The effect of p53-function on the sensitivity to paclitaxel with or without hyperthermia in human colorectal carcinoma cells

C. van Bree; J. H. Savonije; N. A. Franken; J. Haveman; P. J. Bakker

The effect of p53-function on the sensitivity to paclitaxel with or without hyperthermia in human colorectal carcinoma cells

C. van Bree
, J. H. Savonije
, N. A. Franken
, J. Haveman
, P. J. Bakker

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

Abstract

The importance of p53-function for the sensitivity to paclitaxel with and without hyperthermia (HT) was studied in an isogenic cell line system. The inactivation of p53 decreased sensitivity to paclitaxel (1.1-2.5-fold), which correlated with a lower induction of apoptosis. The magnitude of the G2/M arrest after treatment with paclitaxel was similar in all cell lines. The cytotoxicity of paclitaxel was not enhanced by HT in either wild-type p53 or p53-inactivated cells. In conclusion, cellular sensitivity to paclitaxel depends on p53-function by its ability to induce apoptosis. Irrespective of the p53-function HT was not able to enhance the sensitivity to paclitaxel

Original language	English
Pages (from-to)	739-744
Journal	International journal of oncology
Volume	16
Issue number	4
Publication status	Published - 2000

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title = "The effect of p53-function on the sensitivity to paclitaxel with or without hyperthermia in human colorectal carcinoma cells",

abstract = "The importance of p53-function for the sensitivity to paclitaxel with and without hyperthermia (HT) was studied in an isogenic cell line system. The inactivation of p53 decreased sensitivity to paclitaxel (1.1-2.5-fold), which correlated with a lower induction of apoptosis. The magnitude of the G2/M arrest after treatment with paclitaxel was similar in all cell lines. The cytotoxicity of paclitaxel was not enhanced by HT in either wild-type p53 or p53-inactivated cells. In conclusion, cellular sensitivity to paclitaxel depends on p53-function by its ability to induce apoptosis. Irrespective of the p53-function HT was not able to enhance the sensitivity to paclitaxel",

author = "\{van Bree\}, C. and Savonije, \{J. H.\} and Franken, \{N. A.\} and J. Haveman and Bakker, \{P. J.\}",

year = "2000",

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T1 - The effect of p53-function on the sensitivity to paclitaxel with or without hyperthermia in human colorectal carcinoma cells

AU - van Bree, C.

AU - Savonije, J. H.

AU - Franken, N. A.

AU - Haveman, J.

AU - Bakker, P. J.

PY - 2000

Y1 - 2000

N2 - The importance of p53-function for the sensitivity to paclitaxel with and without hyperthermia (HT) was studied in an isogenic cell line system. The inactivation of p53 decreased sensitivity to paclitaxel (1.1-2.5-fold), which correlated with a lower induction of apoptosis. The magnitude of the G2/M arrest after treatment with paclitaxel was similar in all cell lines. The cytotoxicity of paclitaxel was not enhanced by HT in either wild-type p53 or p53-inactivated cells. In conclusion, cellular sensitivity to paclitaxel depends on p53-function by its ability to induce apoptosis. Irrespective of the p53-function HT was not able to enhance the sensitivity to paclitaxel

AB - The importance of p53-function for the sensitivity to paclitaxel with and without hyperthermia (HT) was studied in an isogenic cell line system. The inactivation of p53 decreased sensitivity to paclitaxel (1.1-2.5-fold), which correlated with a lower induction of apoptosis. The magnitude of the G2/M arrest after treatment with paclitaxel was similar in all cell lines. The cytotoxicity of paclitaxel was not enhanced by HT in either wild-type p53 or p53-inactivated cells. In conclusion, cellular sensitivity to paclitaxel depends on p53-function by its ability to induce apoptosis. Irrespective of the p53-function HT was not able to enhance the sensitivity to paclitaxel

M3 - Article

C2 - 10717242

SN - 1019-6439

VL - 16

SP - 739

EP - 744

JO - International journal of oncology

JF - International journal of oncology

IS - 4

ER -

The effect of p53-function on the sensitivity to paclitaxel with or without hyperthermia in human colorectal carcinoma cells

Abstract

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