Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines

Haatisha Jandu; Kristina Aluzaité; Louise Fogh; Sebastian Wingaard Thrane; Julie B Noer; Joanna Proszek; Khoa Nguyen Do; Stine Ninel Hansen; Britt Damsgaard-Hansen; Signe Lykke Nielsen; Magnus Stougaard; Birgitta R. Knudsen; José Moreira; Petra Hamerlik; Madhavsai Gajjar; Marcel Smid; John Martens; John Foekens; Yves Pommier; Nils Brünner; Anne-Sofie Schrohl Rasmussen; Jan Stenvang

doi:10.1186/s12885-016-2071-1

Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines

Haatisha Jandu, Kristina Aluzaité, Louise Fogh, Sebastian Wingaard Thrane, Julie B Noer, Joanna Proszek, Khoa Nguyen Do, Stine Ninel Hansen, Britt Damsgaard-Hansen, Signe Lykke Nielsen, Magnus Stougaard, Birgitta R. Knudsen, José Moreira, Petra Hamerlik, Madhavsai Gajjar, Marcel Smid, John Martens, John Foekens, Yves Pommier, Nils BrünnerAnne-Sofie Schrohl Rasmussen, Jan Stenvang

24 Citations (Scopus)

Abstract

BACKGROUND: Studies in taxane and/or anthracycline refractory metastatic breast cancer (mBC) patients have shown approximately 30 % response rates to irinotecan. Hence, a significant number of patients will experience irinotecan-induced side effects without obtaining any benefit. The aim of this study was to lay the groundwork for development of predictive biomarkers for irinotecan treatment in BC.

METHODS: We established BC cell lines with acquired or de novo resistance to SN-38, by exposing the human BC cell lines MCF-7 and MDA-MB-231 to either stepwise increasing concentrations over 6 months or an initial high dose of SN-38 (the active metabolite of irinotecan), respectively. The resistant cell lines were analyzed for cross-resistance to other anti-cancer drugs, global gene expression, growth rates, TOP1 and TOP2A gene copy numbers and protein expression, and inhibition of the breast cancer resistance protein (ABCG2/BCRP) drug efflux pump.

RESULTS: We found that the resistant cell lines showed 7-100 fold increased resistance to SN-38 but remained sensitive to docetaxel and the non-camptothecin Top1 inhibitor LMP400. The resistant cell lines were characterized by Top1 down-regulation, changed isoelectric points of Top1 and reduced growth rates. The gene and protein expression of ABCG2/BCRP was up-regulated in the resistant sub-lines and functional assays revealed BCRP as a key mediator of SN-38 resistance.

CONCLUSIONS: Based on our preclinical results, we suggest analyzing the predictive value of the BCRP in breast cancer patients scheduled for irinotecan treatment. Moreover, LMP400 should be tested in a clinical setting in breast cancer patients with resistance to irinotecan.

Original language	English
Article number	34
Journal	B M C Cancer
Volume	16
Number of pages	13
ISSN	1471-2407
DOIs	https://doi.org/10.1186/s12885-016-2071-1
Publication status	Published - 22 Jan 2016

Keywords

Faculty of Social Sciences
Breast cancer
Topoisomerase I
Irinotecan
SN-38
Resistance
ABCG2/BCRP

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Jandu, H., Aluzaité, K., Fogh, L., Thrane, S. W., Noer, J. B., Proszek, J., Nguyen Do, K., Hansen, S. N., Damsgaard-Hansen, B., Nielsen, S. L., Stougaard, M., Knudsen, B. R., Moreira, J., Hamerlik, P., Gajjar, M., Smid, M., Martens, J., Foekens, J., Pommier, Y., ... Stenvang, J. (2016). Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines. B M C Cancer, 16, [34]. https://doi.org/10.1186/s12885-016-2071-1

Jandu, H, Aluzaité, K, Fogh, L, Thrane, SW, Noer, JB, Proszek, J, Nguyen Do, K, Hansen, SN, Damsgaard-Hansen, B, Nielsen, SL, Stougaard, M, Knudsen, BR, Moreira, J, Hamerlik, P, Gajjar, M, Smid, M, Martens, J, Foekens, J, Pommier, Y, Brünner, N, Rasmussen, A-SS & Stenvang, J 2016, 'Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines', B M C Cancer, vol. 16, 34. https://doi.org/10.1186/s12885-016-2071-1

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title = "Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines",

abstract = "BACKGROUND: Studies in taxane and/or anthracycline refractory metastatic breast cancer (mBC) patients have shown approximately 30 % response rates to irinotecan. Hence, a significant number of patients will experience irinotecan-induced side effects without obtaining any benefit. The aim of this study was to lay the groundwork for development of predictive biomarkers for irinotecan treatment in BC.METHODS: We established BC cell lines with acquired or de novo resistance to SN-38, by exposing the human BC cell lines MCF-7 and MDA-MB-231 to either stepwise increasing concentrations over 6 months or an initial high dose of SN-38 (the active metabolite of irinotecan), respectively. The resistant cell lines were analyzed for cross-resistance to other anti-cancer drugs, global gene expression, growth rates, TOP1 and TOP2A gene copy numbers and protein expression, and inhibition of the breast cancer resistance protein (ABCG2/BCRP) drug efflux pump.RESULTS: We found that the resistant cell lines showed 7-100 fold increased resistance to SN-38 but remained sensitive to docetaxel and the non-camptothecin Top1 inhibitor LMP400. The resistant cell lines were characterized by Top1 down-regulation, changed isoelectric points of Top1 and reduced growth rates. The gene and protein expression of ABCG2/BCRP was up-regulated in the resistant sub-lines and functional assays revealed BCRP as a key mediator of SN-38 resistance.CONCLUSIONS: Based on our preclinical results, we suggest analyzing the predictive value of the BCRP in breast cancer patients scheduled for irinotecan treatment. Moreover, LMP400 should be tested in a clinical setting in breast cancer patients with resistance to irinotecan.",

keywords = "Faculty of Social Sciences, Breast cancer, Topoisomerase I, Irinotecan, SN-38, Resistance, ABCG2/BCRP",

author = "Haatisha Jandu and Kristina Aluzait{\'e} and Louise Fogh and Thrane, {Sebastian Wingaard} and Noer, {Julie B} and Joanna Proszek and {Nguyen Do}, Khoa and Hansen, {Stine Ninel} and Britt Damsgaard-Hansen and Nielsen, {Signe Lykke} and Magnus Stougaard and Knudsen, {Birgitta R.} and Jos{\'e} Moreira and Petra Hamerlik and Madhavsai Gajjar and Marcel Smid and John Martens and John Foekens and Yves Pommier and Nils Br{\"u}nner and Rasmussen, {Anne-Sofie Schrohl} and Jan Stenvang",

year = "2016",

month = jan,

day = "22",

doi = "10.1186/s12885-016-2071-1",

language = "English",

volume = "16",

journal = "B M C Cancer",

issn = "1471-2407",

publisher = "BioMed Central Ltd.",

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TY - JOUR

T1 - Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines

AU - Jandu, Haatisha

AU - Aluzaité, Kristina

AU - Fogh, Louise

AU - Thrane, Sebastian Wingaard

AU - Noer, Julie B

AU - Proszek, Joanna

AU - Nguyen Do, Khoa

AU - Hansen, Stine Ninel

AU - Damsgaard-Hansen, Britt

AU - Nielsen, Signe Lykke

AU - Stougaard, Magnus

AU - Knudsen, Birgitta R.

AU - Moreira, José

AU - Hamerlik, Petra

AU - Gajjar, Madhavsai

AU - Smid, Marcel

AU - Martens, John

AU - Foekens, John

AU - Pommier, Yves

AU - Brünner, Nils

AU - Rasmussen, Anne-Sofie Schrohl

AU - Stenvang, Jan

PY - 2016/1/22

Y1 - 2016/1/22

N2 - BACKGROUND: Studies in taxane and/or anthracycline refractory metastatic breast cancer (mBC) patients have shown approximately 30 % response rates to irinotecan. Hence, a significant number of patients will experience irinotecan-induced side effects without obtaining any benefit. The aim of this study was to lay the groundwork for development of predictive biomarkers for irinotecan treatment in BC.METHODS: We established BC cell lines with acquired or de novo resistance to SN-38, by exposing the human BC cell lines MCF-7 and MDA-MB-231 to either stepwise increasing concentrations over 6 months or an initial high dose of SN-38 (the active metabolite of irinotecan), respectively. The resistant cell lines were analyzed for cross-resistance to other anti-cancer drugs, global gene expression, growth rates, TOP1 and TOP2A gene copy numbers and protein expression, and inhibition of the breast cancer resistance protein (ABCG2/BCRP) drug efflux pump.RESULTS: We found that the resistant cell lines showed 7-100 fold increased resistance to SN-38 but remained sensitive to docetaxel and the non-camptothecin Top1 inhibitor LMP400. The resistant cell lines were characterized by Top1 down-regulation, changed isoelectric points of Top1 and reduced growth rates. The gene and protein expression of ABCG2/BCRP was up-regulated in the resistant sub-lines and functional assays revealed BCRP as a key mediator of SN-38 resistance.CONCLUSIONS: Based on our preclinical results, we suggest analyzing the predictive value of the BCRP in breast cancer patients scheduled for irinotecan treatment. Moreover, LMP400 should be tested in a clinical setting in breast cancer patients with resistance to irinotecan.

AB - BACKGROUND: Studies in taxane and/or anthracycline refractory metastatic breast cancer (mBC) patients have shown approximately 30 % response rates to irinotecan. Hence, a significant number of patients will experience irinotecan-induced side effects without obtaining any benefit. The aim of this study was to lay the groundwork for development of predictive biomarkers for irinotecan treatment in BC.METHODS: We established BC cell lines with acquired or de novo resistance to SN-38, by exposing the human BC cell lines MCF-7 and MDA-MB-231 to either stepwise increasing concentrations over 6 months or an initial high dose of SN-38 (the active metabolite of irinotecan), respectively. The resistant cell lines were analyzed for cross-resistance to other anti-cancer drugs, global gene expression, growth rates, TOP1 and TOP2A gene copy numbers and protein expression, and inhibition of the breast cancer resistance protein (ABCG2/BCRP) drug efflux pump.RESULTS: We found that the resistant cell lines showed 7-100 fold increased resistance to SN-38 but remained sensitive to docetaxel and the non-camptothecin Top1 inhibitor LMP400. The resistant cell lines were characterized by Top1 down-regulation, changed isoelectric points of Top1 and reduced growth rates. The gene and protein expression of ABCG2/BCRP was up-regulated in the resistant sub-lines and functional assays revealed BCRP as a key mediator of SN-38 resistance.CONCLUSIONS: Based on our preclinical results, we suggest analyzing the predictive value of the BCRP in breast cancer patients scheduled for irinotecan treatment. Moreover, LMP400 should be tested in a clinical setting in breast cancer patients with resistance to irinotecan.

KW - Faculty of Social Sciences

KW - Breast cancer

KW - Topoisomerase I

KW - Irinotecan

KW - SN-38

KW - Resistance

KW - ABCG2/BCRP

U2 - 10.1186/s12885-016-2071-1

DO - 10.1186/s12885-016-2071-1

M3 - Journal article

C2 - 26801902

SN - 1471-2407

VL - 16

JO - B M C Cancer

JF - B M C Cancer

M1 - 34

ER -

Molecular characterization of irinotecan (SN-38) resistant human breast cancer cell lines

Abstract

Keywords

UN SDGs

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