Mutation analysis of the c-mos proto-oncogene in human ovarian teratomas

K. A.F. De Foy; S. A. Gayther; W. H. Colledge; S. Crockett; I. V. Scott; M. J. Evans; B. A.J. Ponder

doi:10.1038/bjc.1998.269

Mutation analysis of the c-mos proto-oncogene in human ovarian teratomas

K. A.F. De Foy, S. A. Gayther, W. H. Colledge, S. Crockett, I. V. Scott, M. J. Evans, B. A.J. Ponder

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

9 Scopus citations

Abstract

Female transgenic mice lacking a functional c-mos proto-oncogene develop ovarian teratomas, indicating that c-mos may behave as a tumour-suppressor gene for this type of tumour. We have analysed the entire coding region of the c-MOS gene in a series of human ovarian teratomas to determine whether there are any cancer-causing alterations. DNA from twenty teratomas was analysed by single-strand conformational analysis (SSCA) and heteroduplex analysis (HA) to screen for somatic and germline mutations. In nine of these tumours the entire gene was also sequenced. A previously reported polymorphism and a single new sequence variant were identified, neither of which we would predict to be disease-causing alterations. These results suggest that mutations in the coding region of the c-MOS gene do not play a significant role in the genesis of human ovarian teratomas.

Original language	English (US)
Pages (from-to)	1642-1644
Number of pages	3
Journal	British Journal of Cancer
Volume	77
Issue number	10
DOIs	https://doi.org/10.1038/bjc.1998.269
State	Published - 1998
Externally published	Yes

Keywords

Ovary
Parthenogenesis
Teratoma
c-mos

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1038/bjc.1998.269

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title = "Mutation analysis of the c-mos proto-oncogene in human ovarian teratomas",

abstract = "Female transgenic mice lacking a functional c-mos proto-oncogene develop ovarian teratomas, indicating that c-mos may behave as a tumour-suppressor gene for this type of tumour. We have analysed the entire coding region of the c-MOS gene in a series of human ovarian teratomas to determine whether there are any cancer-causing alterations. DNA from twenty teratomas was analysed by single-strand conformational analysis (SSCA) and heteroduplex analysis (HA) to screen for somatic and germline mutations. In nine of these tumours the entire gene was also sequenced. A previously reported polymorphism and a single new sequence variant were identified, neither of which we would predict to be disease-causing alterations. These results suggest that mutations in the coding region of the c-MOS gene do not play a significant role in the genesis of human ovarian teratomas.",

keywords = "Ovary, Parthenogenesis, Teratoma, c-mos",

author = "{De Foy}, {K. A.F.} and Gayther, {S. A.} and Colledge, {W. H.} and S. Crockett and Scott, {I. V.} and Evans, {M. J.} and Ponder, {B. A.J.}",

year = "1998",

doi = "10.1038/bjc.1998.269",

language = "English (US)",

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AU - De Foy, K. A.F.

AU - Gayther, S. A.

AU - Colledge, W. H.

AU - Crockett, S.

AU - Scott, I. V.

AU - Evans, M. J.

AU - Ponder, B. A.J.

PY - 1998

Y1 - 1998

N2 - Female transgenic mice lacking a functional c-mos proto-oncogene develop ovarian teratomas, indicating that c-mos may behave as a tumour-suppressor gene for this type of tumour. We have analysed the entire coding region of the c-MOS gene in a series of human ovarian teratomas to determine whether there are any cancer-causing alterations. DNA from twenty teratomas was analysed by single-strand conformational analysis (SSCA) and heteroduplex analysis (HA) to screen for somatic and germline mutations. In nine of these tumours the entire gene was also sequenced. A previously reported polymorphism and a single new sequence variant were identified, neither of which we would predict to be disease-causing alterations. These results suggest that mutations in the coding region of the c-MOS gene do not play a significant role in the genesis of human ovarian teratomas.

AB - Female transgenic mice lacking a functional c-mos proto-oncogene develop ovarian teratomas, indicating that c-mos may behave as a tumour-suppressor gene for this type of tumour. We have analysed the entire coding region of the c-MOS gene in a series of human ovarian teratomas to determine whether there are any cancer-causing alterations. DNA from twenty teratomas was analysed by single-strand conformational analysis (SSCA) and heteroduplex analysis (HA) to screen for somatic and germline mutations. In nine of these tumours the entire gene was also sequenced. A previously reported polymorphism and a single new sequence variant were identified, neither of which we would predict to be disease-causing alterations. These results suggest that mutations in the coding region of the c-MOS gene do not play a significant role in the genesis of human ovarian teratomas.

KW - Ovary

KW - Parthenogenesis

KW - Teratoma

KW - c-mos

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Mutation analysis of the c-mos proto-oncogene in human ovarian teratomas

Abstract

Keywords

ASJC Scopus subject areas

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