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COMBINATION WITH 5-ASA

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CORTIMENT®

IS NOW SUPPORTED BY REAL WORLD EVIDENCE

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Primary Endpoint

Secondary Endpoint

A SIGNIFICANTLY GREATER PERCENTAGE OF PATIENTS ACHIEVED CLINICAL AND ENDOSCOPIC REMISSION AFTER 8 WEEKS COMPARED TO PLACEBO (P=0.049)1

 

Endoscopic remission and histological healing† were significant for CORTIMENT® vs placebo
(20.0 vs 12.3, p=0.02 and 27.0 vs 17.5, p=0.02 respectively)*1

Graph adapted from Rubin D, et al.2017.
*Results from the modified intention to treat population (n=458).
†Objective secondary endpoints.

Primary Endpoint

 

SECONDARY ENDPOINTS*1

 

  • Significantly more patients achieved endoscopic remission and histological healing with
    CORTIMENT® vs placebo at week 8
  • Clinical remission at week 8 was not significantly different for CORTIMENT® vs placebo

Based on an assumption of remission rates of 15% for placebo and 27% for budesonide MMX, a total of 250 patients per group would be expected to provide 90% power to detect a significant difference between the two groups with a two-sided α = 0.05.

Secondary Endpoint

CONTRIBUTE study used a notably stringent definition of remission1

 

Primary endpoint: patients achieving combined clinical and endoscopic remission at week 8

 

A UC-DAI score ≤ 1 with subscale scores of 0 for:

  • Stool frequency
  • Rectal bleeding
  • Mucosal appearance

UC-DAI = UC disease activity index

STUDY SUMMARY

Budesonide multimatrix is efficacious for mesalazine-refractory, mild to moderate ulcerative colitis: A randomised, placebo-controlled trial
Objectives

To compare the efficacy of Cortiment for induction of remission in patients with mild to moderate ulcerative colitis refractory to baseline mesalazine therapy.

Design

A randomised, double-blind, placebo-controlled, multicentre trial conducted in the USA, Canada and Europe

Primary endpoint

The percentage of patients achieving combined clinical and endoscopic remission at week 8

A UC-DAI score ≤1 with subscale scores of 0 for:

  • Stool frequency
  • Rectal bleeding
  • Mucosal appearance
Methods

Patients (n=510) were randomised 1:1 to receive budesonide MMX 9 mg or placebo once daily after breakfast for 8 weeks in an outpatient setting. Patients continued baseline treatment with oral mesalazine ≥ 2.4 g/day.

Secondary Endpoint

The percentage of patients achieving clinical remission [UCDAI subscale scores of 0 for rectal bleeding and stool frequency] and the percentage of patients achieving endoscopic remission [UCDAI subscale score of 0 for mucosal appearance] at Week 8. An exploratory endpoint included the percentage of patients achieving histological healing [histological activity grade of 0] at Week 8

KEY INCLUSION CRITERIA

  • Male or female, aged 18-75 years
  • Active UC with a UC-DAI mucosal appearance subscale score ≥1
  • Mild or moderate UC with a baseline UC-DAI score ≥4 and ≤10, mucosal appearance sub score ≥1, and physician’s rating of disease activity score of 1 or 2
  • Receiving oral mesalazine ≥2.4 g/day (or equivalent) for ≥6 weeks before randomisation

KEY EXCLUSION CRITERIA

  • Limited distal proctitis
  • Diagnosis of Crohn’s disease, indeterminate colitis or infectious colitis
  • A history of pancolitis for ≥8 years or left-sided colitis for ≥15 years without surveillance or liver cirrhosis, hepatic or renal disease insufficiency
  • Use of:
    • Budesonide MMX® oral corticosteroids during the previous 4 weeks
    • Rectal mesalazine or corticosteroid formulation during the previous 2 weeks
    • Immunosuppressive agents during the previous 8 weeks
    • Biologic therapies during the previous 3 months
    • Systemic or rectal steroids, any mesalazine other than the existing oral mesalazine at the same dose a patient was receiving at study initiation
    • Anti-tumour necrosis factor-a agents and other biologics, and immunosuppressants

 

anti-TNF = anti-tumor necrosis factor,
UC-DAI = UC disease activity index

  • Rubin D, et al. J Crohns Colitis. 2017;11(7):785-791.
Further Clinical Efficacy
iSTART
Prescribing Cortiment
Resources

Job Code: UK-COR-2200001 - Date of preparation: January 2022

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