VTX958 for the Treatment of Moderately to Severely Active Crohn's Disease
- Conditions
- Crohn Disease
- Interventions
- Drug: VTX958Drug: VTX958 Placebo
- Registration Number
- NCT05688852
- Lead Sponsor
- Ventyx Biosciences, Inc
- Brief Summary
This is a multicenter, randomized, double-blind placebo-controlled, parallel group study to evaluate the efficacy and safety of VTX958 in participants with moderately to severely active Crohn's Disease.
- Detailed Description
This is a multicenter, randomized, double-blind placebo-controlled, parallel group study to evaluate the efficacy and safety of VTX958 in participants with moderately to severely active Crohn's Disease. Approximately 132 eligible patients will be randomized, and randomization will be stratified by prior use of biologics for the treatment of CD (yes/no).
The study consists of a 30-day Screening Period, a 12-week double-blind Induction Treatment Period, a 40-week double-blind Maintenance Treatment Period, an Open-Label Extension (OLE) of up to 144 weeks, and a 30-day safety Follow-Up Period. The maximum duration of treatment will be 36 months, including the Induction, Maintenance, and OLE Periods. For all participants, a Follow-Up visit will be performed at 30 days after the last dose of study drug.
Objectives Primary Objectives
\* Evaluate the efficacy of VTX958 in achieving reduction in Crohn's Disease Activity Index (CDAI) score and endoscopic response at the end of the Induction Period
Secondary Objectives
* Evaluate the efficacy of VTX958 in inducing clinical and symptomatic response and remission at the end of the Induction Period
* Evaluate the efficacy of VTX958 in inducing endoscopic response and clinical remission at the end of the Induction Period
Recruitment & Eligibility
- Status
- ACTIVE_NOT_RECRUITING
- Sex
- All
- Target Recruitment
- 132
- Men or women, 18 to 75 years of age, inclusive, at the time of consent
- Capable of giving signed informed consent
- Documented diagnosis of CD ≥ 3 months prior to Day 1. The diagnosis of CD must be confirmed by clinical, endoscopic, and histologic evidence.
- Moderately to severely active CD
- Current diagnosis of ulcerative colitis, indeterminate colitis, microscopic colitis, ischemic colitis, or infectious colitis
- Presence of a stoma or ileoanal pouch
- Presence of currently known complications of CD such as symptomatic bowel stricture(s) and >2 missing segments of the following 5 segments: terminal ileum, right colon, transverse colon, left and sigmoid colon, and rectum, fulminant colitis, toxic megacolon or any other manifestation that may require surgery or hospitalization
- Known diagnosis of short gut or bowel syndrome
- Previous exposure to VTX958 or any other TYK2 inhibitor (eg, deucravacitinib) in any study
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description VTX958 Dose A VTX958 - VTX958 Dose B VTX958 - VTX958 Placebo VTX958 Placebo -
- Primary Outcome Measures
Name Time Method Change in mean Crohn's disease Activity Index (CDAI) score from baseline to week 12 During screening to week 12 Change in Mean CDAI (Crohn's disease Activity Index). CDAI is a weighted index comprising eight Crohn's Disease (CD)-related clinical and laboratory variables, to assess CD disease activity. Three of the variables, stool frequency, abdominal pain, and general well-being, are patient-reported measures recorded daily. The total CDAI score is calculated using the sum of each variable times the multiplier. The total score range of the CDAI is from 0 to 600.
The proportion of participants achieving endoscopic response at Week 12 During screening to week 12 SES-CD is an endoscopic grading system is used to assess CD disease activity. The SES-CD assesses 4 endoscopic variables: the size of ulcers, ulcerated surface, affected surface, and presence of narrowing. Each variable score ranging from 0 to 3. The total SES-CD score is calculated using the sum of all parameter scores in 5 segments: terminal ileum, right colon, transverse colon, left colon, and rectum.
- Secondary Outcome Measures
Name Time Method Change from baseline in mean simple endoscopic score in Crohn's disease SES-CD at Week 12 During screening to week 12 Change from baseline in mean simple endoscopic score in Crohn's disease SED-CD at 12 weeks. The SES-CD is an endoscopic grading system is used to assess CD disease activity. The SES-CD assesses 4 endoscopic variables: the size of ulcers, ulcerated surface, affected surface, and presence of narrowing. Each variable score ranging from 0 to 3. The total SES-CD score is calculated using the sum of all parameter scores in 5 segments: terminal ileum, right colon, transverse colon, left colon, and rectum.
Proportion of participants achieving clinical remission at Week 12 During screening to week 12 Clinical remission is defined as a CDAI score \< 150. CDAI is a weighted index comprising eight Crohn's Disease (CD)-related clinical and laboratory variables, to assess CD disease activity. Three of the variables, stool frequency, abdominal pain, and general well-being, are patient-reported measures recorded daily. The total CDAI score is calculated using the sum of each variable times the multiplier. The total score range of the CDAI is from 0 to 600.
Proportion of participants achieving patient-reported outcome 2 (PRO2) remission at Week 12 During screening to week 12 The proportion of participants achieving PRO2 remission at week 12. PRO2 remission is defined is an unweighted CDAI component of daily AP score ≤ 1 and unweighted CDAI component of daily average stool frequency (SF) score ≤ 3
Proportion of participants achieving clinical response at Week 12 During screening to week 12 Proportion of participants achieving clinical response at Week 12. A clinical response is defined as ≥ 100 points reduction from baseline in CDAI score or CDAI score \< 150. CDAI is a weighted index comprising eight Crohn's Disease (CD)-related clinical and laboratory variables, to assess CD disease activity. Three of the variables, stool frequency, abdominal pain, and general well-being, are patient-reported measures recorded daily. The total CDAI score is calculated using the sum of each variable times the multiplier. The total score range of the CDAI is from 0 to 600.
Proportion of participants achieving both endoscopic response (outcome- measure # 2) and clinical remission (outcome measure # 4) at Week 12 During screening to week 12 Proportion of participants achieving both endoscopic response (as described in outcome measure 2) and clinical remission (as described in outcome measure 4) at Week 12.
Trial Locations
- Locations (105)
Local Site # 840105
🇺🇸Garden Grove, California, United States
Local Site # 840109
🇺🇸Lancaster, California, United States
Local Site # 840124
🇺🇸Kissimmee, Florida, United States
Local Site # 840104
🇺🇸Miami, Florida, United States
Local Site # 840108
🇺🇸Orlando, Florida, United States
Local Site # 840125
🇺🇸Orlando, Florida, United States
Local Site # 840112
🇺🇸Atlanta, Georgia, United States
Local Site # 840115
🇺🇸Glenview, Illinois, United States
Local Site # 840107
🇺🇸Gurnee, Illinois, United States
Local Site # 840119
🇺🇸New Albany, Indiana, United States
Local Site # 840127
🇺🇸Louisville, Kentucky, United States
Local Site # 840113
🇺🇸Shreveport, Louisiana, United States
Local Site # 840117
🇺🇸Chevy Chase, Maryland, United States
Local Site # 840118
🇺🇸Rockville, Maryland, United States
Local Site # 840116
🇺🇸Liberty, Missouri, United States
Local Site # 840121
🇺🇸Winston-Salem, North Carolina, United States
Local Site # 840122
🇺🇸Columbus, Ohio, United States
Local Site # 840106
🇺🇸Oklahoma City, Oklahoma, United States
Local Site # 840123
🇺🇸Myrtle Beach, South Carolina, United States
Local Site # 840111
🇺🇸Garland, Texas, United States
Local Site # 840103
🇺🇸Katy, Texas, United States
Local Site # 840110
🇺🇸Lubbock, Texas, United States
Local Site # 840114
🇺🇸Lubbock, Texas, United States
Local Site # 840102
🇺🇸Southlake, Texas, United States
Local Site # 840101
🇺🇸Tyler, Texas, United States
Local Site # 840126
🇺🇸West Jordan, Utah, United States
Local Site # 036106
🇦🇺Concord, Australia
Local Site # 036103
🇦🇺Melbourne, Australia
Local Site # 036104
🇦🇺Melbourne, Australia
Local Site # 036101
🇦🇺Melbourne, Australia
Local Site # 036102
🇦🇺Parkville, Australia
Local Site # 036105
🇦🇺Perth, Australia
Local Site # 076102
🇧🇷Taguatinga, Distrito Federal, Brazil
Local Site # 076104
🇧🇷Porto Alegre, Rio Grande do Su, Brazil
Local Site # 076106
🇧🇷Curitiba, Brazil
Local Site # 076107
🇧🇷Curitiba, Brazil
Local Site # 076101
🇧🇷Santo André, Brazil
Local Site # 076103
🇧🇷São Paulo, Brazil
Local Site # 076105
🇧🇷São Paulo, Brazil
Local Site # 100102
🇧🇬Ruse, Bulgaria
Local Site # 100103
🇧🇬Sofia, Bulgaria
Local Site # 100101
🇧🇬Sofia, Bulgaria
Local Site # 124103
🇨🇦Oakville, Ontario, Canada
Local Site # 124104
🇨🇦Oshawa, Ontario, Canada
Local Site # 124101
🇨🇦Toronto, Ontario, Canada
Local Site # 124102
🇨🇦Woodbridge, Ontario, Canada
Local Site # 203106
🇨🇿Brno, Czechia
Local Site # 203102
🇨🇿Brno, Czechia
Local Site # 203105
🇨🇿Hradec Králové, Czechia
Local Site # 203104
🇨🇿Ostrava, Czechia
Local Site # 203101
🇨🇿Slaný, Czechia
Local Site # 203103
🇨🇿Ústí Nad Labem, Czechia
Local Site # 268105
🇬🇪Tbilisi, Georgia
Local Site # 268103
🇬🇪Tbilisi, Georgia
Local Site # 268101
🇬🇪Tbilisi, Georgia
Local Site # 276102
🇩🇪Tuebingen, Baden-Wuerttemberg, Germany
Local Site # 276105
🇩🇪Ulm, Baden-Wuerttemberg, Germany
Local Site # 276106
🇩🇪Duisburg, North Rhine-Westphalia, Germany
Local Site # 276109
🇩🇪Berlin, Germany
Local Site # 276104
🇩🇪Berlin, Germany
Local Site # 276108
🇩🇪Hessen, Germany
Local Site # 276107
🇩🇪Kiel, Germany
Local Site # 348101
🇭🇺Budapest, Hungary
Local Site # 348102
🇭🇺Békéscsaba, Hungary
Local Site # 348106
🇭🇺Gyöngyös, Hungary
Local Site #348104
🇭🇺Szeged, Hungary
Local Site # 348103
🇭🇺Szekszárd, Hungary
Local Site # 348105
🇭🇺Tatabánya, Hungary
Local Site # 376108
🇮🇱Haifa, Israel
Local Site # 376103
🇮🇱Ashkelon, Israel
Local Site # 376105
🇮🇱Jerusalem, Israel
Local Site # 376107
🇮🇱Jerusalem, Israel
Local Site # 376101
🇮🇱Petah tikva, Israel
Local Site # 376102
🇮🇱Reẖovot, Israel
Local Site # 380104
🇮🇹Milan, Lombardy, Italy
Local Site # 380105
🇮🇹Negrar, Verona, Italy
Local Site # 380101
🇮🇹Bari, Italy
Local Site # 380107
🇮🇹Milan, Italy
Local Site # 380109
🇮🇹Rome, Italy
Local Site # 380106
🇮🇹Turin, Italy
Local Site # 440101
🇱🇹Vilnius, Lithuania
Local Site # 498101
🇲🇩Chisinau, Moldova, Republic of
Local Site # 498102
🇲🇩Chisinau, Moldova, Republic of
Local Site # 616116
🇵🇱Bydgoszcz, Poland
Local Site #616113
🇵🇱Knurów, Poland
Local Site # 616112
🇵🇱Kraków, Poland
Local Site # 616117
🇵🇱Lublin, Poland
Local Site # 616109
🇵🇱Nowy Targ, Poland
Local Site # 616107
🇵🇱Oświęcim, Poland
Local Site # 616115
🇵🇱Poznan, Poland
Local Site # 616104
🇵🇱Rzeszów, Poland
Local Site # 616118
🇵🇱Staszów, Poland
Local Site # 616106
🇵🇱Szczecin, Poland
Local Site # 616102
🇵🇱Warsaw, Poland
Local Site # 616114
🇵🇱Wrocław, Poland
Local Site # 616103
🇵🇱Wrocław, Poland
Local Site # 616108
🇵🇱Wrocław, Poland
Local Site # 616110
🇵🇱Łódź, Poland
Local Site # 616105
🇵🇱Łódź, Poland
Local Site # 616101
🇵🇱Łódź, Poland
Local Site # 703103
🇸🇰Bratislava, Slovakia
Locla Site # 703101
🇸🇰Košice, Slovakia
Local Site # 703106
🇸🇰Martin, Slovakia
Local Site # 703104
🇸🇰Prešov, Slovakia
Local Site # 703102
🇸🇰Šahy, Slovakia