Protein aggregation is a prominent feature of many neurodegenerative disorders including Parkinson's disease (PD). Aggregation of alpha-synuclein (SNCA) may underlie the pathology of PD. They are the main components of Lewy bodies and dystrophic neurites that are the intraneuronal inclusions characteristic of the disease. We have demonstrated that the polyphenol (-)-epi-gallocatechine gallate (EGCG) inhibited SNCA aggregation, which made it a candidate for therapeutic intervention in PD. Three methods were used: SNCA fibril formation inhibition by EGCG in incubates; inhibition of the SNCA fluorophore A-Syn-HiLyte488 binding to plated SNCA in microwells; and inhibition of the A-Syn-HiLyte488 probe binding to aggregated SNCA in postmortem PD tissue. Recombinant human SNCA was incubated under conditions that result in fibril formation. The aggregation was blocked by 100 nM EGCG in a concentration-dependent manner, as shown by an absence of thioflavin T binding. In the microplate assay system, the ED of EGCG inhibition of A-Syn-HiLyte488 binding to coated SNCA was 250 nM. In the PD tissue based assay, SNCA aggregates were recognized by incubation with 7 nM of A-Syn-HiLyte488. This binding was blocked by EGCG in a concentration dependent manner. The SNCA amino acid sites, which potentially interacted with EGCG, were detected on peptide membranes. It was implicated that EGCG binds to SNCA by instable hydrophobic interactions. In this study, we suggested that EGCG could be a potent remodeling agent of SNCA aggregates and a potential disease modifying drug for the treatment of PD and other α-synucleinopathies.
Abstract-The investigation of co-channel interference mitigation techniques (such as, interference cancellation through receiver processing, interference randomization by frequency hopping, and interference avoidance through resource usage restrictions imposed by frequency and power planning) has become a key focus area in achieving dense spectrum reuse in next generation cellular systems such as 3GPP LTE, LTEadvanced, and WiMAX. In this paper, we propose an interference avoidance scheme for LTE downlink that uses dynamic inter-cell coordination facilitated through X2 interface among neighbouring evolved UTRAN nodeBs (eNBs, i.e., LTE base stations). Proposed scheme is evaluated by extensive simulations and compared with a number of reference schemes available in the literature. It has been observed that the proposed scheme attains superior performance in terms of cell-edge and sector throughput compared to those in the reference schemes.
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