Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT04887818 |
| Other study ID # |
REB20-0239 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
Phase 2/Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
June 2021 |
| Est. completion date |
December 2021 |
Study information
| Verified date |
April 2021 |
| Source |
University of Calgary |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Anal fissure is a common anorectal diseases characterized by tear of the anoderm from the
dentate line to the anal verge leading to pain and bleeding during and post defecation. It
may be a benign disease, but patients suffering from disease report significantly impacted
quality of life especially when it becomes chronic. Several treatment modalities have been
studied for chronic anal fissure, and topical calcium channel blockers (CCB) showed promising
benefit and side effect profile in treatment of chronic anal fissure. Topical Diltiazem and
Nifedipine are currently widely used CCBs for chronic anal fissure after multiple studies
showing their benefits compared to different agents or modalities. To the investigators'
knowledge, there is no study comparing the efficacy of topical Diltiazem and Nifedipine
directly. The investigators aim to design a pragmatic randomized clinical trial to compare
the efficacy, and side effect profile of topical Nifedipine and Diltiazem in treatment of
chronic anal fissure.
Description:
Anal fissure is a common anorectal diseases characterized by tear of the anoderm from the
dentate line to the anal verge. It is a benign disease, but symptoms including stabbing pain
during and post defecation, bleeding, and irritation lead to decreased quality of life. Acute
anal fissure are superficial splits, and mostly heal spontaneously within 4 weeks with or
without conservative management including high fibre diet and stool softeners. Chronic anal
fissure is characterized by symptoms lasting longer than 2 months, and clinical findings of
sentinel perianal skin tag, hypertrophied anal papilla, exposure of the underlying internal
anal sphincter or anal cicatrization. The pathophysiology involves hypertonia of the internal
anal sphincter leading to a reduction in mucosal blood flow, therefore poor healing tendency.
Several treatment modalities have been studied for chronic anal fissure. Surgical therapy
(ie. lateral internal sphincterotomy) has shown promising healing rate, but its role as first
line treatment was limited by significant complications including permanent flatus or fecal
incontinence. Chemical sphincterotomy was introduced as a promising first line treatment due
to its safe side effect profile and comparable healing rate. Topical Nitro donor initially
showed a reasonable healing rate, but it was associated with high rate of significant
headache leading to early termination of the therapy.
Calcium channel blockers (CCB) were then introduced to the market due to its known systemic
vasodilator effect. Systemic administration of CCB is associated with various side effects
including hypotension, positional hypotension, and flushing, but the topical agents were
associated with minimal systemic side effects while demonstrating potent local vasodilator
effect. Several randomized clinical trials have shown excellent healing rate, and safe side
effect profile of both topical Diltiazem and Nifedipine. Currently, both agents are
prescribed as the standard of care for first line treatment of symptomatic anal fissure.
To the investigators' knowledge, there is no study comparing the efficacy of topical
Diltiazem and Nifedipine directly. The investigators aim to design a pragmatic randomized
clinical trial to compare the efficacy, and side effect profile of topical Nifedipine and
Diltiazem in treatment of chronic anal fissure.
This study will be a prospective, randomized, double-blinded study involving patients with
chronic anal fissure undergoing 12-week treatment course of 2% Diltiazem ointment with 1.5%
lidocaine vs. 0.3% Nifedipine ointment with 1.5% lidocaine. Patients with IBD, anorectal
surgery, infection, radiation, instrumentation, obstetrical injuries, or patients who are
currently pregnant will be excluded. Both the surgeons and the participants will be blinded
from the agent being used. The participants will be followed up in the clinic at 3 months to
evaluate patient reported outcome and physical exam findings of anal fissure.
Primary outcome is the anal fissure related symptoms reported by the patients upon completion
of the therapy. Physical exam findings will documented and to aid in assessment of the
response to the therapy, but patient reported outcome will be the most important clinical
information to assess efficacy of the therapy. Secondary outcome include rate of side
effects, patient compliance rate, recurrence rate, and time from cure to recurrence.
Recurrence is defined by return of symptoms related to anal fissure in patients who
experienced resolution of symptoms.
