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Evaluation of Efficacy of TOOKAD® (VTP) Versus Active Surveillance for Intermediate Risk Localized Prostate Cancer

Primary Purpose

Localized Prostate Cancer

Status
Withdrawn
Phase
Phase 3
Locations
United States
Study Type
Interventional
Intervention
TOOKAD®
Sponsored by
Steba Biotech S.A.
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Localized Prostate Cancer focused on measuring Prostatic Disease, Genital Neoplasm,male, Urogenital neoplasm, Genital disease,male, Male urogenital disease, Neoplasms, Neoplasms by site, Prostatic neoplasm, Carcinoma

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)MaleDoes not accept healthy volunteers

Inclusion Criteria:

  1. Men 18 years or older.
  2. Men who have chosen Active Surveillance as the treatment for their prostate cancer.
  3. Patients who have had a multiparametric MRI of the prostate performed and have undergone transrectal systematic biopsy plus biopsy of any lesions (or "areas") considered suspicious per the MRI (PIRADS version 2 score of 4 or 5) within 6 months before signing consent.
  4. Unilateral Grade Group 2 (Gleason grade 3+4=7) prostate cancer with a total length of Gleason pattern 4 no more than 2mm when measured in all systematic biopsy cores plus up to 1 core from each targeted biopsy lesion (if more than 1 core is taken from a given lesion the core with the longest length of pattern 4 will be included). Note: the presence and length of Grade Group 1 (Gleason score 3+3=6) cancer in the biopsy will not be considered when determining eligibility.
  5. Prostate cancer clinical stage up to cT2a, N0/Nx, M0/Mx.
  6. Prostate volume ≥20 mL and ≤80 mL
  7. Serum PSA ≤10 ng/mL.
  8. Patients with cT2a and PSA between 10 and 20 ng/mL will have appropriate imaging and work up to sufficiently exclude clinical evidence of bone metastases (e.g., bone scan, whole body MRI, PET scan, or equivalent). Patients with sites considered "suspicious" may be evaluated with confirmatory biopsy to determine eligibility. Patients with sites considered "definite" or "consistent with" bone metastases will be excluded.
  9. Men who are sexually active with women of childbearing potential must use contraceptive method with a failure rate of less than 1% per year. Contraception should be continued for a period of 90 days after the VTP procedure. The individual methods of contraception may be determined in consultation with the investigator.
  10. Signed Informed Consent Form.

Exclusion Criteria:

  1. Grade Group 3, 4 or 5 (≥ Gleason Score 4+3=7) cancer
  2. In patients with Grade Group 2 cancers, a total length of Gleason pattern 4 more than 2mm when measured in all systematic biopsy cores plus up to 1 core from each targeted biopsy lesion (if more than 1 core is taken from a given lesion, include the mm of pattern 4 in the 1 core with the longest length of pattern 4)
  3. Bilateral GG 2 cancer
  4. MRI evidence of extracapsular extension of cancer (MRI read as "definite", "frank" or "gross" ECE, or MRI lesion with >10mm capsular contact, in an area with biopsy proven cancer).
  5. Seminal vesicle invasion on DRE or MRI ("probable" or "consistent with")
  6. Radiographically suspicious lymph node involvement confirmed with biopsy or PET scan.
  7. Any prior or current treatment for prostate cancer, including but not limited to surgery, radiation therapy (external or brachytherapy) or chemotherapy;
  8. Life expectancy less than 10 years;
  9. Participation in another clinical study involving an investigational product that in the opinion of the investigator may interfere with the endpoints or investigational criteria of this study;
  10. Inability to understand the informed consent document, to give consent voluntarily or to complete the study tasks, especially inability to understand and fulfill the health-related QOL questionnaire;
  11. Any history of a definitively ablative procedure for benign prostatic disease, such as benign prostatic hyperplasia, including TURP, whether electrosurgical or thermal laser ablation; or high intensity frequency ultrasound (HIFU) or cryotherapy, for focal or total ablative therapy of the prostate.

  12. Any condition or history of illness or surgery that may pose an additional risk to men undergoing the VTP procedure such as:

    1. Medical conditions that preclude the use of general anesthesia;
    2. Any condition or history of active rectal inflammatory bowel disease or other factors which might increase the risk of fistula formation;
    3. Hormonal manipulation (excluding 5-alpha-reductase inhibitors) that alters androgen production within the previous 6 months;
    4. Oral anticoagulant drugs that could not be withdrawn at least 5 days prior to the VTP procedure or antiplatelet drugs (e.g. aspirin) that could not be withdrawn at least 5 days prior to the VTP procedure and for at least 3 days after VTP;
    5. Renal and hepatic disorders with values of >1.5 times the upper limit of normal (ULN) or blood disorders (upon clinician judgment);
    6. A history of sun hypersensitivity or photosensitive dermatitis.
    7. Any other condition or history of illness or surgery that in the opinion of the investigator might affect the conduct and results of the study or pose additional risks to the patient (e.g., cardiac or respiratory disease precluding general anesthesia, active urethral stricture disease).

Sites / Locations

  • Memorial Sloan-Kettering Cancer Center

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

No Intervention

Arm Label

TOOKAD®

Active Surveillance

Arm Description

TOOKAD® , lyophilized formulation, given at a dose of 4mg/Kg.

Active surveillance is one of the management strategy in men who have intermediate risk localised prostate cancer

Outcomes

Primary Outcome Measures

Rate of objective progression
To evaluate the difference in the rate of objective progression of cancer between men treated with TOOKAD -VTP and men managed with Active Surveillance for localized prostate cancer.

Secondary Outcome Measures

Rate of conversion to radical local or systemic therapy
To confirm the differences between men treated with VTP and men managed with Active Surveillance in overall rate of conversion to radical local or systemic therapy
Rate of conversion to radical local or systemic therapy following objective progression
To confirm the differences between men treated with VTP and men managed with Active Surveillance in overall rate of conversion to radical local or systemic therapy following objective progression
Rate of biopsy progression in the index lobe
To confirm the differences between men treated with VTP and men managed with Active Surveillance in the rate of biopsy progression in the index lobe (the lobe initially diagnosed with GG2 cancer) defined as: Any Grade Group 3 or higher cancer in a biopsy core of the index lobe Increase in total length of Gleason pattern 4 >1mm above baseline and >2mm in total length in a follow-up biopsy of the index lobe
Rate of clinical local or distant progression
The rate of clinical local or distant progression defined as any of the following: Clinical stage ≥ T3N0M0 cancer MRI evidence of extracapsular extension of cancer (MRI read as "definite", "frank" or "gross" ECE, or MRI lesion with >10mm capsular contact) in an area with biopsy proven cancer. Seminal vesicle invasion, identified as "probable" or "definite," on DRE or MRI Radiographically suspicious lymph node involvement confirmed with biopsy or PET scan. Metastatic disease Prostate cancer-specific death
Adverse events and Serious Adverse events
The rate, severity, onset and duration of adverse events (AEs) and serious adverse events (SAEs)
FACT-P - Question GP5 - Bother Related to Adverse Events
The FACT-P is a multidimensional, self-report QoL instrument specifically designed for use with prostate cancer patients. It consists of 27 core items which assess patient function in four domains: Physical, Social/Family, Emotional, and Functional well-being. Only Question GP5 will be assessed to determine bother related to adverse events.
Urinary:PRO-CTCAE - Urinary Questions 61 - 65
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Urinary Questions 61 - 65 will be assessed
Pain: PRO-CTCAE Pain Question 48
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective.Only Pain Question 48 will be assessed
Bowel Symptoms: PRO-CTCAE questions 17 and 18
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Bowel Symptoms questions 17 and 18 will be assessed
Sexual Function: PRO-CTCAE questions 66-68 and 70-72
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Sexual Function questions 66-68 and 70-72 will be assessed
Anxiety = PRO-CTCAE question 54
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective.Only Anxiety question 54 will be assessed
Anxiety = MAX-PC Questions 15-18 - Anxiety related to fear of prostate cancer recurrence
The Memorial Anxiety Scale for Prostate Cancer (MAX-PC) has been developped to facilitate the identification and assessment of men with prostate cancer-related anxiety. This scale consists of three subscales that measure general prostate cancer anxiety, anxiety related to prostate specific antigen (PSA) levels in particular, and fear of recurrence. Only Anxiety Questions 15-18 will be assessed
Assessment feasibility of performing radical, local or systemic treatment
The physician will evaluate the ease or difficulties of radical, local or systemic therapy after VTP procedure using a scale . The instrument to be used to assess feasibility of performing RT will be a 5-point Likert Scale. The question may be similar to the following: "What was the difficulty in performing radical treatment on the subject" and proposed anwers will be: None, Minimal, Moderate, Severe or Extreme
Safety of radical, local or systemic treatment
Safety recorded as incidence of Adverse events and Serious Adverse Events
Biochemical outcomes of radical, local or systemic treatment
Biochemical Response recorded as serum PSA change as absolute measurement in ng/dL and as percentage increase or decrease over time
Clinical recurrence
Clinical recurrence recorded as physician recorded objective recurrence of tumor on physical exam or imaging.
Primary cause for conversion to radical treatment
Identification of the primary cause for conversion to radical treatment as assessed by physician: Pre-defined cancer progression Changes in clinical parameters in absence of objective progression (physicial examination findings, PSA, imaging (MRI, CT, PET), biopsy, or other tests to be documented such as genomic tests) Significant change in anxiety about prostate cancer (Defined as increase of last MAX-PC (Memorial Anxiety Scale for Prostate Cancer)-fear of recurrence score prior to conversion to radical therapy by 3 points or more vs. baseline) in the absence of objective progression or change in clinical parameters Patient preference in absence of objective progression, change in clinical parameters, or documented prostate cancer anxiety
Assessment of PSA Level
Assessment of PSA level in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA serum level to be recorded as ng/ml
Assessment of PSA density
Assessment of PSA density in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA density is calculated as total PSA (ng/ml) divided by prostate volume (ml).
Assessment of PSA kinetics
Assessment of PSA kinetics in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA kinetics is evaluated as change in PSA serum level in ng/ml over time.
Assessment of MRI dynamic characteristics (change in size of initial lesions)
Change in size of initial lesion on MRI in cm3
Assessment of MRI dynamic characteristics (change in PIRADS v2 score of initial lesions)
Change in PIRADS v2 Score of initial lesion
Assessment of MRI dynamic characteristics (Development of new lesions)
Incidence of new lesions discovered
Assessment of MRI dynamic characteristics (Changes in level of suspicion for ECE, SVI, LN metastases)
Changes in imaging results to indicate potential progression of prostate cancer outside the prostate gland (Changes in level of suspicion for Extra Capsular Extension (ECE), Semical vesicle invasion (SVI), Lymph node (LN) metastases used to identify local recurrence, and local, regional or distant progression).

Full Information

First Posted
December 26, 2019
Last Updated
November 10, 2020
Sponsor
Steba Biotech S.A.
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1. Study Identification

Unique Protocol Identification Number
NCT04225299
Brief Title
Evaluation of Efficacy of TOOKAD® (VTP) Versus Active Surveillance for Intermediate Risk Localized Prostate Cancer
Official Title
An Evaluation of the Efficacy of Partial Gland Ablation (PGA) With TOOKAD® Vascular Targeted Photodynamic Therapy (VTP) Versus Active Surveillance for Men With Intermediate Risk Localized Prostate Cancer
Study Type
Interventional

2. Study Status

Record Verification Date
October 2020
Overall Recruitment Status
Withdrawn
Why Stopped
FDA didn't approve the design of the protocol so we didn't start the study
Study Start Date
March 31, 2020 (Anticipated)
Primary Completion Date
March 31, 2030 (Anticipated)
Study Completion Date
July 1, 2030 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Steba Biotech S.A.

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
Multi-center, prospective, randomized controlled clinical trial that will compare two treatment methods (PGA with TOOKAD® VTP and Active Surveillance) for treating localized prostate cancer. The study will include criteria for evaluation, biopsy, eligibility, informed consent, subsequent management and decision making conducted based on data provided locally at each center that follow a set of standardized criteria.
Detailed Description
The primary endpoint requires follow-up through 30 months, but all subjects will be followed for 72 months regardless of initiation of other local or systemic prostate cancer treatments, which will allow assessments of recurrence rates and morbidity after conversion to radical therapy, long-term safety and tolerability, as well as oncologic outcomes. This is multi-center, prospective, randomized controlled phase III clinical trial that will compare two treatment methods (PGA with TOOKAD® VTP and Active Surveillance) for treating localized prostate cancer who meet the inclusion criteria will be approached for participation in the clinical study. Patients consenting to participate will be individually randomized to TOOKAD® VTP or Active Surveillance with a 1:1 ratio. Central randomization will be performed using an independent web-based allocation system. Randomization will be stratified by center using minimization. Ongoing assessment of patients in both arms will be balanced, including follow up examinations, PSA testing, MRI and biopsies at defined intervals. Subjects in the experimental arm will receive the experimental treatment consisting of unilateral TOOKAD® VTP treatment applied to the index lobe containing pattern 4 cancer. The treatment will be administered under general anesthesia. Routine ultrasound examination in the operating room will be performed for morphometric description of the prostate and to facilitate accurate treatment planning and probe placement. Ultrasound will not be used for diagnostic purposes.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Localized Prostate Cancer
Keywords
Prostatic Disease, Genital Neoplasm,male, Urogenital neoplasm, Genital disease,male, Male urogenital disease, Neoplasms, Neoplasms by site, Prostatic neoplasm, Carcinoma

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 3
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Randomized
Enrollment
0 (Actual)

8. Arms, Groups, and Interventions

Arm Title
TOOKAD®
Arm Type
Experimental
Arm Description
TOOKAD® , lyophilized formulation, given at a dose of 4mg/Kg.
Arm Title
Active Surveillance
Arm Type
No Intervention
Arm Description
Active surveillance is one of the management strategy in men who have intermediate risk localised prostate cancer
Intervention Type
Drug
Intervention Name(s)
TOOKAD®
Other Intervention Name(s)
WST11
Intervention Description
TOOKAD® -VTP procedure will consist of an IntraVenous (IV) administration to patients using a 753nm laser light at a fixed power of 150mW/cm and a fixed energy at 200J/cm delivered through transperineal interstitial optical fibers. The needles are positioned in the prostate under ultra sound image guidance
Primary Outcome Measure Information:
Title
Rate of objective progression
Description
To evaluate the difference in the rate of objective progression of cancer between men treated with TOOKAD -VTP and men managed with Active Surveillance for localized prostate cancer.
Time Frame
over 30 months
Secondary Outcome Measure Information:
Title
Rate of conversion to radical local or systemic therapy
Description
To confirm the differences between men treated with VTP and men managed with Active Surveillance in overall rate of conversion to radical local or systemic therapy
Time Frame
over 30 and 72 months
Title
Rate of conversion to radical local or systemic therapy following objective progression
Description
To confirm the differences between men treated with VTP and men managed with Active Surveillance in overall rate of conversion to radical local or systemic therapy following objective progression
Time Frame
over 30 and 72 months
Title
Rate of biopsy progression in the index lobe
Description
To confirm the differences between men treated with VTP and men managed with Active Surveillance in the rate of biopsy progression in the index lobe (the lobe initially diagnosed with GG2 cancer) defined as: Any Grade Group 3 or higher cancer in a biopsy core of the index lobe Increase in total length of Gleason pattern 4 >1mm above baseline and >2mm in total length in a follow-up biopsy of the index lobe
Time Frame
at 30 and 72 months
Title
Rate of clinical local or distant progression
Description
The rate of clinical local or distant progression defined as any of the following: Clinical stage ≥ T3N0M0 cancer MRI evidence of extracapsular extension of cancer (MRI read as "definite", "frank" or "gross" ECE, or MRI lesion with >10mm capsular contact) in an area with biopsy proven cancer. Seminal vesicle invasion, identified as "probable" or "definite," on DRE or MRI Radiographically suspicious lymph node involvement confirmed with biopsy or PET scan. Metastatic disease Prostate cancer-specific death
Time Frame
Screening,Month 12, Month 24,Month 42 and Month 60
Title
Adverse events and Serious Adverse events
Description
The rate, severity, onset and duration of adverse events (AEs) and serious adverse events (SAEs)
Time Frame
Screening-Month 72
Title
FACT-P - Question GP5 - Bother Related to Adverse Events
Description
The FACT-P is a multidimensional, self-report QoL instrument specifically designed for use with prostate cancer patients. It consists of 27 core items which assess patient function in four domains: Physical, Social/Family, Emotional, and Functional well-being. Only Question GP5 will be assessed to determine bother related to adverse events.
Time Frame
Screening,Week 2, Week 4, Week 6, Week 8, Month 3, Month 4, Month 5, Month 6, Month 12, Month 18, Month 24, and Month 36
Title
Urinary:PRO-CTCAE - Urinary Questions 61 - 65
Description
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Urinary Questions 61 - 65 will be assessed
Time Frame
Screening,Week 2, Week 4, Week 6, Week 8, Month 3, Month 4, Month 5, Month 6, Month 12, Month 18, Month 24, and Month 36
Title
Pain: PRO-CTCAE Pain Question 48
Description
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective.Only Pain Question 48 will be assessed
Time Frame
Screening,Week 2, Week 4, Week 6, Week 8, Month 3, Month 4, Month 5, Month 6, Month 12, Month 18, Month 24, and Month 36
Title
Bowel Symptoms: PRO-CTCAE questions 17 and 18
Description
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Bowel Symptoms questions 17 and 18 will be assessed
Time Frame
Screening,Week 4, Week 8, Month 3, Month 6, Month 12, Month 18, Month 24, and Month 36, Month 48, Month 60, and Month 72
Title
Sexual Function: PRO-CTCAE questions 66-68 and 70-72
Description
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective. Only Sexual Function questions 66-68 and 70-72 will be assessed
Time Frame
Screening,Week 4, Week 8, Month 3, Month 6, Month 12, Month 18, Month 24, and Month 36, Month 48, Month 60, and Month 72
Title
Anxiety = PRO-CTCAE question 54
Description
The NCI Patient Reported Outcomes-Common Terminology Criteria for Adverse Events (PRO-CTCAE) is a new patient-reported outcome measurement system developed to characterize the frequency, severity and interference of 78 symptomatic treatment toxicities. These include symptomatic toxicities such as pain, fatigue, nausea, and cutaneous side effects such as rash and hand-foot syndrome, all toxicities that can be meaningfully reported from the patient perspective.Only Anxiety question 54 will be assessed
Time Frame
Screening,Week 4, Week 8, Month 3, Month 6, Month 12, Month 18, Month 24, and Month 36, Month 48, Month 60, and Month 72
Title
Anxiety = MAX-PC Questions 15-18 - Anxiety related to fear of prostate cancer recurrence
Description
The Memorial Anxiety Scale for Prostate Cancer (MAX-PC) has been developped to facilitate the identification and assessment of men with prostate cancer-related anxiety. This scale consists of three subscales that measure general prostate cancer anxiety, anxiety related to prostate specific antigen (PSA) levels in particular, and fear of recurrence. Only Anxiety Questions 15-18 will be assessed
Time Frame
Screening,Month 6, Month 12, Month 18, Month 24, and Month 36, Month 48, Month 60, and Month 72
Title
Assessment feasibility of performing radical, local or systemic treatment
Description
The physician will evaluate the ease or difficulties of radical, local or systemic therapy after VTP procedure using a scale . The instrument to be used to assess feasibility of performing RT will be a 5-point Likert Scale. The question may be similar to the following: "What was the difficulty in performing radical treatment on the subject" and proposed anwers will be: None, Minimal, Moderate, Severe or Extreme
Time Frame
within 90 days after treatment
Title
Safety of radical, local or systemic treatment
Description
Safety recorded as incidence of Adverse events and Serious Adverse Events
Time Frame
within 90 days after treatment
Title
Biochemical outcomes of radical, local or systemic treatment
Description
Biochemical Response recorded as serum PSA change as absolute measurement in ng/dL and as percentage increase or decrease over time
Time Frame
6 weeks and 24 months after treatment
Title
Clinical recurrence
Description
Clinical recurrence recorded as physician recorded objective recurrence of tumor on physical exam or imaging.
Time Frame
6 weeks and 24 months after treatment
Title
Primary cause for conversion to radical treatment
Description
Identification of the primary cause for conversion to radical treatment as assessed by physician: Pre-defined cancer progression Changes in clinical parameters in absence of objective progression (physicial examination findings, PSA, imaging (MRI, CT, PET), biopsy, or other tests to be documented such as genomic tests) Significant change in anxiety about prostate cancer (Defined as increase of last MAX-PC (Memorial Anxiety Scale for Prostate Cancer)-fear of recurrence score prior to conversion to radical therapy by 3 points or more vs. baseline) in the absence of objective progression or change in clinical parameters Patient preference in absence of objective progression, change in clinical parameters, or documented prostate cancer anxiety
Time Frame
Over 30 and 72 months
Title
Assessment of PSA Level
Description
Assessment of PSA level in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA serum level to be recorded as ng/ml
Time Frame
Screening, Day of VTP ,Month 6, Month 18, Month 30, Month 36, Month 48 and Month 72
Title
Assessment of PSA density
Description
Assessment of PSA density in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA density is calculated as total PSA (ng/ml) divided by prostate volume (ml).
Time Frame
Screening, Day of VTP ,Month 6, Month 18, Month 30, Month 36, Month 48 and Month 72
Title
Assessment of PSA kinetics
Description
Assessment of PSA kinetics in predicting or monitoring oncologic outcomes of local recurrence, and local or systemic progression. PSA kinetics is evaluated as change in PSA serum level in ng/ml over time.
Time Frame
Screening, Day of VTP ,Month 6, Month 18, Month 30, Month 36, Month 48 and Month 72
Title
Assessment of MRI dynamic characteristics (change in size of initial lesions)
Description
Change in size of initial lesion on MRI in cm3
Time Frame
Screening, Month 12,Month 24, Month 42 and Month 60
Title
Assessment of MRI dynamic characteristics (change in PIRADS v2 score of initial lesions)
Description
Change in PIRADS v2 Score of initial lesion
Time Frame
Screening, Month 12,Month 24, Month 42 and Month 60
Title
Assessment of MRI dynamic characteristics (Development of new lesions)
Description
Incidence of new lesions discovered
Time Frame
Month 12,Month 24, Month 42 and Month 60
Title
Assessment of MRI dynamic characteristics (Changes in level of suspicion for ECE, SVI, LN metastases)
Description
Changes in imaging results to indicate potential progression of prostate cancer outside the prostate gland (Changes in level of suspicion for Extra Capsular Extension (ECE), Semical vesicle invasion (SVI), Lymph node (LN) metastases used to identify local recurrence, and local, regional or distant progression).
Time Frame
Screening, Month 12,Month 24, Month 42 and Month 60

10. Eligibility

Sex
Male
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Men 18 years or older. Men who have chosen Active Surveillance as the treatment for their prostate cancer. Patients who have had a multiparametric MRI of the prostate performed and have undergone transrectal systematic biopsy plus biopsy of any lesions (or "areas") considered suspicious per the MRI (PIRADS version 2 score of 4 or 5) within 6 months before signing consent. Unilateral Grade Group 2 (Gleason grade 3+4=7) prostate cancer with a total length of Gleason pattern 4 no more than 2mm when measured in all systematic biopsy cores plus up to 1 core from each targeted biopsy lesion (if more than 1 core is taken from a given lesion the core with the longest length of pattern 4 will be included). Note: the presence and length of Grade Group 1 (Gleason score 3+3=6) cancer in the biopsy will not be considered when determining eligibility. Prostate cancer clinical stage up to cT2a, N0/Nx, M0/Mx. Prostate volume ≥20 mL and ≤80 mL Serum PSA ≤10 ng/mL. Patients with cT2a and PSA between 10 and 20 ng/mL will have appropriate imaging and work up to sufficiently exclude clinical evidence of bone metastases (e.g., bone scan, whole body MRI, PET scan, or equivalent). Patients with sites considered "suspicious" may be evaluated with confirmatory biopsy to determine eligibility. Patients with sites considered "definite" or "consistent with" bone metastases will be excluded. Men who are sexually active with women of childbearing potential must use contraceptive method with a failure rate of less than 1% per year. Contraception should be continued for a period of 90 days after the VTP procedure. The individual methods of contraception may be determined in consultation with the investigator. Signed Informed Consent Form. Exclusion Criteria: Grade Group 3, 4 or 5 (≥ Gleason Score 4+3=7) cancer In patients with Grade Group 2 cancers, a total length of Gleason pattern 4 more than 2mm when measured in all systematic biopsy cores plus up to 1 core from each targeted biopsy lesion (if more than 1 core is taken from a given lesion, include the mm of pattern 4 in the 1 core with the longest length of pattern 4) Bilateral GG 2 cancer MRI evidence of extracapsular extension of cancer (MRI read as "definite", "frank" or "gross" ECE, or MRI lesion with >10mm capsular contact, in an area with biopsy proven cancer). Seminal vesicle invasion on DRE or MRI ("probable" or "consistent with") Radiographically suspicious lymph node involvement confirmed with biopsy or PET scan. Any prior or current treatment for prostate cancer, including but not limited to surgery, radiation therapy (external or brachytherapy) or chemotherapy; Life expectancy less than 10 years; Participation in another clinical study involving an investigational product that in the opinion of the investigator may interfere with the endpoints or investigational criteria of this study; Inability to understand the informed consent document, to give consent voluntarily or to complete the study tasks, especially inability to understand and fulfill the health-related QOL questionnaire; Any history of a definitively ablative procedure for benign prostatic disease, such as benign prostatic hyperplasia, including TURP, whether electrosurgical or thermal laser ablation; or high intensity frequency ultrasound (HIFU) or cryotherapy, for focal or total ablative therapy of the prostate. Any condition or history of illness or surgery that may pose an additional risk to men undergoing the VTP procedure such as: Medical conditions that preclude the use of general anesthesia; Any condition or history of active rectal inflammatory bowel disease or other factors which might increase the risk of fistula formation; Hormonal manipulation (excluding 5-alpha-reductase inhibitors) that alters androgen production within the previous 6 months; Oral anticoagulant drugs that could not be withdrawn at least 5 days prior to the VTP procedure or antiplatelet drugs (e.g. aspirin) that could not be withdrawn at least 5 days prior to the VTP procedure and for at least 3 days after VTP; Renal and hepatic disorders with values of >1.5 times the upper limit of normal (ULN) or blood disorders (upon clinician judgment); A history of sun hypersensitivity or photosensitive dermatitis. Any other condition or history of illness or surgery that in the opinion of the investigator might affect the conduct and results of the study or pose additional risks to the patient (e.g., cardiac or respiratory disease precluding general anesthesia, active urethral stricture disease).
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Jonathan Coleman, MD
Organizational Affiliation
Memorial Sloan Kettering Cancer Center
Official's Role
Principal Investigator
Facility Information:
Facility Name
Memorial Sloan-Kettering Cancer Center
City
New York
State/Province
New York
ZIP/Postal Code
10021
Country
United States

12. IPD Sharing Statement

Learn more about this trial

Evaluation of Efficacy of TOOKAD® (VTP) Versus Active Surveillance for Intermediate Risk Localized Prostate Cancer

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