| Literature DB >> 23990866 |
Haifeng Bao1, Patricia A Burke, Jiaqi Huang, Xiaoru Chen, Philip Z Brohawn, Yihong Yao, Robert J Lechleider, Robert S Sikorski, Manuela Buzoianu, Jianliang Zhang, Xiaoqing Shi, Laura K Richman, Theresa M Lavallee.
Abstract
PURPOSE: Clinical development of cancer drugs has a low success rate. Prognostic and predictive biomarkers using minimally invasive approaches hold promise for increasing the probability of success by enabling disease characterization, patient selection and early detection of drug treatment effect. Enumeration and molecular characterization of circulating tumor cells (CTC) may address some of these needs, and thus were evaluated for utility in a Phase I solid tumor clinical study. EXPERIMENTALEntities:
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Year: 2013 PMID: 23990866 PMCID: PMC3749129 DOI: 10.1371/journal.pone.0058557
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Patient characteristics.
| Total patients (N=24) | Patients evaluable for CTC enumeration (N=21) | |
|---|---|---|
| Age (years) | ||
| Median (range) | 65 (39-78) | 64 (39-78) |
| Gender | ||
| Male | 13 (54.2%) | 12 (57.1%) |
| Female | 11 (45.8%) | 9 (42.9%) |
| Tumor category | ||
| Breast cancer | 1 (4.2%) | 1 (4.8%) |
| Colon cancer | 10 (41.7%) | 9 (42.9%) |
| Endometrial caner | 1 (4.2%) | 1 (4.8%) |
| Non-small cell lung caner | 3 (12.5%) | 3 (14.3%) |
| Ovarian cancer | 1 (4.2%) | 1 (4.8%) |
| Prostate cancer | 3 (12.5%) | 3 (14.3%) |
| Others | 5 (20.8%) | 3 (14.3%) |
| Tumor stage at study entry | ||
| I–II | 0 (0%) | 0 (0%) |
| III | 3 (12.5%) | 3 (14.3%) |
| IV | 21 (87.5%) | 18 (85.7%) |
| Lymph nodes | ||
| N0 | 7 (29.2%) | 5 (23.8%) |
| N+ | 14 (58.3%) | 13 (61.9%) |
| Metastasis status | ||
| M0 | 9 (37.5%) | 7 (33.3%) |
| M+ | 12 (50.0%) | 11 (52.4) |
Information of 3 patients was unknown.
Circulating tumor cell detection at baseline.
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| 0 | 10 | 34 | 7 | 33 |
| 1-3 | 8 | 28 | 7 | 33 |
| >3 | 11 | 38 | 7 | 33 |
| Total | 29 | 100 | 21 | 100 |
Figure 1Circulating tumor cell detection and patient stay on treatment time.
Figure 2Kaplan-Meier estimates of probabilities of overall survival (A) and progression-free survival (B) of patients with respect to frequency of CTCs before initiation of therapy.
The red, green, and blue lines represent patients with no CTC, 1-3 CTCs, and above 3 CTCs, respectively.
Figure 3Circulating tumor cell number and disease outcome.
Circulating tumor cell gene expression profiles by quantitative RT-PCR.
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<20 CT
20-25 CT
25.1-29 CT
- Undetected