SEPTA Trial: Stockholm3 Validation Study in a Multi-Ethnic Cohort for ProsTAte Cancer
Description
Brief Summary
Introduction: Prostate cancer (PCa) is the most commonly detected cancer in men and is the
second leading cause of cancer death. Differences in race and ethnicity have been shown to
have differences in PCa incidence, detection, and outcomes. Current prostate cancer screening
involves prostatic specific antigen (PSA) which is a nonspecific protein marker (aka
kallikrein) that can often leads to unnecessary biopsies (up to 74% benign biopsies) and
clinical overdiagnosis (with up to 22% clinically insignificant cancer). Recently more
sophisticated tests have been developed for PCa screening in the United States such as the
Prostate Health Index (PHI) and the 4k (kallikrein) score, as well as clinical models that
use information from the patient clinical history. However, these tests utilize limited serum
protein assays and none of the established screening protocols utilize genetic variables to
help account for the likely inherited risks as seen in different ethnicities.
A recent Swedish, prospective, population-based study, published in the Lancet Oncology,
developed a unique multivariable biopsy outcome prediction model within a Nordic population
of nearly 60,000 men. This model, the Stockholm3, which incorporated plasma protein markers,
germline DNA SNPs as well as clinical variables, was shown to be capable of reducing the
number of biopsies by 44% compared to PSA while maintaining adequate sensitivity for
detection of PCa.
It is unknown whether an approach developed in Sweden that incorporates protein markers,
genetics, clinical variables, and genetic ancestry would be beneficial in a racially diverse
cohort.
Hypothesis: The investigators hypothesize that, a prospectively studied multiethnic cohort of
men with the Stockholm3 test will identify unique and common risk factors that improve
prostate cancer detection.
Aim: To assess the performance of the Stockholm3 test as compared to PSA and to identify
unique features associated with PCa in Black/African American (n=500), Asian (n=500),
White/Caucasian Hispanic (n=500), and White/Caucasian Non-Hispanic (n=500) men.
Methods: The investigators propose a prospectively identified cohort with participating
institutions which have screened positive to undergo a prostate biopsy to have a
retrospective analysis the Stockholm3 test and ancestry markers. Within this cohort the
investigators will examine several predetermined risk factors to investigate their
relationship to prostate cancer.
This blood sample will be tested for quantitative levels of serum protein markers and DNA
will be extracted and will be tested for germline mutations as defined by the Stockholm3 test
and other ancestry informative markers. Results from the study will be presented in such a
way that no individual information will be disclosed.
Detailed Description
Study Design and Procedures:
The research coordinator will explain the information contained within the consent.
Additionally, patient's blood will be drawn prior to their biopsy.
Prior to the biopsy, blood will be collected in x2 ethylenediaminetetraacetic acid (EDTA) 4
ml tubes after obtaining consent from the subjects. One tube will be immediately centrifuged
(10 minutes at 2000G) and plasma decanted to a tube without additives (this typically
produces 1.5 ml of plasma). The decanted tube (with plasma) and the remaining EDTA tube (with
whole blood) is then frozen and stored at the designated participating institutional site. It
will be stored at -20 Celsius until being shipped. The SEPTA specific blood collection is
followed by the following collaborators: Uropartners, University of Illinois at Chicago,
University of Chicago, Rush Medical Center, Montefiore, University of Texas Health Science
Center of San Antonio, Urology Clinics of North Texas, University of Southern California Keck
School of Medicine, Los Angeles County Hospital, Stanford University.
Additional samples from University Health Network (Toronto), Northwestern Medicine, John H.
Stroger, Jr. Hospital of Cook County, and Cook County Health System (Chicago) will be
included from biobanked sources which were prospective collected meeting inclusion and
exclusion criteria.
Patient data will be stored in a REDCap database, hosted on Sweden's secure server. Data will
be stored for the duration of the study, and 5 years afterwards for data analysis purposes.
Consented patients will be tracked by patient logs by each participating institution. The
medical record number will be collected to keep a consistent identifier for data collection
by key site personnel. Once all the patient data is recorded the data will be exported from
REDCap with the MRN removed. There will be no patient identifiers used at the Karolinska
Institute or A3P lab. The following PHI and non-PHI information will be logged of the
patient:
PHI:
Medical record number (MRN)
Non-PHI Demographic data
- Stockholm3 Identification number
- Race
- Zip code
Clinical data
- Total PSA
- Age on sampling date [years]
- Family history of prostate cancer
- Use of 5-alpha reductase inhibitors
- Earlier biopsy conducted
- Prostate volume [Prostate volume as measure with US]
- Digital rectal exam status [Benign/normal, Nodule/induration felt, Asymmetry, Not
performed]
AND
Outcome data - Results from biopsy performed immediately after blood venipuncture, i.e.:
Results will be separated into targeted biopsy cores and systematic biopsy cores
- Gleason Score 1
- Gleason Score 2
- Gleason Sum
- Cancer length (mm) (total and highest grade)
- Number of cores
- Number of positive cores
- Time to perform biopsy after blood draw [days]
- Results from MRI, i.e. Prostate Imaging Reporting & Data System (PIRADS) (0, 1, 2, 3, 4,
5)
Permitted use:
To run the Stockholm3 test defined by Gronberg et al AND Ancestry informative genetic markers
Samples will be shipped to the Uppsala based laboratory (A23 Laboratory) in Sweden for
analysis. Each patient will have two blood samples (plasma and whole blood) and will be
frozen at -20 Celsius. The blood samples will then be tested for quantitative levels of serum
protein levels and DNA will be extracted from white blood cells and will be tested for gene
and small nucleotide polymorphic (SNPs) germline mutations and variants .
Genotyping will be performed using custom genotyping assays. Plasma will be used for protein
analysis. Plasma protein analysis will be performed using a custom protein assays including
total and free PSA, human glandular kallikrein 2 (hK2), microseminoprotein-beta (MSMB), and
Macrophage inhibitory cytokine 1 (MIC-1). PSA will be tested with a commercial assay.
Based on the results from the plasma protein analysis, the genetic analysis and clinical
data, the Stockholm3 Risk Score will be calculated. The participants' samples will be treated
in accordance with the regulations of Sweden at the laboratory based in Uppsala, Sweden.
Results of the tests will not be shared with the patient, nor will the results change or
impact medical decisions.
Expected Risks/Benefits
Anticipated Risks:
As this is retrospective analysis of deidentified patient information as well as deidentified
biospecimens, there are few anticipated risks. A confidentiality breach as well as loss of
privacy are possible, however every effort will be made to minimize this risk.
Anticipated Benefits:
Participants will advance scientific and clinical knowledge. Participants will also receive a
small payment for the time and involvement in the study.
Data Collection and Management Procedures
This study will utilize REDCap (Research Electronic Data Capture), a software toolset and
workflow methodology for electronic collection and management of clinical and research data,
to collect and store data. The Karolinska Institute Information Technology (KI-IT) Department
will be used as a central location for data processing and management. REDCap is hosted by
KI-IT in the Biomedicum (Solnavägen 9, Solna, Sweden 17165)
Data Analysis
Data analysis will be performed by the PI, co-investigators and/or key research personnel.
Quality Control and Quality Assurance
Key research personnel will be responsible for ensuring all data collected adheres to the
protocol.
Data and Safety Monitoring
This study is minimal risk and all efforts will be made to ensure there are no
confidentiality breaches as well as no loss of privacy.
Statistical Considerations
Power analysis This study is being conducted among several sites and thus pooled analysis
will be performed. Based on the framework developed a two-sided alpha of 0.05, 250 men in
each ethnicity gives 80% power to detect 10 percentage points differences in sensitivity
and/or specificity of the Stockholm3 test across different ethnicities. Pooled data from
several sites will allow for comparison between non-Hispanic White, Africa/Black, Asian, and
Hispanic White men. Within each ethnicity group of 250 men, the same sample size gives a 90%
power for detecting differences in area under curve (AUC) between Stockholm3 and PSA for
detection of PC that are at least 10 percentage points (primary aim).
Goal accruement is 500 men within each race/ethnicity, interim analysis will be performed
when 250 men in each race/ethnicity is enrolled.
Data Analysis Descriptive univariate statistics will be used to compare groups. Binary
endpoints will be assessed with a logistic regression model. Statistical analysis will
involve logistic regression modeling, AUC calculation, calibration analyses and calculation
of basic performance characteristics (sensitivity, specificity and predictive values).
Regulatory Requirements
Informed Consent The participants indicate their consent to participate in the study by
signing informed consents for accessing medical records, conducting genetic research and
undergoing venipuncture for blood samples.
Subject Confidentiality Data used for this study will be stored in REDCaps and all data
transferred between institutions will remain deidentified throughout the study.
Unanticipated Problems Any unanticipated problems will be immediately reported to the
Site-specific ethical review board by designated research personnel.
Phase
N/AInclusion and Exclusion Criteria
- All men (age 45.0
- 75.0 years), regardless of race, presenting to a practicing urologist with symptoms that would lead to an evaluation for prostate cancer and who are scheduled to receive a needle biopsy of the prostate
- No prior diagnosis of prostate cancer
- Men who in the three (3) months prior to study participation received any invasive urologic procedure such as biopsy, thermotherapy, microwave therapy, laser therapy, transurethral resection of the prostate (TURP), urethral catheterization, and lower genitourinary tract endoscopy (cystoscopy)
- Men who were subjected to DRE or prostate manipulation within five (5) days (120 hours) prior to blood sampling
Sites
Please contact the trial administrator to learn more about where you can participate in this trial. Please use the contact form on the right side.