Ulcerative Colitis Clinical Trial
Official title:
A Multi-centre Double Blind Randomised Placebo-controlled Study of the Use of Rectal Tacrolimus in the Treatment of Resistant Ulcerative Proctitis
Ulcerative Colitis (UC) is a life-long incurable disease with remissions and exacerbations. Inflammation confined to the rectum occurs in a quarter of patients and can be extremely hard to treat. Many medications have been tried in order to control the inflammation, but they do not always work. One of the newer medications is the immunosuppressing medication, tacrolimus that has been shown to be effective in UC when taken orally. Unfortunately, the oral use of this medication can have numerous serious side effects. In order to overcome these side effects, the use of topical rectal tacrolimus has been examined. Pilot studies in ulcerative proctitis (inflammation confined to the rectum) resistant to conventional therapies have demonstrated a clinical remission in 75% of patients and although the medication was well absorbed through the lining of the bowel, the levels in the blood were very low and no serious side effects were reported. The findings suggest that this preparation is indeed effective for inflammation in the distal bowel and that the method of administration reduces side effects. Further work, however, now needs to be undertaken to validate the original findings.
The Inflammatory Bowel Diseases (IBDs) are life-long conditions often diagnosed between 15
and 35 years of age that are increasing in frequency. In developed countries, IBD prevalence
was about 100-220/100,000 in 2002. More recently the estimated prevalence of CD and UC in
the USA are 201 and 238 per 100,000 respectively. This indicates more than 620,000 CD and
730,000 UC patients in the USA alone. It has also been noted that the incidence of IBD has
been increasing in the ethnic minorities in American over the last two decades and it is
predicted that IBD, which was previously thought of as a 'Caucasian disease', will reach a
comparable levels in Asia as in the Western Countries within 10-15 years. One of the major
costs in IBD treatment is the need for a hospital admission. These have been falling for CD
patients secondary to the increasing use of the biological therapies, however, admissions
for UC have doubled over the last 15 years. IBD now costs the Australian economy of
22,000,000 people over $2.7 billion annually and this is comparable throughout the western
World.
Tacrolimus and cyclosporin are classical calcineurin inhibitors and are widely used as
immunosuppressive medications with promising results in UC. Calcineurin, or protein
phosphatase 2B (PP2B), is a ubiquitously expressed cytosolic Ser/Thr protein phosphatase,
that is highly conserved in eukaryotes. It has the ability to dephosphorylate a broad range
of proteins and can regulate interleukin (IL)-2, IL-4 and interferon (IFN)γ expression, as
well as modulating the activity of transcription factors like NF-κB. Enhanced NF-kB activity
is well described in CD and UC and induces the proinflammatory cytokine IL-1β, IL-6 and TNFα
expression. It is primarily through the reduction in the levels of these cytokines that
clinical remission may be achieved.
The efficacy of oral tacrolimus has been examined in the management of medication resistant
CD and UC. Unfortunately, the majority of these studies have been open labelled with only
one randomised controlled trial reported in UC. This demonstrated a short-term clinical
improvement but without a significant increase in the remission rate, potentially due to low
patient numbers. Despite this, there are numerous open labelled studies in both UC and CD
that suggest efficacy in the short term and with promising longer term data. The evidence
would suggest, however, that the blood trough level should be at least 10ug/L in order to
achieve the best efficacy (therapeutic range 5-20ug/L), but the higher the trough level the
more likely a patient will suffer an adverse effect. These, unfortunately, can be numerous
and include hypertension, nausea and diarrhoea, haematological abnormalities, renal
impairment. Increase in the rate of skin cancers is also a concern, a concern supported by
animal studies.
Use of topical tacrolimus has been effective in the treatment of perioral and perineal
inflammation in paediatric CD patients with resolution of symptoms in 75%. Work examining
topical perianal tacrolimus therapy in adult CD patients also demonstrated clinical
efficacy, and although tacrolimus is absorbed well transdermally, only low trough levels of
tacrolimus were detected in the blood. In these preliminary studies, the use of topical
tacrolimus was associated with very few side effects. Long-term topical use, as with oral
formulations, may be associated with an increased risk of skin cancer formation.
Epidemiological evidence, however, would suggest that the risk is low and localised to the
tacrolimus-treated sun-exposed skin.
The recent pilot study by our group demonstrated that 75% (6/8) of patients with resistant
distal colitis responded and achieved a remission of their disease following 4 and 8 weeks
of tacrolimus rectal ointment8. A dose of 0.3 to 0.5mg/ml 3ml twice a day was identified in
the majority of patients to induce remission. In these patients tacrolimus trough levels
were taken regularly and were either undetectable (<1.5 μg/L) sub-therapeutic (<5 μg/L) or,
at their highest, in the low therapeutic range (therapeutic range 5-20 μg/L). The ointment
was well tolerated without any systemic adverse effects. Use of the same rectal tacrolimus
preparation in further 8 patients was also associated with a clinical response in 6 patients
after 4 weeks of therapy.
The efficacy of topical tacrolimus in UC is further supported by a separate pilot study that
examined topical tacrolimus in patients with resistant distal colitis. In this study a
clinical and histological improvement in 10 of 12 patients by 4 weeks without any major side
effects reported and the preparation was well tolerated.
METHODOLOGY
Study medication and supply:The preparation of the tacrolimus rectal ointment will be
undertaken in respective hospital pharmacy at each centre. Gloves and mask shall be worn
when making the preparation. The concentration of tacrolimus in the ointment shall be 0.5
mg⁄mL. Five millilitres of propylene glycol will be slowly mixed into the desired amount of
tacrolimus powder on a clean glass slab. To this, 70 mL of paraffin liquid BP (LP) will be
gradually added by serial dilution and triturate until evenly mixed. This process will be
repeated with 125 mL of paraffin white soft BP (WSP). The resulting cream will be packed
into tubes and labelled. The preparation will be formulated using the LP ⁄WSP base for ease
of rectal use.
Medication Stability: The cream expires after 30 days at room temperature or 90 days at 4-8
0C
Administration of the study medication: A total of 3ml of the study medication or placebo
will be applied rectally, via an applicator, twice a day by the patient over the 8-week
period. The application will take place prior to retiring to bed and following breakfast in
the morning. For shift workers application will occur just prior to retiring to bed and
following the first meal of the day.
Dosage schedule:
1. Randomisation: Patients will be randomly assigned in a 1:1 ratio to receive the
tacrolimus or placebo.
2. Blinding: The trial patients and the clinical investigators will be blinded to the
randomisation.
Concomitant therapy: Rectal preparation will be ceased a day prior to commencing the trial.
Patients will be continued on the same oral medications they are on at commencement of the
study.
Screening visit: All patients will sign informed consent prior to any data collection.
Patient demographics will be recorded. Stool culture and microscopy, blood pressure (BP),
full blood count (FBC), erythrocyte sedimentation rate (ESR), C-reactive protein (CRP),
urea,electrolytes (U&E) and GFR will be taken and measured locally at each site. Results of
these tests will be faxed through to the central site at Fremantle hospital within 3 days of
collection for review. Faecal calprotectin will be taken and stored at -200C. These
specimens will be sent in batches on dry ice every 3 months to the central site at Fremantle
Hospital for analysis.
Within 7 days prior to week 0 a flexible sigmoidoscopy will be performed. Two sets of photos
will be taken at endoscopy one set distal (within 15cm of the anus) and one set proximal
(15-25cm from the anus). The region depicting the worse level of inflammation will 2
biopsies will be taken from each region for histological analysis. Biopsies will be fixed
and blocked at each hospital site. All the paraffin blocks will be sent to Fremantle
Hospital be noted. Following the photos for histological analysis. Four additional biopsies
will be taken from each region for RNA isolation. The biopsies from each region will be
placed immediately into 2 tubes labelled 'proximal' and 'distal' containing RNAlater and
stored at -80oC. These will then be sent in batches on dry ice every 3 months to the central
site at Fremantle Hospital for analysis. A full Mayo score will calculated to confirm the
presence of active UC (Mayo score between 6 and 12 required for inclusion).
Week 0: A Mayo score will be calculated using the screening endoscopic findings and
treatment initiated. Baseline IBDQ calculated and BP measured
Weeks 2, and 4: A modified Mayo score will be calculated, BP taken, and FBC, ESR, CRP, U&E
as described above and the IBDQ assessed. The faecal calprotectin will be taken and stored
at -200C. Blood for the tacrolimus trough will be taken, the serum collected and this will
be stored at -20oC. The serum will then be sent on dry ice to the central site at Fremantle
Hospital for assessment within 2 days of collection. The medical monitor (CIA) at Fremantle
Hospital will review all the tacrolimus trough levels to ensure patient safety.
Week 8 or withdrawal: A flexible sigmoidoscopy will be undertaken ± 3 days of the week 8
visit (or at early withdrawal) and a full Mayo score calculated. Photos and biopsies will be
taken and processed as detailed at the screening sigmoidoscopy. Routine FBC, U&E, ESR, CRP,
BP measured, and faecal calprotectin as described above
Week 12: Follow-up phone call to assess any adverse events. Each histological specimen will
be assessed centrally at Fremantle Hospital by a blinded specialist gastroenterological
histopathologist. These findings will be correlated with the endoscopic scoring and photos
taken at endoscopy.
Early withdrawal from the study: Patients are free to withdraw from the study at any time.
If the patient is withdrawing due to lack of efficacy of the study preparation 4 weeks or
more following the week 0 visit, they will be eligible for open label use topical tacrolimus
ointment for 4 weeks. A withdrawal flexible sigmoidoscopy will be required prior to the
supply of the topical tacrolimus ointment. Photos will be taken prior to the biopsies as
described for the week 0 and 8 procedures. Routine FBC, U&E, ESR, CRP, BP measured,
tacrolimus trough levels and faecal calprotectin will be taken after 2 weeks of therapy as
described above. These patients will be eligible for analysis for the primary and secondary
end points
Interim Analysis: An interim analysis by an independent statistician and clinician after 20
patients have completed the 8-week visit will be done to confirm the drug safety and to
assess the efficacy. This shall be required prior to allowing the study to continue.
mRNA expression levels: Biopsies (x4) taken from two regions for the distal colon (within
15cm of the anus and 15-25cm from the anus). The region containing the worse inflammation
seen on endoscopic examination at weeks 0 and 8 (or at early withdrawal) will have been
noted. All samples will have been immediately placed in RNA later and stored at -800C prior
to transfer on dry ice to the central site at Fremantle Hospital. Levels of TNFα, IFN-γ,
IL-1β, IL-2, IL4, IL-10 and IL-6 mRNA expression will be determined on each group of
samples. Total RNA will be isolated and DNase-treated using the Qiagen 96 RNeasy® kit
(Qiagen, Clifton Hill, Australia) according to the manufacturer's instructions. The quality
of the RNA samples will be verified, reverse transcription performed and cDNA quantitated by
real-time PCR using QuantiTect SYBR Green Master Mix (Qiagen) on the ABI PRISM 7900HT
(Applied Biosystems). Specific primers for the mRNAs will be used. Dissociation curve
analysis will confirm specificity of amplification and copy numbers will be determined from
plasmid or PCR product standard curves. Target mRNA copy numbers will be normalised against
reference gene copy number for each cDNA sample. The above methods are already available in
CIA's laboratory at Fremantle Hospital. The limit of mRNA detection is 3pg/ml for all
cytokines
Statistical analysis: Comparisons between the mRNA expression in endoscopic biopsies taken
at weeks 0 and 8 (or at withdrawal) in the tacrolimus treatment arm will undertaken and
compared with each other and against those from the placebo control arm at the same time
points. The mRNA expression levels will be correlated with the endoscopic and histological
inflammatory scores. Differences between the groups will be assessed using one-way ANOVA on
log-transformed data. Statistical analysis will be conducted using the Statistical Package
for the Social Sciences (SPSS) version 17. Statistical significance is considered as p<0.05
for all analyses.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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