Human Hsp60 with Its Mitochondrial Import Signal Occurs in Solution as Heptamers and Tetradecamers Remarkably Stable over a Wide Range of Concentrations

Vilasi, Silvia; Carrotta, Rita; Mangione, Maria Rosalia; Campanella, Claudia; Librizzi, Fabio; Randazzo, Loredana; Martorana, Vincenzo; Gammazza, Antonella Marino; Ortore, María Grazia; Vilasi, Annalisa; Pocsfalvi, Gabriella; Burgio, Giosalba; Corona, Davide; Piccionello, Antonio Palumbo; Zummo, Giovanni; Bulone, Donatella; Macario, Everly Conway de; Macario, Alberto J. L.; Biagio, Pier Luigi San; Cappello, Francesco

doi:10.1371/journal.pone.0097657

Cited by 49 publications

(59 citation statements)

References 59 publications

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“…The values for GroEL and mitochondrial Hsp60 (used as standard protein) are of the same order of magnitude of those reported in literature [21,22]. The chromatograph we report in the Supporting Materials is the same previously reported in the paper written by some of us [14], because we used the same stock of commercial enzymes. All the experiments were conducted by diluting naïve Hsp60 from stock solutions to reach the concentration of 4.8 μM and dissolving GroEL in 20 mM Tris pH 8.0 and 10% glycerol (w/w) at 4.8 μM, too.…”

Section: Sample Preparationsupporting

confidence: 57%

“…Higher protein concentrations were obtained with Vivaspin concentrators with a Polyethersulfone membrane and 10 kDa molecular weight cut-offs (Sartorius, Germany). Protein concentration for each experiment was determined by the area under a peak from the corresponding High Performance Liquid Chromatography (HPLC) chromatogram recorded at 280 nm [14]. The concentration determination was performed after Dynamic Light Scattering experiments on the samples, which showed that there were only the oligomeric species considered functional for chaperonins [5,11,14].…”

Section: Sample Preparationmentioning

confidence: 99%

“…Moreover, naïve Hsp60 form could be involved in tumor cells or during inflammatory diseases [13,7]. More recently, the structure and oligomeric state of the naïve Hsp60 have been studied in vitro in a wide range of concentrations, and results have shown that it exists in solution in a dynamic equilibrium between two conformations: heptameric single rings and double ringed tetradecamers [14].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Stability and disassembly properties of human naïve Hsp60 and bacterial GroEL chaperonins

Ricci

Ortore

Vilasi

et al. 2016

Biophysical Chemistry

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Section: Sample Preparationsupporting

confidence: 57%

Section: Sample Preparationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Stability and disassembly properties of human naïve Hsp60 and bacterial GroEL chaperonins

Ricci

Ortore

Vilasi

et al. 2016

Biophysical Chemistry

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“…The other two exible linkers, connecting the N-and C-ending domain to the equatorial-intermediate domains, are from residues 23 to 26 and from 548 to 552. Taking advantage of recent ndings above mentioned, 11 and considering initial attempt to tting SAXS data (see Fig. S5 †), we have considered that, unlike GroEL, naïve-Hsp60 in solution can simultaneously be present as a mixture of tetradecamers and heptamers.…”

Section: Structural Analysis Of Naïve-hsp60mentioning

confidence: 99%

Quaternary structures of GroEL and naïve-Hsp60 chaperonins in solution: a combined SAXS-MD study

et al. 2015

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The quaternary structures of bacterial GroEL and human naïve-Hsp60 chaperonins in physiological conditions have been investigated by an innovative approach based on a combination of synchrotron Small Angle X-ray Scattering (SAXS) in-solution experiments and molecular dynamics (MD) simulations. Low-resolution SAXS experiments over large and highly symmetric oligomers are analyzed on the basis of the high-resolution structure of the asymmetric protein monomers, provided by MD. The results reveal remarkable differences between the solution and the crystallographic structure of GroEL and between the solution structures of GroEL and of its human homologue Hsp60.

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“…Various studies, published over the past several years, have demonstrated new subcellular locations and functions for Hsp60, describing it as a ubiquitous molecule with multiple roles in health and disease [42][43][44]. Moreover, detailed studies of the structure of Hsp60 have been reported that help understand the functions of this multifaceted molecule [45,46].…”

Section: Hsp60mentioning

confidence: 99%

Alzheimer's Disease and Molecular Chaperones: Current Knowledge and the Future of Chaperonotherapy

Gammazza¹,

Bavisotto²,

Barone³

et al. 2016

CPD

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Abstract:Background: Alzheimer's disease (AD) is a dementia, a neurodegenerative condition, and a protein-misfolding disease or proteinopathy, characterized by protein deposits, extracellular plaques and intracellular neurofibrillary tangles, which contain the AD's typical pathological proteins, abnormal -amyloid and hyperphosphorylated tau, respectively, and are located predominantly in the cortex of the frontal, parietal, and temporal brain lobes.

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Human Hsp60 with Its Mitochondrial Import Signal Occurs in Solution as Heptamers and Tetradecamers Remarkably Stable over a Wide Range of Concentrations

Cited by 49 publications

References 59 publications

Stability and disassembly properties of human naïve Hsp60 and bacterial GroEL chaperonins

Stability and disassembly properties of human naïve Hsp60 and bacterial GroEL chaperonins

Quaternary structures of GroEL and naïve-Hsp60 chaperonins in solution: a combined SAXS-MD study

Alzheimer's Disease and Molecular Chaperones: Current Knowledge and the Future of Chaperonotherapy

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