Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer.

Heidi Schwarzenbach; Felix Chun; Imke Lange; Sebastian Carpenter; Miriam Gottberg; Andreas Erbersdobler; Martin Friedrich; Hartwig Huland; Klaus Pantel

Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer.

Standard

Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer. / Schwarzenbach, Heidi; Chun, Felix; Lange, Imke; Carpenter, Sebastian; Gottberg, Miriam; Erbersdobler, Andreas; Friedrich, Martin; Huland, Hartwig; Pantel, Klaus.

in: INT J CANCER, Jahrgang 120, Nr. 7, 7, 2007, S. 1465-1471.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Schwarzenbach, H, Chun, F, Lange, I, Carpenter, S, Gottberg, M, Erbersdobler, A, Friedrich, M, Huland, H & Pantel, K 2007, 'Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer.', INT J CANCER, Jg. 120, Nr. 7, 7, S. 1465-1471. <http://www.ncbi.nlm.nih.gov/pubmed/17205532?dopt=Citation>

APA

Schwarzenbach, H., Chun, F., Lange, I., Carpenter, S., Gottberg, M., Erbersdobler, A., Friedrich, M., Huland, H., & Pantel, K. (2007). Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer. INT J CANCER, 120(7), 1465-1471. [7]. http://www.ncbi.nlm.nih.gov/pubmed/17205532?dopt=Citation

Vancouver

Schwarzenbach H, Chun F, Lange I, Carpenter S, Gottberg M, Erbersdobler A et al. Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer. INT J CANCER. 2007;120(7):1465-1471. 7.

Bibtex

@article{c6644aa1fa0648fa818f76d41d9ba977,

title = "Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer.",

abstract = "Tumor tissues, blood plasma and bone marrow (BM) aspirates of 57 prostate cancer patients (PCa) without clinical signs of overt metastases were assessed for LOH (loss of heterozygosity) by a PCR-based fluorescence microsatellite analysis, using a panel of 15 markers. Additionally, micrometastatic tumor cells in BM were monitored by an immunocytological cytokeratin assay. In total, 25 (44%), 32 (56%) and 41 (72%) of the patients had at least 1 LOH in their blood, BM and tumor samples, respectively. Among the informative cases, the frequency of LOH was highest in blood plasma for the markers D8S360 (18%) and D10S1765 (15%), and in BM plasma for THRB (24%) and D8S137 (22%). Comparison of blood plasma and BM with tumors showed discrepant results in 35% and 45% of patients, respectively. Whereas all LOHs at THRB in BM plasma were also detected in the autologous tumor tissues, LOHs at D6S474 and D11S898 in BM were not retrieved in the tumors. The comparison with established risk factors showed a correlation of borderline significance for LOH at D9S1748 in the BM aspirates (p=0.055) and a significant correlation in the tumor samples (p=0.004) with increasing pathologic Gleason scores. Interestingly, 22% of the PCa patients harbored tumor cells in their BM and tended (p=0.065) to have more frequent LOH (16%) in BM plasma compared to patients without tumor cells (9%). These data demonstrate, for the first time, the presence of free tumor-specific DNA in blood and BM of PCa patients and suggest a possible relationship to BM micrometastasis.",

author = "Heidi Schwarzenbach and Felix Chun and Imke Lange and Sebastian Carpenter and Miriam Gottberg and Andreas Erbersdobler and Martin Friedrich and Hartwig Huland and Klaus Pantel",

year = "2007",

language = "Deutsch",

volume = "120",

pages = "1465--1471",

journal = "INT J CANCER",

issn = "0020-7136",

publisher = "Wiley-Liss Inc.",

number = "7",

}

RIS

TY - JOUR

T1 - Detection of tumor-specific DNA in blood and bone marrow plasma from patients with prostate cancer.

AU - Schwarzenbach, Heidi

AU - Chun, Felix

AU - Lange, Imke

AU - Carpenter, Sebastian

AU - Gottberg, Miriam

AU - Erbersdobler, Andreas

AU - Friedrich, Martin

AU - Huland, Hartwig

AU - Pantel, Klaus

PY - 2007

Y1 - 2007

N2 - Tumor tissues, blood plasma and bone marrow (BM) aspirates of 57 prostate cancer patients (PCa) without clinical signs of overt metastases were assessed for LOH (loss of heterozygosity) by a PCR-based fluorescence microsatellite analysis, using a panel of 15 markers. Additionally, micrometastatic tumor cells in BM were monitored by an immunocytological cytokeratin assay. In total, 25 (44%), 32 (56%) and 41 (72%) of the patients had at least 1 LOH in their blood, BM and tumor samples, respectively. Among the informative cases, the frequency of LOH was highest in blood plasma for the markers D8S360 (18%) and D10S1765 (15%), and in BM plasma for THRB (24%) and D8S137 (22%). Comparison of blood plasma and BM with tumors showed discrepant results in 35% and 45% of patients, respectively. Whereas all LOHs at THRB in BM plasma were also detected in the autologous tumor tissues, LOHs at D6S474 and D11S898 in BM were not retrieved in the tumors. The comparison with established risk factors showed a correlation of borderline significance for LOH at D9S1748 in the BM aspirates (p=0.055) and a significant correlation in the tumor samples (p=0.004) with increasing pathologic Gleason scores. Interestingly, 22% of the PCa patients harbored tumor cells in their BM and tended (p=0.065) to have more frequent LOH (16%) in BM plasma compared to patients without tumor cells (9%). These data demonstrate, for the first time, the presence of free tumor-specific DNA in blood and BM of PCa patients and suggest a possible relationship to BM micrometastasis.

AB - Tumor tissues, blood plasma and bone marrow (BM) aspirates of 57 prostate cancer patients (PCa) without clinical signs of overt metastases were assessed for LOH (loss of heterozygosity) by a PCR-based fluorescence microsatellite analysis, using a panel of 15 markers. Additionally, micrometastatic tumor cells in BM were monitored by an immunocytological cytokeratin assay. In total, 25 (44%), 32 (56%) and 41 (72%) of the patients had at least 1 LOH in their blood, BM and tumor samples, respectively. Among the informative cases, the frequency of LOH was highest in blood plasma for the markers D8S360 (18%) and D10S1765 (15%), and in BM plasma for THRB (24%) and D8S137 (22%). Comparison of blood plasma and BM with tumors showed discrepant results in 35% and 45% of patients, respectively. Whereas all LOHs at THRB in BM plasma were also detected in the autologous tumor tissues, LOHs at D6S474 and D11S898 in BM were not retrieved in the tumors. The comparison with established risk factors showed a correlation of borderline significance for LOH at D9S1748 in the BM aspirates (p=0.055) and a significant correlation in the tumor samples (p=0.004) with increasing pathologic Gleason scores. Interestingly, 22% of the PCa patients harbored tumor cells in their BM and tended (p=0.065) to have more frequent LOH (16%) in BM plasma compared to patients without tumor cells (9%). These data demonstrate, for the first time, the presence of free tumor-specific DNA in blood and BM of PCa patients and suggest a possible relationship to BM micrometastasis.

M3 - SCORING: Zeitschriftenaufsatz

VL - 120

SP - 1465

EP - 1471

JO - INT J CANCER

JF - INT J CANCER

SN - 0020-7136

IS - 7

M1 - 7

ER -