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En studie for å vurdere farmakokinetikken, sikkerheten og effekten av to doser bimekizumab hos deltakere i ungdomsstudier med moderat til alvorlig plakkpsoriasis (BE CONNECTED)

24. april 2026 oppdatert av: UCB Biopharma SRL

En multisenter, åpen, randomisert studie for å vurdere farmakokinetikken, sikkerheten og effekten av to doser bimekizumab hos deltakere i ungdomsstudier med moderat til alvorlig plakkpsoriasis

Formålet med studien er å vurdere farmakokinetikken (PK) til bimekizumab administrert subkutant (sc) hos ungdom med moderat til alvorlig plakkpsoriasis (PSO).

Studieoversikt

Status

Fullført

Forhold

Intervensjon / Behandling

Studietype

Intervensjonell

Registrering (Faktiske)

41

Fase

  • Fase 2

Kontakter og plasseringer

Denne delen inneholder kontaktinformasjon for de som utfører studien, og informasjon om hvor denne studien blir utført.

Studiesteder

  • Canada
      • Calgary, Canada
        • Ps0020 50354
      • St. John's, Canada
        • Ps0020 50357
  • Forente stater
    • Indiana
      • Indianapolis, Indiana, Forente stater, 46250
        • Ps0020 50344
    • Texas
      • Cypress, Texas, Forente stater, 77433
        • Ps0020 50359
  • Polen
      • Bialystok, Polen
        • Ps0020 40626
      • Lodz, Polen
        • Ps0020 40625
      • Rzeszów, Polen
        • Ps0020 40396
      • Warsaw, Polen
        • Ps0020 40335
      • Wroclaw, Polen
        • Ps0020 40333
      • Wroclaw, Polen
        • Ps0020 40334
  • Tyskland
      • Frankfurt, Tyskland
        • Ps0020 40645

Deltakelseskriterier

Forskere ser etter personer som passer til en bestemt beskrivelse, kalt kvalifikasjonskriterier. Noen eksempler på disse kriteriene er en persons generelle helsetilstand eller tidligere behandlinger.

Kvalifikasjonskriterier

Alder som er kvalifisert for studier

12 år til 17 år (Barn)

Tar imot friske frivillige

Nei

Beskrivelse

Inklusjonskriterier:

  • Deltakeren må være ≥12 til <18 år på tidspunktet for signering av det informerte samtykket/samtykket i henhold til lokale forskrifter

  • Deltakeren har hatt en diagnose av moderat til alvorlig plakkpsoriasis (PSO) i minst 3 måneder før screeningbesøket og:

    1. Kroppsoverflate (BSA) påvirket av PSO ≥10 %
    2. Investigator's Global Assessment (IGA)-score ≥3 (på en skala fra 0 til 4)
    3. Psoriasis Area and Severity Index (PASI) score ≥12 ELLER
    4. PASI-score ≥10 pluss minst 1 av følgende:

    Jeg. Klinisk relevant ansiktsinvolvering ii. Klinisk relevant genital involvering iii. Klinisk relevant hånd- og fotinvolvering

  • Deltaker må være kandidat for systemisk PSO-terapi og/eller foto-/kjemoterapi
  • Kroppsvekt ≥30 kg og kroppsmasseindeks for alderspersentil på ≥5 ved baseline
  • Mann eller kvinne En kvinnelig deltaker vil være kvalifisert til å delta hvis hun ikke er gravid, ikke ammer, og en kvinne i fertil alder (WOCBP) godtar å følge prevensjonsveiledningen
  • I stand til å gi/ha foreldre eller juridisk representant gi signert informert samtykke/samtykke (der det er relevant)

Ekskluderingskriterier:

  • Deltakeren har tilstedeværelse av guttat, invers, pustulær eller erytrodermisk PSO eller annen dermatologisk tilstand som kan påvirke den kliniske vurderingen av PSO
  • Deltakeren har en historie med inflammatorisk tarmsykdom (IBD) eller symptomer som tyder på IBD
  • Anamnese med aktiv tuberkulose med mindre den er vellykket behandlet, latent tuberkulose med mindre den er profylaktisk behandlet
  • Deltakeren har en aktiv infeksjon eller historie med infeksjoner (som alvorlig infeksjon, kroniske infeksjoner, opportunistiske infeksjoner, uvanlig alvorlige infeksjoner)
  • Deltaker har laboratorieavvik ved screening
  • Deltakeren har opplevd primær svikt i en eller flere interleukin-17 (IL-17) biologisk responsmodifikator ELLER primær svikt i mer enn 1 biologisk responsmodifikator annet enn en IL-17 biologisk responsmodifikator
  • Tilstedeværelse av aktive selvmordstanker, eller positiv selvmordsatferd
  • Deltakeren har blitt diagnostisert med alvorlig depresjon de siste 6 månedene

Studieplan

Denne delen gir detaljer om studieplanen, inkludert hvordan studien er utformet og hva studien måler.

Hvordan er studiet utformet?

Designdetaljer

  • Primært formål: Behandling
  • Tildeling: Randomisert
  • Intervensjonsmodell: Parallell tildeling
  • Masking: Ingen (Open Label)

Våpen og intervensjoner

Deltakergruppe / Arm
Intervensjon / Behandling
Eksperimentell: Bimekizumab Dose A
Studiedeltakere randomisert til denne armen vil motta bimekizumab (BKZ) dose A på forhåndsspesifiserte tidspunkter i løpet av studien.
Legemiddel: bimekizumab
Studiedeltakere vil motta subkutant administrert bimekizumab (BKZ) på forhåndsspesifiserte tidspunkter i løpet av studien.
Andre navn:
  • UCB4940
  • BKZ
Eksperimentell: Bimekizumab dose B
Studiedeltakere randomisert til denne armen vil motta bimekizumab (BKZ) dose B på forhåndsspesifiserte tidspunkter i løpet av studien.
Legemiddel: bimekizumab
Studiedeltakere vil motta subkutant administrert bimekizumab (BKZ) på forhåndsspesifiserte tidspunkter i løpet av studien.
Andre navn:
  • UCB4940
  • BKZ

Hva måler studien?

Primære resultatmål

Resultatmål
Tiltaksbeskrivelse
Tidsramme
Plasma Concentration of Bimekizumab at Week 0
Tidsramme: Baseline (Week 0)
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 0. PK-PPS = Pharmacokinetic per-protocol set, IMP = investigational medicinal product.
Baseline (Week 0)
Plasma Concentration of Bimekizumab at Week 1
Tidsramme: Week 1
Blood samples were collected to determine the bimekizumab plasma concentration at Week 1.
Week 1
Plasma Concentration of Bimekizumab at Week 4
Tidsramme: Week 4
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 4.
Week 4
Plasma Concentration of Bimekizumab at Week 8
Tidsramme: Week 8
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 8.
Week 8
Plasma Concentration of Bimekizumab at Week 12
Tidsramme: Week 12
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 12.
Week 12
Plasma Concentration of Bimekizumab at Week 16
Tidsramme: Week 16
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 16.
Week 16
Plasma Concentration of Bimekizumab at Week 20
Tidsramme: Week 20
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 20.
Week 20
Plasma Concentration of Bimekizumab at Week 40
Tidsramme: Week 40
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 40.
Week 40
Plasma Concentration of Bimekizumab at Week 64
Tidsramme: Week 64
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 64.
Week 64
Plasma Concentration of Bimekizumab at Week 88
Tidsramme: Week 88
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 88.
Week 88
Plasma Concentration of Bimekizumab at Week 112
Tidsramme: Week 112
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 112.
Week 112
Plasma Concentration of Bimekizumab at Week 124
Tidsramme: Week 124
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 124.
Week 124
Plasma Concentration of Bimekizumab at Safety Follow up (SFU)
Tidsramme: Week 140 (SFU)
Blood samples were collected prior to the scheduled dose to determine the bimekizumab plasma concentration at Week 140 (SFU).
Week 140 (SFU)

Sekundære resultatmål

Resultatmål
Tiltaksbeskrivelse
Tidsramme
Percentage of Participants With Treatment-emergent Adverse Events (TEAEs)
Tidsramme: From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)]
An adverse event (AE) is any untoward medical occurrence in a patient or clinical study participant, temporally associated with the use of IMP, whether or not considered related to the IMP. Treatment-emergent AEs are defined as those AEs that started date on or following the first dose of IMP through the final dose of IMP +20 weeks. The last dose was given 4 weeks prior end of extension period.
From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)]
Percentage of Participants With Serious Treatment-emergent Adverse Events
Tidsramme: From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
An serious adverse event (SAE) must meet 1 or more of the following criteria: Results in death; Is life-threatening; Requires inpatient hospitalization or prolongation of existing hospitalization; Results in persistent disability/incapacity; Is a congenital anomaly/birth defect; Important medical event that, based upon appropriate medical judgment, may jeopardize the patient or subject and may require medical or surgical intervention to prevent 1 of the other outcomes listed in the definition of serious. Treatment-emergent AEs are defined as those AEs that started date on or following the first dose of IMP through the final dose of IMP +20 weeks. The data was rounded to one decimal place. The last dose was given 4 weeks prior end of extension period.
From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
Percentage of Participants With Treatment-emergent Adverse Events (TEAEs) Leading to Discontinuation of Investigational Medicinal Product (IMP)
Tidsramme: From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
An AE is any untoward medical occurrence in a patient or clinical study participant, temporally associated with the use of IMP, whether or not considered related to the IMP. Treatment-emergent AEs are defined as those AEs that started date on or following the first dose of IMP through the final dose of IMP +20 weeks. This measure considers any TEAE leading to permanent discontinuation of IMP regardless of reason. The last dose was given 4 weeks prior end of extension period.
From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
Percentage of Participants With Treatment-emergent Adverse Events (TEAEs) Leading to Withdrawal From the Study
Tidsramme: From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
An AE is any untoward medical occurrence in a patient or clinical study participant, temporally associated with the use of IMP, whether or not considered related to the IMP. Treatment-emergent AEs are defined as those AEs that started date on or following the first dose of IMP through the final dose of IMP +20 weeks. This measure considers any TEAEs leading to withdrawal from the study. The last dose was given 4 weeks prior end of extension period.
From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
Exposure-adjusted Incidence Rates (EAIR) of Selected Safety Topics of Interest
Tidsramme: From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
Selected safety topics of interest (including infection [serious, opportunistic, fungal, and tuberculosis (TB)], inflammatory bowel disease [IBD], and injection site reactions) with onset occurring from day of first dose through 20 weeks after final dose of IMP adjusted by duration of participant exposure to IMP. The exposure-adjusted incidence rate (EAIR) is defined as the number of participants (n) with a specific AE adjusted for the exposure and was scaled to 100 participant-years. The last dose was given 4 weeks prior end of extension period.
From day of first dose (Week 0) through 20 weeks after final dose of IMP (up to Week 140)
Change From Baseline in Vital Signs (Systolic and Diastolic Blood Pressure)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Blood pressure was measured in millimeters of mercury (mmHg).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Vital Signs (Pulse Rate)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Pulse rate was measured in beats per minute (beats/min).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Vital Signs (Temperature)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Temperature (oral, axillary, otic or non-contact forehead) was measured in degrees Celsius (°C).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Platelet Count)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Platelets was measured in number of platelets per liter (10^9/L).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Mean Corpuscular Hemoglobin)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Mean corpuscular hemoglobin (HGB) was measured in picograms (pg).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Mean Corpuscular Volume)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Mean corpuscular volume was measured in femtolitres.
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Erythrocytes)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Erythrocytes was measured in number of red blood cells per liter (10^12/L).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Hemoglobin)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Hemoglobin was measured in grams per liter.
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Hematocrit)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Hematocrit was measured in volume percentage (%) of red blood cells in the blood.
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Clinical Chemistry Parameters (Alkaline Phosphatase, Alanine Aminotransferase, Aspartate Aminotransferase)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Alkaline phosphatase, alanine aminotransferase, aspartate aminotransferase was measured in units per liter.
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Hematology Parameters (Basophils, Eosinophils, Lymphocytes, Monocytes, Neutrophils, Leukocytes)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Basophils, eosinophils, lymphocytes, monocytes, neutrophils and leukocytes was measured in number of white blood cells per liter (10^9/L).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Clinical Chemistry Parameters (Calcium, Potassium, Sodium, Blood Urea Nitrogen, Glucose (Nonfasting)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Calcium, potassium, sodium, blood urea nitrogen, and glucose (non fasting) was measured in millimoles per liter (mmol/L).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Clinical Chemistry Parameters (Creatinine, Total and Direct Bilirubin)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Creatinine and bilirubin was measured in micromols per liter (μmol/L).
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Clinical Chemistry Parameters (Total Protein)
Tidsramme: Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Total protein was measured in gram per liter (g/L)
Baseline (Week 0), Weeks 16, 124, Safety Follow-Up (up to Week 140)
Change From Baseline in Height
Tidsramme: Baseline (Week 0), Weeks 16, 124
Growth assessment, as assessed by the change from Baseline in height.
Baseline (Week 0), Weeks 16, 124
Change From Baseline in Weight
Tidsramme: Baseline (Week 0), Weeks 16, 124
Growth assessment, as assessed by the change from Baseline in weight.
Baseline (Week 0), Weeks 16, 124
Percentage of Participants With Psoriasis Area and Severity Index (PASI) 90 Response at Week 16
Tidsramme: Week 16
Percentage of participants with PASI 90 response at Week 16 is reported. PASI90 response assessments are based on at least 90% improvement in PASI score from Baseline. This is scoring system that averages redness, thickness, and scaliness of psoriatic lesions(on a 0-4 scale), and weights resulting score by area of skin involved. Body divided into 4 areas:head, arms, trunk to groin, and legs to top of buttocks. Assignment of average score for redness, thickness, and scaling for each of 4 body areas with score of 0(none) to 4(very marked). Determining percentage of skin covered with psoriasis(PSO) for each of body areas and converting to 0 to 6 scale. Final PASI=average redness, thickness, and scaliness of psoriatic skin lesions, multiplied by involved PSO area score of respective section, and weighted by percentage of person's affected skin for respective section. Minimum possible PASI score is 0=no disease, maximum score is 72=maximal disease. Data was rounded to one decimal place.
Week 16
Percentage of Participants With Investigator's Global Assessment (IGA) 0/1 (Clear [0]/Almost Clear [1] With at Least 2-category Improvement From Baseline) Response at Week 16
Tidsramme: Week 16
The Investigator's Global Assessment (IGA) measures the overall psoriasis severity following a 5-point scale (0-4), where scale 0= clear, no signs of psoriasis; presence of post-inflammatory hyperpigmentation, scale 1= almost clear, no thickening; normal to pink coloration; no to minimal focal scaling, scale 2= mild thickening, pink to light red coloration and predominately fine scaling, 3= moderate, clearly distinguishable to moderate thickening; dull to bright red, clearly distinguishable to moderate thickening; moderate scaling and 4= severe thickening with hard edges; bright to deep dark red coloration; severe/coarse scaling covering almost all or all lesions. IGA response (Clear or Almost Clear) is defined as clear [0] or almost clear [1] with at least a two-category improvement from Baseline. The data was rounded to one decimal place.
Week 16
Percentage of Participants With Psoriasis Area and Severity Index (PASI) 75 Response at Week 4
Tidsramme: Week 4
Percentage of participants with PASI75 response at Week 4 is reported. PASI75 response assessments are based on at least 75% improvement in PASI score from Baseline. This is scoring system that averages redness, thickness, and scaliness of psoriatic lesions (on a 0-4 scale), and weights resulting score by area of skin involved. Body divided into 4 areas:head, arms, trunk to groin, and legs to top of buttocks. Assignment of an average score for redness, thickness, and scaling for each of 4 body areas with a score of 0 (clear) to 4 (very marked). Determining percentage of skin covered with PSO for each of body areas and converting to 0 to 6 scale. Final PASI=average redness, thickness, and scaliness of psoriatic skin lesions, multiplied by involved psoriasis area score of respective section, and weighted by percentage of person's affected skin for respective section. Minimum possible PASI score is 0=no disease, maximum score is 72=maximal disease. Data was rounded to one decimal place.
Week 4
Percentage of Participants With Anti-bimekizumab Antibody (AbAb) Detection Prior to Investigational Medicinal Product (IMP) Administration
Tidsramme: Baseline (Week 0)
Anti-bimekizumab antibody (AbAb) detection prior to IMP administration. Anti-bimekizumab antibodies was measured using 3-tiered assay approach: screening assay, confirmatory assay, and titration assay. Antidrug antibody (ADAb) positive status: any sample that is positive screen and positive immunodepletion (regardless of availability of a titer value). ADAb negative status: any sample that is either negative screen, or positive screen and negative immunodepletion, and where the bimekizumab concentration is less than or equal to the drug tolerance limit of the validated ADAb assay. ADAb missing status: any sample that is either negative screen or positive screen and negative immunodepletion and where the bimekizumab concentration exceeds the validated ADAb assay drug tolerance limit.
Baseline (Week 0)
Percentage of Participants With Anti-bimekizumab Antibody (AbAb) Detection Following Investigational Medicinal Product (IMP) Administration
Tidsramme: From Baseline (Week 0, post-first dose) to Safety Follow-Up (Week 140)
Anti-bimekizumab antibody (AbAb) detection following IMP administration. Overall ADAb positive is defined as having at least one sample that is confirmed positive following the 1st dose of IMP to SFU (regardless of missing data). Overall ADAb negative is defined as having all samples reported as negative, or has only one missing/inconclusive sample, following the 1st dose of IMP to SFU. Overall ADAb missing if the study participant has more than one missing ADAb sample for any reason and all other available ADAb samples are negative. The data was rounded to one decimal place.
From Baseline (Week 0, post-first dose) to Safety Follow-Up (Week 140)
Change From Baseline in Children's Dermatology Life Quality Index (CDLQI) Response at Week 16
Tidsramme: Baseline, Week 16
The CDLQI is a questionnaire designed to measure the impact of skin diseases on the lives of children. The questionnaire consists of 10 questions that are based on the experiences of children with skin disease. The instrument asks participants about symptoms and feelings, leisure, school or holidays, personal relationships, sleep, and treatment. The questions relate to the impact of the skin disease on the child over the last week, (ie, over the last 7 days). The CDLQI total score ranges from 0 to 30 with higher scores indicating higher impact of skin disease on quality of life (Qol).
Baseline, Week 16

Samarbeidspartnere og etterforskere

Det er her du vil finne personer og organisasjoner som er involvert i denne studien.

Sponsor

UCB Biopharma SRL

Etterforskere

  • Studieleder: UCB Cares, 001 844 599 2273

Studierekorddatoer

Disse datoene sporer fremdriften for innsending av studieposter og sammendragsresultater til ClinicalTrials.gov. Studieposter og rapporterte resultater gjennomgås av National Library of Medicine (NLM) for å sikre at de oppfyller spesifikke kvalitetskontrollstandarder før de legges ut på det offentlige nettstedet.

Studer hoveddatoer

Studiestart (Faktiske)

6. april 2021

Primær fullføring (Faktiske)

12. mars 2025

Studiet fullført (Faktiske)

12. mars 2025

Datoer for studieregistrering

Først innsendt

18. januar 2021

Først innsendt som oppfylte QC-kriteriene

18. januar 2021

Først lagt ut (Faktiske)

22. januar 2021

Oppdateringer av studieposter

Sist oppdatering lagt ut (Faktiske)

18. mai 2026

Siste oppdatering sendt inn som oppfylte QC-kriteriene

24. april 2026

Sist bekreftet

1. april 2026

Mer informasjon

Begreper knyttet til denne studien

Nøkkelord

Ytterligere relevante MeSH-vilkår

Andre studie-ID-numre

  • PS0020
  • 2020-001724-34 (EudraCT-nummer)
  • 2023-509832-24 (Registeridentifikator: EU Clinical Trials)
  • U1111-1303-1875 (Annen identifikator: World Health Organization (WHO))

Plan for individuelle deltakerdata (IPD)

Planlegger du å dele individuelle deltakerdata (IPD)?

JA

IPD-planbeskrivelse

Data fra denne utprøvingen kan bli forespurt av kvalifiserte forskere seks måneder etter produktgodkjenning i USA og/eller Europa, eller global utvikling avbrytes, og 18 måneder etter fullføring av utprøvingen. Etterforskere kan be om tilgang til anonymiserte individuelle data på pasientnivå og redigerte utprøvingsdokumenter som kan omfatte: analyseklare datasett, studieprotokoll, kommentert saksrapportskjema, statistisk analyseplan, datasettspesifikasjoner og klinisk studierapport. Før bruk av dataene må forslag godkjennes av et uavhengig granskningspanel på www.Vivli.org og en signert datadelingsavtale må utføres. Alle dokumenter er kun tilgjengelig på engelsk, i en forhåndsbestemt tid, vanligvis 12 måneder, på en passordbeskyttet portal. Denne planen kan endres hvis risikoen for å identifisere prøvedeltakere på nytt blir bestemt til å være for høy etter at prøven er fullført; i dette tilfellet og for å beskytte deltakerne, vil ikke individuelle pasientdata bli gjort tilgjengelig.

IPD-delingstidsramme

Data fra denne utprøvingen kan bli forespurt av kvalifiserte forskere seks måneder etter at produktgodkjenning i USA og/eller Europa eller global utvikling er avbrutt, og 18 måneder etter at forsøket er fullført.

Tilgangskriterier for IPD-deling

Kvalifiserte forskere kan be om tilgang til anonymiserte IPD og redigerte studiedokumenter som kan omfatte: rådatasett, analyseklare datasett, studieprotokoll, blankt caserapportskjema, kommentert caserapportskjema, statistisk analyseplan, datasettspesifikasjoner og klinisk studierapport. Før bruk av dataene må forslag godkjennes av et uavhengig granskningspanel på www.Vivli.org og en signert datadelingsavtale må utføres. Alle dokumenter er kun tilgjengelig på engelsk, i en forhåndsdefinert tid, vanligvis 12 måneder, på en passordbeskyttet portal.

IPD-deling Støtteinformasjonstype

  • STUDY_PROTOCOL
  • SEVJE
  • CSR

Legemiddel- og utstyrsinformasjon, studiedokumenter

Studerer et amerikansk FDA-regulert medikamentprodukt

Ja

Studerer et amerikansk FDA-regulert enhetsprodukt

Nei

produkt produsert i og eksportert fra USA

Ja

Denne informasjonen ble hentet direkte fra nettstedet clinicaltrials.gov uten noen endringer. Hvis du har noen forespørsler om å endre, fjerne eller oppdatere studiedetaljene dine, vennligst kontakt register@clinicaltrials.gov. Så snart en endring er implementert på clinicaltrials.gov, vil denne også bli oppdatert automatisk på nettstedet vårt. .

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