A Phase 3 Study to Evaluate the Safety and Efficacy of KarXT + KarX-EC for the Treatment of Agitation Associated with Alzheimer’s Disease.

2025-520612-34-00 Protocol CN012-0024 Therapeutic confirmatory (Phase III) Ongoing, recruiting

Start 28 Nov 2025 · Status Ongoing, recruiting · 5 EU/EEA countries · 34 sites · Protocol CN012-0024

Overview

Sponsor-declared trial summary

Phase Therapeutic confirmatory (Phase III)
Status Ongoing, recruiting
Participants planned 354
Countries 5
Sites 34

Agitation Associated with Alzheimer’s Disease

To demonstrate the efficacy of KarXT + KarX-EC compared with placebo in the treatment of participants with agitation associated with AD as measured by the Cohen-Mansfield Agitation Inventory – International Psychogeriatric Association (CMAI-IPA) scale.

Key facts

Sponsor
Bristol-Myers Squibb Services Unlimited Company
Participant type
Patients
Age range
18-64 years, 65+ years
Gender
Male and Female
Therapeutic area
Psychiatry and Psychology [F] - Mental Disorders [F03]
Trial duration
28 Nov 2025 → ongoing
Decision date (initial)
2025-10-22
Transition trial
No
Low-intervention
No
Rare-disease indication
No
Vulnerable population
Yes

External identifiers

EU CT number
2025-520612-34-00
WHO UTN
U1111-1316-5827

Trial design

CTIS Part I — objectives, methods, condition coding

Main objective

Scope: Safety, Efficacy

To demonstrate the efficacy of KarXT + KarX-EC compared with placebo in
the treatment of participants with agitation associated with AD as measured by the
Cohen-Mansfield Agitation Inventory – International Psychogeriatric Association
(CMAI-IPA) scale.

Secondary objectives 1

  1. To demonstrate the efficacy of KarXT + KarX-EC compared with placebo in the treatment of participants with agitation associated with AD as measured by the Clinical Global Impressions – Severity (CGI-S) score.

Conditions and MedDRA coding

Agitation Associated with Alzheimer’s Disease

VersionLevelCodeTermSystem organ class
27.0 LLT 10066844 Behavioral and psychiatric symptoms of dementia 10037175
20.0 PT 10012271 Dementia Alzheimer's type 100000004852

Regulatory references

Scientific advice from competent authorities
Food And Drug Administration
Plan to share IPD
Yes
IPD plan description
BMS will provide access to individual anonymized participant data upon request from qualified researchers, and subject to certain criteria. Additional information regarding Bristol Myers Squibb's data sharing policy and process can be found at: https://www.bms.com/researchers-and-partners/clinical-trials-and-research/disclosure-commitment.html.

Eligibility criteria

Principal inclusion / exclusion criteria as submitted by sponsor

Inclusion criteria 7

  1. A diagnosis of Alzheimer’s disease (AD) in accordance with the 2024 Alzheimer’s Association criteria with one of the the following confirmations of AD pathology: - Historical evidence of AD diagnosis with amyloid positron emission tomography (PET), Aβ42/40 ratio in CSF, pTau181/Aβ42 ratio in CSF or pTau217/Aβ42 ratio in plasma using an Health Authority (HA)-authorized diagnostic assay. - If no historical evidence available: A. A plasma biomarker will be assessed for eligibility if allowed per regulatory requirements. The test cutoff(s) will be based on diagnostic use approval. B. If a plasma biomarker assay cannot be used or if the assay result is inconclusive, conduct one the following: o Amyloid PET o Aβ42/40 ratio or pTau181/Aβ42 ratio in CSF using an HA-authorized diagnostic assay
  2. Mini-Mental State Examination (MMSE) score of 5 to 22, inclusive, at Screening (Visit 1)
  3. Have one identified caregiver who should have sufficient contact (approximately 10 hours a week or more) and is willing to: - Attend all visits and report on participant’s status - Oversee participant compliance with medication and study procedures - Participate in the study assessments and provide IC to participate in the study
  4. History of agitation that meets the International Psychogeriatric Association (IPA) consensus definition for agitation in cognitive disorders with onset at least two weeks prior to Screening (Visit 1).
  5. AD participants are required to have NPI/NPI-NH Agitation/Aggression score ≥ 4 at Screening (Visit 1) and Baseline (Visit 4).
  6. CGI-S ≥ 4, as related to agitation, at Screening (Visit 1) and Baseline (Visit 4)
  7. At least 1 of the following 3 criteria must be established from the CMAI-IPA at Screening (Visit 1) and Baseline (Visit 4; CMAI-IPA Physical/Verbal Aggression Positivity): - 1 or more aggressive behaviors occurring several times per week - 2 or more aggressive behaviors occurring once or twice per week - 3 or more aggressive behaviors occurring less than once per week

Exclusion criteria 3

  1. Medical Conditions  Agitation symptoms that are primarily attributable to a condition other than the AD causing the dementia  History of bipolar disorder, schizophrenia, or schizoaffective disorder  History of (or at high risk for) urinary retention, gastric retention, or narrow-angle glaucoma as evaluated by the Investigator  Risk of suicidal behavior during the study as determined by the Investigator’s clinical assessment and/or C-SSR
  2. Prior/Concomitant Therapy - Recent history of receiving monoamine oxidase inhibitors, anticonvulsants (eg, lamotrigine, divalproex), mood stabilizers (eg, lithium), tricyclic antidepressants (eg, imipramine, desipramine), or any other psychoactive medications except for as needed anxiolytics (eg, lorazepam)  Selective serotonin reuptake inhibitors and serotonin norepinephrine reuptake inhibitors taken at a stable dose for at least 8 weeks prior to Screening (Visit 1) may be permitted  Mirtazapine or trazodone may be used as a hypnotic if started at least 8 weeks prior to Screening (Visit 1)
  3. Other protocol-defined Inclusion/Exclusion criteria apply.

Endpoints

Primary and secondary outcome measures (English text)

Primary endpoints 1

  1. Change from baseline to the end of treatment on the CMAI-IPA total score compared with placebo.

Secondary endpoints 1

  1. Change from baseline to the end of treatment on the CGI-S as it relates specifically to agitation compared with placebo.

Investigational products

Investigational medicinal products (IMPs), comparators, placebo, auxiliary

Test 8

KarX-EC

PRD12408423 · Product

Active substance
Xanomeline Tartrate
Substance synonyms
LY246708 tartrate, 3-(4-(Hexyloxy)-1,2,5-thiadiazol-3-yl)-1,2,5,6-tetrahydro-1-methylpyridine (-)-(+)-tartrate (1:1)
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarX-EC

PRD12408417 · Product

Active substance
Xanomeline Tartrate
Substance synonyms
LY246708 tartrate, 3-(4-(Hexyloxy)-1,2,5-thiadiazol-3-yl)-1,2,5,6-tetrahydro-1-methylpyridine (-)-(+)-tartrate (1:1)
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarX-EC

PRD12408422 · Product

Active substance
Xanomeline Tartrate
Substance synonyms
LY246708 tartrate, 3-(4-(Hexyloxy)-1,2,5-thiadiazol-3-yl)-1,2,5,6-tetrahydro-1-methylpyridine (-)-(+)-tartrate (1:1)
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarX-EC

PRD12408431 · Product

Active substance
Xanomeline Tartrate
Substance synonyms
LY246708 tartrate, 3-(4-(Hexyloxy)-1,2,5-thiadiazol-3-yl)-1,2,5,6-tetrahydro-1-methylpyridine (-)-(+)-tartrate (1:1)
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarXT

PRD12404386 · Product

Active substance
Trospium Chloride
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarXT

PRD12404368 · Product

Active substance
Trospium Chloride
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarXT

PRD12404394 · Product

Active substance
Trospium Chloride
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

KarXT

PRD12404377 · Product

Active substance
Trospium Chloride
Pharmaceutical form
CAPSULE
Route of administration
ORAL
Max daily dose
9999 mg milligram(s)
Max total dose
9999 mg milligram(s)
Max treatment duration
9999 Week(s)
Authorisation status
Not Authorised
MA holder
BRISTOL-MYERS SQUIBB INTERNATIONAL CORPORATION
Paediatric formulation
No
Orphan designation
No

Placebo 2

KarX-EC matching Placebo

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

KarXT matching placebo

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

Bristol-Myers Squibb Services Unlimited Company

87 Total trials 43 Recruiting 35 Ended
Commercial
Sponsor organisation
Bristol-Myers Squibb Services Unlimited Company
Address
Plaza 254, Blanchardstown Corporate Park 2 Blanchardstown Corporate Park 2
City
Dublin 15
Postcode
D15 T867
Country
Ireland

Scientific contact point

Organisation
Bristol-Myers Squibb Services Unlimited Company
Contact name
GSM-CT

Public contact point

Organisation
Bristol-Myers Squibb Services Unlimited Company
Contact name
GSM-CT

Third parties 7

OrganisationCity, countryDuties
Medidata Solutions Inc.
ORG-100016256
 New York, United States Other
Signant Health LLC
ORG-100040732
 Blue Bell, United States Other
Iqvia Holdings Inc.
ORG-100043905
 Durham, United States Other
Labcorp Central Laboratory Services SARL
ORG-100011524
 Meyrin, Switzerland Other, Laboratory analysis
Syneos Health Inc.
ORG-100008382
 Morrisville, United States Other
Greenphire LLC
ORG-100041621
 King Of Prussia, United States Other
Accenture Solutions Private Limited
ORG-100032592
 Bangaluru, India Other

Locations

5 EU/EEA countries · 34 investigational sites

By country

CountryMS statusPlanned subjectsSites
Czechia Ongoing, recruiting 21 7
France Ongoing, recruiting 17 7
Hungary Authorised, recruiting 14 7
Italy Ongoing, recruiting 20 7
Poland Ongoing, recruiting 20 6
Rest of world
Korea, Democratic People's Republic of, Argentina, Ukraine, United Kingdom, Israel, United States, Chile
 262

Investigational sites

Czechia

7 sites · Ongoing, recruiting
Neuropsychiatrie s.r.o.
N/A, Terronska 580/19, Bubenec, Prague 6
Vestra Clinics s.r.o.
N/A, Jiraskova 1389, 516 01, Rychnov Nad Kneznou
A-Shine s.r.o.
N/A, Sumavska 2, Vychodni Predmesti, Plzen 3
Neurohk s.r.o.
N/A, Smetanova 830, 565 01, Chocen
Neuro Health Centrum s.r.o.
NA, Hornikova 2485/34, Lisen, Brno-Lisen
INEP medical s.r.o.
N/A, Krizikova 264/22, Karlin, Prague
AGE Centrum s.r.o.
NA, Na Sibeniku 914/1 Nova Ulice, 779 00, Olomouc

France

7 sites · Ongoing, recruiting
Centre Hospitalier Universitaire De Toulouse
Gérontopole - Centre de Recherche Clinique (CRC), Place Lange, 31059, Toulouse Cedex 9
Hopital Fernand Widal
Centre de neurologie cognitive, 200 Rue Du Faubourg Saint Denis, 75010, Paris
Hopitaux Universitaires de Strasbourg - Hopital de la Robertsau
Centre Mémoire de Ressources et de Recherche (CMRR), 21 rue David Richard, 67000, Strasbourg
Hospices Civils de Lyon (HCL) - Hôpital des Charpennes
Centre de Recherche Clinique Vieillissement Cerveau Fragilité (CRC VCF), 27 rue Garbiel Peri, 69100, Villeurbanne
Centre Hospitalier Et Universitaire De Limoges
Hôpital Dupuytren - Service de médecine gériatrique, 2 Avenue Martin Luther King, 87042, Limoges Cedex 1
Centre Hospitalier Universitaire De Lille
Hopital Roger Salengro - Centre Mémoire de Ressources et de Recerches (CMRR), Avenue Du Professeur Emile Laine, 59037, Lille Cedex
Centre Hospitalier Universitaire De Montpellier
Hopital Gui de Chauliac - Centre Mémoire de Ressources et de Recerches (CMRR), 80 Avenue Augustin Fliche, 34295, Montpellier Cedex 5

Hungary

7 sites · Authorised, recruiting
Dr. Mathe Es Tarsa Bt.
N/A, Szechenyi Ut 8, 6300, Kalocsa
Gyoengyosi Bugat Pal Koerhaz
Pszichiatria, Dozsa Gyorgy Utca 20-22, 3200, Gyongyos
Semmelweis University
Neurológiai Klinika, Balassa J Utca 6, 1083, Budapest
University Of Debrecen
Neurologiai Klinika, Bartok Bela Ut 2-26, 4031, Debrecen
Clinexpert Kft.
N/A, Kaszasdulo Utca 5, 1033, Budapest III
Obudai Egeszseguegyi Centrum Kft.
N/A, Kodaly Zoltan Utca 8/ A, 2400, Dunaujvaros
Gyor-Moson-Sopron Varmegyei Petz Aladar Egyetemi Oktato Korhaz
Pszichiatriai, Mentalhigienes és Addiktologiai Osztaly, Vasvari Pal Utca 2-4, 9024, Gyor

Italy

7 sites · Ongoing, recruiting
Fondazione Policlinico Universitario Agostino Gemelli IRCCS
UOC Medicina Interna Geriatrica, Largo Francesco Vito 1, 00168, Rome
Azienda Socio Sanitaria Territoriale Degli Spedali Civili Di Brescia
S.C. Neurologia, Piazzale Spedali Civili 1, 25123, Brescia
Azienda Ospedaliero Universitaria Pisana
UO Psichiatria, Via Roma 67, 56126, Pisa
Azienda Ospedaliero-Universitaria Sant Andre
NESMOS, Via Di Grottarossa 1035-1039, 00189, Rome
Azienda Ospedaliera Universitaria Federico II Di Napoli
Neuroscience, Via Sergio Pansini 5, 80131, Naples
Istituto Auxologico Italiano
Neurology, Piazzale Brescia 20, 20149, Milan
Azienda Ospedaliero-Universitaria Policlinico Umberto I
Human Neuroscience, Viale Del Policlinico 155, 00161, Rome

Poland

6 sites · Ongoing, recruiting
Rcmed Oddzial Sochaczew
N/A, Aleja 600-Lecia 45, 96-500, Sochaczew
Niepubliczny Zaklad Opieki Zdrowotnej Neuromed M. I M. Nastaj. sp.p.
N/A, Ul. Polnocna 8/3, 20-064, Lublin
Centrum Medyczne Neuromed Sp. z o.o.
N/A, Ul. Jana Biziela 14, 85-163, Bydgoszcz
Centrum In Psyche Spersonalizowanej Psychiatrii i Terapii
N/A, ul. prof Jana Mikusińskiego 1/1, 40-146, Katowice
M2M Med. Sp. z o.o. Sp. j.
N/A, Ul. Lwowska 34, 41-500, Chorzow
Centrum Medyczne Hcp Sp. z o.o.
Oddział Udarowy i Neurologii, Ośrodek Badań Klinicznych, Ul. 28 Czerwca 1956 R. 194, 61-485, Poznan

Country notifications

Trial-start, recruitment-start, end and early-termination notifications submitted per Member State

Country Trial startTrial end Recruitment startRecruitment end Early termination
Czechia 2025-12-22 2026-02-23
France 2025-11-28 2025-12-19
Hungary 2026-05-27
Italy 2025-12-19 2026-03-16
Poland 2025-12-22 2026-01-28

Results and documents

Annex IV summary of results, Annex V layperson summary, and all documents registered in CTIS for this trial

Documents 59 files

Public protocol annexes, IB summaries, regulatory submissions and post-authorisation documents registered in CTIS.

TypeTitleVersion
Protocol (for publication) D1_Protocol 2025-520612-34_redacted PA 01
Protocol (for publication) D4_patient facing documents__statement_under license PL 1
Protocol (for publication) D4_Patient facing documents_Questionnaire_Statement for publication_IT na
Protocol (for publication) D4_Statement on validated questionnaires under licence_CZ N/A
Protocol (for publication) D4_Statement on validated questionnaires under licence_FR 1
Protocol (for publication) D4_Statement on validated questionnaires under license_ENG 1
Protocol (for publication) D4_Statement on validated questionnaires under license_HU 1
Recruitment arrangements (for publication) K1_Recruitment and Informed consent procedure template 1
Recruitment arrangements (for publication) K1_Recruitment arrangement Form_PL 2.0
Recruitment arrangements (for publication) K1_Recruitment arrangements_CZ 1.0
Recruitment arrangements (for publication) K1_Recruitment arrangements_FR 1.0
Recruitment arrangements (for publication) K1_Recruitment arrangements_IT final 1
Recruitment arrangements (for publication) K2_PI to Participant Letter_PL 1.0
Recruitment arrangements (for publication) K2_Recruitment material_PI to Patient Letter_IT 1
Recruitment arrangements (for publication) K2_Recruitment material_Poster_FR 1.0
Recruitment arrangements (for publication) K2_Recruitment material_Recruitment Poster_IT 1
Recruitment arrangements (for publication) K2_Recruitment material_Study Intro Trifold_FR 1.0
Recruitment arrangements (for publication) K2_Recruitment material_Study Intro Trifold_IT 1
Recruitment arrangements (for publication) K2_Study Intro Trifold_PL 1.0
Subject information and informed consent form (for publication) L1_ICF_Genetic_redacted 2
Subject information and informed consent form (for publication) L1_SIS and ICF Adult Assent_IT_Redatto 2
Subject information and informed consent form (for publication) L1_SIS and ICF Assent_FR_New patients_redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF ASSENT_FR_patients included_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF Assent_PL_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF Main_FR_New patients redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF Main_FR_patients included_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF Main_IT_Redatto 3
Subject information and informed consent form (for publication) L1_SIS and ICF Main_PL_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF Optional Future Research_FR 1.1
Subject information and informed consent form (for publication) L1_SIS and ICF Optional Future Research_PL 1.0
Subject information and informed consent form (for publication) L1_SIS and ICF Otional Future Research_IT_Redatto 1
Subject information and informed consent form (for publication) L1_SIS and ICF Pregnant participant_FR 1.0
Subject information and informed consent form (for publication) L1_SIS and ICF Privacy_IT_Redatto 1
Subject information and informed consent form (for publication) L1_SIS and ICF Reimbursement_IT_Redatto 1
Subject information and informed consent form (for publication) L1_SIS and ICF Study Partner_FR_redacted 1.1
Subject information and informed consent form (for publication) L1_SIS and ICF Study Partner_IT_Redatto 1
Subject information and informed consent form (for publication) L1_SIS and ICF Study Partner_PL_Redacted 1.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Adult Assent_Redacted 2
Subject information and informed consent form (for publication) L1_SIS and ICF_Assent_already enrolled participant_CZ_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Assent_new_participant_CZ_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Caregiver_CZ_Redacted 1.1
Subject information and informed consent form (for publication) L1_SIS and ICF_Main_already enrolled participant_CZ_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Main_new participant_CZ_Redacted 2.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Main_Redacted 2
Subject information and informed consent form (for publication) L1_SIS and ICF_Optional Future Research redacted 2
Subject information and informed consent form (for publication) L1_SIS and ICF_Optional Future Research_CZ 1.0
Subject information and informed consent form (for publication) L1_SIS and ICF_Participant Card 1
Subject information and informed consent form (for publication) L1_SIS and ICF_Study Partner_Redacted 1.2
Subject information and informed consent form (for publication) L1_SIS_Genetic_Redacted 2
Subject information and informed consent form (for publication) L2_Other subject information material_IOCBP_CZ 1.1
Subject information and informed consent form (for publication) L2_Other subject information material_Persona Data_CZ 1.0
Subject information and informed consent form (for publication) L2_Other subject information material_Study Participant Alert Card_FR_Redacted 1.0
Subject information and informed consent form (for publication) L3_SIS and ICF_Greephire ID log 1
Synopsis of the protocol (for publication) D1_Protocol synopsis 2025-520612-34_EN 05
Synopsis of the protocol (for publication) D1_Protocol synopsis 2025-520612-34_FR 5.0
Synopsis of the protocol (for publication) D1_Protocol synopsis 2025-520612-34_IT 5
Synopsis of the protocol (for publication) D1_Protocol synopsis_2025-520612-34_CZ 5
Synopsis of the protocol (for publication) D1_Protocol synopsis_2025-520612-34_HU 5.0
Synopsis of the protocol (for publication) D1_Protocol synopsis_2025-520612-34_PL 5.0

Application history

2 submissions — initial application plus substantial / non-substantial modifications

#TypeCodeSubmittedReference MSConclusionDecision date
1 INITIAL IN 2025-06-30 Poland Acceptable with conditions
2025-10-20
 2025-10-22
2 SUBSTANTIAL MODIFICATION SM-1 2025-12-22 Poland Acceptable
2026-03-07
 2026-03-09

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