帕金森病引起的人脑组织/细胞和DNA/染色质空间结构改变的光学检测

IF 2.3
Fatemah Alharthi, Dhruvil Solanki, Ishmael Apachigawo, Santanu Maity, Jianfeng Xiao, Mohammad Moshahid Khan, Prabhakar Pradhan
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引用次数: 0

摘要

帕金森病(PD)是最常见的神经退行性疾病之一,迫切需要早期可靠的生物标志物。亚细胞水平的结构紊乱,特别是在核成分如DNA/染色质中,提供了一个有希望的诊断靶点。在这项研究中,我们应用了两种基于介观物理的光学技术-部分波光谱(PWS)和逆参与比(IPR)来量化死后人脑组织和细胞核的纳米级结构变化。PWS和IPR均显示PD样品的DNA/染色质结构紊乱和质量密度波动显著增加。这些异常可能与α -突触核蛋白在黑质中的病理聚集有关,这是pd相关神经变性的标志。补充组织学分析支持光学结果,证实了微结构破坏的存在。我们的研究结果建立了PWS和IPR作为检测PD早期纳米级变化的敏感光学/光子学工具,为改进诊断和了解疾病进展提供了新的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Optical Detection of the Spatial Structural Alteration in the Human Brain Tissues/Cells and DNA/Chromatin due to Parkinson's Disease.

Parkinson's disease (PD) is one of the most common neurodegenerative disorders, highlighting the urgent need for early, reliable biomarkers. Structural disorder at the subcellular level, particularly in nuclear components such as DNA/chromatin, offers a promising diagnostic target. In this study, we applied two mesoscopic physics-based optical techniques-partial wave spectroscopy (PWS) and inverse participation ratio (IPR)-to quantify nanoscale structural alterations in postmortem human brain tissues and nuclei. Both PWS and IPR revealed a significant increase in structural disorder and mass density fluctuations in DNA/chromatin of PD samples. These abnormalities are potentially linked to the pathological aggregation of alpha-synuclein in the substantia nigra, a hallmark of PD-related neurodegeneration. Complementary histological analyses supported the optical findings, validating the presence of disrupted microarchitecture. Our results establish PWS and IPR as sensitive optical/photonics tools for detecting early nanoscale changes in PD, offering a novel path toward improved diagnosis and understanding of disease progression.

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