Overview
Sponsor-declared trial summary
Phase
Therapeutic confirmatory (Phase III)
Status
Ongoing, recruitment ended
Participants planned
864
Countries
10
Sites
50
Relapsing Multiple Sclerosis (MS)
To demonstrate the superiority of a higher dose of ocrelizumab over the approved dose of ocrelizumab as assessed by risk reduction in composite confirmed disability progression (cCDP) sustained for at least 12 weeks
Key facts
- Sponsor
- F. Hoffmann-La Roche AG
- Participant type
- Patients
- Age range
- 18-64 years
- Gender
- Male and Female
- Therapeutic area
- Diseases [C] - Nervous System Diseases [C10]
- Trial duration
- 20 Oct 2020 → ongoing
- Decision date (initial)
- 2024-02-19
- Transition trial
- Yes
- Low-intervention
- No
- Rare-disease indication
- No
- Vulnerable population
- Yes
- Funding sources
- F. Hoffmann-La Roche AG
External identifiers
- EU CT number
- 2023-506467-34-00
- EudraCT number
- 2020-000893-69
Trial design
CTIS Part I — objectives, methods, condition coding
Main objective
Scope: Safety, Pharmacodynamic, Others, Pharmacokinetic, Efficacy
To demonstrate the superiority of a higher dose of ocrelizumab over the approved dose of ocrelizumab as assessed by risk reduction in composite confirmed disability progression (cCDP) sustained for at least 12 weeks
Secondary objectives 7
- 1. To demonstrate superiority of a higher dose of ocrelizumab over the approved dose of ocrelizumab on the basis of: time to onset of 24-week cCDP (cCDP24); time to onset of cCDP48; time to onset of cCDP12 independent of protocol-defined relapses (PDR), also termed progression independent of relapse activity (PIRA) as per Kappos et al 2020; time to onset of CDP12; time to ≥ 20% increase in 12-week confirmed timed 25-foot walk test (T25FWT); annual rate of percent change from baseline in total brain volume; time to 12-week confirmed 4-point worsening in Symbol Digit Modalities test (SDMT); and time to 12-week confirmed 8-point increase in 12-Item Multiple Sclerosis Walking Scale (MSWS-12)
- 2. To demonstrate that both the approved dose and the higher dose of ocrelizumab can lead to a significant reduction in NfL from baseline by evaluating change in NfL (i.e. ratio to baseline) at Week 48 for patients assigned to the higher dose ocrelizumab group and for patients assigned to the approved dose ocrelizumab group
- 3. To evaluate the safety profile of a higher dose of ocrelizumab compared with the approved dose of ocrelizumab
- 4. To assess the exposure to ocrelizumab in serum in all patients in both study arms
- 5. To characterize the ocrelizumab PD profile
- 6. To evaluate the immune response to ocrelizumab
- 7. To identify biomarkers that are predictive of response to a higher dose of ocrelizumab
Conditions and MedDRA coding
Relapsing Multiple Sclerosis (MS)
| Version | Level | Code | Term | System organ class |
|---|---|---|---|---|
| 20.1 | LLT | 10039720 | Sclerosis multiple | 10029205 |
| 20.1 | PT | 10028245 | Multiple sclerosis | 100000004852 |
| 20.0 | PT | 10048393 | Multiple sclerosis relapse | 100000004852 |
| 21.1 | PT | 10063399 | Relapsing-remitting multiple sclerosis | 100000004852 |
Study design 5 periods
| # | Title | Allocation | Blinding | Roles blinded | Arms |
|---|---|---|---|---|---|
| 1 | Screening Up to 6-week screening period to be evaluated for eligibility
|
Not Applicable | None | ||
| 2 | Double blind treatment (DBT) phase Minimum 120 week double blind treatment (DBT) phase.
|
Randomised Controlled | Double | [{"id":181796,"code":1,"name":"Subject"},{"id":181797,"code":2,"name":"Investigator"}] | |
| 3 | Optional Open-Label Extension Phase 96 weeks (4 doses in total) starting from the first OLE dose
|
Not Applicable | None | ||
| 4 | Safety Follow-Up Phase and B-Cell Monitoring Each patient will be followed for safety for 48 weeks, starting from the last ocrelizumab dose received.
|
Not Applicable | None | ||
| 5 | Optional CSF Biomarker Substudy A CSF BIOMARKER SUBSTUDY WITHIN BN42083
TRIAL, PHASE IIIB MULTICENTER, RANDOMIZED,
DOUBLE-BLIND, CONTROLLED STUDY TO
EVALUATE THE EFFICACY, SAFETY AND
PHARMACOKINETICS OF A HIGHER DOSE OF
OCRELIZUMAB IN ADULTS WITH PRIMARY
PROGRESSIVE MULTIPLE SCLEROSIS
|
Randomised Controlled | Double | [{"id":181802,"code":1,"name":"Subject"},{"id":181801,"code":2,"name":"Investigator"}] |
Eligibility criteria
Principal inclusion / exclusion criteria as submitted by sponsor
Inclusion criteria 6
- 1. Ages 18−55 years at time of screening
- 2. Diagnosis of RMS (i.e., RRMS or aSPMS where patients still experience relapses) in accordance with the revised McDonald Criteria 2017
- 3. At least two documented clinical relapses within the last 2 years prior to screening, or one clinical relapse in the year prior to screening (with no relapse 30 days prior to screening and at baseline)
- 4. Patients must be neurologically stable for at least 30 days prior to randomization and baseline assessments
- 5. Expanded disability status scale (EDSS) score, at screening and baseline, from 0 to 5.5 inclusive
- 6. Documented MRI of brain with abnormalities consistent with MS
Exclusion criteria 6
- 1. History of primary progressive MS at screening
- 2. Any known or suspected active infection at screening or baseline, or any major episode of infection requiring hospitalization or treatment with IV anti microbials within 8 weeks prior to and during screening or treatment with oral anti microbials within 2 weeks prior to and during screening
- 3. History of confirmed or suspected progressive multifocal leukoencephalopathy (PML)
- 4. History of cancer, including hematologic malignancy and solid tumors, within 10 years of screening
- 5. Immunocompromised state
- 6. Known presence of other neurologic disorders that could interfere with the diagnosis of MS or assessments of efficacy and/or safety during the study
Endpoints
Primary and secondary outcome measures (English text)
Primary endpoints 1
- 1. Time to onset of cCDP sustained for at least 12 weeks. Time to onset of cCDP is defined as the first occurrence of a predefined confirmed progression event measured by EDSS, T25FWT or 9-HPT
Secondary endpoints 23
- 1. Time to onset of 24 week cCDP (cCDP24)
- 2. Time to onset of 48-week cCDP (cCDP48)
- 3. Time to onset of cCDP12 independent of protocol-defined relapses (PDR), also termed progression independent of relapse activity (PIRA) as per Kappos et al 2020
- 4. Time to ≥ 20% increase in 12 week confirmed T25FWT
- 5. Time to ≥ 20% increase in 24 week confirmed T25FWT
- 6. Annual rate of percent change from baseline in total brain volume
- 7. Time to 12-week confirmed 4-point worsening in Symbol Digit Modalities test (SDMT)
- 8. Time to 12-week confirmed 8-point increase in 12-Item Multiple Sclerosis Walking Scale (MSWS-12)
- 9. Change in NfL (i.e. ratio to baseline) at Week 48 for patients assigned to the higher dose ocrelizumab group
- 10. Change in NfL (i.e ratio to baseline) at Week 48 for patients assigned to the approved dose ocrelizumab group
- 11. Incidence and severity of adverse events, with severity determined according to the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) Version 5.0
- 12. Change from baseline in clinical laboratory test results (including hematology, chemistry, and Ig levels)
- 13. Change from baseline in vital signs (including systolic and diastolic blood pressure, and pulse rate) following study treatment administration
- 14. Serum concentration of ocrelizumab at specified timepoints
- 15. B-cell levels in blood (including comparing the degree of B-cell depletion between the doses)
- 16. Proportion of participant achieving 5 or less B-cells per microliter of blood
- 17. Proportion of participants achieving 5 or less B-cells per microliter of blood in participants with the high versus low affinity Fcgamma Receptor 3A (FcγR3A) genotype per arm
- 18. Change from Baseline in the anti-drug antibodies (ADAs) levels
- 19. Levels of Neurofilament Light Chain (NfL) in blood
- 20. Levels of interleukin-6 (IL-6) in blood
- 21. Levels of blood B cells
- 22. Levels of Lymphocytes in blood
- 23. Proportion of participants with different DNA genotypes
Investigational products
Investigational medicinal products (IMPs), comparators, placebo, auxiliary
Test 2
Ocrevus 300 mg concentrate for solution for infusion
PRD5771912 · Product
- Active substance
- Ocrelizumab
- Pharmaceutical form
- SOLUTION FOR INFUSION
- Route of administration
- INTRAVENIOUS INFUSION
- Max daily dose
- 1800 mg milligram(s)
- Max total dose
- 23.4 g gram(s)
- Max treatment duration
- 322 Week(s)
- Authorisation status
- Authorised
- ATC code
- L04AA36 — -
- Marketing authorisation
- EU/1/17/1231/002
- MA holder
- ROCHE REGISTRATION GMBH
- MA country
- EU
- Paediatric formulation
- No
- Orphan designation
- No
- Modified vs. Marketing Authorisation
- No
Ocrevus 300 mg concentrate for solution for infusion
PRD5771848 · Product
- Active substance
- Ocrelizumab
- Pharmaceutical form
- SOLUTION FOR INFUSION
- Route of administration
- INTRAVENOUS INFUSION
- Max daily dose
- 1800 mg milligram(s)
- Max total dose
- 23.4 g gram(s)
- Max treatment duration
- 322 Week(s)
- Authorisation status
- Authorised
- ATC code
- L04AA36 — -
- Marketing authorisation
- EU/1/17/1231/001
- MA holder
- ROCHE REGISTRATION GMBH
- MA country
- EU
- Paediatric formulation
- No
- Orphan designation
- No
- Modified vs. Marketing Authorisation
- No
Placebo 1
N/A · Product
- Other product name
- N/A
- Pharmaceutical form
- N/A
- ATC code
- N/A — N/A
- Marketing authorisation
- N/A
- MA holder
- N/A
- MA country
- Iceland
- Paediatric formulation
- No
- Modified vs. Marketing Authorisation
- No
Auxiliary 3
PRD10109599 · Product
- Active substance
- Paracetamol
- Pharmaceutical form
- TABLET
- Route of administration
- ORAL USE
- Max daily dose
- 1 g gram(s)
- Max total dose
- 13 g gram(s)
- Max treatment duration
- 322 Week(s)
- Authorisation status
- Authorised
- ATC code
- N02BE01 — PARACETAMOL
- Marketing authorisation
- PL 16028/0180
- MA holder
- GALPHARM HEALTHCARE LIMITED
- MA country
- XI
- Paediatric formulation
- No
- Orphan designation
- No
- Modified vs. Marketing Authorisation
- No
Methylprednisolone 500 mg powder and solvent for solution for injection/infusion
PRD10716804 · Product
- Active substance
- Methylprednisolone
- Substance synonyms
- 6-METHYLPREDNISOLONE
- Pharmaceutical form
- SOLUTION FOR INJECTION/INFUSION
- Route of administration
- INTRAVENOUS INFUSION
- Max daily dose
- 100 mg milligram(s)
- Max total dose
- 1300 mg milligram(s)
- Max treatment duration
- 322 Week(s)
- Authorisation status
- Authorised
- ATC code
- H02AB04 — METHYLPREDNISOLONE
- Marketing authorisation
- PL 51463/0127
- MA holder
- KENT PHARMA UK LIMITED
- MA country
- XI
- Paediatric formulation
- No
- Orphan designation
- No
- Modified vs. Marketing Authorisation
- No
Diphenhydramine Hydrochloride Tablets 50 mg
PRD1176426 · Product
- Active substance
- Diphenhydramine Hydrochloride
- Pharmaceutical form
- TABLET
- Route of administration
- ORAL AND IV
- Max daily dose
- 50 mg milligram(s)
- Max total dose
- 650 mg milligram(s)
- Max treatment duration
- 322 Week(s)
- Authorisation status
- Authorised
- ATC code
- R06AA02 — DIPHENHYDRAMINE
- Marketing authorisation
- PL 20416/0068
- MA holder
- CRESCENT PHARMA LIMITED
- MA country
- XI
- Paediatric formulation
- No
- Orphan designation
- No
- Modified vs. Marketing Authorisation
- No
Sponsors and contacts
Sponsor organisations, regulatory contacts, third parties
F. Hoffmann-La Roche AG
- Sponsor organisation
- F. Hoffmann-La Roche AG
- Address
- Grenzacherstrasse 124
- City
- Basel
- Postcode
- 4058
- Country
- Switzerland
Scientific contact point
- Organisation
- F. Hoffmann-La Roche AG
- Contact name
- Trial Information System - TISL
Public contact point
- Organisation
- F. Hoffmann-La Roche AG
- Contact name
- Trial Information System - TISL
Third parties 13
| Organisation | City, country | Duties |
|---|---|---|
| PPD Development LP ORG-100011560
|
Richmond, United States | Laboratory analysis |
| Unilabs A/S ORG-100032351
|
Copenhagen Oe, Denmark | Laboratory analysis |
| IQVIA Limited ORG-100008655
|
Reading, United Kingdom | Other |
| MARKEN Germany GmbH ORG-100017196
|
Hamburg, Germany | Other |
| Eresearchtechnology Inc. ORG-100013039
|
Philadelphia, United States | Other |
| Neurorx Research Inc. ORG-100046079
|
Montreal, Canada | Laboratory analysis |
| Syneos Health Inc. ORG-100008382
|
Princeton, United States | Laboratory analysis |
| Roland Henry Lab UCSF; UCSF Department of Neurology, Sandler Neurosciences Center ORL-000003923
|
San Francisco, United States | Laboratory analysis |
| Neurostatus-UHB AG ORG-100046513
|
Basel, Switzerland | Other |
| IQVIA RDS Hellas Single Member S.A. ORG-100048380
|
Chalandri, Greece | On site monitoring |
| Labcorp Central Laboratory Services S.a.r.l. ORG-100011524
|
Meyrin, Switzerland | Laboratory analysis |
| Almac Group Limited ORG-100011829
|
Craigavon, United Kingdom (Northern Ireland) | Interactive response technologies (IRT) |
| Publicis Healthcare Communications Group Limited ORG-100044665
|
London, United Kingdom | Other |
Locations
10 EU/EEA countries · 50 investigational sites
By country
| Country | MS status | Planned subjects | Sites |
|---|---|---|---|
| Belgium | Ended | 8 | 2 |
| Denmark | Ended | 3 | 1 |
| France | Ongoing, recruitment ended | 6 | 4 |
| Germany | Ended | 47 | 8 |
| Greece | Ended | 3 | 1 |
| Hungary | Ended | 21 | 3 |
| Italy | Ended | 33 | 8 |
| Poland | Ongoing, recruitment ended | 183 | 13 |
| Portugal | Ongoing, recruitment ended | 10 | 4 |
| Spain | Ongoing, recruitment ended | 43 | 6 |
| Rest of world
Switzerland, Canada, Peru, Bosnia and Herzegovina, Australia, Russian Federation, Brazil, Turkey, Israel, Mexico, Belarus, Ukraine, United Kingdom, Argentina, United States
|
— | 507 | — |
Investigational sites
Hopital Erasme
Neurology, Lennikse Baan 808, 1070, Anderlecht
Noorderhart
Revalidatie en MS Centrum, Boemerangstraat 2, 3900, Pelt
Centre Hospitalier Universitaire De Bordeaux
Neurology, Place Amelie Raba Leon, 33000, Bordeaux
CHU Gabriel-Montpied
Neurology, 58 Rue Montalembert, 63000, Clermont Ferrand
CHU De Rouen
Neurology, 1 Rue De Germont, Bp 96031, Rouen Cedex
Groupement Des Hopitaux De L'Institut Catholique De Lille
Neurology, Boulevard De Belfort, P. O. Box 387, Lille Cedex
Universitaet Leipzig
Neurologie, Liebigstrasse 20, Zentrum-Suedost, Leipzig
DKD HELIOS Klinik Wiesbaden GmbH
Neurologie, Aukammallee 33, Bierstadt, Wiesbaden
Charite Universitaetsmedizin Berlin KöR
Klinik für Neurologie, Chariteplatz 1, Mitte, Berlin
Universitaetsklinikum Ulm AöR
Klinik für Neurologie, Oberer Eselsberg 45, Eselsberg, Ulm
Universitaetsklinikum Tuebingen AöR
Zentrum für Neurologie, Hoppe-Seyler-Strasse 3, Nordstadt, Tuebingen
Technische Universitat Dresden
Zentrum für klinische Neurowissenschaften, Fetscherstrasse 74, Johannstadt-Nord, Dresden
St. Josef-Hospital
Klinik für Neurologie, Gudrunstrasse 56, Grumme, Bochum
Universitaetsklinikum Schleswig-Holstein
Klinik für Neurologie, Arnold-Heller-Strasse 3, Brunswik, Kiel
401 General Military Hospital Of Athens
Neurology Clinic, Panagioti Kanellopoulou Av 1, 115 25, Athens
Somogy Varmegyei Kaposi Mor Oktato Korhaz
Neurologiai Osztaly, Tallian Gyula Utca 20-32, 7400, Kaposvar
Uno Medical Trials Kft.
Neurologia, Vecsey Karoly Utca 39, 1152, Budapest XV
S-Medicon Kft.
Neurologia, Megyeri Ut 53, 1044, Budapest IV
IRCCS Foundation Istituto Neurologico Carlo Besta
UO Neurologia IV - Neuroimmunologia Malattie Neuromuscolari, Via Giovanni Celoria 11, 20133, Milan
Neurological Centre Of Latium Istituto Di Neuroscienze O In Breve N.C.L. Istituto Di Neuroscienze S.r.l.
Centro sperimentazioni cliniche di NCL, Via Patrica 15, 00178, Rome
Azienda Ospedaliera Policlinico Universitario Tor Vergata
UOSD Sclerosi Multipla, Viale Oxford 81, 00133, Rome
Istituto Neurologico Mediterraneo Neuromed S.p.A.
Dipartimento di Neurologia, Via Atinense N. 18, 86077, Pozzilli
Azienda Ospedaliero-Universitaria Policlinico Umberto I
Dipartimento di Neuroscienze Umane, Viale Del Policlinico 155, 00161, Rome
Universita' Degli Studi G. D'annunzio Di Chieti
Dipartimento di Neuroscienze, Imaging e Scienze Cliniche, Via Dei Vestini 31, 66100, Chieti
Azienda Ospedaliera Universitaria Universita' Degli Studi Della Campania Luigi Vanvitelli
I Clinica Neurologica, Via Santa Maria Di Costantinopoli 104, 80138, Naples
Azienda Ospedaliera Universitaria Universita' Degli Studi Della Campania Luigi Vanvitelli
II Clinica Neurologica, Via Santa Maria Di Costantinopoli 104, 80138, Naples
Nmedis Sp. z o.o.
NA, Ul. Kujawska 5, 35-323, Rzeszow
Centrum Medyczne Neuroprotect
NA, 1 Pietro, Ul. Ulica Klaudyny 16c, Warsaw
Ma-Lek Clinical Sp. z o.o.
NA, Ul. Zaleska 9, 40-571, Katowice
Indywidualna Praktyka Lekarska Prof. dr hab. n. med. Konrad Rejdak
NA, Ul. 1 Maja 14, 20-410, Lublin
Uniwersyteckie Centrum Kliniczne Warszawskiego Uniwersytetu Medycznego
Klinika Neurologii, Ul. Ulica Stefana Banacha 1a, 02-097, Warsaw
Copernicus Podmiot Leczniczy Sp. z o.o.
Oddział Neurologiczny, Ul. Nowe Ogrody 1/6, 80-803, Gdansk
Uniwersytecki Szpital Kliniczny Nr 1 Im Norberta Barlickiego Uniwersytetu Medycznego W Lodzi SPZOZ
Oddział Kliniczny Neurologii, Ul. Dr Stefana Kopcinskiego 22, 90-153, Lodz
Euromedis Sp. z o.o.
NA, Ul. Powstancow Wielkopolskich 33 A, 70-111, Szczecin
Centrum Neurologii Krzysztof Selmaj
NA, ul. Tylna 12, 90-324, Łódź
EMC Instytut Medyczny S.A.
NA, Ul. Grunwaldzka 156, 60-309, Poznan
Instytut Psychiatrii I Neurologii
II Klinika Neurologiczna, Ul. Jana III Sobieskiego 9, 02-957, Warsaw
Neurocentrum Bydgoszcz Sp. z o.o.
NA, Ul. Aleje Prof. Sylwestra Kaliskiego 28/U1, 85-796, Bydgoszcz
Neurologiczny NZOZ Centrum Leczenia SM Ośrodek Badań Klinicznych im. dr n. med. Hanki Hertmanowskiej
NA, ul. Fabianowska 40, 62-064, Plewiska k. Poznania
Centro Hospitalar Universitario De Lisboa Norte E.P.E.
Serviço de Neurologia, Avenida Professor Egas Moniz, 1649-035, Lisbon
CCAB Centro Clinico Academico Braga Associacao
Unidade de Investigação Clínica, Lugar De Sete Fontes S Victor, 4710-243, Braga
Hospital Beatriz Angelo
Neurologia - HBA, Avenida Carlos Teixeira No 3, 2674-514, Loures
Centro Hospitalar De Lisboa Ocidental E.P.E.
Serviço de Neurologia, Rua Da Junqueira 126, 1349-019, Lisbon
Complexo Hospitalario Universitario A Coruna
Neurologia, Lugar Jubias De Arriba 84, 15006, A Coruna
Hospital Alvaro Cunqueiro
Neurologia, Estrada Clara Campoamor No 341, 36312, Vigo
Hospital Universitario Quironsalud Madrid
Neurologia, Calle De Diego De Velazquez 1, 28223, Pozuelo De Alarcon
Hospital Universitario Regional De Malaga
Neurologia, Avenida De Carlos De Haya Sn, 29010, Malaga
Hospital Universitario Puerta Del Mar
Neurologia, Avenida De Ana De Viya 21, 11009, Cadiz
Hospital Universitari Vall D Hebron
Neurologia, Edificio Materno-Infantil, Passeig De La Vall D'hebron 119-129, Barcelona
Country notifications
Trial-start, recruitment-start, end and early-termination notifications submitted per Member State
| Country | Trial start | Trial end | Recruitment start | Recruitment end | Early termination |
|---|---|---|---|---|---|
| Belgium | 2021-01-13 | 2026-03-02 | 2021-01-27 | 2022-09-06 | |
| Denmark | 2021-03-15 | 2025-11-19 | 2021-08-09 | 2022-09-06 | |
| France | 2021-03-10 | 2021-04-29 | 2022-09-06 | ||
| Germany | 2021-02-08 | 2026-03-18 | 2021-03-24 | 2022-09-06 | |
| Greece | 2021-04-22 | 2026-03-04 | 2021-05-12 | 2022-09-06 | |
| Hungary | 2020-10-20 | 2026-03-12 | 2020-11-26 | 2022-09-06 | |
| Italy | 2021-02-02 | 2026-03-30 | 2021-02-04 | 2022-09-06 | |
| Poland | 2020-11-13 | 2020-12-14 | 2022-09-06 | ||
| Portugal | 2021-01-19 | 2021-05-03 | 2022-09-06 | ||
| Spain | 2020-10-23 | 2020-10-26 | 2022-09-06 |
Oversight and notifications
Regulatory notifications under CTR Articles 38, 52, 53, 54 and 77
Unexpected events 1 · Art. 53 CTR
Note: SUSARs are reported via EudraVigilance, not CTIS — events shown here are CTIS-public notifications only.
Unexpected event UE-89991
- Event date
- 2025-07-02
- Date aware
- 2025-06-05
- Submission date
- 2025-07-15
- Member states affected
- Belgium, Denmark, France, Germany, Greece, Hungary, Italy, Portugal, Spain, Poland
- Clinical procedures
- Additional sampling for liver functional tests (LFT) are needed at baseline for all study participants and for monitoring symptomatic participants.
- Event description
- Clinically significant liver injury, without findings of viral hepatitis, requiring screening, monitoring and discontinuation
Results and documents
Annex IV summary of results, Annex V layperson summary, and all documents registered in CTIS for this trial
Documents 124 files
Public protocol annexes, IB summaries, regulatory submissions and post-authorisation documents registered in CTIS.
| Type | Title | Version |
|---|---|---|
| Protocol (for publication) | D1_Protocol 2023-506467-34-00 Redacted | 4 |
| Protocol (for publication) | D1_Protocol 2023-506467-34-00 Redacted GR | 4 |
| Recruitment arrangements (for publication) | K 1 BN42082 Recruitment arrangements ES | 1 |
| Recruitment arrangements (for publication) | K 1 BN42082_Recurit_arrange_Fr | 1 |
| Recruitment arrangements (for publication) | K1_ BN42082_Recurit_arrange_GR_File Note | 1 |
| Recruitment arrangements (for publication) | K1_ Recuritment arrangements | 1 |
| Recruitment arrangements (for publication) | K1_BN42082_Recruitment Arrangements | 1 |
| Recruitment arrangements (for publication) | K1_BN42082_Recurit_arrange_DEU_File Note | 1 |
| Recruitment arrangements (for publication) | K1_BN42082_Recurit_arrange_XXX_File Note | 1 |
| Recruitment arrangements (for publication) | K1_Recruitment_Arrangements_REDACTED | 1 |
| Recruitment arrangements (for publication) | K3_Document Additionnel - for publication | 1 |
| Subject information and informed consent form (for publication) | L1 SIS ICF Covid | 1 |
| Subject information and informed consent form (for publication) | L1 SIS ICF CSF substudy | 3 |
| Subject information and informed consent form (for publication) | L1 SIS ICF Main | 6 |
| Subject information and informed consent form (for publication) | L1 SIS ICF Main LP | 1 |
| Subject information and informed consent form (for publication) | L1 SIS ICF MR Health voluntary | 2 |
| Subject information and informed consent form (for publication) | L1 SIS ICF Ole Phase | 1 |
| Subject information and informed consent form (for publication) | L1 SIS ICF pregnant partner and infant | 1 |
| Subject information and informed consent form (for publication) | L1 SIS ICF RBR | 2 |
| Subject information and informed consent form (for publication) | L1_ Privacy consent form other subjects | NA |
| Subject information and informed consent form (for publication) | L1_ SIS and ICF CSF substudy | 4.0 |
| Subject information and informed consent form (for publication) | L1_ SIS and ICF infant | 2.0 |
| Subject information and informed consent form (for publication) | L1_ SIS and ICF main | 4.0 |
| Subject information and informed consent form (for publication) | L1_ SIS and ICF MRI | 3.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Add COVID-19 | 1.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Genetic | 2.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Infant Health Questionnaire | 2.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Main | 4.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF MRI | 3.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Optional Blood COVID-19 | 1.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Optional CSF Biomarker Substudy | 4.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Optional LP | 4.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF Optional Open Label | 2.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 ICF RBR | 3.0 |
| Subject information and informed consent form (for publication) | L1_BN42082 Reimbursement Information Sheet | 1.1 |
| Subject information and informed consent form (for publication) | L1_GDPR_clean | 18 |
| Subject information and informed consent form (for publication) | L1_GDPR_TC | 18 |
| Subject information and informed consent form (for publication) | L1_ICF Addendum for COVID-19 | 2 |
| Subject information and informed consent form (for publication) | L1_ICF_COVID-19 vaccination | 1 |
| Subject information and informed consent form (for publication) | L1_ICF_CSF SubStudy_OLE | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_CSF_DBT | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_enfant ne | 4 |
| Subject information and informed consent form (for publication) | L1_ICF_IHQ | 3 |
| Subject information and informed consent form (for publication) | L1_ICF_Immune_response | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_Main | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_Main | 8 |
| Subject information and informed consent form (for publication) | L1_ICF_Mandatory Clinical Genetic | 2 |
| Subject information and informed consent form (for publication) | L1_ICF_MRI healthy volunteers | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_OLE | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_OLE | 2 |
| Subject information and informed consent form (for publication) | L1_ICF_RBR | 5 |
| Subject information and informed consent form (for publication) | L1_ICF_RBR | 3 |
| Subject information and informed consent form (for publication) | L1_Main PIS_clean | 7 |
| Subject information and informed consent form (for publication) | L1_Main PIS_TC | 7 |
| Subject information and informed consent form (for publication) | L1_MRI PIS_clean | 4 |
| Subject information and informed consent form (for publication) | L1_MRI PIS_TC | 4 |
| Subject information and informed consent form (for publication) | L1_SIS Addendum for COVID-19 | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF covid addendum | 1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF COVID-19 ICF Addendum_EN | 1.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF COVID-19 ICF Addendum_FR | 1.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF COVID-19 ICF Addendum_NL | 1.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF COVID-19 ICF Addendum_RU | 1.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Healthy Volunteer MRI ICF_GR | 0.4 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF IHQ ICF_EN | 2.1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF IHQ ICF_FR | 2.1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF IHQ ICF_GR | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF IHQ ICF_NL | 2.1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF IHQ ICF_RU | 2.1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_EN | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_FR | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_GR | 4 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_NL | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_RU | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Main ICF_RU | 3 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF MRI Site Qualification ICF_EN | 2.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF MRI Site Qualification ICF_FR | 2.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF MRI Site Qualification ICF_NL | 2.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Optional CSF Substudy ICF_EN | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Optional CSF Substudy ICF_FR | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF Optional CSF Substudy ICF_NL | 4.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF RBR ICF_EN | 3.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF RBR ICF_FR | 3.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF RBR ICF_GR | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF RBR ICF_NL | 3.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF RBR ICF_RU | 3.0 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_COVID19_GER | 1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_COVID19_RUS | 1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_COVID19_UKR | 1 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_CSF Substudy_GER | 3 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Main_GER | 4 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Main_RUS | 4 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Main_UKR | 4 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_MRI_GER | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_OLE_GER | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Pregnant Pat_GER | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Pregnant Pat_RUS | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_Pregnant Pat_UKR | 2 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_RBR_GER | 3 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_RBR_RUS | 3 |
| Subject information and informed consent form (for publication) | L1_SIS and ICF_RBR_UKR | 3 |
| Subject information and informed consent form (for publication) | L1_SIS_COVID-19 vaccination | 1 |
| Subject information and informed consent form (for publication) | L1_SIS_Main | 6 |
| Subject information and informed consent form (for publication) | L1_SIS_Mandatory Clinical Genetic | 2 |
| Subject information and informed consent form (for publication) | L1_SIS_MRI healthy volunteers | 3 |
| Subject information and informed consent form (for publication) | L1_SIS_OLE | 2 |
| Subject information and informed consent form (for publication) | L1_SIS_RBR | 3 |
| Subject information and informed consent form (for publication) | L1_Thank you letter | 1 |
| Subject information and informed consent form (for publication) | L1-ICF_MRI | 6 |
| Subject information and informed consent form (for publication) | L1SIS_IHQ | 3 |
| Subject information and informed consent form (for publication) | L2_GDPR | 10 |
| Subject information and informed consent form (for publication) | L2_ICF Procedure_REDACTED | 1.0 |
| Subject information and informed consent form (for publication) | L2_Sponsor Statement On Use Of ICF Model | 1.0 |
| Subject information and informed consent form (for publication) | Thank letter in the BN42082_V1_Fr | 1 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_DE 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_ENG 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_ES 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_FRBE 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_FRFR 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_GR 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_HU 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_IT 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_NLBE 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_PL 2023-506467-34-00 | 2 |
| Synopsis of the protocol (for publication) | D1_Protocol synopsis_PT 2023-506467-34-00 | 2 |
Application history
13 submissions — initial application plus substantial / non-substantial modifications
| # | Type | Code | Submitted | Reference MS | Conclusion | Decision date |
|---|---|---|---|---|---|---|
| 1 | INITIAL | IN | 2023-12-21 | Poland | Acceptable 2024-02-08
|
2024-02-08 |
| 2 | SUBSTANTIAL MODIFICATION | SM-1 | 2024-04-19 | Poland | Acceptable 2024-06-24
|
2024-06-24 |
| 3 | NON SUBSTANTIAL MODIFICATION | NSM-2 | 2024-08-13 | Poland | Acceptable 2024-06-24
|
2024-08-13 |
| 4 | SUBSTANTIAL MODIFICATION | SM-2 | 2024-08-14 | 2024-09-30 | ||
| 5 | SUBSTANTIAL MODIFICATION | SM-3 | 2024-08-23 | Acceptable | 2024-09-27 | |
| 6 | SUBSTANTIAL MODIFICATION | SM-4 | 2024-12-19 | Poland | Acceptable 2025-03-24
|
2025-03-24 |
| 7 | NON SUBSTANTIAL MODIFICATION | NSM-3 | 2025-04-17 | Poland | Acceptable 2025-03-24
|
2025-04-17 |
| 8 | SUBSTANTIAL MODIFICATION | SM-5 | 2025-06-04 | Acceptable | 2025-06-18 | |
| 9 | SUBSTANTIAL MODIFICATION | SM-6 | 2025-09-19 | Acceptable | 2025-10-08 | |
| 10 | SUBSTANTIAL MODIFICATION | SM-7 | 2025-09-19 | Acceptable | 2025-10-29 | |
| 11 | SUBSTANTIAL MODIFICATION | SM-8 | 2025-10-16 | Acceptable | 2025-11-17 | |
| 12 | SUBSTANTIAL MODIFICATION | SM-9 | 2025-12-17 | Poland | Acceptable 2026-02-12
|
2026-02-12 |
| 13 | SUBSTANTIAL MODIFICATION | SM-10 | 2026-04-22 | Acceptable | 2026-05-11 |