Drug discovery for Alzheimer's disease targeting the transmembrane domain of amyloid precursor protein (AAPTM).

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Authors
Eden, Angela Bailey
Issue Date
2022-08
Type
Electronic thesis
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en_US
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Chemistry
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Abstract
Alzheimer’s Disease (AD) is a neurological disease currently affecting close to 6 million Americans (3). A major neuropathological hallmark of AD is the presence of senile plaques in the cerebral cortex and hippocampus (3). Senile plaques (amyloid plaques) are mainly composed of extracellular aggregates of amyloid β-peptides (Aβs); it has been hypothesized that Aβ deposition initiates a pathological cascade resulting in cognitive decline characteristic of AD (9-11). γ-secretase (GS) cleaves amyloid precursor protein (APP) in its transmembrane domain generating Aβ40 and Aβ42 that aggregate into the insoluble aggregates of senile plaques (5,11). GS has been a target of anti-AD drug discovery projects with limited success (23-25). Two broad spectrum GS inhibitors (GSIs), avagacestat and semagacestat, failed due to worsening cognition in patients in addition to other serious adverse effects largely attributable to the 90 endogenous substrates of GS (23-25). Despite GSIs’ failure, there is compelling evidence that Aβ is a causative agent in AD, including but not limited to: human genetics of familial AD (FAD) (12-14) and Down’s syndrome (30-31). To circumvent issues from GS inhibition we aimed to target the GS substrate in the amyloidogenic pathway, the transmembrane domain of APP (APPTM). Multiple screening methods resulted in two different binders of APPTM that inhibited APPTM cleavage by GS or presenilin homolog (PSH), 6H8 and N1. 6H8, a covalent modifier of APPTM found in a fragment library, modifies C-terminal lysines in APPTM via a Michael addition mechanism. While N1, a non-covalent modifier found by DNA encoded library screen, binds to APPTM though both hydrophobic and electrostatic interactions. 6H8 and N1 inhibit cleavage of APPTM with IC50 values in the low micromolar and tens of nanomolar ranges, respectively. 6H8 may be engineered into a targeted covalent inhibitor while N1, with nanomolar efficacy, is a promising lead compound for lowering amyloid load for managing AD.
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August 2022
School of Science
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Rensselaer Polytechnic Institute, Troy, NY
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