A Structural Motif of Acetylcholinesterase That Promotes Amyloid β-Peptide Fibril Formation

Ferrari, Giancarlo V. De; Canales, Mauricio; Shin, Irina; Weiner, Lev; Silman, Israel; Inestrosa, Nibaldo C.

doi:10.1021/bi0101392

Cited by 388 publications

(296 citation statements)

References 47 publications

(76 reference statements)

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“…It is worthy of note that these moieties, although solvent exposed, lay in close proximity to P283 and F284 (Figure 2 bottom panels B−C), which have already been identified as relevant for binding Aβ. 8 This evidence is in line with the higher experimentally determined potency of 2b,c in inhibiting hAChE induced Aβ aggregation with respect to 2a. As shown in Figure 3, the peptidic aromatic groups of 2b,c may physically hamper Aβ binding to the surface of the enzyme.…”

Section: Introductionsupporting

confidence: 83%

Multifunctional Cholinesterase and Amyloid Beta Fibrillization Modulators. Synthesis and Biological Investigation

Butini¹,

Brindisi²,

Brogi³

et al. 2013

ACS Med. Chem. Lett.

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In order to identify novel Alzheimer's modifying pharmacological tools, we developed bis-tacrines bearing a peptide moiety for specific interference with surface sites of human acetylcholinesterase (hAChE) binding amyloid-beta (Aβ). Accordingly, compounds 2a−c proved to be inhibitors of hAChE catalytic and noncatalytic functions, binding the catalytic and peripheral sites, interfering with Aβ aggregation and with the Aβ self-oligomerization process (2a). Compounds 2a−c in complex with TcAChE span the gorge with the bis-tacrine system, and the peptide moieties bulge outside the gorge in proximity of the peripheral site. These moieties are likely responsible for the observed reduction of hAChE-induced Aβ aggregation since they physically hamper Aβ binding to the enzyme surface. Moreover, 2a was able to significantly interfere with Aβ self-oligomerization, while 2b,c showed improved inhibition of hAChE-induced Aβ aggregation.

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Section: Introductionsupporting

confidence: 83%

Multifunctional Cholinesterase and Amyloid Beta Fibrillization Modulators. Synthesis and Biological Investigation

Butini¹,

Brindisi²,

Brogi³

et al. 2013

ACS Med. Chem. Lett.

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“…[11][12][13][14][15] Multi-target compounds have been usually designed to hit at least Aβ formation and aggregation and AChE activity, 16 especially prompted by the finding that AChE can bind Aβ, thereby promoting its aggregation and increasing its neurotoxicity. [17][18][19] The recognition site of Aβ within AChE is the so-called peripheral anionic site (PAS) and it is located at the entrance of a 20 Å deep narrow gorge that leads to the catalytic anionic site (CAS). 20 The design of inhibitors able to simultaneously reach both sites of AChE, i.e.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and Multitarget Biological Profiling of a Novel Family of Rhein Derivatives As Disease-Modifying Anti-Alzheimer Agents

et al. 2014

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“…Some classes of AChE inhibitors, especially dual binding site inhibitors, are often endowed with Aβ anti-aggregating properties, 38 which arise either from blockade of the AChE peripheral anionic site (PAS) (blockade of AChE-induced Aβ aggregation) [39][40][41] or from a direct interaction with Aβ (blockade of spontaneous Aβ aggregation), in the latter case likely due to the presence of aromatic planar moieties in the inhibitors.…”

Section: Aβ42 and Tau Anti-aggregating Activitymentioning

confidence: 99%

Shogaol–huprine hybrids: Dual antioxidant and anticholinesterase agents with β-amyloid and tau anti-aggregating properties

Pérez-Areales

Pietro

Espargaró³

et al. 2014

Bioorganic & Medicinal Chemistry

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A Structural Motif of Acetylcholinesterase That Promotes Amyloid β-Peptide Fibril Formation

Cited by 388 publications

References 47 publications

Multifunctional Cholinesterase and Amyloid Beta Fibrillization Modulators. Synthesis and Biological Investigation

Multifunctional Cholinesterase and Amyloid Beta Fibrillization Modulators. Synthesis and Biological Investigation

Synthesis and Multitarget Biological Profiling of a Novel Family of Rhein Derivatives As Disease-Modifying Anti-Alzheimer Agents

Shogaol–huprine hybrids: Dual antioxidant and anticholinesterase agents with β-amyloid and tau anti-aggregating properties

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