, nursing, and clerical staff of the Edinburgh breast unit for their cooperation in the study; Dr Jane Prosser for helpful discussions; Ms Lesley Campbell for typing the paper, and Mr Norman Davidson for artwork.",

year = "1990",

month = sep,

day = "29",

doi = "10.1016/0140-6736(90)93236-I",

language = "English (US)",

volume = "336",

pages = "761--763",

journal = "The Lancet",

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T1 - Evidence implicating at least two genes on chromosome 17p in breast carcinogenesis

AU - Coles, C.

AU - Thompson, A. M.

AU - Elder, P. A.

AU - Cohen, B. B.

AU - Mackenzie, I. M.

AU - Cranston, G.

AU - Mackay, J.

AU - Macdonald, M.

AU - Steel, C. M.

AU - Thompson, A. M.

AU - Chetty, U.

AU - Mackay, J.

AU - Nakamura, Y.

AU - Hoyheim, B.

N1 - Funding Information: This study was supported by grants from the UK Breast Cancer Research Trust (C. C.). the Scottish Hospitals Endownment Research Trust (A. M. T., G. C.) and by Edinburgh University Faculty of Medicine Graduate Research Fellowships (A. M. T., J. M.). We thank Prof H. J. Evans, Professor Sir Patrick Forrest and Prof D. C. Carter for their active encouragement of this work; Dr Tom Anderson for histology of the tumours ; the medical, nursing, and clerical staff of the Edinburgh breast unit for their cooperation in the study; Dr Jane Prosser for helpful discussions; Ms Lesley Campbell for typing the paper, and Mr Norman Davidson for artwork.

PY - 1990/9/29

Y1 - 1990/9/29

N2 - The DNA of paired tumour and blood leucocyte samples from a large series of breast cancer patients was analysed to map regions of loss of heterozygosity on chromosome 17. The high frequency of loss of heterozygosity on 17p was confirmed, and a third of informative tumours had also lost an allele at the long arm locus THH59. On the short arm two distinct regions of loss of heterozygosity were identified, in bands p13-3 and p13-1. The latter probably involves the structural gene p53, which has been implicated as an oncogene or as a tumour suppressor in various human cancers. 17p 13-3, however, showed a significantly higher frequency of loss of heterozygosity, and there was no correlation between allele losses at the two sites. Nevertheless, loss of heterozygosity at 17p 13-3 is associated with overexpression of p53 mRNA, suggesting the existence of a gene some 20 megabases telomeric of p53 that regulates its expression. Lesions of this regulatory gene seem to be involved in the majority of breast cancers.

AB - The DNA of paired tumour and blood leucocyte samples from a large series of breast cancer patients was analysed to map regions of loss of heterozygosity on chromosome 17. The high frequency of loss of heterozygosity on 17p was confirmed, and a third of informative tumours had also lost an allele at the long arm locus THH59. On the short arm two distinct regions of loss of heterozygosity were identified, in bands p13-3 and p13-1. The latter probably involves the structural gene p53, which has been implicated as an oncogene or as a tumour suppressor in various human cancers. 17p 13-3, however, showed a significantly higher frequency of loss of heterozygosity, and there was no correlation between allele losses at the two sites. Nevertheless, loss of heterozygosity at 17p 13-3 is associated with overexpression of p53 mRNA, suggesting the existence of a gene some 20 megabases telomeric of p53 that regulates its expression. Lesions of this regulatory gene seem to be involved in the majority of breast cancers.

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JO - The Lancet

JF - The Lancet

IS - 8718

ER -

Evidence implicating at least two genes on chromosome 17p in breast carcinogenesis

Abstract

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