Thioflavin T Hydroxylation at Basic pH and Its Effect on Amyloid Fibril Detection

Foderà, Vito; Groenning, Minna; Vetri, Valeria; Librizzi, Fabio; Spagnolo, S.; Cornett, Claus; Olsen, Lars; Weert, Marco van de; Leone, Maurizio

doi:10.1021/jp805560c

Cited by 108 publications

(108 citation statements)

References 54 publications

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“…Accordingly, it has been shown that the in vitro fibrillation of apoSOD1 displays the characteristic fingerprint of fragmentation-assisted growth (15) with a square root dependence on [D] (7), consistent with the requirement of sample agitation to expedite the reaction (1)(2)(3)(4)10). Analogous fibrillation behavior is found for β2-microglobulin (2), yeast prions Sup35 (16) and Ure2p (17), insulin (18), WW domain (19), TI 127 (20), and α-synuclein (21). The main difference between these proteins seems to be that some are intrinsically disordered and constantly aggregation-competent by lacking the ability to hide sticky sequence material by folding.…”

mentioning

confidence: 63%

“…Growth seems, thus, controlled by the generic mechanical properties of the fibrils themselves rather than by their precise structural composition or environmental location. Fragmentation control is accordingly observed as a general feature on stirring, shaking, or sonication in vitro and for a variety of proteins (2,16,17,19,20) and peptides (18,21,29,30) with little or no sequence similarities. The corresponding source of mechanical stress in vivo (26) could be vascular pounding, cytoskeleton dynamics, spatial restriction of linear growth, or even chaperones in the disaggregation machinery (34).…”

Section: Discussionmentioning

confidence: 99%

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SOD1 aggregation in ALS mice shows simplistic test tube behavior

Lang

Zetterström

Brännström

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

123

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A longstanding challenge in studies of neurodegenerative disease has been that the pathologic protein aggregates in live tissue are not amenable to structural and kinetic analysis by conventional methods. The situation is put in focus by the current progress in demarcating protein aggregation in vitro, exposing new mechanistic details that are now calling for quantitative in vivo comparison. In this study, we bridge this gap by presenting a direct comparison of the aggregation kinetics of the ALS-associated protein superoxide dismutase 1 (SOD1) in vitro and in transgenic mice. The results based on tissue sampling by quantitative antibody assays show that the SOD1 fibrillation kinetics in vitro mirror with remarkable accuracy the spinal cord aggregate buildup and disease progression in transgenic mice. This similarity between in vitro and in vivo data suggests that, despite the complexity of live tissue, SOD1 aggregation follows robust and simplistic rules, providing new mechanistic insights into the ALS pathology and organism-level manifestation of protein aggregation phenomena in general.superoxide dismutase 1 | aggregation | transgenic mice | aggregation kinetics

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mentioning

confidence: 63%

Section: Discussionmentioning

confidence: 99%

SOD1 aggregation in ALS mice shows simplistic test tube behavior

Lang

Zetterström

Brännström

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

123

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“…This hydroxylation can in some cases explain the linear decrease in ThT intensity that is frequently seen after the elongation phase has ended ( Figure 5(B)). While hydroxylation is accelerated by elevated temperatures and basic conditions, it should not be discounted at neutral pH and 37 C: 15 h of incubation at 50 C reduces ThT absorbance by $25% and this is attributed to hydroxylation [95]. Alternatively, fibrillation under extreme conditions, which affect ThT emission properties can be examined using fixed time point assays, where the protein is incubated under extreme conditions and aliquots are withdrawn at fixed time points and diluted into ThTcompatible measuring conditions [96], see following section for more explanation.…”

Section: Extreme Ph Affects Thtmentioning

confidence: 99%

ThT 101: a primer on the use of thioflavin T to investigate amyloid formation

Malmos

Blancas‐Mejia

Weber

et al. 2017

Amyloid

322

243

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Thioflavin T (ThT) has been widely used to investigate amyloid formation since 1989. While concerns have recently been raised about its use as a probe specific for amyloid, ThT still continues to be a very valuable tool for studying kinetic aspects of fibrillation and associated inhibition mechanisms. This review aims to provide a conceptual instruction manual, covering appropriate considerations and pitfalls related to the use of ThT. We start by giving a brief introduction to amyloid formation with focus on the morphology of different aggregate species, followed by a discussion of the quality of protein needed to obtain reliable fibrillation data. After an overview of the photochemical basis for ThT's amyloid binding properties and artifacts that may arise from this, we describe how to plan and analyze ThT assays. We conclude with recommendations for complementary techniques to address shortcomings in the ThT assay.

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“…In contrast to previous studies (Foderà et al 2008), the free base amino acids l-arginine (Arg) or l-lysine (Lys) were used to raise the solution pH. In the control experiments, l-arginine hydrochloride and l-lysine hydrochloride solutions were used to exclude the direct effect of amino acids on the ThT molecule.…”

Section: Uv-vis Absorbance Of Tht In Aqueous and Buffer Solutions Witmentioning

confidence: 99%

“…For instance, in Jha et al (2014), ThT and Nile Red dyes were used to study the pH dependence of amylin fibrillation; the authors of Sabaté et al (2008) investigated the interaction of ThT with fibrils of the prion-forming domain of the fungal HET-s protein at pH 2. The effect of basic pH (made using potassium buffer solutions) on ThT fluorescence was studied in Foderà et al (2008). In that work, the authors showed that a reversible hydroxylation process occurs in alkaline solutions leading to a decrease in the ThT fluorescence signal.…”

Section: Introductionmentioning

confidence: 99%

Effect of acidic and basic pH on Thioflavin T absorbance and fluorescence

et al. 2015

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Thioflavin T (ThT) is a fluorescent dye able to enhance significantly its fluorescence quantum yield upon binding to protein amyloids. ThT assay is widely used to detect and quantify amyloids in a variety of conditions, including solutions with different pH levels. In the present work, the effect of acidic and basic pH on the conformation of the ThT molecule and its absorption and fluorescence properties was studied. The results show that both acidic and basic pH decrease significantly the intensity of ThT absorption in the visible region and fluorescence emission intensity. Low pHs induce an immediate "all-or-nothing" decrease in the ThT signal, while in alkaline solutions the ThT signal decreases gradually over time. pH-induced signal quenching is less in the presence of glycerol or protein aggregates. Two different mechanisms are responsible for the ThT signal quenching-the ThT hydroxylation at basic pH and protonation of the nitrogen atom of the dimethylamino group at acidic pH. ThT assays should be carefully carried out at basic or acidic pH as strong pH dependence of ThT could be responsible for misinterpretation and false positive/negative experimental results. The potential unsuitability of ThT as a probe in solutions with high pH (>9) has been shown.

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Thioflavin T Hydroxylation at Basic pH and Its Effect on Amyloid Fibril Detection

Cited by 108 publications

References 54 publications

SOD1 aggregation in ALS mice shows simplistic test tube behavior

SOD1 aggregation in ALS mice shows simplistic test tube behavior

ThT 101: a primer on the use of thioflavin T to investigate amyloid formation

Effect of acidic and basic pH on Thioflavin T absorbance and fluorescence

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