Effects of the MYC oncogene antagonist, MAD, on proliferation, cell cycling and the malignant phenotype of human brain tumour cells

Jun Chen; Timothy Willingham; Linda R. Margraf; Nicole Schreiber-Agus; Ronald A. Depinho; Perry D. Nisen

doi:10.1038/nm0795-638

Effects of the MYC oncogene antagonist, MAD, on proliferation, cell cycling and the malignant phenotype of human brain tumour cells

Jun Chen, Timothy Willingham, Linda R. Margraf, Nicole Schreiber-Agus, Ronald A. Depinho, Perry D. Nisen

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

99 Scopus citations

Abstract

To investigate how overexpression of MAD, an antagonist of MYC oncogenes influences the malignant phenotype of human cancer cells, an adenovirus vector System was used to transfer the human MAD gene (AdMAD) into human astrocytoma cells. Decreased growth potential of AdMAD-infected cells was evidenced by a decrease in [3H]thymidine incorporation, an increase in cell doubling time and alteration of cell-cyde distribution. Diminlshed malignant potential of AdMAD-infected cells was manifested by their loss of anchorage-independent growth in soft agar and by their inability, in general, to induce tumorigenesis in a xenograft animal model. These studies indicate that adenovirus constructs encoding MAD dramatically inhibit the proliferation and tumorigenicity of human astrocytoma cells and Support the use of MAD for gene therapy of human tumours.

Original language	English (US)
Pages (from-to)	638-643
Number of pages	6
Journal	Nature medicine
Volume	1
Issue number	7
DOIs	https://doi.org/10.1038/nm0795-638
State	Published - Jul 1995
Externally published	Yes

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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title = "Effects of the MYC oncogene antagonist, MAD, on proliferation, cell cycling and the malignant phenotype of human brain tumour cells",

abstract = "To investigate how overexpression of MAD, an antagonist of MYC oncogenes influences the malignant phenotype of human cancer cells, an adenovirus vector System was used to transfer the human MAD gene (AdMAD) into human astrocytoma cells. Decreased growth potential of AdMAD-infected cells was evidenced by a decrease in [3H]thymidine incorporation, an increase in cell doubling time and alteration of cell-cyde distribution. Diminlshed malignant potential of AdMAD-infected cells was manifested by their loss of anchorage-independent growth in soft agar and by their inability, in general, to induce tumorigenesis in a xenograft animal model. These studies indicate that adenovirus constructs encoding MAD dramatically inhibit the proliferation and tumorigenicity of human astrocytoma cells and Support the use of MAD for gene therapy of human tumours.",

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AU - Chen, Jun

AU - Willingham, Timothy

AU - Margraf, Linda R.

AU - Schreiber-Agus, Nicole

AU - Depinho, Ronald A.

AU - Nisen, Perry D.

PY - 1995/7

Y1 - 1995/7

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AB - To investigate how overexpression of MAD, an antagonist of MYC oncogenes influences the malignant phenotype of human cancer cells, an adenovirus vector System was used to transfer the human MAD gene (AdMAD) into human astrocytoma cells. Decreased growth potential of AdMAD-infected cells was evidenced by a decrease in [3H]thymidine incorporation, an increase in cell doubling time and alteration of cell-cyde distribution. Diminlshed malignant potential of AdMAD-infected cells was manifested by their loss of anchorage-independent growth in soft agar and by their inability, in general, to induce tumorigenesis in a xenograft animal model. These studies indicate that adenovirus constructs encoding MAD dramatically inhibit the proliferation and tumorigenicity of human astrocytoma cells and Support the use of MAD for gene therapy of human tumours.

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Effects of the MYC oncogene antagonist, MAD, on proliferation, cell cycling and the malignant phenotype of human brain tumour cells

Abstract

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