4.6 Article

A novel Alzheimer's disease drug candidate targeting inflammation and fatty acid metabolism

Journal

ALZHEIMERS RESEARCH & THERAPY
Volume 9, Issue -, Pages -

Publisher

BMC
DOI: 10.1186/s13195-017-0277-3

Keywords

Alzheimer's disease; Drug candidate; Gene expression; Metabolomics; Bioinformatics

Funding

  1. California Institute for Regenerative Medicine [PCI08086]
  2. National Institutes of Health (NIH) [R01 AG046153]
  3. NIH [R42AL104034, T32 AG000216]
  4. Templeton Foundation
  5. Bruce and Anne Bundy Foundation

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Background: CAD-31 is an Alzheimer's disease (AD) drug candidate that was selected on the basis of its ability to stimulate the replication of human embryonic stem cell-derived neural precursor cells as well as in APPswe/PS1 Delta E9 AD mice. To move CAD-31 toward the clinic, experiments were undertaken to determine its neuroprotective and pharmacological properties, as well as to assay its therapeutic efficacy in a rigorous mouse model of AD. Results: CAD-31 has potent neuroprotective properties in six distinct nerve cell assays that mimic toxicities observed in the old brain. Pharmacological and preliminary toxicological studies show that CAD-31 is brain-penetrant and likely safe. When fed to old, symptomatic APPswe/PS1 Delta E9 AD mice starting at 10 months of age for 3 additional months in a therapeutic model of the disease, there was a reduction in the memory deficit and brain inflammation, as well as an increase in the expression of synaptic proteins. Small-molecule metabolic data from the brain and plasma showed that the major effect of CAD-31 is centered on fatty acid metabolism and inflammation. Pathway analysis of gene expression data showed that CAD-31 had major effects on synapse formation and AD energy metabolic pathways. Conclusions: All of the multiple physiological effects of CAD-31 were favorable in the context of preventing some of the toxic events in old age-associated neurodegenerative diseases.

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