Publication Type Journal Article
Title Tacrine-allyl/propargylcysteine-benzothiazole trihybrids as potential anti-Alzheimer s drug candidates
Authors Asha Hiremathad Karam Chand A. Raquel Esteves Sandra M. Cardoso Rona R. Ramsay Sílvia Chaves Rangappa S. Keri M. Amélia Santos
Groups BIOIN
Journal RSC ADVANCES
Year 2016
Month
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Volume 6
Number 58
Pages 53519-53532
Abstract On continuing our research into new drug candidates for Alzheimer s disease (AD), we have designed, synthesized and evaluated a series of multifunctional trihybrid agents. The design strategy was based on the incorporation of a benzothiazole (BTA) moiety on a series of very recently reported bihybrids, resulting from the conjugation of a tacrine (TAC) with natural based moieties, namely S-allylcysteine (SAC) (garlic constituent) and S-propargylcysteine (SPRC). Thus, in addition to the acetylcholinesterase inhibition (AChEI) and anti-ROS capacity of the bihybrids (TAC-SAC/SPRC), the new trihybrids (TACSAC/ SPRC-BTA) appeared endowed with a 5-fold capacity for inhibition of amyloid beta-peptide (Ab) aggregation. The BTA moiety led also to considerable enhancement of the AChEI on the trihybrids, which molecular modeling suggested as being due to simultaneous binding to the catalytic active site and peripheral anionic site of AChE. The trihybrids were also assessed for MAO inhibition, but resulted in lower activity than expected, ascribed to the low accessibility of the propargyl groups to the enzyme active site. Finally, the effects of the compounds on the viability of neuroblastome cells stressed with A beta(42) and H2O2 showed moderate cell protection. Overall, the performed studies illustrate the importance (and limitations) of enclosing several molecular scaffolds in one molecular entity to allow the modulation of multiple AD targets.
DOI http://dx.doi.org/10.1039/c6ra03455a
ISBN
Publisher ROYAL SOC CHEMISTRY
Book Title
ISSN 2046-2069
EISSN
Conference Name
Bibtex ID ISI:000378563200116
Observations
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