Overview
Sponsor-declared trial summary
Phase
Therapeutic confirmatory (Phase III)
Status
Ended
Participants planned
750
Countries
8
Sites
45
Agitation in Patients With Dementia of the Alzheimer's Type
The primary objective is to evaluate the efficacy, safety, and tolerability of AVP-786 compared to placebo for the treatment of agitation in patients with dementia of the Alzheimer’s type.
Key facts
- Sponsor
- Otsuka Pharmaceutical Development & Commercialization Inc.
- Participant type
- Patients
- Age range
- 18-64 years, 65+ years
- Gender
- Male and Female
- Therapeutic area
- Diseases [C] - Nervous System Diseases [C10]
- Trial duration
- 6 May 2021 → 23 May 2024
- Decision date (initial)
- 2024-04-29
- Transition trial
- Yes
- Low-intervention
- No
- Rare-disease indication
- No
- Vulnerable population
- Yes
External identifiers
- EU CT number
- 2023-504991-31-00
- EudraCT number
- 2020-000799-39
- ClinicalTrials.gov
- NCT04464564
Trial design
CTIS Part I — objectives, methods, condition coding
Main objective
Scope: Safety, Efficacy, Pharmacokinetic
The primary objective is to evaluate the efficacy, safety, and tolerability of AVP-786 compared to placebo for the treatment of agitation in patients with dementia of the Alzheimer’s type.
Secondary objectives 3
- Evaluate the effects of AVP-786 compared to placebo on global assessments of severity and improvement of agitation.
- Evaluate the effects of AVP-786 compared to placebo on neuropsychiatric symptoms.
- Evaluate the effects of AVP-786 compared to placebo on measures of quality of life and resource utilization.
Conditions and MedDRA coding
Agitation in Patients With Dementia of the Alzheimer's Type
| Version | Level | Code | Term | System organ class |
|---|---|---|---|---|
| 20.0 | PT | 10012271 | Dementia Alzheimer's type | 100000004852 |
Eligibility criteria
Principal inclusion / exclusion criteria as submitted by sponsor
Inclusion criteria 14
- Males and females 50 to 90 years of age (inclusive) at the time of informed consent.
- Patients who require pharmacotherapy for the treatment of agitation per the Investigator’s judgment, after: • An evaluation of reversible factors (eg, pain, infection, or polypharmacy), and • A course of nonpharmacological interventions (eg, redirecting behavior, group activities, music therapy).
- Diagnosis of agitation must meet the International Psychogeriatric Association (IPA) provisional definition of agitation.
- NPI-AA total score (frequency × severity) must be ≥ 4 at Screening and Baseline.
- Patient must meet an additional predetermined blinded eligibility criterion.
- Patient has stable cardiac, pulmonary, hepatic, and renal function per the Investigator’s judgment.
- No clinically significant findings on the Screening ECGs based on central review and on the Baseline predose ECG based on the machine read and Investigator’s evaluation.
- Women who are of childbearing potential and are sexually active must use an effective method of birth control for at least 1 month prior to the Baseline, during participation in the study, and for at least 30 days after the last dose of study drug. The following requirements must be met: • Women who are of childbearing potential must use 2 of the following precautions in order to minimize the risk of failure of 1 method of birth control: vasectomy, tubal ligation, vaginal diaphragm, intrauterine device, birth control pills, birth control depot injection, birth control implant, or condom with spermicide or sponge with spermicide. Periodic abstinence (eg, calendar, ovulation, symptothermal, post ovulation methods), declaration of abstinence for the duration of exposure to study drug, or withdrawal are not acceptable methods of contraception. • Women who are sterile (ie, had an oophorectomy and/or hysterectomy), postmenopausal (defined as 12 consecutive months with no menses without an alternative medical cause), or practice true abstinence (when this method is in line with the preferred and usual lifestyle of the patient) are exempt from this requirement. • Women who are lactating, pregnant, or plan to become pregnant are not eligible for participation in the study. (For Slovakia only, the following text replaces the above: Patient must be postmenopausal (defined as 12 consecutive months with no menses without an alternative medical cause or surgically sterile (ie, had an oophorectomy and/or hysterectomy). • Women who are of childbearing potential, lactating, pregnant, or plan to become pregnant are not eligible for participation in the study.)
- For restricted and prohibited concomitant medications, patients willing and able to meet all protocol requirements for duration of stability or washout prior to study entry and during the study (see Table 3 Restricted and Prohibited Concomitant Medications and Appendix 1 Prohibited Concomitant Medications).
- Caregiver must be willing and able to comply with all study procedures, including adherence to administering study drug and not administering any prohibited medications during the study. The caregiver must spend a minimum of 2 hours with the patient per day for at least 4 days per week to qualify as caregiver.
- Patient/caregiver must be willing to sign and receive a copy of patient/caregiver informed consent form (ICF) after the nature and risks of study participation have been fully explained. Patients who are not capable of signing the ICF but are able to provide assent, or the patient’s authorized representative agrees to participation (for patients unable to provide assent) are allowed.
- Diagnosis of probable Alzheimer’s disease according to the 2011 NIA-AA working groups criteria. Either outpatients or residents of an assisted living facility, a skilled nursing home, a dementia unit, or any other type of facility providing long-term care.
- MMSE score between 8 and 24 (inclusive) at Screening and Baseline.
- Patient has clinically significant, moderate-to-severe agitation for at least 2 weeks prior to Screening that interferes with daily routine per the Investigator’s judgment.
Exclusion criteria 17
- Caregiver is unwilling or unable, in the opinion of the Investigator, to comply with study instructions.
- Patient has dementia predominantly of non-Alzheimer’s type (eg, vascular dementia, frontotemporal dementia, Parkinson’s disease, substance-induced dementia).
- Patients with symptoms of agitation that are not secondary to Alzheimer’s dementia (eg, secondary to pain, other psychiatric disorder, or delirium).
- Patients who have been diagnosed with an Axis 1 disorder (Diagnostic and Statistical Manual of Mental Disorders, 5th Edition, Text Revision [DSM-5] criteria) including, but not limited to: • Schizophrenia, schizoaffective disorder, or other psychotic disorders not related to dementia • Bipolar I or II disorder, bipolar disorder not otherwise specified • Current Major Depressive Episode: Patients with a history of major depressive disorder, that is currently not symptomatic, are eligible. Patients currently on a stable dose(s) of allowed antidepressant medication(s) for at least 3 months prior to the Screening visit are eligible.
- Patients with myasthenia gravis (contraindication for quinidine).
- Patients with any personal history of complete heart block, QTc prolongation, or torsades de pointes. a. Screening and Baseline predose QT interval corrected for heart rate using the Fridericia’s formula (QTcF) of > 450 msec for males and > 470 msec for females unless due to ventricular pacing (See Section 8.1.5). Screening ECGs will be based on central review. Baseline predose ECG will be based on the machine read and Investigator’s evaluation; if the QTcF result from the machine read is exclusionary, do not administer study drug and please contact a Medical Monitor. b. Presence of premature ventricular contractions (PVCs) as evaluated by a central reader and deemed clinically significant by the Investigator.
- Patients with any family history of congenital QT interval prolongation syndrome.
- Patients with known hypersensitivity to DM, Q, opiate drugs (codeine, etc), or any other ingredient of the study drug.
- Patients who have ever received DM co-administered with Q or d6-DM co-administered with Q.
- Patients who would be likely to require a prohibited concomitant medication during the study (see Table 3, Restricted and Prohibited Concomitant Medications and Appendix 1 Prohibited Concomitant Medications).
- Patients with co-existent clinically significant or unstable systemic diseases that could confound the interpretation of the safety results of the study (eg, malignancy [except skin basal-cell carcinoma], poorly controlled diabetes, poorly controlled hypertension, unstable pulmonary, renal or hepatic disease, unstable ischemic cardiac disease, dilated cardiomyopathy, or unstable valvular heart disease). Certain other nonmetastatic cancer may be allowed. Each case is to be evaluated individually with a Medical Monitor.
- Patients who are currently participating in or who have participated in other interventional (drug or device) clinical study, or found to be a “Virtually Certain” match in Clinical Trial Subject Database (CTSdatabase) with a patient who has participated in another interventional drug or device study within 30 days of Baseline.
- Patients with history of postural syncope or any history of unexplained syncope (evaluated on a case-by-case basis) within 12 months of Baseline.
- Patients with a history of substance and/or alcohol abuse within 12 months of Baseline.
- Patients determined to have a high imminent risk of falls during the study based on a clinical evaluation by the Investigator.
- Patients with evidence of serious risk of suicide at Screening and Baseline based on the Sheehan Suicidality Tracking Scale (S-STS), ie, a score of 3 or 4 on any one question 2 through 6 or 11, or a score of 2 or higher on any one questions 1a, 7 through 10, or 12, or who in the opinion of the Investigator present a serious risk of suicide.
- Patients who, in the opinion of the Investigator, Medical Monitor, or sponsor, should not participate in the study.
Endpoints
Primary and secondary outcome measures (English text)
Primary endpoints 1
- The primary efficacy endpoint is the change from baseline to the end of the efficacy period in the CMAI total score.
Secondary endpoints 1
- The key secondary efficacy variable is the change from baseline to end of efficacy period in the CGI-S score, as related to agitation. It will be analyzed by the same statistical methodology specified for the analysis of the primary efficacy variable. The procedure to control the overall type I error rate for this key secondary efficacy analysis will be described in the SAP.
Investigational products
Investigational medicinal products (IMPs), comparators, placebo, auxiliary
Test 1
PRD11079714 · Product
- Active substance
- Quinidine Sulfate
- Substance synonyms
- QUINIDINE SULPHATE
- Pharmaceutical form
- CAPSULE
- Route of administration
- ORAL
- Max daily dose
- 85.26 mg milligram(s)
- Max total dose
- 7247.1 mg milligram(s)
- Max treatment duration
- 85 Day(s)
- Authorisation status
- Not Authorised
- MA holder
- OTSUKA PHARMACEUTICAL DEVELOPMENT & COMMERCIALIZATION, INC
- Paediatric formulation
- No
- Orphan designation
- 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
Sponsors and contacts
Sponsor organisations, regulatory contacts, third parties
Otsuka Pharmaceutical Development & Commercialization Inc.
- Sponsor organisation
- Otsuka Pharmaceutical Development & Commercialization Inc.
- Address
- 2440 Research Boulevard
- City
- Rockville
- Postcode
- 20850-3238
- Country
- United States
Scientific contact point
- Organisation
- Otsuka Pharmaceutical Development & Commercialization Inc.
- Contact name
- Public and Scientific Study Contact
Public contact point
- Organisation
- Otsuka Pharmaceutical Development & Commercialization Inc.
- Contact name
- Public and Scientific Study Contact
Third parties 17
| Organisation | City, country | Duties |
|---|---|---|
| Synevo Sp. z o.o. ORG-100047417
|
Lodz, Poland | Other |
| Clinical Trial Media Inc. ORG-100046339
|
Hauppauge, United States | Other |
| Synevo Sp. z o.o. ORG-100047417
|
Gdansk, Poland | Other |
| Syneos Health Inc. ORG-100008382
|
Morrisville, United States | Code 10, Code 11, Code 12, Other, Code 2, Data management, Code 9 |
| Longboat Clinical Limited ORG-100045828
|
Limerick, Ireland | Other |
| Labconnect LLC ORG-100042800
|
Johnson City, United States | Other |
| Celerion Inc. ORG-100029202
|
Lincoln, United States | Other |
| Signant Health Global LLC ORG-100040604
|
Blue Bell, United States | Other |
| Pro-Ficiency LLC ORG-100042038
|
Durham, United States | Other |
| Signature Diagnostics Inc. ORG-100050226
|
Pittsburgh, United States | Other |
| Endpoint Clinical Inc. ORG-100040567
|
San Francisco, United States | Other |
| ADAX raziskave v medicini d.o.o. ORG-100041891
|
Ljubljana, Slovenia | Other |
| Inato ORG-100044345
|
Neuilly Sur Seine Cedex, France | Other |
| Clinical Ink Inc. ORG-100042433
|
Winston Salem, United States | Data management |
| Eresearchtechnology Inc. ORG-100013039
|
Philadelphia, United States | Other |
| Greenphire LLC ORG-100041621
|
King Of Prussia, United States | Other |
| C2n Diagnostics LLC ORG-100049457
|
Saint Louis, United States | Other |
Locations
8 EU/EEA countries · 45 investigational sites
By country
| Country | MS status | Planned subjects | Sites |
|---|---|---|---|
| Belgium | Ended | 17 | 3 |
| Croatia | Ended | 35 | 6 |
| Hungary | Ended | 39 | 8 |
| Ireland | Ended | 11 | 4 |
| Netherlands | Ended | 22 | 1 |
| Slovakia | Ended | 59 | 6 |
| Slovenia | Ended | 35 | 6 |
| Spain | Ended | 30 | 11 |
| Rest of world
United States, Canada, Mexico, Colombia, Chile
|
— | 502 | — |
Investigational sites
Anima
N/A, Alkerstraat 28, 3570, Alken
UZ Leuven
UPC KU Leuven campus Gasthuisberg, Herestraat 49, 3000, Leuven
Hopital Erasme
Neurology, Lennikse Baan 808, 1070, Anderlecht
Poliklinika Neuron
Neurology, Salata 12, 10000, Grad Zagreb
University Hospital Centre Zagreb
Neurology, Ulica Mije Kispatica 12, 10000, Zagreb
BONIFARM d.o.o. za zastupanje i usluge
Neurology, Ulica Aleksandra Hondla 2/10, Zagreb, Grad Zagreb
Klinika za psihijatriju Vrapce
Biological Psychiatry and Psychogeriatrics, Bolnicka Cesta 32, Zagreb, Grad Zagreb
Pula General Hospital Ospedale Generale di Pola
Department of neurology, Santoriova Ulica 24a, Pula, Pula - Pola
Clinical Hospital Centre Rijeka
Clinic for psychiatry, Kresimirova 42, 51000, Rijeka
Semmelweis University
Department of Psychiatry and Pshychotherapy, Balassa J Utca 6, 1083, Budapest
Obudai Egeszseguegyi Centrum Kft.
Department of Psychiatry, Lajos Utca 74-76, 1036, Budapest III
Obudai Egeszseguegyi Centrum Kft.
Department of Psychiatry, Zarda Utca 11-13, 8900, Zalaegerszeg
PsychoTech Kft.
N/A, Endresz Gyorgy Utca 2/2, 7633, Pecs
University Of Szeged
Department of Psychiatry, Koranyi Fasor 8-10, 6720, Szeged
Bacs-Kiskun Varmegyei Oktatokorhaz
Department of Psychiatry, Kossuth Lajos Utca 34, 6300, Kalocsa
Clinexpert Kft.
Department of Psychiatry, Dozsa Gyorgy Utca 15, 3200, Gyongyos
Obudai Egeszseguegyi Centrum Kft.
Department of Psychiatry, Lajos Utca 74-76, 1036, Budapest III
Mercy University Hospital
Geriatric Medicine, Grenville Place, T12 WE28, Cork
Tallaght University Hospital
Cognitive Clinical Trials Unit, Tallaght, D24 NR0A, Dublin 24
St James's Hospital
Global Brain Health Institute, James's Street, D08 NHY1, Dublin 8
St. Finbarr's Hospital
The Assessment and Treatment Centre, Douglas Rd, Ballinlough, Cork
Brain Research Center Den Bosch B.V.
Geriatrics, Statenlaan 37, 5223 LA, 's-Hertogenbosch
Centrum Zdravia R.B.K. s.r.o.
Psychiatricka ambulancia, Pod Papiernou 1286/4, 085 01, Bardejov
Epamed s.r.o.
Psychiatricka ambulancia, Topasova 9, Zapad, Kosice - Zapad
Konzilium s.r.o.
Neurologicka ambulancia, Puskinova 795/8, 018 51, Nova Dubnica
Crystal Comfort s.r.o.
N/A, M R Stefanika 2427, 093 01, Vranov Nad Toplou
MUDr. Beata Dupejova neurologicka ambulancia s.r.o.
N/A, Nova 21, Foncorda, Banska Bystrica
PsychoLine s.r.o.
Psychiatrická ambulancia, Dobsinskeho 4861, 97901, Rimavska Sobota
University Medical Center Ljubljana
Department of Neurology, Zaloska Cesta 7, 1000, Ljubljana
Splosna Bolnisnica Murska Sobota
Department of Neurology, Rakican, Ulica Dr. Vrbnjaka 6, Murska Sobota
Univerzitetni Klinicni Center Maribor
Department of Neurologic Diseases, Ljubljanska Ulica 5, 2000, Maribor
Univerzitetna psihiatricna klinika Ljubljana
Department of Geriatry, Chengdujska Cesta 45, 1000, Ljubljana
Nevrološka ambulanta Kromberk
N/A, Ulica Vinka Vodopivca 21, 5000, Nova Gorica
Psihiatricna Bolnisnica Begunje
Psychiatric Hospital Begunje, Begunje Na Gorenjskem 55, 4275, Begunje Na Gorenjskem
Clinica Montecanal S.L.
Neuroscience, Calle Franz Schubert 2, 50012, Zaragoza
University Hospital Son Espases
Neurology, Carretera Valldemossa 79, 07120, Palma
Hospital Universitario De La Princesa
Neurology, Calle De Diego De Leon 62, 28006, Madrid
Hospital Universitario La Paz
Geriatrics, Paseo Castellana 261, 28046, Madrid
Hospital Universitario Virgen De La Macarena
Neurology, Avenida Del Doctor Fedriani 3, 41009, Sevilla
Hospital Universitario Rio Hortega
Psychiatry and mental health, Calle Dulzaina 2, 47012, Valladolid
Accellacare Espana S.L.
Neurology, Calle Del Marques De La Valdavia 103 Bajo Local, 28100, Alcobendas
Hospital General Universitario Dr. Balmis
Neurology, Avinguda Del Pintor Baeza 12, 03010, Alicante
Complejo Asistencial De Zamora Hospital Provincial De Zamora
Psychiatry, Calle De Hernan Cortes 40, 49020, Zamora
University Hospital Virgen Del Rocio S.L.
Neurology, Avenida De Manuel Siurot S/n, 41013, Sevilla
Hospital Universitario Del Henares
Neurology, Avenida De Marie Curie S/n, 28822, Coslada
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 | 2022-10-05 | 2022-10-05 | 2024-05-10 | ||
| Croatia | 2022-11-15 | 2022-11-15 | 2024-05-10 | ||
| Hungary | 2021-05-27 | 2021-05-27 | 2024-05-10 | ||
| Ireland | 2024-04-29 | 2024-04-29 | 2024-05-10 | ||
| Netherlands | 2022-07-21 | 2022-07-21 | 2024-05-10 | ||
| Slovakia | 2021-07-23 | 2021-07-23 | 2024-05-10 | ||
| Slovenia | 2022-04-06 | 2022-04-06 | 2024-05-10 | ||
| Spain | 2021-05-06 | 2021-05-06 | 2024-05-10 |
Results and documents
Annex IV summary of results, Annex V layperson summary, and all documents registered in CTIS for this trial
Summary of results Art. 37(4) CTR
| Title | Submission date | Status | Type |
|---|---|---|---|
| 20-AVP-786-307 EUCTIS Results _17 March 2025 SUM-80549
|
2025-04-29T22:21:35 | Submitted | Summary of Results |
Layperson summary Annex V
| Title | Submission date | Status | Type |
|---|---|---|---|
| 20-AVP-786-307 Plain Language Summary Final_27Mar2025 | 2025-04-29T22:30:36 | Submitted | Laypersons Summary of Results |
Documents 11 files
Public protocol annexes, IB summaries, regulatory submissions and post-authorisation documents registered in CTIS.
| Type | Title | Version |
|---|---|---|
| Laypersons summary of results (for publication) | 20-AVP-786-307 Plain Language Summary Final | N/A |
| Laypersons summary of results (for publication) | BE_20-AVP-786-307 Plain Language Summary Final_BE-de | N/A |
| Laypersons summary of results (for publication) | BE_20-AVP-786-307 Plain Language Summary Final_BE-fr | N/A |
| Laypersons summary of results (for publication) | BE_20-AVP-786-307 Plain Language Summary Final_BE-nl | N/A |
| Laypersons summary of results (for publication) | ES_20-AVP-786-307 Plain Language Summary Final_es | N/A |
| Laypersons summary of results (for publication) | HR_20-AVP-786-307 Plain Language Summary Final_hr | N/A |
| Laypersons summary of results (for publication) | HU_20-AVP-786-307 Plain Language Summary Final_hu | N/A |
| Laypersons summary of results (for publication) | NL_20-AVP-786-307 Plain Language Summary Final_nl | N/A |
| Laypersons summary of results (for publication) | SI_20-AVP-786-307 Plain Language Summary Final_sl | N/A |
| Laypersons summary of results (for publication) | SK_20-AVP-786-307 Plain Language Summary Final_sk | N/A |
| Summary of results (for publication) | 20-AVP-786-307 EUCTIS Results | N/A |
Application history
1 submissions — initial application plus substantial / non-substantial modifications
| # | Type | Code | Submitted | Reference MS | Conclusion | Decision date |
|---|---|---|---|---|---|---|
| 1 | INITIAL | IN | 2024-03-25 | Spain | Acceptable 2024-04-25
|
2024-04-25 |