The Role of Glycation on the Aggregation Properties of IAPP

Milordini, Giulia; Zacco, Elsa; Percival, Matthew; Puglisi, Rita; Piaz, Fabrizio Dal; Temussi, Piero Andrea; Pastore, Annalisa

doi:10.3389/fmolb.2020.00104

Cited by 15 publications

(11 citation statements)

References 66 publications

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“…Interestingly, only 6% of the aggregates detected using Apt-1 were ThT-active, also at later time points, demonstrating the aptamer's ability to identify less mature oligomers that may be important in the disease pathology of TDP-43 and overcoming the limitations of current methods, such as the identification of oligomers of different size and structure. Other most commonly used approaches for the imaging and morphology studies of protein aggregates are transmission electron microscopy (TEM) 50 and atomic force microscopy (AFM) 51 . Both techniques provide qualitative and quantitative information at the nanometer level, but the former is limited in resolution and the latter requires long and complex sample preparation.…”

Section: Discussionmentioning

confidence: 99%

Probing TDP-43 condensation using an in silico designed aptamer

et al. 2022

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Aptamers are artificial oligonucleotides binding to specific molecular targets. They have a promising role in therapeutics and diagnostics but are often difficult to design. Here, we exploited the catRAPID algorithm to generate aptamers targeting TAR DNA-binding protein 43 (TDP-43), whose aggregation is associated with Amyotrophic Lateral Sclerosis. On the pathway to forming insoluble inclusions, TDP-43 adopts a heterogeneous population of assemblies, many smaller than the diffraction-limit of light. We demonstrated that our aptamers bind TDP-43 and used the tightest interactor, Apt-1, as a probe to visualize TDP-43 condensates with super-resolution microscopy. At a resolution of 10 nanometers, we tracked TDP-43 oligomers undetectable by standard approaches. In cells, Apt-1 interacts with both diffuse and condensed forms of TDP-43, indicating that Apt-1 can be exploited to follow TDP-43 phase transition. The de novo generation of aptamers and their use for microscopy opens a new page to study protein condensation.

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Section: Discussionmentioning

confidence: 99%

Probing TDP-43 condensation using an in silico designed aptamer

et al. 2022

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“…The kinetics of PHF6 (Ac-VQIVYK-NH 2 ) aggregation upon incubation with or without various concentrations of the inhibitors, NQ, DA, or NQDA (PHF6: inhibitor = 5 : 1, 1 : 1, and 1 : 5) was monitored by thioflavin S (ThS) fluorescence assay. Prior to the assay, PHF6 was monomerized by treating it with HFIP, a commonly used method to monomerize amyloidogenic proteins including Aβ 42 in AD and amylin polypeptide associated with diabetes type 2 [39,40]. The nature of the PHF6 monomers was verified immediately thereafter (at time zero) by CD (see below).…”

Section: Inhibition Of Phf6 Aggregation By Nqdamentioning

confidence: 99%

Inhibition of tau amyloid formation and disruption of its preformed fibrils by Naphthoquinone–Dopamine hybrid

et al. 2021

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Misfolding and aggregation of tau protein, into pathological amyloids, are hallmarks of a group of neurodegenerative diseases collectively termed tauopathies and their modulation may be therapeutically valuable. Herein, we describe the synthesis and characterization of a dopaminebased hybrid molecule, naphthoquinone-dopamine (NQDA). Using thioflavin S assay, CD, transmission electron microscopy, dynamic light scattering, Congo Red birefringence, and large unilamellar vesicle leakage assays, we demonstrated its efficacy in inhibiting the in vitro aggregation of key tau-derived amyloidogenic fragments, PHF6 (VQIVYK) and PHF6* (VQIINK), prime drivers of aggregation of full-length tau in disease pathology. Isothermal titration calorimetry analysis revealed that the interaction between NQDA and PHF6 is spontaneous and has significant binding efficiency driven by both entropic and enthalpic processes. Furthermore, NQDA efficiently disassembled preformed fibrils of PHF6 and PHF6* into nontoxic species. Molecular dynamic simulations supported the in vitro results and provided a plausible mode of binding of NQDA with PHF6 fibril. NQDA was also capable of inhibiting the aggregation of full-length tau protein and disrupting its preformed fibrils in vitro in a dose-dependent manner. In a comparative study, the IC 50 value (50% inhibition of fibril formation) of NQDA in inhibiting the aggregation of PHF6 (25 µM) was~17 µM, which is lower than for other bona fide amyloid inhibitors, naphthoquinone-tryptophan, rosmarinic acid, epigallocatechin gallate,~21,~77, or~19 µM, respectively. Comparable superiority of NQDA was observed for inhibition of PHF6*. These findings suggest that NQDA can be a useful scaffold for designing new therapeutics for Alzheimer's disease and other tauopathies.

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“…Moreover, the AGE-modified IAPP, such as normal IAPP, is able to interact with synthetic membranes and also to exhibit cytotoxicity [ 124 ]. Recently, glycation of IAPP has been studied in the presence of MGO as glycating agent [ 125 ]. In this study, MGO has been shown to efficiently react only with IAPP Lys1 inducing both a slowdown of the IAPP aggregation process and changes in the aggregate morphology [ 125 ].…”

Section: Glycation Role In Amyloid Aggregationmentioning

confidence: 99%

“…Recently, glycation of IAPP has been studied in the presence of MGO as glycating agent [ 125 ]. In this study, MGO has been shown to efficiently react only with IAPP Lys1 inducing both a slowdown of the IAPP aggregation process and changes in the aggregate morphology [ 125 ]. This study suggests that, although the only AGE-modified residue is Lys1 as in the CML-derived IAPP, differences in the AGEs produced and in the experimental conditions may play a key role in the dynamic effects induced by glycation on the aggregation process.…”

Section: Glycation Role In Amyloid Aggregationmentioning

confidence: 99%

Understanding the Role of Protein Glycation in the Amyloid Aggregation Process

Sirangelo

2021

IJMS

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Protein function and flexibility is directly related to the native distribution of its structural elements and any alteration in protein architecture leads to several abnormalities and accumulation of misfolded proteins. This phenomenon is associated with a range of increasingly common human disorders, including Alzheimer and Parkinson diseases, type II diabetes, and a number of systemic amyloidosis characterized by the accumulation of amyloid aggregates both in the extracellular space of tissues and as intracellular deposits. Post-translational modifications are known to have an active role in the in vivo amyloid aggregation as able to affect protein structure and dynamics. Among them, a key role seems to be played by non-enzymatic glycation, the most unwanted irreversible modification of the protein structure, which strongly affects long-living proteins throughout the body. This study provided an overview of the molecular effects induced by glycation on the amyloid aggregation process of several protein models associated with misfolding diseases. In particular, we analyzed the role of glycation on protein folding, kinetics of amyloid formation, and amyloid cytotoxicity in order to shed light on the role of this post-translational modification in the in vivo amyloid aggregation process.

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The Role of Glycation on the Aggregation Properties of IAPP

Cited by 15 publications

References 66 publications

Probing TDP-43 condensation using an in silico designed aptamer

Probing TDP-43 condensation using an in silico designed aptamer

Inhibition of tau amyloid formation and disruption of its preformed fibrils by Naphthoquinone–Dopamine hybrid

Understanding the Role of Protein Glycation in the Amyloid Aggregation Process

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