Ignite Creation Date:
2024-10-26 @ 3:41 PM
Last Modification Date:
2024-10-26 @ 3:41 PM
Study NCT ID:
NCT06625450
Status:
NOT_YET_RECRUITING
Last Update Posted:
None
First Post:
2024-10-02
Brief Title:
TOFACITINIB vs TOFACITINIB WITH MESALAMINE IN ULCERATIVE COLITIS
Sponsor:
None
Organization:
None
Study Overview
Official Title:
TOFACITINIB COMPARED TO TOFACITINIB WITH MESALAMINE FOR MAINTENANCE OF REMISSION IN ULCERATIVE COLITIS A RANDOMIZED CONTROLLED TRIAL
Status:
NOT_YET_RECRUITING
Status Verified Date:
2024-10
Last Known Status:
None
Delayed Posting:
No
If Stopped, Why?:
Not Stopped
Has Expanded Access:
No
If Expanded Access, NCT#:
N/A
Has Expanded Access, NCT# Status:
N/A
Acronym:
None
Brief Summary:
All the trials using tofacitinib for maintenance of remission in UC have allowed the use of concomitant therapies except glucocorticoids Mesalamine a drug used in mild-to-moderate UC is often continued in patients receiving other drugs for maintenance In this study we plan to compare the effect of withdrawing mesalamine and continuing monotherapy with tofacitinib versus continuing dual therapy with tofacitinib and mesalamine We hypothesize that the continuation of tofacitinib monotherapy after withdrawing mesalamine will be as efficacious and safe as continuation of the combination in remission maintenance in UC
Detailed Description:
Inflammatory bowel disease IBD is a chronic inflammatory condition of bowel having a relapsing and remitting course It has two major forms ulcerative colitis UC and Crohns disease CD Other less common forms include microcytic colitis primary collagenous colitis and lymphocytic colitis Ulcerative colitis is a form of IBD in which there is continuous involvement of the colon with the inflammation initiating from the rectum and then progressively involving variable lengths of the large intestine Both genetic predisposition and environmental factors play a role A dysregulated immune response gut microbiota and epithelial barrier defects are implicated in the pathogenesis of UC
The usual presentation is bloody diarrhoea Diagnosis is based on clinical endoscopic and histological findings The aim of treatment in ulcerative colitis is to induce clinical biochemical and endoscopic remission and to maintain it on a long-term Various treatment options include 5-ASA glucocorticoids thiopurines biologicals and small molecules 5-ASA is used both in inducing and maintaining remission in UC As per the American Gastroenterology Association AGA guidelines 5-ASA is used as the first line agent for inducing remission in mild to moderate UC 1 It has also been extensively evaluated in the maintenance of remission 2 In an initial multicentre study 264 subjects with UC in remission for 1 month were randomized into a mesalamine and a placebo arm Endoscopic remission at 6 months was the primary endpoint defining treatment success In both the intention-to-treat and per protocol analyses mesalamine was significantly better than placebo for remission maintenance the end of 6 months Since then several studies have demonstrated the efficacy of different preparations of mesalamine in maintaining remission in ulcerative colitis
Tofacitinib has also been studied in the OCTAVE trials for both induction and maintenance of remission in UC In the OCTAVE induction 1 and 2 trials tofacitinib was compared to placebo for induction of remission in moderate-to-severe UC and it was found to be better than placebo Various meta-analyses also confirmed the same The OCTAVE sustain proved tofacitinib to be better than placebo in maintaining UC in remission at both the studied doses 10 mg twice daily and 5 mg twice daily All the trials using tofacitinib for maintenance of remission in UC have allowed the use of concomitant therapies except glucocorticoids Mesalamine a drug used in mild-to-moderate UC is often continued in patients receiving other drugs for maintenance Recent guidelines have emphasised the importance of low-cost healthcare as there is increasing pressure on healthcare budgets worldwide 3 A study in the United Kingdom suggested that mesalamine accounts for up to 25 of the total healthcare costs in UC with an average annual maintenance prescription estimated to be 740 or 850 4 While mesalamine is safe and well-tolerated it has rare but serious idiosyncratic adverse effects including pancreatitis Around 3 of patients even report a paradoxical worsening of diarrhoea 5 The negative impact of polypharmacy must also be taken into consideration with non-compliance often linked to higher pill burdens 6 In fact the burden of a more complex medication regimen has been associated with poorer outcomes in both UC with real-world compliance as low as 50 7 Furthermore compliance to topical 5-ASA therapy is even worse than oral therapy 8 Thus there is a clear need to explore the withdrawal of 5-ASA from the UC treatment regimen
Two studies have evaluated the outcomes of withdrawal of oral 5-ASA in patients concomitantly treated with immunomodulators Both studies showed no difference in relapse rates between patients with ulcerative colitis receiving either azathioprine monotherapy or combination of azathioprine and oral 5-ASA therapy with better compliance in azathioprine monotherapy group 9 10 No randomized controlled trial RCT has yet evaluated the withdrawal of 5-ASA in patients treated with either biologic therapy or tofacitinib However a recent cohort study from two national population-based databases from the United States and Denmark showed no increase in the risk of adverse clinical events after withdrawing oral 5-ASA within 90 days of initiating anti-TNF therapy compared to those who continued 5-ASA 11 No RCT or prospective study has evaluated the outcome of 5-ASA withdrawal in patients receiving tofacitinib therapy Indirect evidence from subgroup analysis of RCTs suggests that concomitant 5-ASA therapy does not increase the likelihood of maintaining clinical remission after escalation to tofacitinib 12
The usual presentation is bloody diarrhoea Diagnosis is based on clinical endoscopic and histological findings The aim of treatment in ulcerative colitis is to induce clinical biochemical and endoscopic remission and to maintain it on a long-term Various treatment options include 5-ASA glucocorticoids thiopurines biologicals and small molecules 5-ASA is used both in inducing and maintaining remission in UC As per the American Gastroenterology Association AGA guidelines 5-ASA is used as the first line agent for inducing remission in mild to moderate UC 1 It has also been extensively evaluated in the maintenance of remission 2 In an initial multicentre study 264 subjects with UC in remission for 1 month were randomized into a mesalamine and a placebo arm Endoscopic remission at 6 months was the primary endpoint defining treatment success In both the intention-to-treat and per protocol analyses mesalamine was significantly better than placebo for remission maintenance the end of 6 months Since then several studies have demonstrated the efficacy of different preparations of mesalamine in maintaining remission in ulcerative colitis
Tofacitinib has also been studied in the OCTAVE trials for both induction and maintenance of remission in UC In the OCTAVE induction 1 and 2 trials tofacitinib was compared to placebo for induction of remission in moderate-to-severe UC and it was found to be better than placebo Various meta-analyses also confirmed the same The OCTAVE sustain proved tofacitinib to be better than placebo in maintaining UC in remission at both the studied doses 10 mg twice daily and 5 mg twice daily All the trials using tofacitinib for maintenance of remission in UC have allowed the use of concomitant therapies except glucocorticoids Mesalamine a drug used in mild-to-moderate UC is often continued in patients receiving other drugs for maintenance Recent guidelines have emphasised the importance of low-cost healthcare as there is increasing pressure on healthcare budgets worldwide 3 A study in the United Kingdom suggested that mesalamine accounts for up to 25 of the total healthcare costs in UC with an average annual maintenance prescription estimated to be 740 or 850 4 While mesalamine is safe and well-tolerated it has rare but serious idiosyncratic adverse effects including pancreatitis Around 3 of patients even report a paradoxical worsening of diarrhoea 5 The negative impact of polypharmacy must also be taken into consideration with non-compliance often linked to higher pill burdens 6 In fact the burden of a more complex medication regimen has been associated with poorer outcomes in both UC with real-world compliance as low as 50 7 Furthermore compliance to topical 5-ASA therapy is even worse than oral therapy 8 Thus there is a clear need to explore the withdrawal of 5-ASA from the UC treatment regimen
Two studies have evaluated the outcomes of withdrawal of oral 5-ASA in patients concomitantly treated with immunomodulators Both studies showed no difference in relapse rates between patients with ulcerative colitis receiving either azathioprine monotherapy or combination of azathioprine and oral 5-ASA therapy with better compliance in azathioprine monotherapy group 9 10 No randomized controlled trial RCT has yet evaluated the withdrawal of 5-ASA in patients treated with either biologic therapy or tofacitinib However a recent cohort study from two national population-based databases from the United States and Denmark showed no increase in the risk of adverse clinical events after withdrawing oral 5-ASA within 90 days of initiating anti-TNF therapy compared to those who continued 5-ASA 11 No RCT or prospective study has evaluated the outcome of 5-ASA withdrawal in patients receiving tofacitinib therapy Indirect evidence from subgroup analysis of RCTs suggests that concomitant 5-ASA therapy does not increase the likelihood of maintaining clinical remission after escalation to tofacitinib 12
Study Oversight
Has Oversight DMC:
None
Is a FDA Regulated Drug?:
None
Is a FDA Regulated Device?:
None
Is an Unapproved Device?:
None
Is a PPSD?:
None
Is a US Export?:
None
Is an FDA AA801 Violation?:
None