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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT04374253
Other study ID # WN42171
Secondary ID 2020-000766-42
Status Terminated
Phase Phase 3
First received
Last updated
Start date January 26, 2021
Est. completion date March 6, 2023

Study information

Verified date April 2024
Source Hoffmann-La Roche
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is an open-label, multicenter, rollover study to evaluate the safety, tolerability, and efficacy of long-term administration of open-label gantenerumab in participants with AD who completed Study WN29922 or WN39658, either the double-blind or open-label extension (OLE) part.


Description:

Participants who were in the active arm in the double blind part and those who have completed OLE part in the parent study, will continue receive open-label gantenerumab 510 mg sub-cutaneously (SC) every 2 weeks (Q2W). Participants who are naive to gantenerumab treatment will be required to undergo the 3 step uptitration scheme as in the parent study before receiving target dose of open label gantenerumab.


Recruitment information / eligibility

Status Terminated
Enrollment 1382
Est. completion date March 6, 2023
Est. primary completion date March 6, 2023
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - Completed Study WN29922 or WN39658, either its double-blind part or OLE part, and did not discontinue study drug early - The participant should be capable of completing assessments either alone or with the help of the caregiver - Availability of a person (referred to as the "caregiver") - For women of childbearing potential: agreement to remain abstinent (refrain from heterosexual intercourse) or use contraception methods with a failure rate of <1% per year (bilateral tubal ligation, male sterilization, hormonal contraceptives that inhibit ovulation, hormone-releasing intrauterine devices, and copper intrauterine devices) during the treatment period and for at least 16 weeks after the final dose of gantenerumab - Agreement not to donate blood or blood products for transfusion for the duration of the study and for 1 year after final dose of study drug Exclusion Criteria: - Pregnant or breastfeeding, or intending to become pregnant during the study or within at least 16 weeks after the final dose of study drug - Prematurely discontinued from Study WN29922 or WN39658 - Any medical condition that may jeopardize the participant's safety if he or she continues to receive study treatment - Received any investigational treatment other than gantenerumab during or since completion of Study WN29922 or WN39658, either its double-blind or OLE part - Evidence of disseminated leptomeningeal hemosiderosis - Evidence of intracerebral macrohemorrhage - Use of prohibited medication - Evidence of ARIA-E on the last MRI scan report in Study WN29922 or WN39658, either its double-blind or OLE part

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Gantenerumab
Group 1 participants who were in the active arm in the double blind part in the parent study (WN29922 or WN39658), will continue to receive open-label gantenerumab 510 mg SC, Q2W. Participants who are naive to gantenerumab treatment will be required to undergo the 3 step uptitration scheme before receiving target dose of open label gantenerumab, 510 mg SC, Q2W.
Gantenerumab
Group 2 participants who have completed OLE part in the parent study (WN29922 or WN39658), will continue to receive open-label gantenerumab 510 mg SC, Q2W

Locations

Country Name City State
Argentina Hospital Italiano Caba
Argentina Universidad Maimonides Caba
Argentina Instituto Geriatrico Nuestra Señora de las Nieves Capital Federal
Argentina CEN Centro Especializado en Neurociencias Cordoba
Argentina Instituto Kremer Córdoba
Argentina Instituto de Neurociencias San Agustín S.A. La Plata
Argentina Fundación Scherbovsky; General Department Mendoza
Australia St Vincent's Hospital Sydney; Neurology Darlinghurst New South Wales
Australia Central Coast Neurosciences Research Erina New South Wales
Australia Heidelberg Repatriation Hospital; Medical and Cognitive Research Centre Heidelberg West Victoria
Australia Southern Neurology Kogarah New South Wales
Australia Australian Alzheimer's Research Foundation Nedlands Western Australia
Australia The Queen Elizabeth Hospital; Neurology Woodville South Australia
Belgium AZ Sint Blasius (Dendermonde) Dendermonde
Belgium UZ Gent Gent
Belgium Jessa Zkh (Campus Virga Jesse) Hasselt
Brazil Hospital Nossa Senhora das Graças; Setor de Pesquisa em Neurologia Curitiba PR
Brazil Instituto de Neurologia de Curitiba Curitiba PR
Brazil Clinica Clinilive ltda Maringa PR
Brazil Hospital das Clinicas - UFRGS Porto Alegre RS
Brazil Hospital das Clinicas - FMUSP_X; Neurologia Sao Paulo SP
Canada Center for Diagnosis and Research on Alzheimer's disease Greenfield Park Quebec
Canada Parkwood Hospital; Geriatric Medicine London Ontario
Canada Alpha Recherche Clinique Quebec
Canada Baycrest Health Sciences Toronto Ontario
Canada Sunnybrook Health Sciences Centre Toronto Ontario
Canada The Medical Arts Health Research Group - West Vancouver Vancouver British Columbia
Canada Devonshire Clinical Research Woodstock Ontario
Chile Psicomed Estudios Médicos Antofagasta
Chile Biomedica Research Group Santiago
Chile Especialidades Medicas LYS Santiago
China Beijing Tian Tan Hospital,Capital Medical University Beijing City
Denmark Aarhus Universitetshospital; Neurologisk Afd. F, Demensklinikken Aarhus N
Denmark Rigshospitalet, Hukommelsesklinikken København Ø
Denmark Svendborg Sygehus; Neurologisk afdeling N, Demensklinik Fyn Svendborg
Finland Terveystalo Ruoholahti Helsinki
Finland Itä-Suomen yliopisto, Kuopion kampus Kuopio
France CHU Amiens Hopital Sud; Neurologie Amiens Cedex1
France Hôpital Avicenne; Centre de Recherche Clinique Bobigny Cedex
France Groupement Hospitalier Est - Hôpital Neurologique; Neurologie A (U502) Bron cedex
France CHU de la Timone - Hopital d Adultes; Service de Neurologie Marseille
France Hôpital Lariboisière Paris
France CHU Poitiers - Hopital La Miletrie Poitiers
France CHU Strasbourg Hôpital Hautepierre Strasbourg
France Gerontopole; Centre de Recherche clinique Toulouse
France Hopital des Charpennes Villeurbanne
Germany Ambulates Gesundheitszentrum der Charité GmbH; MVZ Neurologie Campus Benjamin Franklin Berlin
Germany ECRC Experimental and Clinical Research Center, Charité Campus Berlin Buch, Memory Clinic Berlin
Germany Universitätsklinikum Köln; Klinik und Poliklinik für Psychiatrie und Psychotherapie Köln
Germany PANAKEIA - Arzneimittelforschung Leipzig GmbH Leipzig
Germany Universitätsmedizin derJohannes Gutenberg-Universität Mainz;Klinik für Psychiatrie und Psychotherapi Mainz
Germany Klinikum rechts der Isar der TU München; Klinik für Psychiatrie und Psychotherapie München
Germany Universitätsklinikum Münster; Klinik und Poliklinik für Neurologie Münster
Germany Universitätsklinikum Rostock Zentrum für Nervenheilkunde Rostock
Germany Universitätsklinikum Ulm; Klinik für Neurologie Ulm
Germany Studienzentrum Nordwest Dr med Joachim Springub Herr Wolfgang Schwarz Westerstede
Germany Forschungszentrum Ruhr Witten
Hungary Semmelweis University; Department of Neurology Budapest
Italy IRCCS ?Centro S. Giovanni di Dio? Fatebenefratelli -UO Alzheimer Brescia Lombardia
Italy IRCCS Ospedale San Raffaele; Centro Disturbi della Memoria Milano Lombardia
Italy Nuovo Ospedale Civile S. Agostino-Estense; Clinica Neurologica ? Dipartimento di Neuroscienze Modena Emilia-Romagna
Italy ASST DI MONZA; Neurologia Monza Lombardia
Italy Dipartimento delle Patologie Emergenti; Azienda Ospedaliera Universitaria Policlinico Paolo Giaccone Palermo Sicilia
Italy IRCCS Neuromed; Neurologia I-Centro studio e cura delle demenze e UVA Pozzilli Molise
Italy Fondazione Santa Lucia IRCCS; Neurologia e Riabilitazione Neurologica Roma Lazio
Italy Ospedale San Giovanni Calibita Fatebenefratell;Neurologia Roma Lazio
Italy Umberto I Policlinico di Roma-Università di Roma La Sapienza Roma Lazio
Italy AO Città della Salute e della Scienza Osp.S.Giov.Battista Molinette; SC Geriatria Torino Piemonte
Japan Nagoya Ekisaikai Hospital Aichi
Japan National Center for Geriatrics and Gerontology Aichi
Japan Yachiyo Hospital Aichi
Japan Inage Neurology and Memory Clinic Chiba
Japan Juntendo University Urayasu Hospital Chiba
Japan Medical Corporation Hakuyokai Kashiwado Hospital Chiba
Japan Tokyo Bay Advanced Medical and Makuhari Clinic Chiba
Japan Fukuoka University Hospital Fukuoka
Japan Southern Tohoku Medical Clinic Fukushima
Japan National Hospital Organization Hiroshima-Nishi Medical Center Hiroshima
Japan Hyogo Prefectural HarimaHimeji General Medical Center Hyogo
Japan Kobe University Hospital Hyogo
Japan Matsui Dietary and Dementia Clinic Hyogo
Japan Tsukazaki Hospital Hyogo
Japan Kagawa Prefectural Central Hospital Kagawa
Japan Shonan Kamakura General Hospital Kanagawa
Japan Rakuwakai Otowa Hospital Kyoto
Japan Uji Takeda Hospital Kyoto
Japan Okayama Kyokuto Hospital Okayama
Japan Rijikai Medical Corporation Katayama Medical Clinic Okayama
Japan Kishiwada Tokushukai Hospital Osaka
Japan MI Clinic Osaka
Japan National Hospital Organization Hizen Psychiatric Medical Center Saga
Japan NHO Shizuoka Institute of Epilepsy and Neurological Disorders Shizuoka
Japan Shizuoka City Shimizu Hospital Shizuoka
Japan Jichiidai Station Brain Clinic Tochigi
Japan Medical corporation Ichiekai Itsuki Hospital Tokushima
Japan Tokushima Hospital Tokushima
Japan National Center of Neurology and Psychiatry Tokyo
Japan Nozomi Memory Clinic Tokyo
Japan P-One Clinic Tokyo
Japan Tokyo Medical and Dental University Hospital Tokyo
Japan Tokyo Medical University Hospital Tokyo
Japan Yamagata Tokusyukai Hospital Yamagata
Korea, Republic of Dong-A University Hospital Busan
Korea, Republic of Myongji Hospital Gyeonggi-do
Korea, Republic of Gachon University Gil Medical Center Incheon
Korea, Republic of Inha University Hospital Incheon
Korea, Republic of Seoul National University Bundang Hospital Seongnam-si
Korea, Republic of Asan Medical Center Seoul
Korea, Republic of Ewha Womans University Hospital (Seoul) Seoul
Korea, Republic of Hanyang University Seoul Hospital Seoul
Korea, Republic of Konkuk University Medical Center Seoul
Korea, Republic of Samsung Medical Center Seoul
Korea, Republic of Seoul St Mary's Hospital Seoul
Lithuania Vilnius University Hospital Santariskiu Clinics; Neurology Vilnius
Mexico Mexico Centre for Clinical Research Ciudad de México Mexico CITY (federal District)
Mexico Hospital Angeles de Culiacán, Neurociencias Estudios Clínicos SC Culiacán Sinaloa
Mexico AVIX Investigación Clínica S.C Monterrey Nuevo LEON
Mexico Hospital Universitario Dr Jose Eleuterio Gonzalez UANL; Depto.de NeurologíaPta.BajaConsulta Monterrey Nuevo LEON
Netherlands Brain Research Center B.V Amsterdam
Peru Hospital IV Alberto Sabogal Sologuren; Unidad de Investigacion Bellavista
Peru Clinica Internacional; Unidad De Investigacion Lima
Peru Hospital Nacional Dos de Mayo; Unidad de Investigacion de Neurologia Lima
Poland O?rodek Badawczo-Naukowo-Dydaktyczny Chorób Ot?piennych w ?cinawie ?cinawa
Poland Podlaskie Centrum Psychogeriatrii Bia?ystok
Poland NZOZ Vitamed Bydgoszcz
Poland NEURO-CARE Sp. z o.o. Sp. Komandytowa Katowice
Poland KO-MED Centra Kliniczne Lublin II Lublin
Poland Neurologiczny NZOZ Centrum Leczenia SM; Osrodek Badan Klinicznych Plewiska
Poland Senior Sp. Z O.O. Poradnia Psychogeriatryczna Sopot
Poland mMED Maciej Czarnecki Warszawa
Poland Pratia S.A. Warszawa
Poland NZOZ WCA Wroc?aw
Portugal Hospital de Braga; Servico de Neurologia Braga
Portugal HUC; Servico de Neurologia Coimbra
Portugal Hospital da Senhora da Oliveira-Guimarães; Serviço de Neurologia Guimarães
Portugal Hospital Geral de Santo Antonio; Servico de Neurologia Porto
Puerto Rico Santa Cruz Behavioral PSC Bayamon
Puerto Rico University of Puerto Rico - Medical Science Campus; Internal Medicine San Juan
Russian Federation State autonomous institution of healthcare Inter-regional clinical and diagnostic center Kazan Tatarstan
Russian Federation Vertebronevrologiya LLC Kazan Tatarstan
Russian Federation FSBHI Siberian Clinical Center of the Federal Medical and Biological Agency Krasnoyarsk Krasnojarsk
Russian Federation City Clin Hosp n.a. S.P.Botkin Moscow Moskovskaja Oblast
Russian Federation University ?linic of headaches Moscow Moskovskaja Oblast
Russian Federation City Polyclinic No. 2 of the Department of Healthcare of the City of Moscow Moskva Moskovskaja Oblast
Russian Federation FSBMEI HPE "Military Medical Academy n.a. S.M. Kirov" of the MoD of the RF Sankt-peterburg Sankt Petersburg
Russian Federation MHI City Clinical Hospital #2 named after V.I. Razumovsky; Psychiatric Saratov
Russian Federation Nebbiolo Center for Clinical Trials Tomsk
Spain Hospital General Universitario de Albacete; Servicio de Neurología Albacete
Spain Fundación ACE; Servicio de Neurología Barcelona
Spain Hospital Clinic i Provincial; Servicio de Neurologia Barcelona
Spain Hospital de la Santa Creu i Sant Pau; Servicio de Neurologia Barcelona
Spain Hospital del Mar; Servicio de Neurologia Barcelona
Spain Hospital Vall d'Hebron; Servicio de Neurología Barcelona
Spain Hospital Universitario Reina Sofia; Servicio de Neurologia Cordoba
Spain Policlínica Guipuzcoa; Servicio de Neurología Donostia-san Sebastian Guipuzcoa
Spain Hospital General Universitario de Elche; Servicio de Neurología Elche Alicante
Spain CAE OROITU; Servicio de Neurología Getxo Vizcaya
Spain Hospital Universitari de Bellvitge; Servicio de Neurologia L'Hospitalet de Llobregat Barcelona
Spain Hospital Universitario de Santa Maria; Servicio de Neurología Lleida Lerida
Spain Hospital San Pedro; Servicio de Neurología Logroño LA Rioja
Spain Hospital Ramon y Cajal; Servicio de Neurologia Madrid
Spain Hospital Ruber Internacional; Servicio de Neurología Madrid
Spain Hospital Universitario 12 de Octubre; Servicio de Neurologia Madrid
Spain Universitario de La Princesa; Servicio de Neurología Madrid
Spain HM Universitario Puerta del Sur CINAC (C.Integ.Neuroc);; Servicio de Psiquiatría Móstoles Madrid
Spain Clinica Universitaria de Navarra Pamplona Navarra
Spain Clinica Universitaria de Navarra; Servicio de Neurología Pamplona Navarra
Spain Hospital Virgen del Puerto. Servicio de Neurología Plasencia Caceres
Spain Hospital Quiron de Madrid; Servicio de Neurologia Pozuelo de Alarcon Madrid
Spain Complejo Asistencial Universitario de Salamanca; Servicio de Psiquiatría Salamanca
Spain Hospital General De Catalunya; Servicio de Neurologia Sant Cugat del Valles Barcelona
Spain Hospital Universitario Marques de Valdecilla; Servicio de Neurología SANtander Cantabria
Spain Hospital Victoria Eugenia; Servico Neurología Sevilla
Spain Hospital Virgen del Rocío; Servicio de Neurología Sevilla
Spain Hospital Mutua De Terrasa; Servicio de Neurologia Terrassa Barcelona
Spain Hospital Universitario Dr. Peset; Servicio de Neurologia Valencia
Spain Hospital Universitario la Fe; Servicio de Neurologia Valencia
Spain Complejo Asistencial de Zamora; Servicio Psiquiatria Zamora
Spain Servicio de Neurología Hospital Viamed Montecanal. Zaragoza
Sweden Skånes Universitetssjukhus Malmö, Minneskliniken Malmö
Sweden Sahlgrenska Academy University,Neuroscience and Physiology;Departmt of Psychiatry and Neurochemistry Mölndal
Sweden KAROLINSKA UNI HOSPITAL, HUDDINGE; Mottagning Kognitiv Forskning, M54 Stockholm
Taiwan Changhua Christian Hospital; Neurology Changhua County
Taiwan Kaohsiung Medical University Hospital; Neurology Kaohsiung
Taiwan Chang Gung Memorial Foundation - Kaohsiung - Neurology Niaosong Dist.
Taiwan China Medical University Hospital; Neurology North Dist.
Taiwan National Taiwan University Hospital; Neurology Taipei
Taiwan Chang Gung Memorial Foundation - Linkou - Neurology Taoyuan
Turkey Ondokuz Mayis Univ. Med. Fac.; Neurology Samsun
United Kingdom The Rice Centre; Royal United Hospital Bath
United Kingdom Re:Cognition Health Birmingham Birmingham
United Kingdom The Fritchie Centre, Charlton Lane Centre, Charlon Lane, Leckhampton; The Fritchie Centre Cheltenham
United Kingdom Surrey and Borders NHS Foundation Trust; Research and Development Department Chertsey
United Kingdom Ninewells Hospital Dundee
United Kingdom Queen Elizabeth University Hospital - PPDS Glasgow
United Kingdom Charing Cross Hospital London
United Kingdom Re:Cognition Health London London
United Kingdom St George?s Hospital London
United Kingdom Campus for Ageing and Vitality Newcastle
United Kingdom Royal Hallamshire Hospital Sheffield Teaching Hospitals NHS Foundation Trust Sheffield
United Kingdom University Southampton NHS Foundation Trust; Wessex Neurologica Centre Southampton
United States Abington Neurological Associates Abington Pennsylvania
United States Emory University Atlanta Georgia
United States JEM Research LLC Atlantis Florida
United States Senior Adults Specialty Research Austin Texas
United States American Health Network Institute, LLC Avon Indiana
United States Missouri Memory Center Bolivar Missouri
United States Brigham and Womens Hospital; Center for Alzheimer Research & Treatment Boston Massachusetts
United States Accel Research Sites - CRU Tampa Bradenton Florida
United States Bradenton Research Center Bradenton Florida
United States Behavioral Health Research Charlotte North Carolina
United States University of Virginia Charlottesville Virginia
United States Cleveland Clinic; Cleveland Lou Ruvo Center for Brain Health ? Neurological Institute Cleveland Ohio
United States Ohio State University; College of Medicine Columbus Ohio
United States Kerwin Medical Center Dallas Texas
United States Neurology Consultants of Dallas; Research Department Dallas Texas
United States Brain Matters Research, Inc. Delray Beach Florida
United States Health Initiatives Research, PLLC Fayetteville Arkansas
United States Precise Research Centers Flowood Mississippi
United States Fort Wayne Neurological Center Fort Wayne Indiana
United States Fullerton Neurology and Headache Center Fullerton California
United States Neurology Center of North Orange County Fullerton California
United States Center for Advanced Research & Education Gainesville Georgia
United States Alzheimers Disease & Memory Disorders Center; Department of Neurology Baylor College of Medicine Houston Texas
United States The University of Texas Health Science Center at Houston Houston Texas
United States Irvine Center for Clinical Research Irvine California
United States University of Mississippi Medical Center Jackson Mississippi
United States The Clinical Trial Center, LLC Jenkintown Pennsylvania
United States Neurological Associates of Long Island, PC Lake Success New York
United States Cleveland Clinic Lou Ruvo; Center for Brain Research Las Vegas Nevada
United States UW Wisconsin-Madison Madison Wisconsin
United States ClinCloud, LLC Maitland Florida
United States Alzheimer's Memory Center Matthews North Carolina
United States Allied Biomedical Research Institute, Inc Miami Florida
United States Optimus U Corp Miami Florida
United States Yale University School Of Medicine New Haven Connecticut
United States Columbia University Medical Center New York New York
United States Boston Center for Memory Newton Massachusetts
United States Sentara Neurology Specialists Norfolk Virginia
United States Research Center for Clinical Studies, Inc. Norwalk Connecticut
United States Renstar Medical Research Ocala Florida
United States University of Nebraska Medical Center; Dept of Neurological Sciences Omaha Nebraska
United States Banner Alzheimer?s Institute Phoenix Arizona
United States Barrow Neurological Institute Phoenix Arizona
United States Summit Research Network Inc. Portland Oregon
United States Raleigh Neurology Associates Raleigh North Carolina
United States Desert Valley Research Redlands California
United States National Clinical Research Inc.-Richmond Richmond Virginia
United States AD-CARE, University of Rochester Medical Center Rochester New York
United States Sutter Medical Group, Neurology Sacramento California
United States Washington University School of Medicine Saint Louis Missouri
United States Wasatch Clinical Research, LLC Salt Lake City Utah
United States Syrentis Clinical Research Santa Ana California
United States Intercoastal Medical Group Sarasota Florida
United States California Neuroscience Research Medical Group, Inc Sherman Oaks California
United States Southern California Research LLC Simi Valley California
United States Southern Illinois University, School of Medicine Springfield Illinois
United States The Cognitive and Research Center of New Jersey Springfield New Jersey
United States Richmond Behavioral Associates Staten Island New York
United States Banner Sun Health Research Insitute Sun City Arizona
United States Infinity Clinical Research, LLC Sunrise Florida
United States SUNY Upstate Medical University Syracuse New York
United States Axiom Clinical Research of Florida Tampa Florida
United States Advanced Memory Research Institute of NJ Toms River New Jersey
United States Georgetown University Medical Center Washington District of Columbia
United States Alzheimer?s Research and Treatment Center Wellington Florida
United States Via Christi Research Wichita Kansas
United States Wake Forest University Winston-Salem North Carolina

Sponsors (1)

Lead Sponsor Collaborator
Hoffmann-La Roche

Countries where clinical trial is conducted

United States,  Argentina,  Australia,  Belgium,  Brazil,  Canada,  Chile,  China,  Denmark,  Finland,  France,  Germany,  Hungary,  Italy,  Japan,  Korea, Republic of,  Lithuania,  Mexico,  Netherlands,  Peru,  Poland,  Portugal,  Puerto Rico,  Russian Federation,  Spain,  Sweden,  Taiwan,  Turkey,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants With at Least One Adverse Event (AE) and Serious Adverse Event (SAE) An AE is any untoward medical occurrence in a clinical investigation participant administered a pharmaceutical product, regardless of casual attribution. A SAE is any AE that is fatal, life threatening, requires or prolongs inpatient hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect in a neonate/infant born to a mother exposed to study drug or a significant medical event in the investigator's judgment. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants With Post-baseline Suicidal Ideation or Suicidal Behavior as Measured Using Columbia-Suicide Severity Rating Scale (C-SSRS) Score C-SSRS= assesses lifetime suicidality of participant (at baseline) & any new instances of suicidality (since last visit). Structured interview prompts recollection of suicidal ideation (intensity of ideation, behavior, & attempts with actual/potential lethality). Categories have yes/no responses, include Wish to be Dead; Non-specific Active Suicidal Thoughts; Active Suicidal Ideation with Any Methods (Not Plan) without Intent to Act; Active Suicidal Ideation with Some Intent to Act, without Specific Plan; Active Suicidal Ideation with Specific Plan and Intent, Preparatory Acts and Behavior; Aborted/Interrupted Attempt; Actual Attempt (non-fatal); Completed Suicide. Suicidal ideation/behavior= "yes" to any of listed categories. Score of 0= no suicide risk. Score of 1 or higher= suicidal ideation or behavior. Categories with non-zero values are only reported here. First dosing visit in OLE (first dosing in current study or OLE period of parent GRADUATE studies)=baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants With at Least One Amyloid-Related Imaging Abnormalities-Edema (ARIA-E) Confirmed by MRI ARIA are an identified risk with anti-amyloid antibodies, including gantenerumab. These changes can be identified on brain MRI. In ARIA-E, (E for oedema or effusion), oedema can be seen in different areas of the brain on MRI, representing fluid leakage into the brain parenchyma or sulcal spaces. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants With at Least One Amyloid-Related Imaging Abnormalities-Haemosiderin Deposition (ARIA-H) Confirmed by MRI ARIA are an identified risk with anti-amyloid antibodies, including gantenerumab. These changes can be identified on brain MRI. ARIA-H (H for hemosiderosis) are small foci of signal loss observed on MRI sequences sensitive for paramagnetic tissue properties and comprise cerebral microbleeds (small foci of bleeding in the brain parenchyma) and leptomeningeal hemosiderosis (small foci of bleeding on the surface of the brain). These changes also occur sporadically in AD. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants With Injection-Site Reactions (ISRs) An AE is any unfavorable and unintended sign, symptom, or disease temporally associated with the use of a pharmaceutical product, regardless of casual attribution. Local injection reactions (or injection site reactions) are defined as AEs related to the injection site that occur during or within 24 hours after study drug administration that are judged to be related to the study drug injection. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants Who Discontinued the Study Due an AE An AE is any untoward medical occurrence in a clinical investigation participant administered a pharmaceutical product, regardless of casual attribution. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Primary Number of Participants With at Least One Adverse Event of Special Interest (AESI) An AE is any untoward medical occurrence in a clinical investigation participant administered a pharmaceutical product, regardless of casual attribution. AEs that were considered to be of special interest for this study included cases of potential drug-induced liver injury that include an elevated ALT or AST in combination with either an elevated bilirubin or clinical jaundice, as defined by Hy's Law and suspected transmission of an infectious agent by the study drug. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
Secondary Change From Baseline Over Time in Clinical Dementia Rating - Global Score (CDR-GS) CDR was derived through semi-structured interview with the participant and an appropriate informant, and it rated impairment across six domains: memory, orientation, judgment, and problem solving, community affairs, home and hobbies, and personal care on a 5-point scale for which 0=normal, 0.5=very mild dementia, 1=mild dementia, 2=moderate dementia, and 3= severe dementia. The score range for the CDR-GS is from 0 to 3 and a high score on the CDR-GS would indicate a high disease severity. A negative change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Clinical Dementia Rating (CDR) - Sum of Boxes (SB) CDR was derived through semi-structured interview with the participant and an appropriate informant, and it rated impairment across six domains: memory, orientation, judgment, and problem solving, community affairs, home and hobbies, and personal care on a 5-point scale for which 0=no impairment, 0.5=questionable impairment, and 1, 2, and 3=mild, moderate, and severe impairment, respectively. The CDR-SB is based on summing each of the domain box scores with total score ranging from 0-18 with higher scores reflecting greater cognitive and functional impairment. A negative change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Mini-Mental State Examination (MMSE) Score MMSE is a rater-administered performance-based outcome (PerfO) that includes a set of standardized questions used to evaluate possible cognitive impairment and help stage the severity level of this impairment. The questions target six areas: orientation, registration, attention, short-term recall, language, and constructional praxis/visuospatial abilities. Total score ranges from 0-30, with lower scores indicating greater impairment. A positive change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Alzheimer Disease Assessment Scale-Cognition, Subscale 11 (ADAS-Cog11) Score ADAS-Cog11 was designed to measure cognitive symptom change in participants with Alzheimer's Disease (AD) and consisted of 11 tasks. The standard 11 items (and corresponding score range) were: word recall (0-10), commands (0-5), constructional praxis (0-5), naming objects and fingers (0-5), ideational praxis (0-5), orientation (0-8), word recognition (0-12), spoken language ability (0-5), comprehension of spoken language (0-5), word-finding difficulty (0-5), and remembering test instructions (0-5). The test included 7 performance items and 4 clinician-rated items. The ADAS-Cog11 total score was the sum of all 11 individual items, with a total score ranging from 0 (no impairment) to 70 (severe impairment). Higher scores indicated more severe cognitive impairment. A negative change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Alzheimer Disease Assessment Scale-Cognition, Subscale 13 (ADAS-Cog13) Score The ADAS-Cog13 total score includes all of the items in the ADAS-Cog11 in addition to delayed word recall and the number cancellation. For the ADAS-cog 13 the range is 0-85 (score range for Delayed Word Recall [DWR] score is 0-10 and for Number Cancellation [NC] is 0-5, thus the score is ADAS-cog 11[0-70] plus the scores for DWR and NC). A higher score indicates worse performance. A negative change from baseline indicates improvement in cognitive function. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Verbal Fluency Task Score VFT is a rater administered PerfO that measures speed and flexibility of verbal thought with a total score that ranges from 0-99 (lower scores indicating lower performance). A positive change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change From Baseline Over Time in Coding (Digit Symbol Substitution Test [DSST]) Subset Coding, also called DSST is a rater administered PerfO that measures speed of processing and associative memory with a total score that ranges from 0-135 (lower scores indicating lower performance). The DSST was adapted from the Wechsler Adult Intelligence Scale. The 120-second version of the test was used in this study. Positive change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change in Functional Activities Questionnaire (FAQ) Score FAQ is a rater-administered observer-reported outcome (ObsRO) (informant-based measure) that measures a participant's functional ability to perform complex higher-order activities. The observer provides performance ratings of the target person on ten complex higher-order activities. Total score that ranges from 0-30, with higher scores reflecting greater functional impairment. A negative change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Change in Alzheimer Disease Cooperative Study Group-Activities of Daily Living (ADCS-ADL) Score ADCS-ADL is a 23-item rater-administered, ObsRO that captures a participant's ability to perform basic activities of daily living (e.g., eating and toileting) and more complex ADL or instrumental activities of daily living (iADL, e.g., using the telephone, managing finances, preparing a meal). Total score ranges from 0-78, with higher scores reflecting better functioning. A positive change from baseline indicates improvement. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). Baseline (OLE Day 1), Weeks 24, 36, 52, 76 and 104
Secondary Number of Participants With Anti-drug Antibody (ADA) to Gantenerumab The number of participants with positive results for ADA against gantenerumab at any of the post-baseline assessment time-points were reported. Evaluable participant during OLE was participant with an ADA assay result from at least one sample during OLE. Treatment Emergent ADA = A participant with a negative or missing baseline ADA result(s) and at least one positive post-baseline ADA result. The first dosing visit in the OLE (first dosing in current study or first dosing in the OLE period of the parent GRADUATE studies) was considered as baseline (OLE Day 1). From Baseline (OLE Day 1) up to 14 weeks after the last dose (up to 134 weeks)
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