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How structure shapes (dys)function A perspective to understanding brain region-specific degeneration in prion disease

机译:结构如何形成(功能障碍)功能以了解病毒疾病中特定于大脑区域的变性

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Structure is a key determinant of function, with the nervous system being no exception. For example, in the nervous system the physiological properties of different synapses may be understood by comparing their structures. However, it is not clear whether specific structural properties of some neurons might play a role in driving their selective removal during chronic neurodegeneration or whether the structural properties might underpin why particular types of synapses or other neuronal compartments are more susceptible to degeneration (i.e., become dysfunctional) in certain brain regions than in others. Our recent study of the ultrastructure of the hippocampus and the cerebellum revealed that early synaptic loss is not a ubiquitous event in a brain undergoing chronic neurodegeneration. The prominent structural differences in proximity of the synaptic environment that are brought about by a degree of synaptic ensheathment by glial cells may help explain why Purkinje cell synapses remain intact, while pyramidal cell synapses progressively degenerate. The intrinsic structural organization of the hippocampal neuropil could contribute to the susceptibility of synapses to extracellular protein misfolding by a relatively higher degree of synaptic exposure to the extracellular environment. We suggest that neuronal structure may determine more than function; it might also predict dysfunction.
机译:结构是功能的关键决定因素,神经系统也不例外。例如,在神经系统中,不同突触的生理特性可以通过比较它们的结构来理解。但是,尚不清楚某些神经元的特定结构性质是否可能在驱动其在慢性神经退行性变过程中的选择性去除中发挥作用,或者该结构性质是否可能支撑为什么特定类型的突触或其他神经元区室更易变性(即变得某些大脑区域的功能异常)。我们最近对海马和小脑超微结构的研究表明,在经历慢性神经变性的大脑中,早期突触丧失并非普遍存在。由胶质细胞一定程度的突触包被引起的突触环境附近的显着结构差异可能有助于解释为什么浦肯野细胞突触保持完整,而锥体细胞突触逐渐退化。海马神经细胞的固有结构组织可能通过相对较高程度的突触暴露于细胞外环境而导致突触对细胞外蛋白错误折叠的敏感性。我们建议神经元的结构可能比功能更重要。它也可能预测功能障碍。

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