Combining modelling and mutagenesis studies of synaptic vesicle protein 2A to identify a series of residues involved in racetam binding

Shi, Jiye; Anderson, Dina; Lynch, Berkley A.; Castaigne, Jean‐Gabriel; Foerch, Patrik; Lebon, Florence

doi:10.1042/bst0391341

Cited by 23 publications

(41 citation statements)

References 42 publications

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“…The subsequent complexes were then simulated using molecular dynamics in an attempt to further characterize SV2A–racetam binding site interactions. Despite the short timescale simulations and the challenge and caveats of modeling the extramembranous domains, the studies support the putative binding pocket observed by Shi et al [85] and Lee et al [86], and, furthermore, identified additional hydrophobic and hydrogen bond interactions with T456, S665 and L689, which may be important for ligand recognition within the putative racetam binding site.…”

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivsupporting

confidence: 79%

“…These predictions were subsequently borne out by SDM performed on W454A and D670A in conjunction with binding affinity assays [86]. Taken together with the studies of Shi et al [85], the outward-open conformation of SV2A (i.e. with the putative binding site exposed to the interior of the synaptic vesicle) presents a levetiracetam-binding pocket that is in greater agreement with the SDM experiments.…”

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 68%

“…Although the sequence identity between SV2A and other MFS proteins is very low, typically <20 %, homology models have been constructed using available MFS x-ray structures as templates. In an early study Shi et al [85] selected three residues—F658, G659 and V661—based on their alignment with functionally relevant residues in LacY for site-directed mutagenesis (SDM) studies with levetiracetam and structurally-related analogs such as ucb 30889, collectively referred to as racetams, to elucidate residues that are important for racetam binding. Furthermore, Shi et al [85] constructed an SV2A homology model using the LacY crystal structure as a template, and in conjunction with racetam docking studies they proposed additional residues for SDM studies.…”

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 99%

“…In an early study Shi et al [85] selected three residues—F658, G659 and V661—based on their alignment with functionally relevant residues in LacY for site-directed mutagenesis (SDM) studies with levetiracetam and structurally-related analogs such as ucb 30889, collectively referred to as racetams, to elucidate residues that are important for racetam binding. Furthermore, Shi et al [85] constructed an SV2A homology model using the LacY crystal structure as a template, and in conjunction with racetam docking studies they proposed additional residues for SDM studies. In total, through binding affinity experiments, 14 mutants were found to be implicated in racetam binding (F277A, W300A, W300F, Y462A, K694A, G303A, F658A, V661A, I663A, W666A, N667A, S294A, M301A, G659A) and were proposed to encompass the SV2A racetam binding site.…”

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 99%

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Synaptic Vesicle Glycoprotein 2A Ligands in the Treatment of Epilepsy and Beyond

Löscher¹,

et al. 2016

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The synaptic vesicle glycoprotein SV2A belongs to the major facilitator superfamily (MFS) of transporters and is an integral constituent of synaptic vesicle membranes. SV2A has been demonstrated to be involved in vesicle trafficking and exocytosis, processes crucial for neurotransmission. The anti-seizure drug levetiracetam was the first ligand to target SV2A and displays a broad spectrum of anti-seizure activity in various preclinical models. Several lines of preclinical and clinical evidence, including genetics and protein expression changes, support an important role of SV2A in epilepsy pathophysiology. While the functional consequences of SV2A ligand binding are not fully elucidated, studies suggest that subsequent SV2A conformational changes may contribute to seizure protection. Conversely, the recently discovered negative SV2A modulators, such as UCB0255, counteract the anti-seizure effect of levetiracetam and display procognitive properties in preclinical models. More broadly, dysfunction of SV2A may also be involved in Alzheimer’s disease and other types of cognitive impairment, suggesting potential novel therapies for levetiracetam and its congeners. Furthermore, emerging data indicate that there may be important roles for two other SV2 isoforms (SV2B and SV2C) in the pathogenesis of epilepsy, as well as other neurodegenerative diseases. Utilization of recently developed SV2A positron emission tomography ligands will strengthen and reinforce the pharmacological evidence that SV2A is a druggable target, and will provide a better understanding of its role in epilepsy and other neurological diseases, aiding in further defining the full therapeutic potential of SV2A modulation.

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Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivsupporting

confidence: 79%

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 68%

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 99%

Section: Sv2a As a Target For Anti-seizure Drugs: Levetiracetam Brivmentioning

confidence: 99%

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Synaptic Vesicle Glycoprotein 2A Ligands in the Treatment of Epilepsy and Beyond

Löscher¹,

et al. 2016

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“…The importance of SV receptors is more evident when this cellular membrane receptor is bound to neurotransmissors, drugs and neurotoxins, such as tetanus toxin and botulinium neurotoxin (BoNTA), especially the type A (BoNTA), that in therapeutic doses and for endocytosis lets to improve conditions as epilepsy and cancer in a more specific manner (Arnon et al, 2001;Karsenty et al, 2009;de Groot et al, 2010;Montal, 2010;Blum et al, 2012;Shi et al, 2011) and lead to apoptosis (Choi et al, 2007). BoNTA has been successfully used in the treatment of refractory detrusor overactivity.…”

Section: Introductionmentioning

confidence: 99%

Synaptic Vesicle Protein 2 (SV2) Isoforms

Bandala

Miliar-García²,

Mejía-Barradas

et al. 2012

Asian Pacific Journal of Cancer Prevention

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New molecular markers of cancer had emerged with novel applications in cancer prevention and therapeutics, including for breast cancer of unknown causes, which has a high impact on the health of women worldwide. The purpose of this research was to detemine protein and mRNA expression of synaptic vesicle 2 (SV2) isoforms A, B and C in breast cancer cell lines. Cultured cell lines MDA-MB-231, SKBR3, T47D were lysed and their protein and mRNA expression analyzed by real-time PCR and western blot technique, respectively. SV2A, B proteins were identified in non-tumor (MCF-10A) and tumor cell lines (MDA-MB-231 and T47D) while SV2C only was found in the T47D cell line. Furthermore, the genomic expression was consistent with protein expression for a such cell line, but in MDA-MB-231 there was no SV2B genomic expression, and the SV2C mRNA and protein were not found in the non tumoral cell line. These findings suggest a possible cellular transdifferentiation to neural character in breast cancer, of possible relevance to cancer development, and point to possible use of SV2 as molecular marker and a vehicle for cancer treatment with botulinum toxin.

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Mechanisms of Antiepileptic Drug Action

Walker¹,

Surges²

2015

The Treatment of Epilepsy

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Combining modelling and mutagenesis studies of synaptic vesicle protein 2A to identify a series of residues involved in racetam binding

Cited by 23 publications

References 42 publications

Synaptic Vesicle Glycoprotein 2A Ligands in the Treatment of Epilepsy and Beyond

Synaptic Vesicle Glycoprotein 2A Ligands in the Treatment of Epilepsy and Beyond

Synaptic Vesicle Protein 2 (SV2) Isoforms

Mechanisms of Antiepileptic Drug Action

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