2014
DOI: 10.1523/jneurosci.1405-14.2014
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Combined Treatment with a BACE Inhibitor and Anti-Aβ Antibody Gantenerumab Enhances Amyloid Reduction in APPLondonMice

Abstract: Therapeutic approaches for prevention or reduction of amyloidosis are currently a main objective in basic and clinical research on Alzheimer's disease. Among the agents explored in clinical trials are anti-A␤ peptide antibodies and secretase inhibitors. Most anti-A␤ antibodies are considered to act via inhibition of amyloidosis and enhanced clearance of existing amyloid, although secretase inhibitors reduce the de novo production of A␤. Limited information is currently available on the efficacy and potential a… Show more

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Cited by 86 publications
(61 citation statements)
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“…Preclinical data suggest combining therapeutics targeting the amyloid cascade (anti-Aβ and BACEi) significantly enhances reduction of amyloid load and plaque number beyond either monotherapy alone (66, 67). The existing and NexGen arms will be testing individual therapeutics that are a possible first combination (68-71), and the DIAN-TU trial platform’s multiple monotherapies and pooled placebo allow an opportunity to test combinations alongside monotherapy.…”
Section: Methods and Resultsmentioning
confidence: 99%
“…Preclinical data suggest combining therapeutics targeting the amyloid cascade (anti-Aβ and BACEi) significantly enhances reduction of amyloid load and plaque number beyond either monotherapy alone (66, 67). The existing and NexGen arms will be testing individual therapeutics that are a possible first combination (68-71), and the DIAN-TU trial platform’s multiple monotherapies and pooled placebo allow an opportunity to test combinations alongside monotherapy.…”
Section: Methods and Resultsmentioning
confidence: 99%
“…These combinations may be multiple mechanisms to lower Aβ burden, such as a BACE inhibitor to decrease the production of Aβ 1-42 monomer combined with an antibody that targets aggregated forms of Aβ. Recent animal studies suggest that these approaches might be synergistic in decreasing Aβ, and may have the added benefit in humans of allowing lower doses of each therapeutic to avoid treatment associated adverse events (Jacobsen et al, 2014). Ultimately, it would be ideal to combine anti-Aβ and anti-Tau treatments, particularly in early symptomatic patients.…”
Section: Introductionmentioning
confidence: 99%
“…For example, SCA type 1 (SCA1) is caused by ataxin-1 protein (ATXN1) with an abnormally expanded polyglutamine stretch and is characterized by neurodegeneration in a wide range of the central and the peripheral nervous systems (reviewed in [2]). Since amyloid fibrils are believed to be toxic forms, reduction of those fibrils is theoretically a major target for biochemical treatments against neurodegenerative disorders [3]. However, no effective drugs for polyglutamine diseases have been explored using biochemical approaches.…”
Section: Introductionmentioning
confidence: 99%