Amyloid beta (Aβ or Abeta) is a peptide of 36–43 amino acids that is processed from the Amyloid precursor protein. While best known as a component of amyloid plaques in association with Alzheimer's disease, evidence has been found that Aβ is a highly multifunctional peptide with significant non-pathological activity.[1] Aβ is the main component of deposits found in the brains of patients with Alzheimer's disease
Beta Amyloid~Identification of potential bivalent inhibitors from natural compounds for acetylcholinesterase through in silico screening using multiple pharmacophores.
The symptomatic cure observed in the treatment of Alzheimer's disease
(AD) by FDA approved drugs could possibly be due to their specificity
against the active site of acetylcholinesterase (AChE) and not by
targeting its pathogenicity. The AD pathogenicity involved in AChE
protein is mainly due to amyloid beta
peptide aggregation, which is triggered specifically by peripheral
anionic site (PAS) of AChE. In the present study, a workflow has been
developed for the identification and prioritization of potential
compounds that could interact not only with the catalytic site but also
with the PAS of AChE. To elucidate the essential structural elements of
such inhibitors, pharmacophore models were constructed using PHASE,
based on a set of fifteen best known AChE inhibitors. All these models
on validation were further restricted to the best seven. These were
transferred to PHASE database screening platform for screening 89,425
molecules deposited at the "ZINC natural product database". Novel lead
molecules retrieved were subsequently subjected to molecular docking and
ADME profiling. A set of 12 compounds were identified with high
pharmacophore fit values and good predicted biological activity scores.
These compounds not only showed higher affinity for catalytic residues,
but also for Trp86 and Trp286, which are important, at PAS of AChE. The
knowledge gained from this study, could lead to the discovery of
potential AChE inhibitors that are highly specific for AD treatment as
they are bivalent lead molecules endowed with dual binding ability for
both catalytic site and PAS of AChE
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