Tetrahydrofurobenzofuran cymserine, a potent butyrylcholinesterase inhibitor and experimental Alzheimer drug candidate, enzyme kinetic analysis

Kamal, MA; Qu, X; Yu, QS; Tweedie, D; Holloway, HW; Li, Y; Tan, Y; Greig, NH

Tetrahydrofurobenzofuran cymserine, a potent butyrylcholinesterase inhibitor and experimental Alzheimer drug candidate, enzyme kinetic analysis

Kamal, MA

Qu, X Yu, QS Tweedie, D Holloway, HW Li, Y Tan, Y

Greig, NH

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Publication Type:: Journal Article
Citation:: Journal of Neural Transmission, 2008, 115 (6), pp. 889 - 898
Issue Date:: 2008-06-01

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Field	Value	Language
dc.contributor.author	Kamal, MA https://orcid.org/0000-0003-0088-0565	en_US
dc.contributor.author	Qu, X	en_US
dc.contributor.author	Yu, QS	en_US
dc.contributor.author	Tweedie, D	en_US
dc.contributor.author	Holloway, HW	en_US
dc.contributor.author	Li, Y	en_US
dc.contributor.author	Tan, Y https://orcid.org/0000-0001-9221-330X	en_US
dc.contributor.author	Greig, NH	en_US
dc.date.available	2008-01-14	en_US
dc.date.issued	2008-06-01	en_US
dc.identifier.citation	Journal of Neural Transmission, 2008, 115 (6), pp. 889 - 898	en_US
dc.identifier.issn	0300-9564	en_US
dc.identifier.uri	http://hdl.handle.net/10453/9736
dc.description.abstract	Synaptic loss, particularly related to the forebrain cholinergic system, is considered to be an early event that leads to Alzheimer's disease (AD) and has led to the development of acetylcholinesterase inhibitors (AChE-Is) as the mainstay of treatment for several degenerative disorders that culminate in dementia. The primary dose-limiting toxicities of all clinically available AChE-Is are, similar to useful actions on cognition, cholinergically mediated and they ultimately limit the value of this drug class in achieving anything but symptomatic improvements. In addition, AChE levels in brain areas associated with AD decline with disease progression, which likely ultimately limits the therapeutic utility of this drug class. New research indicates that selective inhibition of butyrylcholinesterase (BuChE), a closely related enzyme that is markedly elevated in AD brain, increases acetylcholine (ACh) and augments cognition in rodents free of the characteristic undesirable actions of AChE-Is. BuChE inhibition hence represents an innovative treatment approach for AD, and agents are currently being synthesized to optimally achieve this. The novel compound, tetrahydrofurobenzofuran cymserine (THFBFC), is derived from our effort to produce a potent and BuChE-selective inhibitor as a candidate to test the hypothesis that BuChE-Is would be efficacious and better tolerated than AChE-Is in AD. Herein, we applied innovative enzyme kinetic analyses to characterize the quantitative interaction of THFBFC with human BuChE. These provided values for the agent's IC50, together with specific new kinetic constants, such as KT50, KT1/2, RI, oKRT, oPmax, KPT and PT1/2, to aid define target concentrations for clinical translation. Additional classical kinetic parameters, including Ki, Km or Ks, kcat or Vmax and Vmi were also determined. THFBFC proved to be a potent competitive inhibitor of human BuChE and, like its isomer dihydrobenzodioxepine cymserine, is a potentially interesting AD drug candidate. © 2008 Springer-Verlag.	en_US
dc.relation.ispartof	Journal of Neural Transmission	en_US
dc.relation.isbasedon	10.1007/s00702-008-0022-y	en_US
dc.subject.classification	Neurology & Neurosurgery	en_US
dc.subject.mesh	Serum	en_US
dc.subject.mesh	Humans	en_US
dc.subject.mesh	Alzheimer Disease	en_US
dc.subject.mesh	Physostigmine	en_US
dc.subject.mesh	Furans	en_US
dc.subject.mesh	Butyrylcholinesterase	en_US
dc.subject.mesh	Enzyme Inhibitors	en_US
dc.subject.mesh	Drug Evaluation, Preclinical	en_US
dc.subject.mesh	Binding, Competitive	en_US
dc.subject.mesh	Molecular Structure	en_US
dc.subject.mesh	Kinetics	en_US
dc.title	Tetrahydrofurobenzofuran cymserine, a potent butyrylcholinesterase inhibitor and experimental Alzheimer drug candidate, enzyme kinetic analysis	en_US
dc.type	Journal Article
utslib.citation.volume	6	en_US
utslib.citation.volume	115	en_US
utslib.for	1109 Neurosciences	en_US
utslib.for	1701 Psychology	en_US
dc.location.activity	ISI:000256472400014	en_US
pubs.embargo.period	Not known	en_US
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Faculty of Science/School of Life Sciences
pubs.organisational-group	/University of Technology Sydney/Strength - CHT - Health Technologies
utslib.copyright.status	closed_access
pubs.issue	6	en_US
pubs.publication-status	Published	en_US
pubs.volume	115	en_US

Abstract:

Synaptic loss, particularly related to the forebrain cholinergic system, is considered to be an early event that leads to Alzheimer's disease (AD) and has led to the development of acetylcholinesterase inhibitors (AChE-Is) as the mainstay of treatment for several degenerative disorders that culminate in dementia. The primary dose-limiting toxicities of all clinically available AChE-Is are, similar to useful actions on cognition, cholinergically mediated and they ultimately limit the value of this drug class in achieving anything but symptomatic improvements. In addition, AChE levels in brain areas associated with AD decline with disease progression, which likely ultimately limits the therapeutic utility of this drug class. New research indicates that selective inhibition of butyrylcholinesterase (BuChE), a closely related enzyme that is markedly elevated in AD brain, increases acetylcholine (ACh) and augments cognition in rodents free of the characteristic undesirable actions of AChE-Is. BuChE inhibition hence represents an innovative treatment approach for AD, and agents are currently being synthesized to optimally achieve this. The novel compound, tetrahydrofurobenzofuran cymserine (THFBFC), is derived from our effort to produce a potent and BuChE-selective inhibitor as a candidate to test the hypothesis that BuChE-Is would be efficacious and better tolerated than AChE-Is in AD. Herein, we applied innovative enzyme kinetic analyses to characterize the quantitative interaction of THFBFC with human BuChE. These provided values for the agent's IC50, together with specific new kinetic constants, such as KT50, KT1/2, RI, oKRT, oPmax, KPT and PT1/2, to aid define target concentrations for clinical translation. Additional classical kinetic parameters, including Ki, Km or Ks, kcat or Vmax and Vmi were also determined. THFBFC proved to be a potent competitive inhibitor of human BuChE and, like its isomer dihydrobenzodioxepine cymserine, is a potentially interesting AD drug candidate. © 2008 Springer-Verlag.

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