Clinical Trial Details
— Status: Active, not recruiting
Administrative data
| NCT number |
NCT02594072 |
| Other study ID # |
ASSERT |
| Secondary ID |
|
| Status |
Active, not recruiting |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
April 2016 |
| Est. completion date |
December 2024 |
Study information
| Verified date |
November 2023 |
| Source |
University of British Columbia |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Two radiation therapy techniques are commonly used for the treatment of intermediate and high
risk prostate cancer: brachytherapy and external beam radiation therapy (EBRT). However, both
have limitations. Brachytherapy, in which radioactive seeds are inserted into the prostate,
produces excellent outcomes but is invasive and not all patients are eligible or willing to
receive this treatment. EBRT, while gentle at the time of delivery, tends to be very
prolonged and may have poorer outcomes than brachytherapy. This study will examine the use of
stereotactic ablative radiotherapy (SABR), in which patients are given only a few, high dose
radiation treatments. Treatments are short, non-invasive, applicable to patients not able to
do brachytherapy, and may be more effective than conventional EBRT. This study will compare
SABR with EBRT in terms of the rates of acute and late toxicities for each treatment,
disease-free survival, and health-related quality of life measures.
Description:
The current study is a randomized phase II study comparing high speed, single arc,
LINAC-based prostate stereotactic ablative radiotherapy (SABR) with conventional external
beam radiation treatment (EBRT), along with androgen suppression (AS), in men with
intermediate and high risk prostate cancer, who are either unsuitable for or unwilling to
have brachytherapy. The two primary objectives of the study are to assess the feasibility of
randomization, and to compare the rates of acute and late toxicities. Should randomization
prove feasible, and toxicities comparable, a future phase 3 trial will be pursued.
Primary objectives:
1. To determine the proportion of eligible patients who are willing to be randomized
2. To estimate and compare the proportions of acute and late toxicities, focussing on grade
3 and 4 complications of the treatment interventions as delivered in the British
Columbia (BC) Cancer Agency
Secondary objectives:
1. To compare the disease free survival as reflected in biochemical relapse free survival
at five years between the two interventions
2. To compare the health related quality of life as reflected in changes on the EPIC
questionnaire between the two interventions
3. To quantify the degree of intra-fraction motion with the proposed SABR technique
Research Method
To determine the willingness of eligible patients to be randomized, a screening log
documenting the number of eligible subjects approached for participation will be maintained.
Subjects who are approached but who decline participation will undergo a short interview by
the Clinical Research Associate as to the reason for non-participation. The Clinical Research
Associate will read from a script with statements to make sure that subjects who refuse the
trial know that they are free to provide or not provide the reasons for declining the trial
and that their answers will not affect the care they will receive. They will be asked to list
up to five reasons for non-participation in the trial. At the conclusion of the trial,
qualitative analyses will be done for the reason of non-participation.
The two radiation treatment protocols, conventional EBRT and SABR, will be compared in a
randomized, phase II study.
Patients with biopsy-proven intermediate or high risk prostate cancer will be accrued. T3 or
T4 disease, men with International Prostate Symptom Score >20 and prostate volume > 90 cc are
not eligible. Men with high risk disease must have a <15% risk of pelvic lymph node
involvement to be eligible.
Eligible subjects will be identified by the treating oncologist and enrolled through the
clinical trials unit of the participating regional cancer centre. Once the consent form is
signed, a Study Entry Form will be sent to the trial administrative centre located at the
Vancouver Island Centre of the BC Cancer Agency. A Patient Identification Number will be
assigned and the patient will be randomized to a treatment arm. This study proposes that
eighty (80) patients be randomized in a 1:1 ratio.
Subjects randomized to Arm 1 (conventional EBRT) will receive 73.68 Gy in 28 fractions (5
treatment days per week over 5.5 weeks).
Subjects randomized to Arm 2 (SABR) will receive a prescribed dose of 36.25 Gy in 5 fractions
over 5 weeks (one treatment day per week).
Subjects randomized to the SABR arm will undergo an additional procedure prior to radiation
treatment to place gold seed fiducials (placement of gold seed fiducials is optional in the
EBRT arm and is at the discretion of the treating centre).
Androgen-Deprivation Therapy (ADT) will be administered to all patients on both treatment
arms. ADT will consist of luteinizing hormone-releasing hormone (LHRH) agonist monotherapy,
but total androgen blockade is also permitted at the discretion of the treating oncologist.
The total duration of ADT will be 6 months for men with intermediate risk disease, and 18
months for those with high risk disease. ADT is to be initiated prior to the start of RT.
PATIENT ASSESSMENTS AND FOLLOWUP
Pre-radiotherapy assessment:
All patients must have a biopsy indicating prostate adenocarcinoma within 365 days of trial
registration. A full history and physical examination, with digital rectal examination, must
be done within 60 days of registration. CT scan of the abdomen and pelvis and nuclear
medicine bone scan must be done within 60 days of registration. Baseline PSA and testosterone
must be done not more than 60 days before registration and repeated in the week before
radiotherapy to document response to androgen deprivation therapy. Physician assessment must
be done within 60 days of randomization. Baseline QOL assessment (EPIC), prostate symptom
score (IPSS), and sexual health inventory (SHIM) are to be done prior to the start of
radiotherapy.
Assessments during radiotherapy:
All patients will be seen by a radiation oncologist (or clinical associate) weekly during
radiotherapy. QOL assessment (EPIC), IPSS/SHIM, and adverse events assessment (CTCAEv4,
modified Radiation Therapy Oncology Group (RTOG)/SOMA) will be done during week 5 of
radiotherapy for both Arms 1 and 2.
Post-radiotherapy assessment and follow-up:
All patients will be assessed 2 weeks and 8 weeks post-radiotherapy, then every 6 months
until 2 years, and then yearly until year 5. At each of these time points patients will
undergo physician assessment, PSA/testosterone, QOL assessment (EPIC), IPSS/SHIM, and adverse
events assessment (CTCAEv4, modified RTOG/SOMA).
Data Analysis
Actuarial rates of acute (defined as occurring ≤ 6 months after initiation of treatment) and
late (defined as occurring > 6 months after initiation of treatment) as well as the
prevalence of late toxicities at 1, 2 and 5 years will be determined. Grade 3 and 4
toxicities will be compared between intervention groups using exact test statistics (SAS FREQ
procedure, SAS Gary, NC). Stratified analyses will also use the SAS FREQ procedure and
Zelen's exact test for equal odds ratios, exact confidence limits for the common odds ratio,
and an exact test for the common odds ratio. Quality of life scores and EPIC scales will be
compared between interventions using the t-test statistic.
