Bhaskara Sreenivas scite author profile

The development of polyphenols as drugs for Alzheimer's disease (AD) is thwarted by their meagre brain availability due to instability and poor druglikeness. Here we describe the successful development of stable, druglike polyphenolic analogues of the current AD drug rivastigmine, that have high apparent blood-brain barrier permeabilities and multifunctional properties for AD treatment. The compounds inhibit cholinesterases and amyloid beta (Aβ) fibrillation, protect against Aβ 42-induced toxicity in vitro, and demonstrate efficacy in vivo in a transgenic Caenorhabditis elegans model expressing Aβ 42 , with potencies similar to rivastigmine and natural polyphenols. The results suggest that a tertiary amine substituent is amenable for developing water-soluble, membrane-permeable polyphenols, and its incorporation adjacent to a hydroxy group is favourable for intramolecular hydrogen bonding that facilitates membrane permeability. Carbamylation of one hydroxy group protects the polyphenols from degradation and mostly improves their membrane permeability. These design strategies may assist in the development of polyphenol-based drugs.

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Latent Variate Factorial Principal Component Analysis of Microelectrode Recording of Subthalamic Nuclei Neural Signals with Deep Brain Stimulator in Parkinson Disease

Raju

Lavanya

Sreenivas

2018

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Discovery of drug‐like acetylcholinesterase inhibitors by rapid virtual screening of a 6.9 million compound database

Miles

Sreenivas

et al. 2021

Chem Biol Drug Des

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Cholinesterase inhibitors remain the mainstay of Alzheimer's disease treatment, and the search for new inhibitors with better efficacy and side effect profiles is ongoing. Virtual screening (VS) is a powerful technique for searching large compound databases for potential hits. This study used a sequential VS workflow combining ligand‐based VS, molecular docking and physicochemical filtering to screen for central nervous system (CNS) drug‐like acetylcholinesterase inhibitors (AChEIs) amongst the 6.9 million compounds of the CoCoCo database. Eleven in silico hits were initially selected, resulting in the discovery of an AChEI with a Ki of 3.2 µM. In vitro kinetics and in silico molecular dynamics experiments informed the selection of an additional seven analogues. This led to the discovery of two further AChEIs, with Ki values of 2.9 µM and 0.65 µM. All three compounds exhibited reversible, mixed inhibition of acetylcholinesterase. Importantly, the in silico physicochemical filter facilitated the discovery of CNS drug‐like compounds, such that all three inhibitors displayed high in vitro blood‐brain barrier model permeability.

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Miles¹,

Ng²,

Sreenivas³

et al. 2021

Chem Biol Drug Des

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Design of robust image watermarking technique based on shearlet transform and QR matrix decomposition

Subramani

Narayanan²,

Kamalanathan

et al. 2020

Journal of Interdisciplinary Mathematics

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