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Parkinson's Disease (PD) is characterized by the accumulation of Lewy bodies in dopaminergic neurons. The main protein component of Lewy bodies, α-synuclein (αS), is also firmly linked to PD through the identification of a number of single point mutations that are autosomal dominant for early-onset disease. Consequently, the misfolding and subsequent aggregation of αS is thought to be a key stage in the development and progression of PD. Therefore, modulating the aggregation pathway of αS is an attractive therapeutic target. Owing to the fact that all but one of the familial mutations is located in the preNAC 45-54 region of αS, we previously designed a semi-rational library using this sequence as a design scaffold. The 45-54 peptide library was screened using a protein-fragment complementation assay approach, leading to the identification of the 4554W peptide. The peptide was subsequently found to be effective in inhibiting primary nucleation of αS, the earliest stage of the aggregation pathway. Here, we build upon this previous work by screening the same 45-54 library against five of the known αS single-point mutants that are associated with early-onset PD (A30P, E46K, H50Q, G51D, and A53T). These point mutations lead to a rapid acceleration of PD pathology by altering either the rate or type of aggregates formed. All ultimately lead to earlier disease onset and were therefore used to enforce increased assay stringency during the library screening process. The ultimate aim was to identify a peptide that is effective against not only the familial αS variant from which it has been selected but that is also effective against WT αS. Screening resulted in five peptides that shared common residues at some positions, while deviating at others. All reduced aggregation of the respective target, with several also identified to be effective at reducing aggregation when incubated with other variants. In addition, our results demonstrate that a previously optimized peptide, 4554W(N6A), is highly effective against not only WT αS but also several of the single-point mutant forms and hence is a suitable baseline for further work toward a PD therapeutic.
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http://dx.doi.org/10.1021/acschemneuro.2c00190 | DOI Listing |
Drug Test Anal
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Department of Laboratory Medicine, Karolinska Institute, Stockholm, Sweden.
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September 2025
Department of Chemistry and Biotechnology, Faculty of Science and Technology, Kochi University, 2-5-1 Akebono-cho, Kochi City, Kochi, 780-8520, Japan. Electronic address:
The development of on-site Hg analysers is crucial for the rapid evaluation of Hg concentrations in environmental research. However, the fabrication of Hg analysers requires simplification of analytical procedures and device miniaturisation. Based on the above requirements, our research group previously investigated enclosed quartz cell cold vapour atomic absorption spectrometry (EQC-CV-AAS) as a base technique for an on-site Hg analyser.
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September 2025
Fermentation and Microbial Biotechnology Division, CSIR-Indian Institute of Integrative Medicine, Canal Road, Jammu-Tawi, 180001, India.
Trichoderma species exhibit remarkable versatility in adaptability and in occupying habitats with lifestyles ranging from mycoparasitism and saprotrophy to endophytism. In this study, we present the first high-quality whole-genome assembly and annotation of T. lixii using Illumina HiSeq technology to explore the mechanisms of endophytic lifestyle and plant colonization.
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August 2025
Cardiovascular Medicine, Moscow Multidisciplinary Clinical Center Kommunarka, Moscow, RUS.
Simulation-based training is transforming the education of vascular surgeons in the management of aortic aneurysms (AAs), addressing limitations in traditional apprenticeship models amid declining open surgical volumes and increasing reliance on complex endovascular techniques. This review explores the current landscape of simulation technologies, including computational modeling, fluid-structure interaction, patient-specific 3D printing, artificial intelligence, and robotic platforms. These tools enable high-fidelity, anatomically accurate, and physiologically realistic training environments.
View Article and Find Full Text PDFFood Res Int
November 2025
College of Food Science, Shenyang Agricultural University, Shenyang, Liaoning 110866, PR China. Electronic address:
Tussah pupa protein (TPP), rich in diverse bioactive components and demonstrating extensive physiological activities, has attracted attention in food processing. However, its limited emulsion stability restricts application potential, requiring improvement of techno-functional properties. The effects of myofibrillar protein (MP) compounding coupled with ultrasonic treatment on the emulsifying properties and nutritional value of TPP were systematically investigated from a multi-scale perspective in this study.
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