&lt;p&gt;Review on the Structures and Activities of Transthyretin Amyloidogenesis Inhibitors&lt;/p&gt;

Guo, Xiaohua; Liu, Zhaowen; Zheng, Yizhou; Li, Yamei; Li, Linfu; Liu, Hai; Chen, Zhixi; Wu, Longhuo

doi:10.2147/dddt.s237252

Cited by 17 publications

(10 citation statements)

References 114 publications

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“…Currently, more than 400 crystallographic structures of TTR are deposited in the Protein Data Bank ( ) [ 17 ], most of them in complex with small-molecule ligands. This comprehensive work has allowed a full characterization of the TTR binding sites [ 18 , 19 , 20 ]. A relevant feature of these sites is the presence of three sets of symmetry-related depressions termed halogen-binding pockets (HBPs: HBP1 and HBP1’, HBP2 and HBP2’ and HBP3 and HBP3’), which accommodate the iodine atoms of the thyroid hormones in their complexes with TTR [ 21 ].…”

Section: Introductionmentioning

confidence: 99%

Repurposing Benzbromarone for Familial Amyloid Polyneuropathy: A New Transthyretin Tetramer Stabilizer

Cotrina¹,

Oliveira

Leite

et al. 2020

IJMS

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Transthyretin (TTR) is a homotetrameric protein involved in human amyloidosis, including familial amyloid polyneuropathy (FAP). Discovering small-molecule stabilizers of the TTR tetramer is a therapeutic strategy for these diseases. Tafamidis, the only approved drug for FAP treatment, is not effective for all patients. Herein, we discovered that benzbromarone (BBM), a uricosuric drug, is an effective TTR stabilizer and inhibitor against TTR amyloid fibril formation. BBM rendered TTR more resistant to urea denaturation, similarly to iododiflunisal (IDIF), a very potent TTR stabilizer. BBM competes with thyroxine for binding in the TTR central channel, with an IC50 similar to IDIF and tafamidis. Results obtained by isothermal titration calorimetry (ITC) demonstrated that BBM binds TTR with an affinity similar to IDIF, tolcapone and tafamidis, confirming BBM as a potent binder of TTR. The crystal structure of the BBM-TTR complex shows two molecules binding deeply in the thyroxine binding channel, forming strong intermonomer hydrogen bonds and increasing the stability of the TTR tetramer. Finally, kinetic analysis of the ability of BBM to inhibit TTR fibrillogenesis at acidic pH and comparison with other stabilizers revealed that benzbromarone is a potent inhibitor of TTR amyloidogenesis, adding a new interesting scaffold for drug design of TTR stabilizers.

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Section: Introductionmentioning

confidence: 99%

Repurposing Benzbromarone for Familial Amyloid Polyneuropathy: A New Transthyretin Tetramer Stabilizer

Cotrina¹,

Oliveira

Leite

et al. 2020

IJMS

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“…Familial amyloid polyneuropathy (FAP) is another TTR amyloidosis and is usually associate to Val30Met point mutation [106]. One therapeutic strategy against TTR amyloidosis is the tetramer stabilization by small molecules such as bisaryl [109,110] or monoaryl [111][112][113] structure-based compounds or natural molecules [114,115].…”

Section: Transthyretin (Ttr)mentioning

confidence: 99%

The Positive Side of the Alzheimer’s Disease Amyloid Cross-Interactions: The Case of the Aβ 1-42 Peptide with Tau, TTR, CysC, and ApoA1

et al. 2020

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Alzheimer’s disease (AD) represents a progressive amyloidogenic disorder whose advancement is widely recognized to be connected to amyloid-β peptides and Tau aggregation. However, several other processes likely contribute to the development of AD and some of them might be related to protein-protein interactions. Amyloid aggregates usually contain not only single type of amyloid protein, but also other type of proteins and this phenomenon can be rationally explained by the process of protein cross-seeding and co-assembly. Amyloid cross-interaction is ubiquitous in amyloid fibril formation and so a better knowledge of the amyloid interactome could help to further understand the mechanisms of amyloid related diseases. In this review, we discuss about the cross-interactions of amyloid-β peptides, and in particular Aβ1-42, with other amyloids, which have been presented either as integrated part of Aβ neurotoxicity process (such as Tau) or conversely with a preventive role in AD pathogenesis by directly binding to Aβ (such as transthyretin, cystatin C and apolipoprotein A1). Particularly, we will focus on all the possible therapeutic strategies aiming to rescue the Aβ toxicity by taking inspiration from these protein-protein interactions.

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“…Therefore, in the present paper, we review the previous studies of various inhibitors acting on different proteins in light of the molecular mechanism of action and kinetics of aggregation. A number of other reviews have also been published focusing on the various aspects of fibril formation inhibition, namely on the diversity of the chemical structure of inhibitors [ 3 , 21 , 22 ], on polymer materials showing inhibitory activity [ 17 , 23 ], on peptide-based inhibitors [ 24 ], or particularly on human beta-amyloid inhibitors and treatment strategies of Alzheimer’s disease [ 25 , 26 , 27 ] and transthyretin amyloidogenesis inhibitors [ 28 ].…”

Section: Introductionmentioning

confidence: 99%

Molecular Mechanisms of Inhibition of Protein Amyloid Fibril Formation: Evidence and Perspectives Based on Kinetic Models

Sedov

Khaibrakhmanova

2022

IJMS

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Inhibition of fibril formation is considered a possible treatment strategy for amyloid-related diseases. Understanding the molecular nature of inhibitor action is crucial for the design of drug candidates. In the present review, we describe the common kinetic models of fibril formation and classify known inhibitors by the mechanism of their interactions with the aggregating protein and its oligomers. This mechanism determines the step or steps of the aggregation process that become inhibited and the observed changes in kinetics and equilibrium of fibril formation. The results of numerous studies indicate that possible approaches to antiamyloid inhibitor discovery include the search for the strong binders of protein monomers, cappers blocking the ends of the growing fibril, or the species absorbing on the surface of oligomers preventing nucleation. Strongly binding inhibitors stabilizing the native state can be promising for the structured proteins while designing the drug candidates targeting disordered proteins is challenging.

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<p>Review on the Structures and Activities of Transthyretin Amyloidogenesis Inhibitors</p>

Cited by 17 publications

References 114 publications

Repurposing Benzbromarone for Familial Amyloid Polyneuropathy: A New Transthyretin Tetramer Stabilizer

Repurposing Benzbromarone for Familial Amyloid Polyneuropathy: A New Transthyretin Tetramer Stabilizer

The Positive Side of the Alzheimer’s Disease Amyloid Cross-Interactions: The Case of the Aβ 1-42 Peptide with Tau, TTR, CysC, and ApoA1

Molecular Mechanisms of Inhibition of Protein Amyloid Fibril Formation: Evidence and Perspectives Based on Kinetic Models

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