Development and evaluation of the MiCheck test for aggressive prostate cancer

Neal D. Shore; Christopher M. Pieczonka; R. Jonathan Henderson; James L. Bailen; Daniel R. Saltzstein; Raoul S. Concepcion; Jennifer L. Beebe-Dimmer; Julie J. Ruterbusch; Rachel A. Levin; Sandra Wissmueller; Thao Ho Le; David Gillatt; Daniel W. Chan; Douglas H. Campbell; Bradley J. Walsh

doi:10.1016/j.urolonc.2020.03.010

Development and evaluation of the MiCheck test for aggressive prostate cancer

Neal D. Shore, Christopher M. Pieczonka, R. Jonathan Henderson, James L. Bailen, Daniel R. Saltzstein, Raoul S. Concepcion, Jennifer L. Beebe-Dimmer, Julie J. Ruterbusch, Rachel A. Levin, Sandra Wissmueller, Thao Ho Le, David Gillatt, Daniel W. Chan, Douglas H. Campbell, Bradley J. Walsh

School of Medicine

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

1 Scopus citations

Abstract

Background: A clinical need exists for a biomarker test to accurately delineate aggressive prostate cancer (AgCaP), and thus better assist clinicians and patients decision-making on whether to proceed to prostate biopsy. Objectives: To develop a blood test for AgCaP and compare to PSA, %free PSA, proPSA, and prostate health index (PHI) tests. Design, settings and participants: Patient samples from the MiCheck-01 trial were used for development of the MiCheck test. Methods: Serum analyte concentrations for cellular growth factors were determined using a custom-made Luminex-based R&D Systems multianalyte kit. Outcome measurements and statistical analysis: Bayesian model averaging and random forest approaches were used to identify clinical factors and growth factors able to distinguish between men with AgCaP (Gleason Score [GS] ≥3+4) from those with non-AgCaP (GS 3+3). Logistic regression and Monte Carlo cross-validation identified variable combinations in order to able to maximize differentiation of AgCaP from non-AgCaP. Results: The MiCheck logistic regression model was developed and comprises the following variables: serum prostate-specific antigen (PSA), patient age, Digital Rectal Exam (DRE) status, Leptin, IL-7, vascular endothelial growth factor, and Glypican-1. The model differentiated AgCaP from non-AgCaP with an area under the curve of 0.83 and was superior to PSA, %free PSA and PHI in all patient groups, regardless of PSA range. Applying the MiCheck test to all evaluable biopsy patients from the MiCheck-01 study demonstrated that up to 30% of biopsies could be avoided while delaying diagnosis of only 6.8% of GS ≥3+4 cancers, 5% of GS ≥4+3 cancers and no cancers of GS 8 or higher. Conclusions: The MiCheck test outperforms PSA, %free PSA and PHI tests in differentiating AgCaP vs. non-AgCaP patients. The MiCheck test could result in a significant number of biopsies being avoided with a low number of patients experiencing a delayed diagnosis.

Original language	English (US)
Pages (from-to)	683.e11-683.e18
Journal	Urologic Oncology: Seminars and Original Investigations
Volume	38
Issue number	8
DOIs	https://doi.org/10.1016/j.urolonc.2020.03.010
State	Published - Aug 2020

Keywords

Aggressive
Biomarker
Clinical study
Prostate

ASJC Scopus subject areas

Urology
Oncology

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10.1016/j.urolonc.2020.03.010

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Shore, N. D., Pieczonka, C. M., Henderson, R. J., Bailen, J. L., Saltzstein, D. R., Concepcion, R. S., Beebe-Dimmer, J. L., Ruterbusch, J. J., Levin, R. A., Wissmueller, S., Le, T. H., Gillatt, D., Chan, D. W., Campbell, D. H., & Walsh, B. J. (2020). Development and evaluation of the MiCheck test for aggressive prostate cancer. Urologic Oncology: Seminars and Original Investigations, 38(8), 683.e11-683.e18. https://doi.org/10.1016/j.urolonc.2020.03.010

Shore, ND, Pieczonka, CM, Henderson, RJ, Bailen, JL, Saltzstein, DR, Concepcion, RS, Beebe-Dimmer, JL, Ruterbusch, JJ, Levin, RA, Wissmueller, S, Le, TH, Gillatt, D, Chan, DW, Campbell, DH & Walsh, BJ 2020, 'Development and evaluation of the MiCheck test for aggressive prostate cancer', Urologic Oncology: Seminars and Original Investigations, vol. 38, no. 8, pp. 683.e11-683.e18. https://doi.org/10.1016/j.urolonc.2020.03.010

@article{2d74e7730ed84886907208839d269927,

title = "Development and evaluation of the MiCheck test for aggressive prostate cancer",

abstract = "Background: A clinical need exists for a biomarker test to accurately delineate aggressive prostate cancer (AgCaP), and thus better assist clinicians and patients decision-making on whether to proceed to prostate biopsy. Objectives: To develop a blood test for AgCaP and compare to PSA, %free PSA, proPSA, and prostate health index (PHI) tests. Design, settings and participants: Patient samples from the MiCheck-01 trial were used for development of the MiCheck test. Methods: Serum analyte concentrations for cellular growth factors were determined using a custom-made Luminex-based R&D Systems multianalyte kit. Outcome measurements and statistical analysis: Bayesian model averaging and random forest approaches were used to identify clinical factors and growth factors able to distinguish between men with AgCaP (Gleason Score [GS] ≥3+4) from those with non-AgCaP (GS 3+3). Logistic regression and Monte Carlo cross-validation identified variable combinations in order to able to maximize differentiation of AgCaP from non-AgCaP. Results: The MiCheck logistic regression model was developed and comprises the following variables: serum prostate-specific antigen (PSA), patient age, Digital Rectal Exam (DRE) status, Leptin, IL-7, vascular endothelial growth factor, and Glypican-1. The model differentiated AgCaP from non-AgCaP with an area under the curve of 0.83 and was superior to PSA, %free PSA and PHI in all patient groups, regardless of PSA range. Applying the MiCheck test to all evaluable biopsy patients from the MiCheck-01 study demonstrated that up to 30% of biopsies could be avoided while delaying diagnosis of only 6.8% of GS ≥3+4 cancers, 5% of GS ≥4+3 cancers and no cancers of GS 8 or higher. Conclusions: The MiCheck test outperforms PSA, %free PSA and PHI tests in differentiating AgCaP vs. non-AgCaP patients. The MiCheck test could result in a significant number of biopsies being avoided with a low number of patients experiencing a delayed diagnosis.",

keywords = "Aggressive, Biomarker, Clinical study, Prostate",

author = "Shore, {Neal D.} and Pieczonka, {Christopher M.} and Henderson, {R. Jonathan} and Bailen, {James L.} and Saltzstein, {Daniel R.} and Concepcion, {Raoul S.} and Beebe-Dimmer, {Jennifer L.} and Ruterbusch, {Julie J.} and Levin, {Rachel A.} and Sandra Wissmueller and Le, {Thao Ho} and David Gillatt and Chan, {Daniel W.} and Campbell, {Douglas H.} and Walsh, {Bradley J.}",

note = "Publisher Copyright: {\textcopyright} 2020 Elsevier Inc.",

year = "2020",

month = aug,

doi = "10.1016/j.urolonc.2020.03.010",

language = "English (US)",

volume = "38",

pages = "683.e11--683.e18",

journal = "Urologic Oncology: Seminars and Original Investigations",

issn = "1078-1439",

publisher = "Elsevier Inc.",

number = "8",

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T1 - Development and evaluation of the MiCheck test for aggressive prostate cancer

AU - Shore, Neal D.

AU - Pieczonka, Christopher M.

AU - Henderson, R. Jonathan

AU - Bailen, James L.

AU - Saltzstein, Daniel R.

AU - Concepcion, Raoul S.

AU - Beebe-Dimmer, Jennifer L.

AU - Ruterbusch, Julie J.

AU - Levin, Rachel A.

AU - Wissmueller, Sandra

AU - Le, Thao Ho

AU - Gillatt, David

AU - Chan, Daniel W.

AU - Campbell, Douglas H.

AU - Walsh, Bradley J.

PY - 2020/8

Y1 - 2020/8

N2 - Background: A clinical need exists for a biomarker test to accurately delineate aggressive prostate cancer (AgCaP), and thus better assist clinicians and patients decision-making on whether to proceed to prostate biopsy. Objectives: To develop a blood test for AgCaP and compare to PSA, %free PSA, proPSA, and prostate health index (PHI) tests. Design, settings and participants: Patient samples from the MiCheck-01 trial were used for development of the MiCheck test. Methods: Serum analyte concentrations for cellular growth factors were determined using a custom-made Luminex-based R&D Systems multianalyte kit. Outcome measurements and statistical analysis: Bayesian model averaging and random forest approaches were used to identify clinical factors and growth factors able to distinguish between men with AgCaP (Gleason Score [GS] ≥3+4) from those with non-AgCaP (GS 3+3). Logistic regression and Monte Carlo cross-validation identified variable combinations in order to able to maximize differentiation of AgCaP from non-AgCaP. Results: The MiCheck logistic regression model was developed and comprises the following variables: serum prostate-specific antigen (PSA), patient age, Digital Rectal Exam (DRE) status, Leptin, IL-7, vascular endothelial growth factor, and Glypican-1. The model differentiated AgCaP from non-AgCaP with an area under the curve of 0.83 and was superior to PSA, %free PSA and PHI in all patient groups, regardless of PSA range. Applying the MiCheck test to all evaluable biopsy patients from the MiCheck-01 study demonstrated that up to 30% of biopsies could be avoided while delaying diagnosis of only 6.8% of GS ≥3+4 cancers, 5% of GS ≥4+3 cancers and no cancers of GS 8 or higher. Conclusions: The MiCheck test outperforms PSA, %free PSA and PHI tests in differentiating AgCaP vs. non-AgCaP patients. The MiCheck test could result in a significant number of biopsies being avoided with a low number of patients experiencing a delayed diagnosis.

AB - Background: A clinical need exists for a biomarker test to accurately delineate aggressive prostate cancer (AgCaP), and thus better assist clinicians and patients decision-making on whether to proceed to prostate biopsy. Objectives: To develop a blood test for AgCaP and compare to PSA, %free PSA, proPSA, and prostate health index (PHI) tests. Design, settings and participants: Patient samples from the MiCheck-01 trial were used for development of the MiCheck test. Methods: Serum analyte concentrations for cellular growth factors were determined using a custom-made Luminex-based R&D Systems multianalyte kit. Outcome measurements and statistical analysis: Bayesian model averaging and random forest approaches were used to identify clinical factors and growth factors able to distinguish between men with AgCaP (Gleason Score [GS] ≥3+4) from those with non-AgCaP (GS 3+3). Logistic regression and Monte Carlo cross-validation identified variable combinations in order to able to maximize differentiation of AgCaP from non-AgCaP. Results: The MiCheck logistic regression model was developed and comprises the following variables: serum prostate-specific antigen (PSA), patient age, Digital Rectal Exam (DRE) status, Leptin, IL-7, vascular endothelial growth factor, and Glypican-1. The model differentiated AgCaP from non-AgCaP with an area under the curve of 0.83 and was superior to PSA, %free PSA and PHI in all patient groups, regardless of PSA range. Applying the MiCheck test to all evaluable biopsy patients from the MiCheck-01 study demonstrated that up to 30% of biopsies could be avoided while delaying diagnosis of only 6.8% of GS ≥3+4 cancers, 5% of GS ≥4+3 cancers and no cancers of GS 8 or higher. Conclusions: The MiCheck test outperforms PSA, %free PSA and PHI tests in differentiating AgCaP vs. non-AgCaP patients. The MiCheck test could result in a significant number of biopsies being avoided with a low number of patients experiencing a delayed diagnosis.

KW - Aggressive

KW - Biomarker

KW - Clinical study

KW - Prostate

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Development and evaluation of the MiCheck test for aggressive prostate cancer

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