Male Erectile Disorder, Prostate Cancer, Therapy-related Toxicity, Urinary Incontinence
Conditions
Keywords
urinary incontinence, male erectile disorder, therapy-related toxicity, stage I prostate cancer, stage IIB prostate cancer, stage IIA prostate cancer
Brief summary
RATIONALE: Prospective trials using hemi-ablation with high intensity focused ultrasound (HIFU) (Sonablate 500) have demonstrated feasibility, safety, and encouraging functional outcomes and early cancer control with 90% of men achieving trifecta status (no erectile dysfunction, leak-free pad-free continence, cancer control). However, these trials have involved small numbers of patients with men selected for good baseline function. A multi-centre prospective trial within a larger cohort of men that better represents the patient population with prostate cancer (external validity) is required.
Detailed description
Verification of a new therapy as favourable, or equivalent, in outcome to 'standard' care is ideally sought through comparison with another matched control group. Randomised controlled trials (RCTs) offer the best method for minimising systematic bias and revealing the true effect of an intervention or drug. However, RCTs involving treatments of localised prostate cancer have had a historically poor patient uptake, as the reference 'gold' standard of care is not known. In addition, RCTs are expensive to run and involve huge infra-structural support. A number of trials in the USA have been forced to close due to lack of recruitment. The ProStart trial in the UK has also had to close for the same reason. It has been acknowledged by the Food and Drug Agency in the USA that comparative randomized trials will be problematic in this area due to lack of physician and patient equipoise. A randomized trial may be feasible if a pragmatic design is adopted but prior to acceptance of such a design, the number of centres with expertise in this complex intervention (mp-MRI, TTPM, focal HIFU) will need to be increased. Observational studies are a commonly used alternative to ascertain the effectiveness of a treatment. They are used to observe a treatment effect in a selected group of patients who are presumed to derive benefit from the treatment given. Although methodologically not as robust, and therefore prone to bias, they have some benefits over RCTs. The principal ones are those of enhanced external validity (many patients do not wished to be randomised and therefore refuse participation), and more rapid accrual compared to a randomised design. For this reasons, a single arm medium term follow-up cohort intervention study has been designed. At the time of writing the safety and tolerability aspects of focal therapy by HIFU are known as a result of the Phase I/II studies carried out at UCLH. The results have been presented and exist in the public domain in abstract form but have not yet been published (presented in tables above). These early studies were powered to detect a change in the proportion of men who could obtain an erection sufficient for penetration compared to their status prior to their treatment. The very low event rate for both erectile dysfunction and incontinence indicates that the 'proof of concept' has been demonstrated for focal therapy. Moreover, we can be relatively confident that, in expert hands, focal HIFU is safe. Therefore, a multi-centre study is now required involving a larger group of patients for the following reasons: 1. To evaluate medium term cancer control using histological parameters. Stage two of INDEX will evaluate conversion to radical and systemic therapies and link men to national databases to determine survival in 5 and 10 years. 2. To confirm that focal therapy can lead to low rates of genitourinary and rectal toxicity and minimal impact on quality of life within a large and more representative cohort of patients (greater precision around outcome measures). 3. To demonstrate that the skills (characterization through template prostate mapping and MRI as well as the treatment related skills) acquired by the team at UCLH are indeed transferable to other providers. 4. To calculate costs of care and to model potential cost-effectiveness in comparison to alternative therapies. If this single arm intervention study demonstrates acceptable outcomes to support the findings of the Phase I/II studies, it is anticipated that this preliminary study will lead onto a Phase III evaluation of focal therapy, prior to more widespread use of this technology.
Interventions
OTHERquestionnaire administration
PROCEDUREassessment of therapy complications
PROCEDUREquality-of-life assessment
PROCEDUREtransperineal prostate biopsy
PROCEDUREtransrectal prostate biopsy
Sponsors
University College, London
Study design
Allocation
NA
Intervention model
SINGLE_GROUP
Primary purpose
TREATMENT
Masking
NONE
Intervention model description
Multi-Centre Prospective Single Arm Intervention Trial
Eligibility
Sex/Gender
MALE
Age
No minimum to 90 Years
Healthy volunteers
No
Inclusion criteria
1. Histologically proven prostate cancer on trans-rectal or transperineal template prostate biopsies. 2. Prostate biopsy (either TRUS or MRI Targeted or Template): * TRUS biopsy: up to burden bilateral disease with maximum 3mm one biopsy on non-dominant side is allowable. * MRI targeted and/or Template biopsy within 12 months of entry showing: * unilateral disease minimum 3mm of Gleason 3+3 or any Gleason 3+4 or 4+3 but not exceeding Gleason 4+3 overall OR * bilateral disease presence of clinically significant cancer on only one side (as determined by histological rules described above) Gleason ≤7 which is concordant with the MRI findings. 3. Stage T1-T2cN0M0 disease, as determined by local guidelines (radiological T3a permitted). 4. Serum PSA \</=20ng/ml 5. Life expectancy of \>/=10 years. 6. Signed informed consent by patient. 7. An understanding of the English language sufficient to understand
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Conversion to radical therapy and/or requiring systemic therapy and/or developing metastases and/or dying of prostate cancer | 5 years | To determine the proportion of men converting to radical therapy and/or requiring systemic therapy and/or developing metastases and/or dying of prostate cancer following focal therapy for localised prostate cancer using HIFU |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| rate of erectile dysfunction | 12 months | The presence of severe erectile dysfunction at 12 months, as measured by the IIEF-5 questionnaire with or without the use of phosphodiesterase-5 inhibitors, in those with absence of severe erectile dysfunction at baseline |
| time to return of erectile function | 24 months | Time to return of erectile function (absence of severe ED on IIEF-15 questionnaire) |
| rate of urinary incontinence (pad free, leak free and pad-free alone) | 12 months | Presence of urinary incontinence (any pad usage plus any leakage of urine) as determined by the UCLA-EPIC urinary continence questionnaire, at 12 months, in those men with no urinary incontinence at baseline |
| time to return of continence (pad free, leak free and pad-free alone) | 24 months | Time to return of urinary continence (as determined by UCLA-EPIC Urinary domain questionnaire) |
| rate of loss of ejaculation | 24 months | rate of loss of ejaculation (as determined by IIEF-15 questionnaire) |
| rate of loss of orgasm | 24 months | rate of loss of orgasm (as determined by IIEF-15 questionnaire) |
| rate of pain during intercourse | 24 months | rate of pain during intercourse (as determined by IIEF-15 questionnaire) |
| rate of bowel toxicity | 24 months | UCLA-EPIC Bowel Function Questionnaire |
| number of men using phosphodiesterase-5 inhibitors to maintain erectile function | 24 months | Need for phosphodiesterase-5 inhibitors to maintain erectile function sufficient for penetration up to 24 months |
| anxiety levels | 24 months | EQ-5D Quality of Life Questionnaire |
| general health related quality of life | 24 months | General and prostate health related quality of life measured using EQ-5D Quality of Life questionnaire |
| proportion of men achieving trifecta status at 12 months | 12months | Achievement of trifecta status (no severe ED, pad-free leak-free continence, cancer control with absence of clinically significant cancer) at 12 months in those men with good baseline function |
| proportion of men achieving trifecta status at 24 months | 24 months | Achievement of trifecta status (no severe ED, pad-free leak-free continence, cancer control with absence of clinically significant cancer) at 24 months in those men with good baseline function |
| rate of secondary prostate cancer intervention (prostatectomy, radiotherapy, androgen ablation, whole-gland HIFU or cryosurgery) | 24 months | rate of secondary prostate cancer intervention (prostatectomy, radiotherapy, androgen ablation, whole-gland HIFU or cryosurgery) |
| risk factors for failure defined as a) presence of any cancer and b) clinically significant cancer at study end | 24 months | risk factors for failure defined as a) presence of any cancer and b) clinically significant |
| biochemical (PSA) kinetics including determining the optimal biochemical definition of failure | 24 months | biochemical (PSA) kinetics including determining the optimal biochemical definition of |
| describe composite outcomes of failure | 24 months | describe composite outcomes of failure |
| Cost-effectiveness | 5years | To determine the costs of treatment and model potential cost effectiveness using comparative cancer control and functional outcomes at 5 years compared to other cohort trials involving the management of localized prostate cancer |
| rate of lower urinary tract symptoms | 24 months | Grading of lower urinary tract symptoms as determined by IPSS scores |
Countries
United Kingdom
Outcome results
None listed