Overview
The goal of this clinical study is to to improve diagnosis, follow-up and treatment for patients with disseminated prostate cancer.
The aim is to isolate tumour cells before image diagnostic methods find the metastases. In addition, investigators will use this method to characterise the tumour cells at the "single-cell" level to understand both the metastasis process, early resistance mechanisms and thus find new treatment targets to optimise individualised treatment.
Research subjects who either have disseminated disease at diagnosis or have recurrence after surgery (with minimal dissemination) will be included. A control population of young men without cancer will also be recruited to distinguish tumor-specific changes from normal signals using these new methods.
Description
In this prospective clinical study, led by Umeå University, all research subjects will undergo apheresis and subjects with cancer will also undergo multiple radiological examinations to both identify apheresis and subsequent experimental protocols for isolation of tumor cells, immune cells and other components from the blood. The goal is to increase the sensitivity of identifying circulating tumor cells in early-stage metastatic prostate cancer for molecular characterization without biopsies of metastases. By doing this on multiple occasions in primary metastatic prostate cancer, investigators will identify early resistance mechanisms to given treatment and also investigate immune changes to standard treatment of metastatic prostate cancer (castration). Through qualitative approach, investigators will identify healthy and risk factors for managing the diagnosis of metastatic prostate cancer and the experience of undergoing apheresis to identify circulating tumor cells (CTC) in the blood, with the aim of identifying possible risks for mental health with this research.
Eligibility
Inclusion Criteria:
-The patient (arm 1 and arm 2) must have a health status that minimises the already low risks of the apheresis treatment, have the logistical possibilities to come to the visits according to the study and be planned for treatment according to standard treatment in Sweden today.
For arm 1, 2 and 3:
- Venous blood vessels enabling apheresis
- ECOG-performance status 0-2
- Concentration of av potassium, calcium and magnesium in blood within normal range
- Testosterone>1,7 nmol/L
- Hb>90 g/L
- TPK >50x10exp9 /L
- LPK >1x10exp9 /L
- Bilirubin <1,4 x upper limit for normal (unless the subject suffers from Gilberts disease)
- ALAT or ASAT <2,4 x above limit for normal
- Creatinine <2 mg/dL (<177µmol/L)
Additional inclusion criteria for Arm 1 - Metastatic prostate cancer
One of the following criteria:
- PSA >100ng/ml
- Skeletal metastases with high risk of prostate cancer (regardless of PSA-value)
Additional inclusion criteria for Arm 2 - PSA relapse after operation
All of the three following criteria must be fulfilled:
- Prostatectomy
- PSA >0.2ng/ml
- PSA doubling time <18 months (according to www.mskcc.org/nomograms/prostate/psa_doubling_time)
Additional inclusion criteria for Arm 3 - Healthy research subjects (control group)
All of the following two criteria must be fulfilled:
- Previously healthy (no ongoing medication)
- No history of cancer
Exclusion Criteria for arm 1, 2 and 3:
- Overall, research subjects must not have any other cancer disease or risk factors for undergoing apheresis treatment
- Weight <50 kg
- Medical castration last 6 months (or previous surgical castration)
- Antiandrogen treatment in the last 6 months
- Previous myocardial infarction, stroke, chronic heart failure, atrial fibrillation or multiple deep vein thromboses
- Heart rate <45
- Systolic blood pressure below 100
- Ongoing diagnosed chronic inflammation