Solvent Microenvironments and Copper Binding Alters the Conformation and Toxicity of a Prion Fragment

Inayathullah, Mohammed; Satheeshkumar, K. S.; Malkovskiy, Andrey V.; Carre, Antoine L.; Sivanesan, Senthilkumar; Hardesty, Jasper O.; Rajadas, Jayakumar

doi:10.1371/journal.pone.0085160

Cited by 8 publications

(4 citation statements)

References 89 publications

(103 reference statements)

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“…We also found that Zn 2+ and Cu 2+ significantly inhibited PrP106–126 oligomerization using the thioflavin T (ThT) fluorescence assay, far-ultraviolet circular dichroism (CD) spectroscopy, and atomic force microscopy (AFM) imaging. Although Cu 2+ and Zn 2+ reportedly facilitate the aggregation of AβP [ 91 ], our results coincide with other studies, which indicate that PrP-induced conformational changes and toxicity are attenuated by Cu [ 92 , 93 ]. Moreover, Cu 2+ reportedly inhibits the aggregation of human islet amyloid peptide (amylin) [ 94 ], Thus, it is highly possible that Cu 2+ exhibits complex effects on the oligomerization of amyloidogenic proteins.…”

Section: Toxic Functions Of Prp and Neurometalssupporting

confidence: 91%

Neurometals in the Pathogenesis of Prion Diseases

Kawahara

Kato-Negishi

Tanaka

2021

IJMS

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Prion diseases are progressive and transmissive neurodegenerative diseases. The conformational conversion of normal cellular prion protein (PrPC) into abnormal pathogenic prion protein (PrPSc) is critical for its infection and pathogenesis. PrPC possesses the ability to bind to various neurometals, including copper, zinc, iron, and manganese. Moreover, increasing evidence suggests that PrPC plays essential roles in the maintenance of homeostasis of these neurometals in the synapse. In addition, trace metals are critical determinants of the conformational change and toxicity of PrPC. Here, we review our studies and other new findings that inform the current understanding of the links between trace elements and physiological functions of PrPC and the neurotoxicity of PrPSc.

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Section: Toxic Functions Of Prp and Neurometalssupporting

confidence: 91%

Neurometals in the Pathogenesis of Prion Diseases

Kawahara

Kato-Negishi

Tanaka

2021

IJMS

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“…Solution conditions previously have been found to have significant effects on peptide conformations. For example, the prion protein, PrP has been found to adopt different conformations, specifically with respect to the proportions of α-helical and β-sheet structures, in aqueous solutions, in surfactant solutions, and following sonication . Similarly, secondary structure and aggregation of Aβ peptides has been found to be influenced by solvent conditions.…”

Section: Resultsmentioning

confidence: 99%

“…For example, the prion protein, PrP has been found to adopt different conformations, specifically with respect to the proportions of α-helical and β-sheet structures, in aqueous solutions, in surfactant solutions, and following sonication. 109 Similarly, secondary structure and aggregation of Aβ peptides has been found to be influenced by solvent conditions. In early studies by Shen and Murphy, Aβ(1−39) was not found to have any detectable β-sheet content in neat dimethyl sulfoxide (DMSO); however, in 0.1% trifluoroacetate the peptide contained approximately 1 / 3 β-sheet, and approximately 2 / 3 β-sheet in 35% acetonitrile/0.1% trifluoroacetate, which is thought to be most similar to the fibrillar form of the peptide under physiological conditions.…”

Section: Effect Of Solution Conditions On Cu(ii)mentioning

confidence: 99%

X-ray Absorption Spectroscopy Investigations of Copper(II) Coordination in the Human Amyloid β Peptide

et al. 2019

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Alzheimer’s disease (AD) is the main cause of age-related dementia and currently affects approximately 5.7 million Americans. Major brain changes associated with AD pathology include accumulation of amyloid beta (Aβ) protein fragments and formation of extracellular amyloid plaques. Redox-active metals mediate oligomerization of Aβ, and the resultant metal-bound oligomers have been implicated in the putative formation of harmful, reactive species that could contribute to observed oxidative damage. In isolated plaque cores, Cu(II) is bound to Aβ via histidine residues. Despite numerous structural studies of Cu(II) binding to synthetic Aβ in vitro, there is still uncertainty surrounding Cu(II) coordination in Aβ. In this study, we used X-ray absorption spectroscopy (XAS) and high energy resolution fluorescence detected (HERFD) XAS to investigate Cu(II) coordination in Aβ(1–42) under various solution conditions. We found that the average coordination environment in Cu(II)Aβ(1–42) is sensitive to X-ray photoreduction, changes in buffer composition, peptide concentration, and solution pH. Fitting of the extended X-ray absorption fine structure (EXAFS) suggests Cu(II) is bound in a mixture of coordination environments in monomeric Aβ(1–42) under all conditions studied. However, it was evident that on average only a single histidine residue coordinates Cu(II) in monomeric Aβ(1–42) at pH 6.1, in addition to 3 other oxygen or nitrogen ligands. Cu(II) coordination in Aβ(1–42) at pH 7.4 is similarly 4-coordinate with oxygen and nitrogen ligands, although an average of 2 histidine residues appear to coordinate at this pH. At pH 9.0, the average Cu(II) coordination environment in Aβ(1–42) appears to be 5-coordinate with oxygen and nitrogen ligands, including two histidine residues.

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“…39 It is well known that the hydrophobic 112-125 region of hPrP undergoes random coil to α-helix transition in the presence of membrane like environments (surfactant or lipid micelles) and structuring solvents. [43][44][45][46][47] Similarly to what happens to other amyloidogenic proteins, like Aβ and αS, this structural rearrangement strongly impacts Cu 2+ binding modes in terms of both donor atoms and affinity. 47,48 As we recently demonstrated, the interaction of hPrP91-127 with anionic micelles facilitates simultaneous copper coordination to both His96 and His111, which on the other hand behaves as separate metal anchoring sites in the absence of micelle environment.…”

Section: Introductionmentioning

confidence: 97%

The effect of a membrane-mimicking environment on the interactions of Cu²⁺with an amyloidogenic fragment of chicken prion protein

et al. 2017

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Prion proteins (PrP) from different species have the ability to tightly bind Cu ions. Copper coordination sites are located in the disordered and flexible N-terminal region which contains several His anchoring sites. Among them, two His residues are found in the so called amyloidogenic PrP region which is believed to play a key role in the process leading to oligomer and fibril formation. Both chicken and human amyloidogenic regions have a hydrophobic C-terminal region rich in Ala and Val amino acids. Recent findings revealed that this domain undergoes random coil to α-helix structuring upon interaction with membrane models. This interaction might strongly impact metal binding abilities either in terms of donor sets or affinity. In this study we investigated Cu interaction with an amyloidogenic fragment, chPrP105-140, derived from chicken prion protein (chPrP), in different solution environments. The behavior of the peptide and its metal complexes was analyzed in water and in the presence of negative and positive charged membrane mimicking environments formed by sodium dodecyl sulfate (SDS) and dodecyl trimethyl ammonium chloride (DTAC) micelles. The metal coordination sphere, the metal binding affinity and stoichiometry were evaluated by combining spectroscopic and potentiometric methods. Finally we compare copper(ii) interactions with human and chicken amyloidogenic fragments. Our results indicate that the chicken amyloidogenic fragment is a stronger copper ligand than the human amyloidogenic fragment.

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Solvent Microenvironments and Copper Binding Alters the Conformation and Toxicity of a Prion Fragment

Cited by 8 publications

References 89 publications

Neurometals in the Pathogenesis of Prion Diseases

Neurometals in the Pathogenesis of Prion Diseases

X-ray Absorption Spectroscopy Investigations of Copper(II) Coordination in the Human Amyloid β Peptide

The effect of a membrane-mimicking environment on the interactions of Cu²⁺with an amyloidogenic fragment of chicken prion protein

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Solvent Microenvironments and Copper Binding Alters the Conformation and Toxicity of a Prion Fragment

Cited by 8 publications

References 89 publications

Neurometals in the Pathogenesis of Prion Diseases

Neurometals in the Pathogenesis of Prion Diseases

X-ray Absorption Spectroscopy Investigations of Copper(II) Coordination in the Human Amyloid β Peptide

The effect of a membrane-mimicking environment on the interactions of Cu2+with an amyloidogenic fragment of chicken prion protein

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The effect of a membrane-mimicking environment on the interactions of Cu²⁺with an amyloidogenic fragment of chicken prion protein