The basis for intrinsic drug resistance or sensitivity to methotrexate

J. R. Bertino; J. Lin; G. Pizzorno; Wei Li Wei Wei Li; Y. M. Chang

doi:10.1016/0065-2571(89)90107-6

The basis for intrinsic drug resistance or sensitivity to methotrexate

J. R. Bertino, J. Lin, G. Pizzorno, Wei Li Wei Wei Li, Y. M. Chang

Cancer Institute of New Jersey (CINJ), Basic Research

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

6 Scopus citations

Abstract

Natural resistance to MTX in three different types of malignant cells is discussed. Two causes of resistance found were impaired drug uptake and impaired polyglutamylation. These resistance mechanisms have also been described to occur in cell lines with acquired resitance to this drug. In cells with acquired drug resistance, these phenotypic changes may reflect mutations in genes associated with transport of MTX or the enzyme DHFR, or in some circumstances reversion of the cell to a different phenotype without a mutational event. In cells with intrinsic resistance, the genetic mechanism responsible for these phenotypes is not known. Alternate treatment programs, e.g., with TMTX, or with TMTX and CPG₂, a folate depleting enzyme, are under evaluation for these MTX resistant neoplasms.

Original language	English (US)
Pages (from-to)	277-285
Number of pages	9
Journal	Advances in Enzyme Regulation
Volume	29
Issue number	C
DOIs	https://doi.org/10.1016/0065-2571(89)90107-6
State	Published - 1989

All Science Journal Classification (ASJC) codes

Molecular Medicine
Molecular Biology
Genetics
Cancer Research

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10.1016/0065-2571(89)90107-6

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title = "The basis for intrinsic drug resistance or sensitivity to methotrexate",

abstract = "Natural resistance to MTX in three different types of malignant cells is discussed. Two causes of resistance found were impaired drug uptake and impaired polyglutamylation. These resistance mechanisms have also been described to occur in cell lines with acquired resitance to this drug. In cells with acquired drug resistance, these phenotypic changes may reflect mutations in genes associated with transport of MTX or the enzyme DHFR, or in some circumstances reversion of the cell to a different phenotype without a mutational event. In cells with intrinsic resistance, the genetic mechanism responsible for these phenotypes is not known. Alternate treatment programs, e.g., with TMTX, or with TMTX and CPG2, a folate depleting enzyme, are under evaluation for these MTX resistant neoplasms.",

author = "Bertino, {J. R.} and J. Lin and G. Pizzorno and {Wei Wei Li}, {Wei Li} and Chang, {Y. M.}",

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doi = "10.1016/0065-2571(89)90107-6",

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T1 - The basis for intrinsic drug resistance or sensitivity to methotrexate

AU - Bertino, J. R.

AU - Lin, J.

AU - Pizzorno, G.

AU - Wei Wei Li, Wei Li

AU - Chang, Y. M.

PY - 1989

Y1 - 1989

N2 - Natural resistance to MTX in three different types of malignant cells is discussed. Two causes of resistance found were impaired drug uptake and impaired polyglutamylation. These resistance mechanisms have also been described to occur in cell lines with acquired resitance to this drug. In cells with acquired drug resistance, these phenotypic changes may reflect mutations in genes associated with transport of MTX or the enzyme DHFR, or in some circumstances reversion of the cell to a different phenotype without a mutational event. In cells with intrinsic resistance, the genetic mechanism responsible for these phenotypes is not known. Alternate treatment programs, e.g., with TMTX, or with TMTX and CPG2, a folate depleting enzyme, are under evaluation for these MTX resistant neoplasms.

AB - Natural resistance to MTX in three different types of malignant cells is discussed. Two causes of resistance found were impaired drug uptake and impaired polyglutamylation. These resistance mechanisms have also been described to occur in cell lines with acquired resitance to this drug. In cells with acquired drug resistance, these phenotypic changes may reflect mutations in genes associated with transport of MTX or the enzyme DHFR, or in some circumstances reversion of the cell to a different phenotype without a mutational event. In cells with intrinsic resistance, the genetic mechanism responsible for these phenotypes is not known. Alternate treatment programs, e.g., with TMTX, or with TMTX and CPG2, a folate depleting enzyme, are under evaluation for these MTX resistant neoplasms.

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JO - Advances in Biological Regulation

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The basis for intrinsic drug resistance or sensitivity to methotrexate

Abstract

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