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JLK inhibitors: isocoumarin compounds as putative probes to selectively target the gamma-secretase pathway.

Frédéric Checler, Checler Frédéric,Cristine Alves da Costa, Alves da Costa Cristine,Erwan Ayral,Ayral Erwan,David Andrau,Andrau David, Cécile Dumanchin,Dumanchin Cécile,Michael Farzan, Farzan Michael, Jean-François Hernandez,Hernandez Jean-François, J Martinez,Solveig Lefranc-Jullien, Lefranc-Jullien Solveig,Philippe Marambaud, Marambaud Philippe, Andrea Pasini,Pasini Andrea, Agnès Petit,Petit Agnès,Christopher Phiel,Phiel Christopher, Philippe Robert,Robert Philippe,Peter St George-Hyslop,St George-Hyslop Peter, Sherwin Wilk,Wilk Sherwin

Current Alzheimer Research(2005)

Cited 12|Views6
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Abstract
Alzheimer's disease is characterized by the extracellular deposition of the amyloid beta-peptide that derives from its precursor betaAPP by sequential actions of beta- and gamma- secretases, respectively. Recent studies aimed at identifying these enzymes have been reported as it is thougth that their inhibition should hopefully lead to reduce Abeta load in the AD brains. beta-secretase seems to be due to BACE1, a novel membrane-bound aspartyl protease. gamma-secretase identification is still a matter of controversy. Invalidation of presenilin genes was reported to impair both gamma-secretase-mediated Abeta production and Notch cleavage leading to NICD production. This observation together with another biochemical and pharmacological evidences led to suggest that presenilins could be the genuine long-searched gamma-secretase that would be responsible for both APP and Notch cleavages. We have designed novel non peptidic potential inhibitors of gamma-secretase (referred to as JLK inhibitors) and examined their ability to prevent Abeta40 and Abeta42 secretions as well as NICD production. Three out of a series of these agents drastically lower the recoveries of both Abeta40 and Abeta42 produced by betaAPP-expressing cell lines and concomitantly protect intracellular C99 and C83 recoveries. These inhibitors also prevent Abeta40/42 productions by C99-expressing cells. Interestingly, these inhibitors were totally unable to affect the DeltaENotch cleavage leading to NICD generation. Here, we also further characterize the pharmacological properties and specificity of these JLK inhibitors.
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Key words
isocoumarin compounds,g-secretase
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