Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms

Heather J. Chalfin; Stephanie A. Glavaris; Paymaneh D. Malihi; Jamie M. Sperger; Michael A. Gorin; Changxue Lu; C. Rory Goodwin; Yan Chen; Emily A. Caruso; Ruth Dumpit; Peter Kuhn; Joshua M. Lang; Peter S. Nelson; Jun Luo; Kenneth J. Pienta

doi:10.1016/j.juro.2018.01.033

Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms

Heather J. Chalfin, Stephanie A. Glavaris, Paymaneh D. Malihi, Jamie M. Sperger, Michael A. Gorin, Changxue Lu, C. Rory Goodwin, Yan Chen, Emily A. Caruso, Ruth Dumpit, Peter Kuhn, Joshua M. Lang, Peter S. Nelson, Jun Luo, Kenneth J. Pienta

School of Medicine

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

Purpose: Prostate circulating tumor cells escape into peripheral blood and enter bone marrow as disseminated tumor cells, representing an early step before conventionally detectable metastasis. It is unclear how frequently this occurs in localized disease and existing detection methods rely on epithelial markers with low specificity and sensitivity. We used multiple methodologies of disseminated tumor cell detection in bone marrow harvested at radical prostatectomy. Materials and Methods: Bone marrow was harvested from 208 clinically localized cases, 16 controls and 5 metastatic cases with peripheral blood obtained from 37 metastatic cases. Samples were evaluated at 4 centers with 4 distinct platforms using antibody enrichment with the AdnaTest (Qiagen®) or VERSA (versatile exclusion based rare sample analysis), or whole sample interrogation with the RareCyte platform (Seattle, Washington) or HD-SCA (high definition single cell assay) using traditional epithelial markers and prostate specific markers. We investigated the sensitivity and specificity of these markers by evaluating expression levels in control and metastatic cases. Results: EpCAM, NKX3.1 and AR were nonspecifically expressed in controls and in most samples using AdnaTest with no relation to perioperative variables. Only 1 patient with localized disease showed positive results for the prostate specific marker PSA. With the VERSA platform no localized case demonstrated disseminated tumor cells. With the RareCyte and HD-SCA platforms only a single patient had 1 disseminated tumor cell. Conclusions: Evaluation across multiple platforms revealed that epithelial markers are nonspecific in bone marrow and, thus, not suitable for disseminated tumor cell detection. Using prostate specific markers disseminated tumor cells were typically not detected in patients with localized prostate cancer.

Original language	English (US)
Pages (from-to)	1494-1501
Number of pages	8
Journal	Journal of Urology
Volume	199
Issue number	6
DOIs	https://doi.org/10.1016/j.juro.2018.01.033
State	Published - Jun 2018

Keywords

biomarkers
bone marrow
circulating
neoplasm metastasis
neoplastic cells
prostatic neoplasms
tumor

ASJC Scopus subject areas

Urology

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10.1016/j.juro.2018.01.033

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Chalfin, H. J., Glavaris, S. A., Malihi, P. D., Sperger, J. M., Gorin, M. A., Lu, C., Goodwin, C. R., Chen, Y., Caruso, E. A., Dumpit, R., Kuhn, P., Lang, J. M., Nelson, P. S., Luo, J., & Pienta, K. J. (2018). Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms. Journal of Urology, 199(6), 1494-1501. https://doi.org/10.1016/j.juro.2018.01.033

Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms. / Chalfin, Heather J.; Glavaris, Stephanie A.; Malihi, Paymaneh D. et al.
In: Journal of Urology, Vol. 199, No. 6, 06.2018, p. 1494-1501.

Research output: Contribution to journal › Article › peer-review

Chalfin, HJ, Glavaris, SA, Malihi, PD, Sperger, JM, Gorin, MA, Lu, C, Goodwin, CR, Chen, Y, Caruso, EA, Dumpit, R, Kuhn, P, Lang, JM, Nelson, PS, Luo, J & Pienta, KJ 2018, 'Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms', Journal of Urology, vol. 199, no. 6, pp. 1494-1501. https://doi.org/10.1016/j.juro.2018.01.033

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title = "Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms",

abstract = "Purpose: Prostate circulating tumor cells escape into peripheral blood and enter bone marrow as disseminated tumor cells, representing an early step before conventionally detectable metastasis. It is unclear how frequently this occurs in localized disease and existing detection methods rely on epithelial markers with low specificity and sensitivity. We used multiple methodologies of disseminated tumor cell detection in bone marrow harvested at radical prostatectomy. Materials and Methods: Bone marrow was harvested from 208 clinically localized cases, 16 controls and 5 metastatic cases with peripheral blood obtained from 37 metastatic cases. Samples were evaluated at 4 centers with 4 distinct platforms using antibody enrichment with the AdnaTest (Qiagen{\textregistered}) or VERSA (versatile exclusion based rare sample analysis), or whole sample interrogation with the RareCyte platform (Seattle, Washington) or HD-SCA (high definition single cell assay) using traditional epithelial markers and prostate specific markers. We investigated the sensitivity and specificity of these markers by evaluating expression levels in control and metastatic cases. Results: EpCAM, NKX3.1 and AR were nonspecifically expressed in controls and in most samples using AdnaTest with no relation to perioperative variables. Only 1 patient with localized disease showed positive results for the prostate specific marker PSA. With the VERSA platform no localized case demonstrated disseminated tumor cells. With the RareCyte and HD-SCA platforms only a single patient had 1 disseminated tumor cell. Conclusions: Evaluation across multiple platforms revealed that epithelial markers are nonspecific in bone marrow and, thus, not suitable for disseminated tumor cell detection. Using prostate specific markers disseminated tumor cells were typically not detected in patients with localized prostate cancer.",

keywords = "biomarkers, bone marrow, circulating, neoplasm metastasis, neoplastic cells, prostatic neoplasms, tumor",

author = "Chalfin, {Heather J.} and Glavaris, {Stephanie A.} and Malihi, {Paymaneh D.} and Sperger, {Jamie M.} and Gorin, {Michael A.} and Changxue Lu and Goodwin, {C. Rory} and Yan Chen and Caruso, {Emily A.} and Ruth Dumpit and Peter Kuhn and Lang, {Joshua M.} and Nelson, {Peter S.} and Jun Luo and Pienta, {Kenneth J.}",

note = "Publisher Copyright: {\textcopyright} 2018 American Urological Association Education and Research, Inc.",

year = "2018",

month = jun,

doi = "10.1016/j.juro.2018.01.033",

language = "English (US)",

volume = "199",

pages = "1494--1501",

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T1 - Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms

AU - Chalfin, Heather J.

AU - Glavaris, Stephanie A.

AU - Malihi, Paymaneh D.

AU - Sperger, Jamie M.

AU - Gorin, Michael A.

AU - Lu, Changxue

AU - Goodwin, C. Rory

AU - Chen, Yan

AU - Caruso, Emily A.

AU - Dumpit, Ruth

AU - Kuhn, Peter

AU - Lang, Joshua M.

AU - Nelson, Peter S.

AU - Luo, Jun

AU - Pienta, Kenneth J.

PY - 2018/6

Y1 - 2018/6

N2 - Purpose: Prostate circulating tumor cells escape into peripheral blood and enter bone marrow as disseminated tumor cells, representing an early step before conventionally detectable metastasis. It is unclear how frequently this occurs in localized disease and existing detection methods rely on epithelial markers with low specificity and sensitivity. We used multiple methodologies of disseminated tumor cell detection in bone marrow harvested at radical prostatectomy. Materials and Methods: Bone marrow was harvested from 208 clinically localized cases, 16 controls and 5 metastatic cases with peripheral blood obtained from 37 metastatic cases. Samples were evaluated at 4 centers with 4 distinct platforms using antibody enrichment with the AdnaTest (Qiagen®) or VERSA (versatile exclusion based rare sample analysis), or whole sample interrogation with the RareCyte platform (Seattle, Washington) or HD-SCA (high definition single cell assay) using traditional epithelial markers and prostate specific markers. We investigated the sensitivity and specificity of these markers by evaluating expression levels in control and metastatic cases. Results: EpCAM, NKX3.1 and AR were nonspecifically expressed in controls and in most samples using AdnaTest with no relation to perioperative variables. Only 1 patient with localized disease showed positive results for the prostate specific marker PSA. With the VERSA platform no localized case demonstrated disseminated tumor cells. With the RareCyte and HD-SCA platforms only a single patient had 1 disseminated tumor cell. Conclusions: Evaluation across multiple platforms revealed that epithelial markers are nonspecific in bone marrow and, thus, not suitable for disseminated tumor cell detection. Using prostate specific markers disseminated tumor cells were typically not detected in patients with localized prostate cancer.

AB - Purpose: Prostate circulating tumor cells escape into peripheral blood and enter bone marrow as disseminated tumor cells, representing an early step before conventionally detectable metastasis. It is unclear how frequently this occurs in localized disease and existing detection methods rely on epithelial markers with low specificity and sensitivity. We used multiple methodologies of disseminated tumor cell detection in bone marrow harvested at radical prostatectomy. Materials and Methods: Bone marrow was harvested from 208 clinically localized cases, 16 controls and 5 metastatic cases with peripheral blood obtained from 37 metastatic cases. Samples were evaluated at 4 centers with 4 distinct platforms using antibody enrichment with the AdnaTest (Qiagen®) or VERSA (versatile exclusion based rare sample analysis), or whole sample interrogation with the RareCyte platform (Seattle, Washington) or HD-SCA (high definition single cell assay) using traditional epithelial markers and prostate specific markers. We investigated the sensitivity and specificity of these markers by evaluating expression levels in control and metastatic cases. Results: EpCAM, NKX3.1 and AR were nonspecifically expressed in controls and in most samples using AdnaTest with no relation to perioperative variables. Only 1 patient with localized disease showed positive results for the prostate specific marker PSA. With the VERSA platform no localized case demonstrated disseminated tumor cells. With the RareCyte and HD-SCA platforms only a single patient had 1 disseminated tumor cell. Conclusions: Evaluation across multiple platforms revealed that epithelial markers are nonspecific in bone marrow and, thus, not suitable for disseminated tumor cell detection. Using prostate specific markers disseminated tumor cells were typically not detected in patients with localized prostate cancer.

KW - biomarkers

KW - bone marrow

KW - circulating

KW - neoplasm metastasis

KW - neoplastic cells

KW - prostatic neoplasms

KW - tumor

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SN - 0022-5347

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JO - Journal of Urology

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Prostate Cancer Disseminated Tumor Cells are Rarely Detected in the Bone Marrow of Patients with Localized Disease Undergoing Radical Prostatectomy across Multiple Rare Cell Detection Platforms

Abstract

Keywords

ASJC Scopus subject areas

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