Sara Linse
Professor
Kinetic fingerprints differentiate the mechanisms of action of anti-Aβ antibodies
Author
Summary, in English
The amyloid cascade hypothesis, according to which the self-assembly of amyloid-β peptide (Aβ) is a causative process in Alzheimer’s disease, has driven many therapeutic efforts for the past 20 years. Failures of clinical trials investigating Aβ-targeted therapies have been interpreted as evidence against this hypothesis, irrespective of the characteristics and mechanisms of action of the therapeutic agents, which are highly challenging to assess. Here, we combine kinetic analyses with quantitative binding measurements to address the mechanism of action of four clinical stage anti-Aβ antibodies, aducanumab, gantenerumab, bapineuzumab and solanezumab. We quantify the influence of these antibodies on the aggregation kinetics and on the production of oligomeric aggregates and link these effects to the affinity and stoichiometry of each antibody for monomeric and fibrillar forms of Aβ. Our results reveal that, uniquely among these four antibodies, aducanumab dramatically reduces the flux of Aβ oligomers.
Department/s
- Biochemistry and Structural Biology
- Clinical Memory Research
- MultiPark: Multidisciplinary research focused on Parkinson´s disease
Publishing year
2020-12
Language
English
Pages
1125-1133
Publication/Series
Nature Structural and Molecular Biology
Volume
27
Issue
12
Document type
Journal article
Publisher
Nature Publishing Group
Topic
- Clinical Laboratory Medicine
Status
Published
Research group
- Clinical Memory Research
ISBN/ISSN/Other
- ISSN: 1545-9993