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路易体病理的位点特异性播种在皮质中诱导出不同的运动前细胞和树突状易损性。

Site-specific seeding of Lewy pathology induces distinct pre-motor cellular and dendritic vulnerabilities in the cortex.

作者信息

Khan Hammad F, Dutta Sayan, Scott Alicia N, Xiao Shulan, Yadav Saumitra, Chen Xiaoling, Aryal Uma K, Kinzer-Ursem Tamara L, Rochet Jean-Christophe, Jayant Krishna

机构信息

Weldon School of Biomedical Engineering, West Lafayette, Indiana, IN, USA.

Purdue Institute for Integrative Neuroscience, Purdue University, West Lafayette, IN, USA.

出版信息

Nat Commun. 2024 Dec 30;15(1):10775. doi: 10.1038/s41467-024-54945-0.

Abstract

Circuit-based biomarkers distinguishing the gradual progression of Lewy pathology across synucleinopathies remain unknown. Here, we show that seeding of α-synuclein preformed fibrils in mouse dorsal striatum and motor cortex leads to distinct prodromal-phase cortical dysfunction across months. Our findings reveal that while both seeding sites had increased cortical pathology and hyperexcitability, distinct differences in electrophysiological and cellular ensemble patterns were crucial in distinguishing pathology spread between the two seeding sites. Notably, while beta-band spike-field-coherence reflected a significant increase beginning in Layer-5 and then spreading to Layer-2/3, the rate of entrainment and the propensity of stochastic beta-burst dynamics was markedly seeding location-specific. This beta dysfunction was accompanied by gradual superficial excitatory ensemble instability following cortical, but not striatal, preformed fibrils injection. We reveal a link between Layer-5 dendritic vulnerabilities and translaminar beta event dysfunction, which could be used to differentiate symptomatically similar synucleinopathies.

摘要

区分路易体病理在突触核蛋白病中逐渐进展的基于回路的生物标志物仍然未知。在此,我们表明在小鼠背侧纹状体和运动皮层中接种α-突触核蛋白预形成纤维会在数月内导致不同的前驱期皮质功能障碍。我们的研究结果表明,虽然两个接种部位的皮质病理和过度兴奋性均增加,但电生理和细胞集合模式的明显差异对于区分两个接种部位之间的病理传播至关重要。值得注意的是,虽然β波段棘波-场相干性反映了从第5层开始并随后扩散到第2/3层的显著增加,但夹带速率和随机β爆发动力学的倾向在接种位置上具有明显的特异性。这种β功能障碍伴随着在注射皮质而非纹状体预形成纤维后逐渐出现的浅层兴奋性集合不稳定性。我们揭示了第5层树突易损性与跨层β事件功能障碍之间的联系,这可用于区分症状相似的突触核蛋白病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b78/11685769/37b9c68a1eae/41467_2024_54945_Fig1_HTML.jpg

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