Lysine-Specific Molecular Tweezers Are Broad-Spectrum Inhibitors of Assembly and Toxicity of Amyloid Proteins

Sinha, Sharmistha; Lopes, Dahabada H. J.; Du, Zhongtao; Pang, Eric; Shanmugam, Akila; Lomakin, Aleksey; Talbiersky, Peter; Tennstaedt, Annette; McDaniel, Kirsten; Bakshi, Reena; Kuo, Pei-Yi; Ehrmann, Michael; Benedek, George B.; Loo, Joseph A.; Klärner, Frank‐Gerrit; Schräder, Thomas; Wang, Chunyu; Bitan, Gal

doi:10.1021/ja206279b

Cited by 266 publications

(513 citation statements)

References 58 publications

(106 reference statements)

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“…Previously, we showed that CLR01 bound to Aβ40 at distinct sites, Lys16, Lys28, and to a low extent Arg5, 16 consistent with its putative mechanism of action. Because EGCG showed similar or stronger inhibitory effects, we asked whether it bound to similar sites on Aβ.…”

Section: ■ Results and Discussionsupporting

confidence: 72%

“…At low CLR01 concentrations, these changes occurred predominantly around the three cationic bindings sites, and as the concentration of CLR01 increased, gradually the entire spectrum was affected ( Figure 5B), likely due to Aβ selfassembly into nontoxic oligomers. 16 In contrast, only slight resonance perturbation was found in Aβ40:EGCG spectra at ratios up to 1:4 compared to Aβ40 alone ( Figure 5A and B). The resonances affected the most were in the regions Aβ(11− 15), Aβ(16−23), and Aβ(31−33), yet due to the low magnitude of the perturbation these data are difficult to interpret.…”

Section: ■ Results and Discussionmentioning

confidence: 84%

“…respectively, 16 only weak interaction of EGCG with Aβ40 monomers was observed at concentration ratios up to 1:4, respectively ( Figure 5). At this concentration ratio, the highest ratio studied, the maximum chemical shift induced by EGCG was ∼8 times smaller than the equivalent chemical shift changes in the Aβ40 spectrum in the presence of a similar concentration of CLR01 ( Figure 5B).…”

Section: ■ Results and Discussionmentioning

confidence: 95%

“…22 Relative to other inhibitors, most of which have been found empirically, the putative mechanism of action of CLR01 is quite well understood. CLR01 binds to Lys residues with micromolar affinity 16,23 and interferes with a combination of hydrophobic and electrostatic interactions that are important in the self-assembly of most amyloidogenic proteins, including Aβ 24−26 and tau. 27−30 This mode of action is a novel, processspecific mechanism plausibly applicable to most amyloidogenic proteins.…”

mentioning

confidence: 99%

“…Structural investigation using electron capture dissociation mass spectrometry and solution-state NMR has confirmed that CLR01 indeed binds to the two Lys residues and to a lesser extent to the single Arg residue, already in Aβ monomers. 16 Here, we asked how the activity of the artificial Lys-receptor, CLR01, which was explored as an inhibitor of amyloid proteins' assembly based on a mechanistic rationale, compared with those of the natural compounds, scyllo-inositol and EGCG. On the basis of the distinct structures of these three compounds (Figure 1), it is unlikely that they have a similar mode of interaction with Aβ.…”

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confidence: 99%

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Comparison of Three Amyloid Assembly Inhibitors: The Sugar scyllo-Inositol, the Polyphenol Epigallocatechin Gallate, and the Molecular Tweezer CLR01

Sinha

Maiti³

et al. 2012

ACS Chem. Neurosci.

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Many compounds have been tested as inhibitors or modulators of amyloid β-protein (Aβ) assembly in hope that they would lead to effective, disease-modifying therapy for Alzheimer's disease (AD). These compounds typically were either designed to break apart β-sheets or selected empirically. Two such compounds, the natural inositol derivative scyllo-inositol and the green-tea-derived flavonoid epigallocatechin gallate (EGCG), currently are in clinical trials. Similar to most of the compounds tested thus far, the mechanism of action of scyllo-inositol and EGCG is not understood. Recently, we discovered a novel family of assembly modulators, Lys-specific molecular tweezers, which act by binding specifically to Lys residues and modulate the selfassembly of amyloid proteins, including Aβ, into formation of nontoxic oligomers by a process-specific mechanism (Sinha, S., Lopes, D. H., Du, Z., Pang, E. S., Shanmugam, A., Lomakin, A., Talbiersky, P., Tennstaedt, A., McDaniel, K., Bakshi, R., Kuo, P. Y., Ehrmann, M., Benedek, G. B., Loo, J. A., Klarner, F. G., Schrader, T., Wang, C., and Bitan, G. (2011) Lysine-specific molecular tweezers are broad-spectrum inhibitors of assembly and toxicity of amyloid proteins. J. Am. Chem. Soc. 133, 16958−16969). Here, we compared side-by-side the capability of scyllo-inositol, EGCG, and the molecular tweezer CLR01 to inhibit Aβ aggregation and toxicity. We found that EGCG and CLR01 had comparable activity whereas scyllo-inositol was a weaker inhibitor. Exploration of the binding of EGCG and CLR01 to Aβ using heteronuclear solution-state NMR showed that whereas CLR01 bound to the two Lys and single Arg residues in Aβ monomers, only weak, nonspecific binding was detected for EGCG, leaving the binding mode of the latter unresolved.

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Section: ■ Results and Discussionsupporting

confidence: 72%

Section: ■ Results and Discussionmentioning

confidence: 84%

Section: ■ Results and Discussionmentioning

confidence: 95%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Comparison of Three Amyloid Assembly Inhibitors: The Sugar scyllo-Inositol, the Polyphenol Epigallocatechin Gallate, and the Molecular Tweezer CLR01

Sinha

Maiti³

et al. 2012

ACS Chem. Neurosci.

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131

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Intrinsically Disordered Proteins

Uversky

2020

Structural Biology in Drug Discovery

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Many functional proteins do not have well defined folded structures. In recent years, both experimental and computational approaches have been developed to study the conformational behaviour of this type of protein. It has been shown previously that experimental RDCs (residual dipolar couplings) can be used to study the backbone sampling of disordered proteins in some detail. In these studies, the backbone structure was modelled using a common geometry for all amino acids. In the present paper, we demonstrate that experimental RDCs are also sensitive to the specific geometry of each amino acid as defined by energyminimized internal coordinates. We have modified the FM (flexible-Meccano) algorithm that constructs conformational ensembles on the basis of a statistical coil model, to account for these differences. The modified algorithm inherits the advantages of the FM algorithm to efficiently sample the potential energy landscape for coil conformations. The specific geometries incorporated in the new algorithm result in a better reproduction of experimental RDCs and are generally applicable for further studies to characterize the conformational properties of intrinsically disordered proteins. In addition, the internal-coordinate based algorithm is an order of magnitude more efficient, and facilitates side-chain construction, surface osmolyte simulation, spin-label distribution sampling and proline cis/trans isomer simulation.

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Molecular Tweezers

2018

Molecular Devices

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Lysine-Specific Molecular Tweezers Are Broad-Spectrum Inhibitors of Assembly and Toxicity of Amyloid Proteins

Cited by 266 publications

References 58 publications

Comparison of Three Amyloid Assembly Inhibitors: The Sugar scyllo-Inositol, the Polyphenol Epigallocatechin Gallate, and the Molecular Tweezer CLR01

Comparison of Three Amyloid Assembly Inhibitors: The Sugar scyllo-Inositol, the Polyphenol Epigallocatechin Gallate, and the Molecular Tweezer CLR01

Intrinsically Disordered Proteins

Molecular Tweezers

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