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Candidate anti-A beta fluorene compounds selected from analogs of amyloid imaging agents.


ABSTRACT: Alzheimer's disease (AD) is characterized by depositions of beta-amyloid (A beta) aggregates as amyloid in the brain. To facilitate diagnosis of AD by radioligand imaging, several highly specific small-molecule amyloid ligands have been developed. Because amyloid ligands display excellent pharmacokinetics properties and brain bioavailability, and because we have previously shown that some amyloid ligands bind the highly neurotoxic A beta oligomers (A beta O) with high affinities, they may also be valuable candidates for anti-A beta therapies. Here we identified two fluorene compounds from libraries of amyloid ligands, initially based on their ability to block cell death secondary to intracellular A beta O. We found that the lead fluorenes were able to reduce the amyloid burden including the levels of A beta O in cultured neurons and in 5xFAD mice. To explain these in vitro and in vivo effects, we found that the lead fluorenes bind and destabilize A beta O as shown by electron paramagnetic resonance spectroscopy studies, and block the harmful A beta O-synapse interaction. These fluorenes and future derivatives, therefore, have a potential use in AD therapy and research.

SUBMITTER: Hong HS 

PROVIDER: S-EPMC2888733 | biostudies-literature | 2010 Oct

REPOSITORIES: biostudies-literature

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Candidate anti-A beta fluorene compounds selected from analogs of amyloid imaging agents.

Hong Hyun-Seok HS   Maezawa Izumi I   Budamagunta Madhu M   Rana Sandeep S   Shi Aibin A   Vassar Robert R   Liu Ruiwu R   Lam Kit S KS   Cheng R Holland RH   Hua Duy H DH   Voss John C JC   Jin Lee-Way LW  

Neurobiology of aging 20081120 10


Alzheimer's disease (AD) is characterized by depositions of beta-amyloid (A beta) aggregates as amyloid in the brain. To facilitate diagnosis of AD by radioligand imaging, several highly specific small-molecule amyloid ligands have been developed. Because amyloid ligands display excellent pharmacokinetics properties and brain bioavailability, and because we have previously shown that some amyloid ligands bind the highly neurotoxic A beta oligomers (A beta O) with high affinities, they may also b  ...[more]

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