Amyloid Peptide Pores and the Beta Sheet Conformation

Kagan, Bruce L.; Thundimadathil, Jyothi

doi:10.1007/978-1-4419-6327-7_13

Cited by 60 publications

(62 citation statements)

References 94 publications

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“…At the same time the charge and polarity of E73 is strongly correlated with the dynamics and conformation of the membrane environment, suggesting that the dynamics of the lipids might be connected with global protein motions. This finding is interesting as lipid-protein interactions are known to be important for the structure and function of integral membrane proteins (47)(48)(49)(50)(51)(52). In particular, VDAC1 gating and ionic selectivity have been shown to be dependent on lipid composition (53).…”

Section: μS-ms Dynamics Are Significantly Increased For the N-terminamentioning

confidence: 90%

Functional dynamics in the voltage-dependent anion channel

Villinger

Briones

Giller

et al. 2010

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

105

129

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The voltage-dependent anion channel (VDAC), located in the outer mitochondrial membrane, acts as a gatekeeper for the entry and exit of mitochondrial metabolites. Here we reveal functional dynamics of isoform one of VDAC (VDAC1) by a combination of solution NMR spectroscopy, Gaussian network model analysis, and molecular dynamics simulation. Micro-to millisecond dynamics are significantly increased for the N-terminal six β-strands of VDAC1 in micellar solution, in agreement with increased B-factors observed in the same region in the bicellar crystal structure of VDAC1. Molecular dynamics simulations reveal that a charge on the membrane-facing glutamic acid 73 (E73) accounts for the elevation of N-terminal protein dynamics as well as a thinning of the nearby membrane. Mutation or chemical modification of E73 strongly reduces the micro-to millisecond dynamics in solution. Because E73 is necessary for hexokinase-I-induced VDAC channel closure and inhibition of apoptosis, our results imply that microto millisecond dynamics in the N-terminal part of the barrel are essential for VDAC interaction and gating.membrane protein | molecular dynamics | NMR spectroscopy | protein-lipid interactions | structure D ynamics of proteins provide the essential link between structure and function. Membrane protein dynamics are gaining more attention due to an increasing number of high-resolution structures. A versatile experimental method for the study of membrane protein dynamics is NMR spectroscopy, providing atomic resolution information from nanoseconds to seconds (for an overview see ref. 1). In addition, when a three-dimensional structure is available, insight into fast dynamics of proteins, which occur on the nanosecond time scale, might be gained from molecular dynamics (MD) simulation and elastic network models (2, 3).NMR studies have revealed large conformational changes essential for the physiological function of α-helical membrane proteins, such as the interaction of phospholamban with effectors modulating heart muscle contractility (4, 5) and antimicrobial peptides adopting different conformations in membranes or solution (6, 7). Less well characterized are motions of outer membrane β-barrels. A pioneering solution NMR study revealed μs-ms interconversion of the catalytic loop of PagP between an excited and a nonexcited state, enabling both ligand binding and enzymatic catalysis (8). Nonenzymatic β-barrel channels exhibit more general dynamic features, such as loop flexibility and slow conformational exchange towards the extracellular barrel edges, altogether indicating relevance for substrate conductance and gating (9-11).The voltage-dependent anion channel (VDAC) is one of the few β-barrel membrane proteins, the structure of which has been determined to date (12-14). Serving as the major pass-through for metabolites between mitochondria and the cytosol (15), the highly abundant channel is regarded as a key regulator of cellular energy metabolism (16). Metabolite flow is regulated by a voltage-dependent conformational c...

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Section: μS-ms Dynamics Are Significantly Increased For the N-terminamentioning

confidence: 90%

Functional dynamics in the voltage-dependent anion channel

Villinger

Briones

Giller

et al. 2010

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

105

129

View full text Add to dashboard Cite

show abstract

“…The mitochondrial dysfunction present in Alzheimer's disease is likely caused, in part, by oligomers of Ab interacting with mitochondrial proteins or phospholipids (Crouch et al, 2005;Kagan and Thundimadathil, 2010). However, there is also evidence of mitochondrial dysfunction caused by full length APP (Hansson Petersen et al, 2008), hyperphosphorylated tau (Eckert et al, 2010), or truncated apolipoprotein A4 (ApoE4) (Chen et al, 2011).…”

Section: Introductionmentioning

confidence: 97%

Caffeine increases mitochondrial function and blocks melatonin signaling to mitochondria in Alzheimer's mice and cells

et al. 2012

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“…área innominata) suele presentar pérdida neuronal, formación de estos ovillos y ausencia de placas de Aβ 19 . Otra característica es la presencia de hilos de neurópilo, depósitos de amiloide (vasos sanguíneos cerebrales y meníngeos), degeneración gránulo-vacuolar en las células piramidales del hipocampo, cuerpos de Hirano, gliosis reactiva, aumento de las células de la microglia y alteraciones pseudoespongiformes 20 . Recientemente se ha propuesto que los depó-sitos amorfos amiloideos vinculados con canales amiloideos serían los principales causantes de la fisiopatología de la EA 20 .…”

Section: Descripción Histopatológicaunclassified

Evaluación de la enfermedad de Alzheimer en etapa temprana: biomarcadores y pruebas neuropsicológicas

Lanfranco

Manríquez-Navarro

et al. 2012

Rev. méd. Chile

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Amyloid Peptide Pores and the Beta Sheet Conformation

Cited by 60 publications

References 94 publications

Functional dynamics in the voltage-dependent anion channel

Functional dynamics in the voltage-dependent anion channel

Caffeine increases mitochondrial function and blocks melatonin signaling to mitochondria in Alzheimer's mice and cells

Evaluación de la enfermedad de Alzheimer en etapa temprana: biomarcadores y pruebas neuropsicológicas

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