Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy.

Markus Hambek; Christian Werner; Mehran Baghi; Wolfgang Gstöttner; Rainald Knecht

Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy.

Standard

Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy. / Hambek, Markus; Werner, Christian; Baghi, Mehran; Gstöttner, Wolfgang; Knecht, Rainald.

In: ANTICANCER RES, Vol. 26, No. 2, 2, 2006, p. 1091-1095.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Hambek, M, Werner, C, Baghi, M, Gstöttner, W & Knecht, R 2006, 'Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy.', ANTICANCER RES, vol. 26, no. 2, 2, pp. 1091-1095. <http://www.ncbi.nlm.nih.gov/pubmed/16619511?dopt=Citation>

APA

Hambek, M., Werner, C., Baghi, M., Gstöttner, W., & Knecht, R. (2006). Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy. ANTICANCER RES, 26(2), 1091-1095. [2]. http://www.ncbi.nlm.nih.gov/pubmed/16619511?dopt=Citation

Vancouver

Hambek M, Werner C, Baghi M, Gstöttner W, Knecht R. Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy. ANTICANCER RES. 2006;26(2):1091-1095. 2.

Bibtex

@article{112caad7ce3c4372aea4897310b2fc92,

title = "Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy.",

abstract = "OBJECTIVES: In recent years, new chemotherapy regimens with promising activity, especially in first-line therapy (induction chemotherapy) of head and neck cancer (SCCHN), have been developed. Nevertheless, a major problem concerning the response of SCCHN to chemotherapy is the high percentage of resting cells (G0-phase cells) being resistant to chemotherapy. To overcome this phenomenon, the capacity of several cytokines to switch on cells into the division cycle and progress to the chemosensitive phases (S-, M-phases) was investigated. MATERIALS AND METHODS: Interleukin-6, serotonin, granulocyte colony stimulating factor (G-CSF) and epidermal growth factor (EGF) were used to stimulate G0-phase squamous cell cancer cells (Detroit 562, A431, UM-SCC 10B) for re-entry into the cell cycle to enhance the response to cisplatin. The proportion of G0-phase cells was detected through multicolor FACS analysis and Ki-67 staining. RESULTS: Cell cycle re-entry was most effective after combination treatment with serotonin + EGF. The proportion of G0-phase cells was significantly reduced after stimulation with serotonin + EGF (p <0.05). Corresponding to cell cycle re-entry, the cytotoxic effect of cisplatin was significantly (p <0.04) enhanced in the prestimulated compared to the control cells (cisplatin mono-treatment). CONCLUSION: Our investigations demonstrated for the first time that sensitizing G0-phase squamous cell carcinoma cells for chemotherapy is possible by prestimulation with target cytokines. Considering that up to 95% of tumor cells are in the resting (G0) phase of the cell cycle at the initiation of chemotherapy, prestimulation with EGF and serotonin could contribute to a synchronization of cancer cells. This would clearly enhance the cytotoxic effect.",

author = "Markus Hambek and Christian Werner and Mehran Baghi and Wolfgang Gst{\"o}ttner and Rainald Knecht",

year = "2006",

language = "Deutsch",

volume = "26",

pages = "1091--1095",

journal = "ANTICANCER RES",

issn = "0250-7005",

publisher = "International Institute of Anticancer Research",

number = "2",

}

RIS

TY - JOUR

T1 - Prestimulation of head and neck cancer cells with growth factors enhances treatment efficacy.

AU - Hambek, Markus

AU - Werner, Christian

AU - Baghi, Mehran

AU - Gstöttner, Wolfgang

AU - Knecht, Rainald

PY - 2006

Y1 - 2006

N2 - OBJECTIVES: In recent years, new chemotherapy regimens with promising activity, especially in first-line therapy (induction chemotherapy) of head and neck cancer (SCCHN), have been developed. Nevertheless, a major problem concerning the response of SCCHN to chemotherapy is the high percentage of resting cells (G0-phase cells) being resistant to chemotherapy. To overcome this phenomenon, the capacity of several cytokines to switch on cells into the division cycle and progress to the chemosensitive phases (S-, M-phases) was investigated. MATERIALS AND METHODS: Interleukin-6, serotonin, granulocyte colony stimulating factor (G-CSF) and epidermal growth factor (EGF) were used to stimulate G0-phase squamous cell cancer cells (Detroit 562, A431, UM-SCC 10B) for re-entry into the cell cycle to enhance the response to cisplatin. The proportion of G0-phase cells was detected through multicolor FACS analysis and Ki-67 staining. RESULTS: Cell cycle re-entry was most effective after combination treatment with serotonin + EGF. The proportion of G0-phase cells was significantly reduced after stimulation with serotonin + EGF (p <0.05). Corresponding to cell cycle re-entry, the cytotoxic effect of cisplatin was significantly (p <0.04) enhanced in the prestimulated compared to the control cells (cisplatin mono-treatment). CONCLUSION: Our investigations demonstrated for the first time that sensitizing G0-phase squamous cell carcinoma cells for chemotherapy is possible by prestimulation with target cytokines. Considering that up to 95% of tumor cells are in the resting (G0) phase of the cell cycle at the initiation of chemotherapy, prestimulation with EGF and serotonin could contribute to a synchronization of cancer cells. This would clearly enhance the cytotoxic effect.

AB - OBJECTIVES: In recent years, new chemotherapy regimens with promising activity, especially in first-line therapy (induction chemotherapy) of head and neck cancer (SCCHN), have been developed. Nevertheless, a major problem concerning the response of SCCHN to chemotherapy is the high percentage of resting cells (G0-phase cells) being resistant to chemotherapy. To overcome this phenomenon, the capacity of several cytokines to switch on cells into the division cycle and progress to the chemosensitive phases (S-, M-phases) was investigated. MATERIALS AND METHODS: Interleukin-6, serotonin, granulocyte colony stimulating factor (G-CSF) and epidermal growth factor (EGF) were used to stimulate G0-phase squamous cell cancer cells (Detroit 562, A431, UM-SCC 10B) for re-entry into the cell cycle to enhance the response to cisplatin. The proportion of G0-phase cells was detected through multicolor FACS analysis and Ki-67 staining. RESULTS: Cell cycle re-entry was most effective after combination treatment with serotonin + EGF. The proportion of G0-phase cells was significantly reduced after stimulation with serotonin + EGF (p <0.05). Corresponding to cell cycle re-entry, the cytotoxic effect of cisplatin was significantly (p <0.04) enhanced in the prestimulated compared to the control cells (cisplatin mono-treatment). CONCLUSION: Our investigations demonstrated for the first time that sensitizing G0-phase squamous cell carcinoma cells for chemotherapy is possible by prestimulation with target cytokines. Considering that up to 95% of tumor cells are in the resting (G0) phase of the cell cycle at the initiation of chemotherapy, prestimulation with EGF and serotonin could contribute to a synchronization of cancer cells. This would clearly enhance the cytotoxic effect.

M3 - SCORING: Zeitschriftenaufsatz

VL - 26

SP - 1091

EP - 1095

JO - ANTICANCER RES

JF - ANTICANCER RES

SN - 0250-7005

IS - 2

M1 - 2

ER -