PMID- 35532913
OWN - NLM
STAT- MEDLINE
DCOM- 20220615
LR  - 20230510
IS  - 2168-6157 (Electronic)
IS  - 2168-6149 (Print)
IS  - 2168-6149 (Linking)
VI  - 79
IP  - 6
DP  - 2022 Jun 1
TI  - Safety, Tolerability, and Immunogenicity of the ACI-24 Vaccine in Adults With 
      Down Syndrome: A Phase 1b Randomized Clinical Trial.
PG  - 565-574
LID - 10.1001/jamaneurol.2022.0983 [doi]
AB  - IMPORTANCE: Individuals with Down syndrome (DS) are at high risk of developing 
      Alzheimer disease due to an increased dose of the amyloid precursor protein gene, 
      APP, which leads to increased levels of full-length APP and its products, 
      including amyloid-beta (Abeta). The liposome-based antiamyloid ACI-24 vaccine is 
      intended to treat neurological disorders caused by misfolded Abeta pathological 
      protein. However, the safety, tolerability, and immunogenicity of the ACI-24 
      vaccine among adults with DS have not been fully examined. OBJECTIVE: To assess 
      the safety and tolerability of the ACI-24 vaccine among adults with DS as well as 
      its ability to induce immunogenicity measured by anti-Abeta immunoglobulin G titers. 
      DESIGN, SETTING, AND PARTICIPANTS: This multicenter double-blind 
      placebo-controlled dose-escalation phase 1b randomized clinical trial was 
      conducted at 3 US academic medical centers with affiliated Down syndrome clinics 
      between March 30, 2016, and June 29, 2020. A total of 20 adults with DS were 
      screened; of those, 16 adults were eligible to participate. Eligibility criteria 
      included men or women aged 25 to 45 years with cytogenetic diagnosis of either 
      trisomy 21 or complete unbalanced translocation of chromosome 21. Between April 
      27, 2016, and July 2, 2018, participants were randomized 3:1 into 2 dose-level 
      cohorts (8 participants per cohort, with 6 participants receiving the ACI-24 
      vaccine and 2 receiving placebo) in a 96-week study. Participants received 48 
      weeks of treatment followed by an additional 48 weeks of safety follow-up. 
      INTERVENTIONS: Participants were randomized to receive 7 subcutaneous injections 
      of ACI-24, 300 mug or 1000 mug, or placebo. MAIN OUTCOMES AND MEASURES: Primary 
      outcomes were measures of safety and tolerability as well as antibody titers. 
      RESULTS: Among 16 enrolled participants, the mean (SD) age was 32.6 (4.4) years; 
      9 participants were women, and 7 were men. All participants were White, and 1 
      participant had Hispanic or Latino ethnicity. Treatment adherence was 100%. There 
      were no cases of meningoencephalitis, death, or other serious adverse events 
      (AEs) and no withdrawals as a result of AEs. Most treatment-emergent AEs were of 
      mild intensity (110 of 132 events [83.3%]) and unrelated or unlikely to be 
      related to the ACI-24 vaccine (113 of 132 events [85.6%]). No amyloid-related 
      imaging abnormalities with edema or cerebral microhemorrhage and no evidence of 
      central nervous system inflammation were observed on magnetic resonance imaging 
      scans. Increases in anti-Abeta immunoglobulin G titers were observed in 4 of 12 
      participants (33.3%) receiving ACI-24 (2 receiving 300 mug and 2 receiving 1000 
      mug) compared with 0 participants receiving placebo. In addition, a greater 
      increase was observed in plasma Abeta1-40 and Abeta1-42 levels among individuals 
      receiving ACI-24. CONCLUSIONS AND RELEVANCE: In this study, the ACI-24 vaccine 
      was safe and well tolerated in adults with DS. Evidence of immunogenicity along 
      with pharmacodynamic and target engagement were observed, and anti-Abeta antibody 
      titers were not associated with any adverse findings. These results support 
      progression to clinical trials using an optimized formulation of the ACI-24 
      vaccine among individuals with DS. TRIAL REGISTRATION: ClinicalTrials.gov 
      Identifier: NCT02738450.
FAU - Rafii, Michael S
AU  - Rafii MS
AD  - Alzheimer's Therapeutic Research Institute, Keck School of Medicine, University 
      of Southern California, San Diego, San Diego.
FAU - Sol, Olivier
AU  - Sol O
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Mobley, William C
AU  - Mobley WC
AD  - Department of Neuroscience, University of California, San Diego, San Diego.
FAU - Delpretti, Saskia
AU  - Delpretti S
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Skotko, Brian G
AU  - Skotko BG
AD  - Down Syndrome Program, Division of Medical Genetics and Metabolism, Department of 
      Pediatrics, Massachusetts General Hospital, Boston.
FAU - Burke, Anna D
AU  - Burke AD
AD  - Barrow Neurological Institute, Phoenix, Arizona.
FAU - Sabbagh, Marwan N
AU  - Sabbagh MN
AD  - Barrow Neurological Institute, Phoenix, Arizona.
FAU - Yuan, Shauna H
AU  - Yuan SH
AD  - Department of Neurology, University of Minnesota, Minneapolis.
FAU - Rissman, Robert A
AU  - Rissman RA
AD  - Department of Neuroscience, University of California, San Diego, San Diego.
FAU - Pulsifer, Margaret
AU  - Pulsifer M
AD  - Down Syndrome Program, Division of Medical Genetics and Metabolism, Department of 
      Pediatrics, Massachusetts General Hospital, Boston.
FAU - Evans, Casey
AU  - Evans C
AD  - Down Syndrome Program, Division of Medical Genetics and Metabolism, Department of 
      Pediatrics, Massachusetts General Hospital, Boston.
FAU - Evans, A Carol
AU  - Evans AC
AD  - Department of Neuroscience, University of California, San Diego, San Diego.
FAU - Beth, Gregory
AU  - Beth G
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Fournier, Nicolas
AU  - Fournier N
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Gray, Julian A
AU  - Gray JA
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Dos Santos, Antonio Melo
AU  - Dos Santos AM
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Hliva, Valerie
AU  - Hliva V
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Vukicevic, Marija
AU  - Vukicevic M
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Kosco-Vilbois, Marie
AU  - Kosco-Vilbois M
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Streffer, Johannes
AU  - Streffer J
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Pfeifer, Andrea
AU  - Pfeifer A
AD  - AC Immune SA, Lausanne, Switzerland.
FAU - Feldman, Howard H
AU  - Feldman HH
AD  - Department of Neuroscience, University of California, San Diego, San Diego.
AD  - Alzheimer's Disease Cooperative Study, University of California, San Diego, San 
      Diego.
LA  - eng
SI  - ClinicalTrials.gov/NCT02738450
GR  - RF1 AG073979/AG/NIA NIH HHS/United States
PT  - Clinical Trial, Phase I
PT  - Journal Article
PT  - Multicenter Study
PT  - Randomized Controlled Trial
PT  - Research Support, N.I.H., Extramural
PL  - United States
TA  - JAMA Neurol
JT  - JAMA neurology
JID - 101589536
RN  - 0 (Amyloid beta-Peptides)
RN  - 0 (Immunoglobulin G)
RN  - 0 (Vaccines)
SB  - IM
MH  - Adult
MH  - *Alzheimer Disease
MH  - Amyloid beta-Peptides
MH  - Double-Blind Method
MH  - *Down Syndrome
MH  - Female
MH  - Humans
MH  - Immunoglobulin G
MH  - Male
MH  - *Vaccines
PMC - PMC9086937
COIS- Conflict of Interest Disclosures: Dr Rafii reported receiving grants from the 
      National Institutes of Health (NIH) and personal fees from AC Immune during the 
      conduct of the study and personal fees from Alzheon and Keystone Bio outside the 
      submitted work. Dr Sol reported receiving personal fees from AC Immune outside 
      the submitted work. Dr Mobley reported receiving grants from AC Immune, the 
      LuMind IDSC Foundation, and the NIH and personal fees from AC Immune during the 
      conduct of the study; grants from AC Immune, Annovis Bio, and Samumed (now 
      Biosplice Therapeutics); personal fees from AC Immune, Alzheon, Annovis Bio, 
      Cortexyme, Pfizer, and Samumed (now Biosplice Therapeutics); serving as a board 
      member of ProMIS Neurosciences; owning stock options in CuraSen Therapeutics; and 
      owning a patent for a gamma secretase modulator (licensed to the University of 
      California, San Diego [UCSD]) outside the submitted work. Dr Delpretti reported 
      receiving grants from the LuMind IDSC Foundation and the NIH and personal fees 
      from AC Immune during the conduct of the study and receiving personal fees from 
      AC Immune outside the submitted work. Dr Skotko reported receiving grants from 
      UCSD during the conduct of the study; grants from F. Hoffmann-La Roche and the 
      LuMind IDSC Foundation; personal fees from the Gerson Lehrman Group; and 
      royalties from Woodbine House and serving on the honorary board of directors of 
      the Massachusetts Down Syndrome Congress and the professional advisory committee 
      of the National Center for Prenatal and Postnatal Down Syndrome Resources outside 
      the submitted work. Dr Sabbagh reported receiving personal fees from Biogen, 
      Cortexyme, Eisai Co, Eli Lilly and Company, Qynapse, Renew Research, Roche, and 
      T3D Therapeutics and owning stock in Alzheon, Athira Pharma, Cognoptix, and 
      uMethodHealth outside the submitted work. Dr Evans reported receiving grants from 
      the LuMind IDCS Foundation during the conduct of the study. Dr Beth reported 
      receiving grants from the LuMind IDCS Foundation and the NIH and personal fees 
      from AC Immune during the conduct of the study and receiving personal fees from 
      AC Immune outside the submitted work. Dr Fournier reported receiving grants from 
      the LuMind IDSC Foundation and the NIH and personal fees from AC Immune during 
      the conduct of the study and receiving personal fees from AC Immune outside the 
      submitted work. Dr Gray reported receiving grants from AC Immune, the LuMind IDSC 
      Foundation and the NIH and personal fees from AC Immune during the conduct of the 
      study and receiving personal fees from AC Immune outside the submitted work. Dr 
      Melo dos Santos reported receiving grants from the LuMind IDSC Foundation and the 
      NIH and personal fees from AC Immune during the conduct of the study and 
      receiving personal fees from AC Immune outside the submitted work. Dr Hliva 
      reported receiving grants from the LuMind IDSC Foundation and the NIH and 
      personal fees from AC Immune during the conduct of the study and receiving 
      personal fees from AC Immune outside the submitted work. Dr Vukicevic reported 
      receiving grants from the LuMind IDSC Foundation and the NIH and personal fees 
      from AC Immune during the conduct of the study and receiving personal fees from 
      AC Immune outside the submitted work. Dr Kosco-Vilbois reported receiving grants 
      from the LuMind IDSC Foundation and the NIH and personal fees from AC Immune 
      during the conduct of the study. Dr Streffer reported receiving grants from the 
      LuMind IDSC Foundation and the NIH and personal fees from AC Immune during the 
      conduct of the study and receiving personal fees from AC Immune outside the 
      submitted work. Dr Pfeifer reported receiving personal fees from AC Immune during 
      the conduct of the study and outside the submitted work. Dr Feldman reported 
      receiving grants from AC Immune and the NIH during the conduct of the study and 
      receiving grants from Annovis Bio, Biohaven Pharmaceutical Holding Company, the 
      LuMind IDSC Foundation, and Vivoryon Therapeutics and personal fees from the 
      World Events Forum and serving as a consultant for Arkuda Therapeutics, Axon 
      Neuroscience, Biosplice Therapeutics, Janssen Pharmaceuticals, Novo Nordisk, 
      Roche/Genentech, Samus Therapeutics, and the Tau Consortium outside the submitted 
      work. No other disclosures were reported.
EDAT- 2022/05/10 06:00
MHDA- 2022/06/16 06:00
PMCR- 2023/05/09
CRDT- 2022/05/09 11:33
PHST- 2022/05/10 06:00 [pubmed]
PHST- 2022/06/16 06:00 [medline]
PHST- 2022/05/09 11:33 [entrez]
PHST- 2023/05/09 00:00 [pmc-release]
AID - 2792226 [pii]
AID - noi220019 [pii]
AID - 10.1001/jamaneurol.2022.0983 [doi]
PST - ppublish
SO  - JAMA Neurol. 2022 Jun 1;79(6):565-574. doi: 10.1001/jamaneurol.2022.0983.