Inhibiting and Remodeling Toxic Amyloid-Beta Oligomer Formation Using a Computationally Designed Drug Molecule That Targets Alzheimer’s Disease

Matthew A. Downey; Maxwell J. Giammona; Christian A. Lang; Steven K. Buratto; Ambuj K. Singh; Michael T. Bowers

doi:https://doi.org/10.1007/s13361-018-1975-1

doi.org/10.1007/s13361-018-1975-1

Inhibiting and Remodeling Toxic Amyloid-Beta Oligomer Formation Using a Computationally Designed Drug Molecule That Targets Alzheimer’s Disease

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..., Michael T. Bowers

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Journal of the American Society for Mass Spectrometry3.20

Volume: 30, Issue: 1, Pages: 85 - 93

Published: Apr 30, 2018

Abstract

Alzheimer’s disease (AD) is rapidly reaching epidemic status among a burgeoning aging population. Much evidence suggests the toxicity of this amyloid disease is most influenced by the formation of soluble oligomeric forms of amyloid β-protein, particularly the 42-residue alloform (Aβ42). Developing potential therapeutics in a directed, streamlined approach to treating this disease is necessary. Here we utilize the joint pharmacophore space (JPS)...

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Paper Details

Title

Inhibiting and Remodeling Toxic Amyloid-Beta Oligomer Formation Using a Computationally Designed Drug Molecule That Targets Alzheimer’s Disease

DOI

doi.org/10.1007/s13361-018-1975-1

Published Date

Apr 30, 2018

Journal

Journal of the American Society for Mass Spectrometry

Volume

30

Issue

1

Pages

85 - 93

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