Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study

BACKGROUND: Presence of disseminated tumor cells (DTCs) in bone marrow (BM) after completion of systemic adjuvant treatment predicts reduced survival in breast cancer. The present study explores the use of DTCs to identify adjuvant insufficiently treated patients to be offered secondary adjuvant tre...

Descripción completa

Detalles Bibliográficos
Autores principales: Synnestvedt, Marit, Borgen, Elin, Wist, Erik, Wiedswang, Gro, Weyde, Kjetil, Risberg, Terje, Kersten, Christian, Mjaaland, Ingvil, Vindi, Lise, Schirmer, Cecilie, Nesland, Jahn Martin, Naume, Bjørn
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3576235/
https://www.ncbi.nlm.nih.gov/pubmed/23259667
http://dx.doi.org/10.1186/1471-2407-12-616
_version_ 1782259818322460672
author Synnestvedt, Marit
Borgen, Elin
Wist, Erik
Wiedswang, Gro
Weyde, Kjetil
Risberg, Terje
Kersten, Christian
Mjaaland, Ingvil
Vindi, Lise
Schirmer, Cecilie
Nesland, Jahn Martin
Naume, Bjørn
author_facet Synnestvedt, Marit
Borgen, Elin
Wist, Erik
Wiedswang, Gro
Weyde, Kjetil
Risberg, Terje
Kersten, Christian
Mjaaland, Ingvil
Vindi, Lise
Schirmer, Cecilie
Nesland, Jahn Martin
Naume, Bjørn
author_sort Synnestvedt, Marit
collection PubMed
description BACKGROUND: Presence of disseminated tumor cells (DTCs) in bone marrow (BM) after completion of systemic adjuvant treatment predicts reduced survival in breast cancer. The present study explores the use of DTCs to identify adjuvant insufficiently treated patients to be offered secondary adjuvant treatment intervention, and as a surrogate marker for therapy response. METHODS: A total of 1121 patients with pN1-3 or pT1c/T2G2-3pN0-status were enrolled. All had completed primary surgery and received 6 cycles of anthracycline-containing chemotherapy. BM-aspiration was performed 8-12 weeks after chemotherapy (BM1), followed by a second BM-aspiration 6 months later (BM2). DTC-status was determined by morphological evaluation of immunocytochemically detected cytokeratin-positive cells. If DTCs were present at BM2, docetaxel (100 mg/m(2), 3qw, 6 courses) was administered, followed by DTC-analysis 1 month (BM3) and 13 months (BM4) after the last docetaxel infusion. RESULTS: Clinical follow-up (FU) is still ongoing. Here, the descriptive data from the study are presented. Of 1085 patients with a reported DTC result at both BM1 and BM2, 94 patients (8.7%) were BM1 positive and 83 (7.6%) were BM2 positive. The concordance between BM1 and BM2 was 86.5%. Both at BM1 and BM2 DTC-status was significantly associated with lobular carcinomas (p = 0.02 and p = 0.03, respectively; chi-square). In addition, DTC-status at BM2 was also associated with pN-status (p = 0.009) and pT-status (p = 0.03). At BM1 28.8% and 12.8% of the DTC-positive patients had ≥2 DTCs and ≥3 DTCs, respectively. At BM2, the corresponding frequencies were 47.0% and 25.3%. Of 72 docetaxel-treated patients analyzed at BM3 and/or BM4, only 15 (20.8%) had persistent DTCs. Of 17 patients with ≥3 DTCs before docetaxel treatment, 12 patients turned negative after treatment (70.6%). The change to DTC-negativity was associated with the presence of ductal carcinoma (p = 0.009). CONCLUSIONS: After docetaxel treatment, the majority of patients experienced disappearance of DTCs. As this is not a randomized trial, the results can be due to effects of adjuvant (docetaxel/endocrine/trastuzumab) treatment and/or limitations of the methodology. The clinical significance of these results awaits mature FU data, but indicates a possibility for clinical use of DTC-status as a residual disease-monitoring tool and as a surrogate marker of treatment response. TRIAL REGISTRATION: Clin Trials Gov NCT00248703
format Online
Article
Text
id pubmed-3576235
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-35762352013-02-20 Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study Synnestvedt, Marit Borgen, Elin Wist, Erik Wiedswang, Gro Weyde, Kjetil Risberg, Terje Kersten, Christian Mjaaland, Ingvil Vindi, Lise Schirmer, Cecilie Nesland, Jahn Martin Naume, Bjørn BMC Cancer Research Article BACKGROUND: Presence of disseminated tumor cells (DTCs) in bone marrow (BM) after completion of systemic adjuvant treatment predicts reduced survival in breast cancer. The present study explores the use of DTCs to identify adjuvant insufficiently treated patients to be offered secondary adjuvant treatment intervention, and as a surrogate marker for therapy response. METHODS: A total of 1121 patients with pN1-3 or pT1c/T2G2-3pN0-status were enrolled. All had completed primary surgery and received 6 cycles of anthracycline-containing chemotherapy. BM-aspiration was performed 8-12 weeks after chemotherapy (BM1), followed by a second BM-aspiration 6 months later (BM2). DTC-status was determined by morphological evaluation of immunocytochemically detected cytokeratin-positive cells. If DTCs were present at BM2, docetaxel (100 mg/m(2), 3qw, 6 courses) was administered, followed by DTC-analysis 1 month (BM3) and 13 months (BM4) after the last docetaxel infusion. RESULTS: Clinical follow-up (FU) is still ongoing. Here, the descriptive data from the study are presented. Of 1085 patients with a reported DTC result at both BM1 and BM2, 94 patients (8.7%) were BM1 positive and 83 (7.6%) were BM2 positive. The concordance between BM1 and BM2 was 86.5%. Both at BM1 and BM2 DTC-status was significantly associated with lobular carcinomas (p = 0.02 and p = 0.03, respectively; chi-square). In addition, DTC-status at BM2 was also associated with pN-status (p = 0.009) and pT-status (p = 0.03). At BM1 28.8% and 12.8% of the DTC-positive patients had ≥2 DTCs and ≥3 DTCs, respectively. At BM2, the corresponding frequencies were 47.0% and 25.3%. Of 72 docetaxel-treated patients analyzed at BM3 and/or BM4, only 15 (20.8%) had persistent DTCs. Of 17 patients with ≥3 DTCs before docetaxel treatment, 12 patients turned negative after treatment (70.6%). The change to DTC-negativity was associated with the presence of ductal carcinoma (p = 0.009). CONCLUSIONS: After docetaxel treatment, the majority of patients experienced disappearance of DTCs. As this is not a randomized trial, the results can be due to effects of adjuvant (docetaxel/endocrine/trastuzumab) treatment and/or limitations of the methodology. The clinical significance of these results awaits mature FU data, but indicates a possibility for clinical use of DTC-status as a residual disease-monitoring tool and as a surrogate marker of treatment response. TRIAL REGISTRATION: Clin Trials Gov NCT00248703 BioMed Central 2012-12-22 /pmc/articles/PMC3576235/ /pubmed/23259667 http://dx.doi.org/10.1186/1471-2407-12-616 Text en Copyright ©2012 Synnestvedt et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Synnestvedt, Marit
Borgen, Elin
Wist, Erik
Wiedswang, Gro
Weyde, Kjetil
Risberg, Terje
Kersten, Christian
Mjaaland, Ingvil
Vindi, Lise
Schirmer, Cecilie
Nesland, Jahn Martin
Naume, Bjørn
Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title_full Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title_fullStr Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title_full_unstemmed Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title_short Disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. Descriptive results from an intervention study
title_sort disseminated tumor cells as selection marker and monitoring tool for secondary adjuvant treatment in early breast cancer. descriptive results from an intervention study
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3576235/
https://www.ncbi.nlm.nih.gov/pubmed/23259667
http://dx.doi.org/10.1186/1471-2407-12-616
work_keys_str_mv AT synnestvedtmarit disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT borgenelin disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT wisterik disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT wiedswanggro disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT weydekjetil disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT risbergterje disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT kerstenchristian disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT mjaalandingvil disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT vindilise disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT schirmercecilie disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT neslandjahnmartin disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy
AT naumebjørn disseminatedtumorcellsasselectionmarkerandmonitoringtoolforsecondaryadjuvanttreatmentinearlybreastcancerdescriptiveresultsfromaninterventionstudy

Ejemplares similares