The Lipid-binding Domain of Wild Type and Mutant α-Synuclein

Georgieva, Elka R.; Ramlall, Trudy F.; Borbat, Peter P.; Freed, Jack H.; Eliezer, David

doi:10.1074/jbc.m110.157214

Cited by 132 publications

(98 citation statements)

References 75 publications

(60 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These helices are stabilized by interaction with a variety of phospholipid bilayers, though α-synuclein interacts preferentially with membranes of high curvature and an abundance of acidic phospholipids, properties consistent with those of synaptic vesicles (Davidson et al, 1998; Zhu et al, 2003). Upon interaction with membranes of low curvature α-synuclein adopts a distinct secondary structure characterized by a single extended helix that includes both previously described helical domains and the linker region (amino acids 38–44) (Ferreon et al, 2009; Georgieva et al, 2010; Trexler and Rhoades, 2009). All known mutations associated with familial PD (A30P, E46K, H50Q, G51D, A53E, and A53T) are found in the N-terminal domain (Krüger et al, 2008; Lesage et al, 2013; Pasanen et al, 2014; Polymeropoulos et al, 1997; Proukakis et al, 2013; Zarranz et al, 2004).…”

Section: α-Synuclein Structural Flexibilitymentioning

confidence: 99%

Dynamic structural flexibility of α-synuclein

Mor

Ugras

Daniels

et al. 2016

Neurobiology of Disease

View full text Add to dashboard Cite

α-Synuclein is a conserved, abundantly expressed protein that is partially localized in pre-synaptic terminals in the central nervous system. The precise biological function(s) and structure of α-synuclein are under investigation. Recently, the native conformation and the presence of naturally occurring multimeric assemblies have come under debate. These are important deliberations because α-synuclein assembles into highly organized amyloid-like fibrils and non-amyloid amorphous aggregates that constitute the neuronal inclusions in Parkinson’s disease and related disorders. Therefore understanding the nature of the native and pathological conformations is pivotal from the standpoint of therapeutic interventions that could maintain α-synuclein in its physiological state. In this review, we will discuss the existing evidence that define the physiological states of α-synuclein and highlight how the inherent structural flexibility of this protein may be important in health and disease.

show abstract

Section: α-Synuclein Structural Flexibilitymentioning

confidence: 99%

Dynamic structural flexibility of α-synuclein

Mor

Ugras

Daniels

et al. 2016

Neurobiology of Disease

View full text Add to dashboard Cite

show abstract

“…Experiments have identified two predominant states for monomeric α S bound to anionic membranes, a horseshoe-like broken helix identified with NMR and EPR (Ulmer et al, 2005; Drescher et al, 2008; Rao et al, 2010) where a kink brings together the two helical segments, and an extended kink-free helix conformation without a kink postulated by ESR and DEER experiments (Jao et al, 2004; Georgieva et al, 2008; Jao et al, 2008; Trexler and Rhoades, 2009). It has been suggested that the extended and broken-helix conformations could interconvert (Georgieva et al, 2010; Robotta et al, 2011; Lokappa and Ulmer, 2011), potentially in a lipid-dependent fashion (Borbat et al, 2006; Middleton and Rhoades, 2010). Outside of coarse-grained simulations (Braun et al, 2012; Braun and Sachs, 2015), this conformational diversity had not been sampled, and presented a prime candidate for using the HMMM model to investigate the specific lipid interactions that determine the membrane-bound structure of α S.…”

Section: Applications Of Hmmm To Membrane-associated Phenomenamentioning

confidence: 99%

Efficient Exploration of Membrane-Associated Phenomena at Atomic Resolution

et al. 2015

View full text Add to dashboard Cite

Biological membranes constitute a critical component in all living cells. In addition to providing a conducive environment to a wide range of cellular processes, including transport and signaling, mounting evidence has established active participation of specific lipids in modulating membrane protein function through various mechanisms. Understanding lipid-protein interactions underlying these mechanisms at a sufficiently high resolution has proven extremely challenging, partly due to the semi-fluid nature of the membrane. In order to address this challenge computationally, multiple methods have been developed, including an alternative membrane representation termed HMMM (highly mobile membrane mimetic) in which lateral lipid diffusion has been significantly enhanced without compromising atomic details. The model allows for efficient sampling of lipid-protein interactions at atomic resolution, thereby significantly enhancing the effectiveness of molecular dynamics simulations in capturing membrane-associated phenomena. In this review, after providing an overview of HMMM model development, we will describe briefly successful application of the model to study a variety of membrane processes, including lipid-dependent binding and insertion of peripheral proteins, the mechanism of phospholipid insertion into lipid bilayers, and characterization of optimal tilt angle of transmembrane helices. We conclude with practical recommendations for proper usage of the model in simulation studies of membrane processes.

show abstract

“…1A). The protein adopts a predominantly broken or continuous α-helical structure upon binding high- or low-curvature membranes, respectively (Chandra et al, 2003; Ferreon et al, 2009; Georgieva et al, 2010; Trexler and Rhoades, 2009; Ulmer et al, 2005). Interactions involving an N-terminal segment spanning residues 1–25 are critical for membrane binding and for the adoption of an α-helical structure (Bartels et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

Effects of impaired membrane interactions on α-synuclein aggregation and neurotoxicity

Ysselstein

Joshi

Mishra

et al. 2015

Neurobiology of Disease

162

View full text Add to dashboard Cite

The post-mortem brains of individuals with Parkinson’s disease (PD) and other synucleinopathy disorders are characterized by the presence of aggregated forms of the presynaptic protein α-synuclein (aSyn). Understanding the molecular mechanism of aSyn aggregation is essential for the development of neuroprotective strategies to treat these diseases. In this study, we examined how interactions between aSyn and phospholipid vesicles influence the protein’s aggregation and toxicity to dopaminergic neurons. Two-dimensional NMR data revealed that two familial aSyn mutants, A30P and G51D, populated an exposed, membrane-bound conformer in which the central hydrophobic region was dissociated from the bilayer to a greater extent than in the case of wild-type aSyn. A30P and G51D had a greater propensity to undergo membrane-induced aggregation and elicited greater toxicity to primary dopaminergic neurons compared to the wild-type protein. In contrast, the non-familial aSyn mutant A29E exhibited a weak propensity to aggregate in the presence of phospholipid vesicles or to elicit neurotoxicity, despite adopting a relatively exposed membrane-bound conformation. Our findings suggest that the aggregation of exposed, membrane-bound aSyn conformers plays a key role in the protein’s neurotoxicity in PD and other synucleinopathy disorders.

show abstract

The Lipid-binding Domain of Wild Type and Mutant α-Synuclein

Cited by 132 publications

References 75 publications

Dynamic structural flexibility of α-synuclein

Dynamic structural flexibility of α-synuclein

Efficient Exploration of Membrane-Associated Phenomena at Atomic Resolution

Effects of impaired membrane interactions on α-synuclein aggregation and neurotoxicity

Contact Info

Product

Resources

About