Psoriasis Clinical Trial
Official title:
A Multicenter, Randomized, Double-blinded Study Evaluating the Pharmacokinetics, Efficacy and Safety of Multiple Switches Between Ustekinumab and ABP 654 Compared With Continued Use of Ustekinumab in Subjects With Moderate to Severe Plaque Psoriasis
| Verified date | January 2024 |
| Source | Amgen |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
The purpose of the study is to evaluate pharmacokinetic similarity, efficacy, safety and immunogenicity of multiple switches between ustekinumab and ABP 654 compared with continued use of ustekinumab in participants with moderate to severe plaque psoriasis.
| Status | Completed |
| Enrollment | 494 |
| Est. completion date | February 28, 2023 |
| Est. primary completion date | February 28, 2023 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years to 75 Years |
| Eligibility | Inclusion Criteria: - Participant has stable moderate to severe plaque psoriasis for at least 6 months - Participant has a score of PASI = 12, involvement of = 10% body surface area and static Physician Global Assessment = 3 at screening and at baseline - Participant is a candidate for phototherapy or systemic therapy - Participant has previous failure, inadequate response, intolerance, or contraindication to at least 1 conventional antipsoriatic systemic therapy - Female participant should have a negative serum pregnancy test during screening and a negative urine pregnancy test at baseline - Participant or legally acceptable representative is capable of giving signed Institutional Review Board (IRB)/Independent Ethics Committee (IEC) informed consent - Participant has no known history of latent or active tuberculosis - Participant with a positive purified protein derivative (PPD) test and a history of Bacillus Calmette-Guérin (BCG) vaccination is allowed with a negative Quantiferon/T-spot test - Participant with a positive PPD test or participant with a positive or indeterminate Quantiferon/T-spot test is allowed if he/she has all the following: - No symptoms per tuberculosis worksheet provided by the sponsor, Amgen Inc. - Documented history of adequate prophylaxis initiation prior to receiving investigational product in accordance with local recommendations - No known exposure to a case of active tuberculosis after most recent prophylaxis - No evidence of active tuberculosis on chest radiograph within 3 months prior to the first dose of investigational product Exclusion Criteria: - Participant has erythrodermic psoriasis, pustular psoriasis, guttate psoriasis, medication induced psoriasis, or other skin conditions at the time of screening (eg, eczema) that would interfere with evaluations of the effect of investigational product of psoriasis - Participant has an active infection or history of infections - Participant has uncontrolled, clinically significant systemic disease, such as uncontrolled diabetes mellitus, cardiovascular disease, renal disease, liver disease, or hypertension - Participant has a mean QT internal or abnormal long QT syndrome corrected using Fridericia's formula (QTcF) of > 450 msec (for male participant) or > 470 msec (for female participant) at baseline that, in the opinion of the Investigator, is abnormal or clinically significant - Participant has moderate to severe heart failure (New York Heart Associate class III/IV) - Participant has known hypersensitivity to the investigational product or to any of the excipients - Participant has laboratory abnormalities at screening - Participant has had previous treatment with any agent specifically targeting interleukin (IL)-12 or IL-23 within 1 year prior to enrollment - Participant has received biologic treatment for psoriasis within the previous month or 5 drug half-lives (whichever is longer) prior to enrollment - Participant has received any investigational agents within the previous month or 5 half-lives (whichever is longer) prior to enrollment - Participant has received non-biologic systemic psoriasis therapy within 4 weeks prior to enrollment - Participant has received ultraviolet A phototherapy (with or without psoralen) or excimer laser within 4 weeks prior to enrollment, or ultraviolet B phototherapy within 2 weeks prior to enrollment - Participant has received topical psoriasis treatment within 2 weeks prior to enrollment - Participant has received other investigational procedures within 4 weeks prior to enrollment and during the course of the study - Female participant is pregnant or breastfeeding or planning to become pregnant while participating in the study and for at least 5 months after the last dose of investigational product - Sexually active participants and their partners who are of childbearing potential and not agreeing to use adequate protocol defined contraception methods while participating in the study and for 5 months after the last dose of investigational product |
| Country | Name | City | State |
|---|---|---|---|
| Canada | CCA Medical Research | Ajax | Ontario |
| Canada | SimcoDerm Medical and Surgical Dermatology Center | Barrie | Ontario |
| Canada | Dr. Irina Turchin PC Inc. | Fredericton | New Brunswick |
| Canada | Guelph Dermatology Research | Guelph | Ontario |
| Canada | Dr Wei Jing Loo Medicine Professional Corporation | London | Ontario |
| Canada | Lynderm Research Inc | Markham | Ontario |
| Canada | DermEdge Research Inc. | Mississauga | Ontario |
| Canada | Dr. S. K. Siddha Medicine Professional Corporation - Doctor's Office | Newmarket | Ontario |
| Canada | North York Research Inc. - Dermatology | North York | Ontario |
| Canada | Dermatology Ottawa Research Centre | Ottawa | Ontario |
| Canada | Enverus Medical Research | Surrey | British Columbia |
| Canada | Research Toronto | Toronto | Ontario |
| Canada | K. Papp Clinical Research Inc. | Waterloo | Ontario |
| Canada | Wiseman Dermatology Research Inc. | Winnipeg | Manitoba |
| Estonia | Confido Private Medical Clinic - General Practice/Medicine | Tallinn | Harjumaa |
| Estonia | Innomedica OÜ | Tallinn | |
| Estonia | Clinical Research Center | Tartu | Tartumaa |
| Estonia | Tartu University Hospital | Tartu | Tartumaa |
| Georgia | ,,KANVENI - Scientific/Research National Center of Dermatology and Venereology LLC | Tbilisi | |
| Georgia | ,,Tbilisi Cancer center"LTD | Tbilisi | T'bilisi |
| Georgia | Acad.Fridon Todua Medical Center- Research Institute of Clinical Medicine | Tbilisi | T'bilisi |
| Georgia | LTD Aversi Clinic | Tbilisi | T'bilisi |
| Georgia | LTD Israeli-Georgian Medical Research Clinic Helsicore | Tbilisi | T'bilisi |
| Germany | Dermazentrum Augsburg | Augsburg | Bayern |
| Germany | Fachklinik Bad Bentheim | Bad Bentheim | Niedersachsen |
| Germany | Charite - Campus Charite Mitte (CCM) - Dermatologie & Allergologie - Dermatologie & Allergologie | Berlin | |
| Germany | Rothhaar Studien GmbH | Berlin | |
| Germany | Klinische Forschung Dresden GmbH | Dresden | Sachsen |
| Germany | Universitätsklinikum Carl Gustav Carus | Dresden | Sachsen |
| Germany | Universitätsklinikum Frankfurt am Main - Klinik für Dermatol | Frankfurt/Main | Hessen |
| Germany | Derma-Study-Center-FN | Friedrichshafen | Baden-Württemberg |
| Germany | UK-SH - Lübeck | Lübeck | Schleswig-Holstein |
| Germany | Dermatologische Gemeinschaftspraxis Dres.Scholz Sebastian Schilling | Mahlow | Brandenburg |
| Germany | Praxis Hoffmann | Witten | Nordrhein-Westfalen |
| Hungary | Qualiclinic Kft | Budapest | Pest |
| Hungary | UNOMEDICALTRIALS Kft | Budapest | Pest |
| Hungary | Debreceni Egyetem Klinikai Központ Nagyerdei Campus | Debrecen | Hajdú-Bihar |
| Hungary | Brgyógyászati és Allergológiai Magánrendelés | Szolnok | Jász-Nagykun-Szolnok |
| Latvia | J.Kisis LtD | Riga | Rga |
| Latvia | Riga 1st hospital, Clinic of Dermatology and STD | Riga | Rga |
| Latvia | Smite Aija doctor practice in dermatology, venereology | Talsi | |
| Poland | RENEW CLINIC Spolka Jawna | Bialystok | |
| Poland | Centrum Medyczne Pratia Bydgoszcz | Bydgoszcz | |
| Poland | MICS Centrum Medyczne Bydgoszcz | Bydgoszcz | |
| Poland | Centrum Medyczne Pratia Gdynia | Gdynia | |
| Poland | Barbara Rewerska Diamond Clinic | Krakow | |
| Poland | Centrum Medyczne ALL-MED Badania Kliniczne | Krakow | Maopolskie |
| Poland | Centrum Medyczne Plejady | Krakow | Maopolskie |
| Poland | Centrum Medyczne PROMED | Krakow | |
| Poland | Krakowskie Centrum Medyczne Sp. z o.o. | Krakow | |
| Poland | ETG Siedlce | Siedlce | |
| Poland | RCMed Oddzial Sochaczew | Sochaczew | |
| Poland | Twoja Przychodnia - Szczecinskie Centrum Medyczne | Szczecin | |
| Poland | Centrum Medyczne Evimed | Warszawa | |
| Poland | MICS Centrum Medyczne Warszawa | Warszawa | Mazowieckie |
| Poland | RCMed Oddzia Warszawa | Warszawa | |
| Poland | DermMedica Sp. z o.o. | Wroclaw | |
| United States | Hamilton Research, LLC | Alpharetta | Georgia |
| United States | Zenith Research Inc. | Beverly Hills | California |
| United States | DS Research | Clarksville | Indiana |
| United States | Austin Institute for Clinical Research, Inc. | Dripping Springs | Texas |
| United States | Psoriasis Treatment Center of Central New Jersey | East Windsor | New Jersey |
| United States | Hamzavi Dermatology | Fort Gratiot | Michigan |
| United States | Center for Dermatology Clinical Research, Inc. | Fremont | California |
| United States | Burke Pharmaceutical Research | Hot Springs | Arkansas |
| United States | Encore Research Group-Jacksonville Center for Clinical Resea | Jacksonville | Florida |
| United States | Altus Research, Inc. | Lake Worth | Florida |
| United States | International Dermatology Research, Inc. | Miami | Florida |
| United States | Minnesota Clinical Study Center | New Brighton | Minnesota |
| United States | Quest Dermatology Research | Northridge | California |
| United States | Skin Specialists PC | Omaha | Nebraska |
| United States | Leavitt Medical Associates of Florida d/b/a Ameriderm Research | Ormond Beach | Florida |
| United States | Riverchase Dermatology and Cosmetic Surgery | Pembroke Pines | Florida |
| United States | Austin Institute for Clinical Research, Inc - Dermatology | Pflugerville | Texas |
| United States | Oregon Medical Research Center | Portland | Oregon |
| United States | ActivMed Practices & Research, LLC. | Portsmouth | New Hampshire |
| United States | MediSearch Clinical Trials | Saint Joseph | Missouri |
| United States | Progressive Clinical Research [Texas] | San Antonio | Texas |
| United States | Advanced Medical Research PC | Sandy Springs | Georgia |
| United States | Southern California Dermatology, Inc | Santa Ana | California |
| United States | Olympian Clinical Research | Tampa | Florida |
| United States | Kansas Medical Clinic, PA | Topeka | Kansas |
| United States | The Dermatology Group, PC | Verona | New Jersey |
| United States | Center for Clinical Studies, LTD., LLP | Webster | Texas |
| United States | Integrated Clinical Trial Services Inc. | West Des Moines | Iowa |
| United States | Dundee Dermatology | West Dundee | Illinois |
| United States | Wilmington Dermatology Center | Wilmington | North Carolina |
| United States | Clinical Pharmacology Study Group | Worcester | Massachusetts |
| Lead Sponsor | Collaborator |
|---|---|
| Amgen |
United States, Canada, Estonia, Georgia, Germany, Hungary, Latvia, Poland,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Area Under the Plasma Concentration Time Curve (AUC) Over the Dosing Interval (AUCtau) Between Week 52 and Week 64 | AUCtau from time 0 (week 52) over the dosing interval up to week 64 is presented. Pharmacokinetic (PK) parameters are based on ABP 654 in the switching group and on ustekinumab in the continued-use group. | Blood samples were taken pre-dose week 52; and at 2 days, 7 days, 10 days, 2 weeks, 4 weeks, 8 weeks, and 12 weeks after the week 52 dose | |
| Primary | Maximum Observed Serum Concentration (Cmax) Between Week 52 and Week 64 | Cmax between week 52 and week 64 is presented. PK parameters are based on ABP 654 in the switching group and on ustekinumab in the continued-use group. | Blood samples were taken pre-dose week 52; and at 2 days, 7 days, 10 days, 2 weeks, 4 weeks, 8 weeks, and 12 weeks after the week 52 dose | |
| Secondary | Time of Maximum Serum Concentration (Tmax) Between Week 52 and Week 64 | Tmax between week 52 and week 64 is presented. PK parameters are based on ABP 654 in the switching group and on ustekinumab in the continued-use group. | Blood samples were taken pre-dose week 52; and at 2 days, 7 days, 10 days, 2 weeks, 4 weeks, 8 weeks, and 12 weeks after the week 52 dose | |
| Secondary | Serum Trough Concentration at Steady-state (Ctrough,ss) at Week 28, Week 40, and Week 52 | Ctrough,ss at weeks 28, 40, and 52 are presented. PK parameters are based on ABP 654 in the switching group and on ustekinumab in the continued-use group. | Blood samples were taken pre-dose week 28, week 40, and week 52 | |
| Secondary | PASI Percent Improvement From Baseline at Week 64 | The PASI is a measure of the average redness (erythema), thickness (induration), and scaliness (scaling), each graded on a 0 to 4 scale of the lesions, weighted by the area of involvement. PASI combines the assessment of the severity of lesions and the area affected into a single score in the range 0 (no disease) to 72 (maximal disease). PASI percent improvement is defined as 100 x (value at baseline - value at post-baseline visit) / value at baseline. A positive value indicates PASI improvement. Baseline data were derived based on observed data and at week 64 were derived based on multiple imputation (MI) data. Baseline was defined as the last non-missing assessment taken prior to the first dose of investigational product for the study. | Baseline (day 1) and week 64 | |
| Secondary | PASI 75 Response at Week 64 | The PASI is a measure of the average redness (erythema), thickness (induration), and scaliness (scaling), each graded on a 0 to 4 scale of the lesions, weighted by the area of involvement. PASI combines the assessment of the severity of lesions and the area affected into a single score in the range 0 (no disease) to 72 (maximal disease). PASI response was defined as a participant meeting or surpassing a pre-specified threshold for percent improvement in PASI score compared to the baseline PASI score. An improvement of at least 75% qualified a participant as being a PASI 75 responder. Missing PASI 75 responses at week 64 were imputed by non-responder imputation (NRI). Baseline was defined as the last non-missing assessment taken prior to the first dose of investigational product for the study. | Baseline (day 1) and week 64 | |
| Secondary | PASI 100 Response at Week 64 | The PASI is a measure of the average redness (erythema), thickness (induration), and scaliness (scaling), each graded on a 0 to 4 scale of the lesions, weighted by the area of involvement. PASI combines the assessment of the severity of lesions and the area affected into a single score in the range 0 (no disease) to 72 (maximal disease). PASI response was defined as a participant meeting or surpassing a pre-specified threshold for percent improvement in PASI score compared to the baseline PASI score. An improvement of 100% qualified a participant as being a PASI 100 responder. Missing PASI 100 responses at week 64 were imputed by NRI. Baseline was defined as the last non-missing assessment taken prior to the first dose of investigational product for the study. | Baseline (day 1) and week 64 | |
| Secondary | Number of Participants With Treatment-emergent Adverse Events (TEAEs): Post-randomization Period | TEAEs during the post-randomization period were defined as AEs that started on or after the first dose of investigational product post-randomization and prior to the end of study. The number of participants who experienced any TEAE, and who experienced a serious TEAE are presented. A serious TEAE was defined as any untoward medical occurrence that meets at least 1 of the following serious criteria: resulted in death (fatal), was life-threatening, required inpatient hospitalization or prolongation of existing hospitalization, resulted in persistent or significant disability/incapacity, congenital anomaly/birth defect, or other medically important serious event. | Week 28 to week 64 | |
| Secondary | Number of Participants With Events of Interest (EOI): Post-randomization Period | The treatment-emergent EOIs prespecified for this study included serious systemic hypersensitivity reactions, facial palsy, pustular psoriasis, erythrodermic psoriasis, serious infections (including mycobacterial and salmonella infections), malignancy, cardiovascular events, reversible posterior leukoencephalopathy syndrome (RPLS), serious depression including suicidality, and venous thromboembolism. | Week 28 to week 64 | |
| Secondary | Number of Participants With Antidrug Antibodies (ADAs): Post-randomization Period | The number of participants developing binding or neutralizing ADAs during the post-randomization period is defined as the number of participants in the safety analysis set who had a positive result post-randomization and had never tested positive (i.e., negative or no results) prior to the first dose of post-randomization investigational product and who have at least one ADA result post randomization. A transient antibody results was defined as a positive result during the post-randomization period with a negative result at the participant's last visit tested within the respective study period. Baseline was defined as the last non-missing assessment taken prior to the first dose of investigational product for the study. | Baseline (pre-dose day 1), week 4, week 16, week 28, week 40, week 52 and week 64 |
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