Multi-center study evaluating circulating tumor cells as a surrogate for response to treatment and overall survival in metastatic breast cancer (original) (raw)
- Hiroshi Yagata1,
- Shinji Ohno2,
- Hiroshi Yamaguchi2,
- Hiroji Iwata3,
- Nobuyuki Tsunoda3,
- Yoshinori Ito4,
- Nahomi Tokudome4,
- Masakazu Toi5,
- Katsumasa Kuroi6 &
- …
- Eiji Suzuki6
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Abstract
Background
Evaluating circulating tumor cells (CTCs) is one way to predict outcome and monitor treatment in patients with MBC. In this prospective study, we evaluated CTCs in predicting treatment efficacy and overall survival (OS) using the CellSearch™ System (Veridex, LLC, Raritan, NJ).
Methods
One hundred nineteen patients with MBC with measurable disease were enrolled. Samples of 7.5 ml of blood from 107 eligible patients were tested for CTCs before starting therapy (baseline), after one cycle of therapy (3–4 weeks) and at 12 weeks. We compared CTC levels and imaging at baseline and at 12 weeks. Next, we determined the hazard ratios (HR) by comparing cases with zero CTCs to those with one or more CTCs. Moreover, HR was calculated when comparing cases that had greater than or equal to a certain number of CTCs to those with less than the number of CTCs.
Results
This study shows the incidence of detection of CTCs in patients with metastatic breast cancers. Of the patients, 64.4% (76/118) had one or more CTCs, and 37.3% (44/118) had five or more CTCs. First we set the baseline number of CTCs as 100%. Of the seven cases whose level of CTCs decreased more than 90%, six (85.7%) demonstrated a positive response (complete response and partial response) by imaging after one cycle (3–4 weeks later). For the patients whose CTC levels increased above 100% after one cycle (3–4 weeks later), 7 of 11 (63.6%) had progressive disease (PD). The HR for cases with five to ten CTCs was greater than 1.00 [HR = 2.450; 95% confidence interval (CI) 0.727–8.248]. Statistical significance was observed when comparing patients who had ≥3 CTCs to those with <3 CTCs (P = 0.0273). When comparing cases with ≥5 CTCs to those with <5 CTCs, the hazard ratio was 3.069 (95% CI 1.496–6.295; P = 0.0022).
Conclusions
Because the change in the number of CTCs was highly correlated with results from imaging before and after therapy, CTCs can be considered a biomarker that may predict the effect of treatment earlier than imaging modalities.
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Acknowledgments
This study was sponsored and designed by the sponsor (Ortho-Clinical Diagnostics KK, Tokyo, Japan) in collaboration with clinical investigators. Data on CTCs were also collected and verified by the sponsor.
Author information
Authors and Affiliations
- Department of Breast Surgical Oncology, St. Luke’s International Hospital, 9-1 Akashi-cho, Chuo-ku, Tokyo, 104-8560, Japan
Seigo Nakamura & Hiroshi Yagata - Kyushu Cancer Center, Fukuoka, Japan
Shinji Ohno & Hiroshi Yamaguchi - Aichi Cancer Center, Aichi, Japan
Hiroji Iwata & Nobuyuki Tsunoda - Japan Foundation of Cancer Research Ariake Hospital, Tokyo, Japan
Yoshinori Ito & Nahomi Tokudome - Kyoto University Hospital, Kyoto, Japan
Masakazu Toi - Tokyo Metropolitan Komagome Hospital, Tokyo, Japan
Katsumasa Kuroi & Eiji Suzuki
Authors
- Seigo Nakamura
You can also search for this author inPubMed Google Scholar - Hiroshi Yagata
You can also search for this author inPubMed Google Scholar - Shinji Ohno
You can also search for this author inPubMed Google Scholar - Hiroshi Yamaguchi
You can also search for this author inPubMed Google Scholar - Hiroji Iwata
You can also search for this author inPubMed Google Scholar - Nobuyuki Tsunoda
You can also search for this author inPubMed Google Scholar - Yoshinori Ito
You can also search for this author inPubMed Google Scholar - Nahomi Tokudome
You can also search for this author inPubMed Google Scholar - Masakazu Toi
You can also search for this author inPubMed Google Scholar - Katsumasa Kuroi
You can also search for this author inPubMed Google Scholar - Eiji Suzuki
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Corresponding author
Correspondence toSeigo Nakamura.
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Nakamura, S., Yagata, H., Ohno, S. et al. Multi-center study evaluating circulating tumor cells as a surrogate for response to treatment and overall survival in metastatic breast cancer.Breast Cancer 17, 199–204 (2010). https://doi.org/10.1007/s12282-009-0139-3
- Received: 24 February 2009
- Accepted: 24 April 2009
- Published: 01 August 2009
- Issue Date: July 2010
- DOI: https://doi.org/10.1007/s12282-009-0139-3