Advice
Overview for healthcare professionals
Overview for healthcare professionals
Regulatory status of 0.2% glyceryl trinitrate
Topical 0.2% glyceryl trinitrate ointment does not currently have a UK licence for treating chronic anal fissures, or for any other indication. Therefore, its use is unlicensed.
In line with the guidance from the General Medical Council (GMC), it is the responsibility of the prescriber to determine the clinical need of the patient and the suitability of using unlicensed 0.2% glyceryl trinitrate ointment.
Topical 0.4% glyceryl trinitrate ointment (Rectogesic 4 mg/g rectal ointment, ProStrakan) is licensed in the UK for the relief of pain associated with chronic anal fissure in adults for a maximum of 8 weeks (see the Rectogesic 4 mg/g rectal ointment summary of product characteristics). It is not indicated for the healing of chronic anal fissure and is not recommended for use in children and young people under 18 years because of a lack of data on safety and efficacy.
The summary of product characteristics states that headache is very commonly reported by people using 0.4% glyceryl trinitrate ointment for chronic anal fissure (frequency greater than 1 in 2). Although this can be treated with analgesics such as paracetamol, headaches may be severe (frequency 1 in 5 people) and cause people to discontinue treatment. Dizziness and nausea are also commonly reported (frequency greater than 1 in 100, but less than 1 in 10).
According to the Scottish Medicines Consortium's assessments (2005 to 2008), 0.4% glyceryl trinitrate ointment was appraised but not recommended for use in NHS Scotland for the relief of pain associated with chronic anal fissure.
The Association of Coloproctology of Great Britain and Ireland has suggested that the strength of glyceryl trinitrate (0.2% or 0.4%) does not influence the efficacy but increases the incidence of side effects, particularly headache (Cross et al. 2008). Additionally, it has suggested that 0.2% glyceryl trinitrate ointment (twice daily) is an option for children with anal fissure. There is currently no licensed medical treatment option for this age group.
Other glyceryl trinitrate formulations (tablets, patches, sprays or intravenous infusions) are licensed for treating and preventing angina and other heart conditions (British national formulary, January 2013).
Evidence statements
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A Cochrane systematic review (assessed as up-to-date November 2011) found that glyceryl trinitrate (pooled strengths, range unclear) was marginally, but statistically significantly, better than placebo in healing chronic anal fissure (48.9% compared with 35.5%) but late recurrence was common, occurring in about 50% of people whose fissures were initially cured.
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No direct evidence was identified that compared the efficacy of 0.2% with 0.4% glyceryl trinitrate ointment in healing chronic anal fissure or reducing pain symptoms in adults.
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Indirect comparisons from 2 small randomised controlled trials (RCTs; Scholefield et al. 2003 and Carapeti et al. 1999; only 47 and 23 adults respectively were analysed in the 0.2% ointment groups in each trial) provided very limited evidence that 0.2% glyceryl trinitrate ointment might be as effective as 0.4% glyceryl trinitrate ointment at healing anal fissure after an 8-week treatment period in adults. However, in 1 of these (Scholefield et al. 2003), neither strength of glyceryl trinitrate showed a statistically significant difference from placebo in healing rate.
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One small RCT (Scholefield et al. 2003; 181 people analysed) provided limited evidence that lower strengths of glyceryl trinitrate were associated with fewer reported headaches in adults. The study found a statistically significant trend across glyceryl trinitrate ointment strengths of 0.1%, 0.2% and 0.4%.
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It is not known whether applying less ointment of the same strength, rather than reducing the strength of ointment applied, might have an effect on the incidence or headache.
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No evidence was identified that looked at the effect of using 0.2% glyceryl trinitrate ointment in children or young people under 18 years.
Summary of the evidence
This section gives a brief summary of the main evidence. A more thorough analysis is given in the Evidence review section.
This evidence summary is based on published evidence and does not include evidence from unpublished studies submitted for the regulatory approval of 0.4% glyceryl trinitrate ointment.
Both a literature search and a Cochrane systematic review of non-surgical therapy for anal fissure identified 3 small RCTs recruiting adults (n=309 analysed) and 1 pilot RCT recruiting children (n=15 analysed) that included trial arms using different strengths of glyceryl trinitrate ointment to treat chronic anal fissure.
Efficacy
The Cochrane review (75 studies, 5031 patients) of non-surgical therapy for anal fissure included a total of 18 RCTs in 1315 people, mostly adults, involving glyceryl trinitrate. It found that, overall, glyceryl trinitrate (pooled strengths, range unclear) was marginally, but statistically significantly, better than placebo in healing chronic anal fissure (48.9% compared with 35.5%, p<0.0009) but late recurrence was common, occurring in approximately 50% of people whose fissures were initially cured. Of interest for this evidence summary, it pooled results from 4 RCTs to compare 'high' and 'low' strengths of topical glyceryl trinitrate ointment to treat chronic anal fissure in adults and children (n=324 analysed). High and low cut-offs were not defined in the review but glyceryl trinitrate ointment strengths in the individual trials ranged from 0.05% to 0.6%. The meta-analysis found no significant difference in fissure healing between the different strengths of glyceryl trinitrate used (low strength compared with high strength pooled odds ratio [OR] 0.91, 95% confidence interval [CI] 0.57 to 1.45).
This Cochrane review did not report a direct comparison of topical 0.2% with 0.4% glyceryl trinitrate, and no pooled estimate of effect was reported for the outcomes of pain reduction or adverse events due to headaches. The RCTs that were included in the Cochrane review for glyceryl trinitrate strength comparison are discussed below.
Key outcomes for 2 of the RCTs (Scholefield et al. 2003 and Carapeti et al. 1999) are summarised in tables 1 and 2 respectively. The RCT by Bailey et al. (2002) is not included in the tables because it presented most of its key outcomes in a graphical format only, therefore exact figures were not available. The RCT by Simpson et al. (2003) is not included in the tables because it did not use 0.2% or 0.4% glyceryl trinitrate ointment.
Children
No evidence was identified to assess the efficacy or safety of using 0.2% glyceryl trinitrate ointment in children and young people under 18 years. Only 1 pilot RCT (n=15) was identified but this used 0.1% and 0.05% glyceryl trinitrate ointment (Simpson et al. 2003). The authors' rationale for using these lower strength ointments was that the optimum therapeutic strength of glyceryl trinitrate ointment had not been established.
Adults
No studies were identified that were designed specifically to compare the efficacy of 0.2% with 0.4% glyceryl trinitrate ointment for chronic anal fissure, such as an RCT sufficiently powered to detect these differences or a non-inferiority trial.
Three small RCTs (Scholefield et al. 2003, Carapeti et al. 1999 and Bailey et al. 2002) were identified that tested different strengths of glyceryl trinitrate (0.1%, 0.2%, 0.4% and 0.2%–0.6% escalating weekly by 0.1%) against placebo in adults with chronic anal fissure. All included a local twice-daily application of glyceryl trinitrate ointment for 8 weeks and the primary outcome in all studies was fissure healing. This was assessed at 8 weeks in Scholefield et al. (2003) and Bailey et al. (2002) and at 10 weeks (8 weeks treatment, 2 weeks after treatment) in Carapeti et al. (1999). However, no statistical tests were carried out to assess differences between the glyceryl trinitrate strengths for this primary outcome.
One RCT (Carapeti et al. 1999) attempted to assess for statistically significant differences in secondary outcomes between glyceryl trinitrate strengths (table 2). However, it was small (n=70) and was not statistically powered to detect anything but large differences between glyceryl trinitrate strengths.
Indirect comparisons from 2 small RCTs (Scholefield et al. 2003 and Carapeti et al. 1999; tables 1 and 2, only 47 and 23 adults respectively were analysed in the 0.2% ointment groups in each trial) provided very limited evidence that 0.2% glyceryl trinitrate ointment might be as effective as 0.4% glyceryl trinitrate at healing anal fissure after an 8-week treatment period in adults. However, in 1 of these (Scholefield et al. 2003), neither strength showed a statistically significant difference from placebo in healing rate.
The 3 RCTs reported relatively high healing rates in placebo arms after 8 weeks (32% [7/22] in Carapeti et al. 1999, 37.5% [18/48] in Scholefield et al. 2003 and 50% [patient numbers not reported] in Bailey et al. 2002) suggesting a high spontaneous healing rate. In Scholefield et al. (2003), placebo healing rate reduced from 37.5% (18/48) to 24.3% (9/37) when a stricter definition of chronicity was used. Therefore, heterogeneity in chronic fissure definition may influence reported fissure healing rates.
Using the stricter definition of chronicity, Scholefield et al. (2003) found statistically significantly higher healing rates after 8 weeks in people using 0.1% glyceryl trinitrate ointment (50.0%, 21/42, p=0.05) and 0.4% ointment (56.7%, 17/30, p=0.03) compared with placebo (24.3%, 9/37) and for the trend of all glyceryl trinitrate groups combined compared with placebo (p=0.03). However, the 0.2% glyceryl trinitrate group on its own did not show statistically significant differences from placebo (36.1%, 13/36, p=0.91).
Table 1 Summary of the trial: Scholefield et al. (2003)
0.2% glyceryl trinitrate ointment |
0.4% glyceryl trinitrate ointment |
Placebo |
Analysis |
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Randomised |
n=51 |
n=46 |
n=51 |
0.2%, 0.4% and placebo arms only |
|
ITT population |
n=47 |
n=37 |
n=48 |
Patients who had used some of the study medication and were assessed for healing at the end of the study |
|
Primary outcome: complete healing at 8 weeksa |
40.4% (19/47) 95% CI 26% to 56% |
54.1% (20/37) 95% CI 37% to 71% |
37.5% (18/48) 95% CI 24% to 53% |
|
|
Sub-analysis: |
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Randomised |
n=36 |
n=30 |
n=37 |
ITT data restricted to people who had more than 1 of 5 features of chronicityb |
|
Complete healing at 8 weeks |
36.1% (13/36) 95% CI 21% to 54% |
56.7% (17/30) 95% CI 37% to 75% |
24.3% (9/37) 95% CI 12% to 41% |
|
|
Safety: |
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Randomised |
n=47 |
n=37 |
n=48 |
ITT (0.2% and 0.4% arms only) |
|
Headache |
36.1% (17/47) |
67.5% (25/37) |
12.5% (6/48) |
|
|
Severe headache |
6.4% (3/47) |
24.3% (9/37) |
4.2% (2/48) |
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Abbreviations: CI, confidence interval; ITT, intention to treat; n, number of patients; SD, standard deviation. a Assessed by visual inspection and measurement of length and width of fissure. b Recognised features of chronicity included sentinel skin tag, hypertrophied anal papillae, exposed internal anal sphincter, fibrotic lateral fissure or fibrotic anal sphincter. |
Table 2 Summary of trial:
Carapeti et al. (1999)
0.2% glyceryl trinitrate ointment |
0.2% to 0.6% glyceryl trinitrate ointment weekly 0.1% increments |
Placebo |
Analysis |
|
Randomised |
n=24 |
n=24 |
n=22 |
ITT |
Analysed |
n=23 |
n=23 |
n=22 |
Analysed samplea |
Primary outcome: fissure healing at 10 weeks (8 weeks treatment, 2 weeks post treatment)b |
65% (15/23) |
70% (16/23) |
32% (7/22) |
|
Selected secondary outcomes: |
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Mean pain score (baseline to 8 weeks) |
Not reported, presented graphically |
Not reported, presented graphically |
Not reported, presented graphically |
|
Symptomatic recurrence of fissure initially healed |
33% (5/15) |
25% (4/16) |
43% (3/7) |
|
Safety: |
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Analysed |
n=23 |
n=23 |
n=22 |
Analysed samplea |
Patients reporting headaches |
65% (15/23) |
78% (18/23) |
27% (6/22) |
No significant difference between glyceryl trinitrate groups (p=0.5) but statistically significant difference between glyceryl trinitrate and placebo (p<0.001) |
Abbreviations: ITT, intention to treat; n, number of patients. a After randomisation: n=1 excluded from 0.2% glyceryl trinitrate group because of lack of fissure on baseline examination, n=1 excluded from 0.2%–0.6% because of failure to attend. b Assessed by clinical examination, anal manometry and laser Doppler flowmetry. |
Safety
One small RCT (Scholefield et al. 2003, 181 adults analysed) provided limited evidence that lower glyceryl trinitrate ointment strength was associated with fewer reported headaches over an 8-week treatment period in adults. It showed a statistically significant trend linking increasing glyceryl trinitrate strength (0.1%, 0.2% and 0.4% used) to more frequently reported headache. Frequency of reported headache (baseline to 8 weeks) was 12.5% (6/48) with placebo, 18.3% (9/49) with 0.1% glyceryl trinitrate, 36.1% (17/47) with 0.2% glyceryl trinitrate, and 67.5% (25/37) with 0.4% glyceryl trinitrate (p value for trend less than 0.01).
No statistical test for trend was reported comparing glyceryl trinitrate strength with the frequency of severe headaches reported in the same trial. The frequency of severe headache was 4.2% (2/48) with placebo, 2.0% (1/49) with 0.1% glyceryl trinitrate, 6.4% (3/47) with 0.2% glyceryl trinitrate, and 24.3% (9/37) with 0.4% glyceryl trinitrate.
It is not known whether applying less ointment of the same strength, rather than reducing the strength of ointment applied, might have an effect on the incidence or headache.
Cost effectiveness and cost
NHS electronic drug tariff (January 2013) data indicate that (unlicensed) 0.2% glyceryl trinitrate rectal ointment costs £57.75 for the minimum 30 g volume and an extra £1.62 for every extra gram above 30 g. The price listed for Rectogesic (0.4% glyceryl trinitrate, 4 mg/g rectal ointment, ProStrakan) is lower at £34.80 for 30 g.
No studies were identified that assessed cost effectiveness of 0.2% glyceryl trinitrate ointment compared with 0.4% glyceryl trinitrate ointment.