Minimally Invasive Prostatic Vapor Ablation for the Treatment of BPH in Large Prostates (Rezūm XL)
Status: | Recruiting |
---|---|
Healthy: | No |
Age Range: | 50 - Any |
Updated: | 3/15/2019 |
Start Date: | May 30, 2018 |
End Date: | December 30, 2022 |
Contact: | Laura Olson |
Email: | laura.olson2@bsci.com |
Phone: | 612-231-6525 |
Minimally Invasive Prostatic Vapor Ablation - Multicenter, Single Arm Study for the Treatment of BPH in Large Prostates (Rezūm XL)
Prospective, multicenter, single arm clinical trial designed to evaluate the safety of the
Rezūm System in treating subjects with symptomatic BPH for prostate sizes >80cm3 and ≤150
cm3.
Rezūm System in treating subjects with symptomatic BPH for prostate sizes >80cm3 and ≤150
cm3.
Inclusion Criteria:
1. Male subjects > 50 years of age who have symptomatic BPH.
2. International Prostate Symptom Score (IPSS) score ≥ 13.
3. Peak urinary flow rate (Qmax): ≥ 5ml/sec to ≤ 12 ml/sec with minimum voided volume of
≥ 125 ml.
4. Post-void residual (PVR) ≤300 ml.
5. Prostate volume >80 cm3 to ≤150 cm3
Exclusion Criteria:
Urology:
1. Any prior invasive prostate intervention (e.g., "Radiofrequency" thermotherapy,
balloon, microwave thermotherapy, "Prostatic Urethral Lift", "Transurethral
Resection", or laser) or other surgical interventions of the prostate.
2. Undergone a prostate biopsy within 60 days prior to the scheduled treatment date or
has an imminent need for surgery.
3. Verified acute bacterial prostatitis within last 12 months documented by culture.
4. Active or history of epididymitis within the past 3 months.
5. Urethral strictures, bladder neck contracture, unusual anatomy or muscle spasms that
would prevent the introduction and use of the Rezūm device.
6. Diagnosed bladder, urethral or ureteral stones or active stone passage in the past 6
months, provided that stones that are known to be in the kidney and have been stable
for a period exceeding 3 months are permissible.
7. Subject interested in maintaining fertility.
8. Use of the following medications where the dose is not stable (stable dose defined as
the same medication and dose in the last three months):
1. Beta-blockers;
2. Anticonvulsants;
3. Antispasmodics;
4. Antihistamines;
5. Alpha blockers for BPH and anticholinergics or cholinergics;
6. Type II, 5-alpha reductase inhibitor (e.g., finasteride (Proscar, Propecia));
7. Dual 5-alpha reductase inhibitor (e.g., dutasteride (Avodart));
8. Estrogen, drug-producing androgen suppression, or anabolic steroids;
9. PD5 Inhibitors (e.g., Viagra, Levitra or Cialis)
9. Subjects who have had an incidence of spontaneous urinary retention either treated
with indwelling transurethral catheter or suprapubic catheter 6 months prior to
baseline. A provoked episode now resolved is still admissible
10. Evidence of atonic neurogenic bladder evaluated by a baseline urodynamic assessment.
11. Visible hematuria with subject urine sample without a known contributing factor.
12. Presence of a penile implant or stent(s) in the urethra or prostate
13. Active urinary tract infection by culture within 7 days of treatment or two documented
independent urinary tract infections of any type in the past 6 months.
Gastroenterology:
14. Previous pelvic irradiation or radical pelvic surgery.
15. Previous rectal surgery (other than hemorrhoidectomy) or known history of rectal
disease.
Nephrology:
16. Compromised renal function defined as serum creatinine > 2.0 mg/dl.
17. Hydronephrosis (Grade 2 or higher).
Oncology:
18. Prostate cancer testing:
If PSA is > 2.5 ng/ml and ≤ 10 ng/ml with free PSA <25%, prostate cancer for the
subject must be/had been ruled out through a negative biopsy prior to enrollment
- Males 50-59 years - PSA is >2.5 ng/ml and ≤10 ng/ml with free PSA <25%,
- Males 60+ years - PSA is >4 ng/ml and ≤10 ng/ml, with free PSA <25%
19. History of confirmed malignancy or cancer of the prostate or bladder; however, high
grade prostatic intraepithelial "PIN" is acceptable.
20. History of cancer in non-genitourinary system that is not considered cured (except
basal cell or squamous cell carcinoma of the skin). A potential participant is
considered cured if there has been no evidence of cancer within five years of
enrollment.
Cardiology:
21. History of clinically significant congestive heart failure (i.e., NYHA Class III and
IV).
22. Cardiac arrhythmias that are not controlled by medication and/or medical device.
23. An episode of unstable angina pectoris, a myocardial infarction, transient ischemic
attack, or a cerebrovascular accident within the past six months.
Pulmonology:
24. History of significant respiratory disease where hospitalization for the disease is
required.
Hematology:
25. Diagnosed or suspected bleeding disorder, or coagulopathies.
26. Use of antiplatelet or anticoagulant medication except low dose aspirin (<100mg/day)
within 10 days prior to treatment.
Endocrinology:
27. History of diabetes not controlled by a stable dose of medication over the past three
months, provided that patients with a hemoglobin A1c <8.0% are allowed.
Immunology:
28. History of immunosuppressive conditions (e.g., AIDS, post-transplant).
Neurology:
29. Any cognitive or psychiatric condition that interferes with or precludes direct and
accurate communication with the study investigator regarding the study or affect the
ability to complete the study quality of life questionnaires.
30. Diagnosed or suspected primary neurologic conditions such as multiple sclerosis or
Parkinson's disease or other neurological diseases known to affect bladder function,
sphincter function or poor detrusor muscle function (< 25% of accepted and established
nomograms).
General:
31. Currently enrolled in any other pre-approval investigational study in the US (does not
apply to long-term post-market studies unless these studies might clinically interfere
with the current study endpoints (e.g., limit use of study-required medication, etc.).
32. Any significant medical history that would pose an unreasonable risk or make the
subject unsuitable for the study.
33. Inability to provide a legally effective "Informed Consent Form" and/or comply with
all the required follow-up requirements.
We found this trial at
5
sites
San Antonio, Texas 78229
Principal Investigator: Christopher H. Cantrill, MD
Phone: 210-617-4116
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Jeffersonville, Indiana 47130
Principal Investigator: James L. Bailen, MD
Phone: 812-206-8162
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Scottsdale, Arizona 85255
Principal Investigator: Micheal F. Darson, MD
Phone: 480-661-2662
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7505 Osler Drive
Towson, Maryland 21204
Towson, Maryland 21204
Principal Investigator: Richard M. Levin, MD
Phone: 443-471-5750
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