ROBUST III- Re-Establishing Flow Via Drug Coated Balloon For The Treatment Of Urethral Stricture Disease
Status: | Recruiting |
---|---|
Healthy: | No |
Age Range: | 18 - Any |
Updated: | 4/3/2019 |
Start Date: | June 22, 2018 |
End Date: | November 2024 |
Contact: | Laura Moffett |
Email: | moffettl@urotronic.com |
Phone: | 763-285-7489 |
ROBUST III - Re-Establishing Flow Via Drug Coated Balloon For The Treatment Of Urethral Stricture Disease - A Randomized Control Trial
ROBUST III is a prospective, multi-center, randomized controlled adaptive sample size
clinical trial to establish the safety and effectiveness for the Optilume Stricture Drug
Coated Balloon (DCB).
clinical trial to establish the safety and effectiveness for the Optilume Stricture Drug
Coated Balloon (DCB).
ROBUST III is a prospective, multi-center, single blind randomized controlled clinical trial
in a 2:1 allocation of treatment versus control device.
This study is an adaptive design with an interim analysis for sample size re-estimation
performed after 60 subjects have been enrolled. The interim analysis will be be undertaken
following completion of the 6-month follow-up data from these subjects. Based on the results
of the interim analysis, the final total sample size required for the study will be
re-estimated. A minimum of 140 subjects, and a maximum of 200 subjects (pending the
re-estimation) will be enrolled in the study. A Data Monitoring Committee (DMC) will review
the interim analysis results, including the sample size re-estimation and make
recommendations related to trial continuation to the sponsor.
in a 2:1 allocation of treatment versus control device.
This study is an adaptive design with an interim analysis for sample size re-estimation
performed after 60 subjects have been enrolled. The interim analysis will be be undertaken
following completion of the 6-month follow-up data from these subjects. Based on the results
of the interim analysis, the final total sample size required for the study will be
re-estimated. A minimum of 140 subjects, and a maximum of 200 subjects (pending the
re-estimation) will be enrolled in the study. A Data Monitoring Committee (DMC) will review
the interim analysis results, including the sample size re-estimation and make
recommendations related to trial continuation to the sponsor.
Inclusion Criteria:
1. Male subjects ≥ 18 years' old
2. Visual confirmation of stricture via cystoscopy or urethrogram
3. Single, tandem or diffuse anterior urethral stricture(s), less than or equal to 3.0 cm
total length measured by retrograde urethrogram. (Stricture length is defined as the
distance between the most distal edge of the stricture to the most proximal edge of
the stricture).
4. Two or more prior dilation treatments of the same stricture, including DVIU (Direct
Vision Internal Urethrotomy), but no prior urethroplasty.
5. Significant symptoms of stricture such as frequency of urination, dysuria, urgency,
hematuria, slow flow, feeling of incomplete emptying, recurrent urinary tract
infections (UTI's).
6. International Prostrate Symptoms Score (IPSS) score of 13 or higher (assumed to be
"35" if suprapubic catheter is present)
7. Lumen diameter <12F by urethrogram
8. Qmax <15 ml/sec (assumed to be "0" if suprapubic catheter is present)
9. Guidewire must be able to cross the lesion
Exclusion Criteria:
1. Subjects with diffuse stricture length, greater than 3.0 cm in total length.
(Stricture length is defined as the distance between the most distal edge of the
stricture to the most proximal edge of the stricture).
2. Subjects with a history of hypersensitivity reactions to TAXOL, on medication that may
have negative interaction with paclitaxel, with solid tumors who have a baseline
neutrophil counts of <1500 cells/mm3 or subjects with AIDS-related Kaposi's sarcoma
with baseline neutrophile counts of <1000 cells/mm3.
3. Subjects who had an indwelling suprapubic catheter longer than three (3) months total
prior to enrollment.
4. Previous urethroplasty within the anterior urethra
5. Stricture due to bacterial urethritis or untreated gonorrhea
6. Stricture dilated or incised within the last six (6) weeks (urethral catheterization
is not considered dilation)
7. Presence of local adverse factors, including abnormal prostate making catheterization
difficult, urethral false passage or fistula.
8. Presence of signs of obstructive voiding symptoms not directly attributable to the
stricture at the discretion of the physician
9. Diagnosis of untreated and unresolved BPH or BNC
10. Prior diagnosis of stress urinary incontinence (SUI).
11. History of radical prostatectomy
12. History of pelvic radiation
13. Diagnosis of carcinoma of the urethra, bladder or prostate within the last five (5)
years
14. Active kidney, bladder, urethral or ureteral stone passage in the last six (6) weeks
or concern of stone passage in the next 6 weeks at the discretion of the investigator.
15. Diagnosis of chronic renal failure and treatment with hemodialysis
16. New diagnosis of OAB (overactive bladder) within the last six (6) months
17. Use of alpha blockers, beta blockers, OAB (Overactive Bladder) medication,
anticonvulsants (drugs that prevent or reduce the severity and frequency of seizures),
and antispasmodics where the dose is not stable. (Stable dose is defined as having the
same medication and dose in the last six months.)
18. Dependence on Botox (onabotulinumtoxinA) in urinary system
19. Presence of an artificial urinary sphincter, or stent(s) in the urethra or prostate
20. Known neurogenic bladder, sphincter abnormalities, or poor detrusor muscle function
21. Diagnosed with Lichen Sclerosus, or stricture due to balanitis xerotica obliterans
(BXO)
22. Previous hypospadias repair
23. History of cancer in non-genitourinary system which 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 (5) years of
enrollment
24. 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
25. Unwilling to use protected sex for thirty (30) days' post treatment
26. Unwilling to abstain or use protected sex for ninety (90) days post treatment if
sexual partner is of child bearing potential.
27. Inability to provide Informed Consent Form (ICF) and/or comply with all the required
follow-up requirements
28. Participation in other pre-market studies or treatment with an investigational drug or
device. Long term follow up or post market study of an approved device is allowed.
29. Current active infection in the urinary system
30. Current uncontrolled diabetes (hemoglobin A1c > 7.0%) or evidence of poor wound
healing due to diabetes
31. 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.
32. Visible hematuria in subject's urine sample without known contributing factor
33. Invisible hematuria (or significant microscopic hematuria, i.e. hematuria of ≥ 3
RBC's/HPF) that may be caused by a clinically significant disease unless it is
attributed to the urethral stricture disease or other causes which are benign and not
requiring treatment.
We found this trial at
19
sites
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Cheektowaga, New York 14225
Principal Investigator: Kent Chevli, MD
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545 Health Boulevard
Daytona Beach, Florida 32114
Daytona Beach, Florida 32114
Principal Investigator: Jeffrey Dann, MD
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7580 Buckingham Boulevard
Hanover, Maryland 21076
Hanover, Maryland 21076
Principal Investigator: Kaiser Robertson, MD
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Minneapolis, Minnesota 55445
Principal Investigator: Sean Elliott, MD
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New York, New York 10032
Principal Investigator: Steven Brandes, MD
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Seattle, Washington 98104
Principal Investigator: Judith Hagedorn, MD
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West Columbia, South Carolina 29169
Principal Investigator: Brian Willard, MD
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