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通过原子力和荧光显微镜测绘神经元细胞骨架的温度响应。

Temperature response of the neuronal cytoskeleton mapped via atomic force and fluorescence microscopy.

机构信息

Department of Physics and Astronomy and Center for Nanoscopic Physics, Tufts University, 4 Colby Street, Medford, MA 02155, USA.

出版信息

Phys Biol. 2013 Oct;10(5):056002. doi: 10.1088/1478-3975/10/5/056002. Epub 2013 Aug 22.

Abstract

Neuronal cells change their growth properties in response to external physical stimuli such as variations in external temperature, stiffness of the growth substrate, or topographical guidance cues. Detailed knowledge of the mechanisms that control these biomechanical responses is necessary for understanding the basic principles that underlie neuronal growth and regeneration. Here, we present elasticity maps of living cortical neurons (embryonic rat) as a function of temperature, and correlate these maps to the locations of internal structural components of the cytoskeleton. Neurons display a significant increase in the average elastic modulus upon a decrease in ambient temperature from 37 to 25 °C. We demonstrate that the dominant mechanism by which the elasticity of the neurons changes in response to temperature is the stiffening of the actin components of the cytoskeleton induced by myosin II. We also report a reversible shift in the location and composition of the high-stiffness areas of the neuron cytoskeleton with temperature. At 37 °C the areas of the cell displaying high elastic modulus overlap with the tubulin-dense regions, while at 25 °C these high-stiffness areas correspond to the actin-dense regions of the cytoskeleton. These results demonstrate the importance of considering temperature effects when investigating cytoskeletal dynamics in cells.

摘要

神经元细胞会根据外部物理刺激改变其生长特性,例如外部温度变化、生长基质的硬度或地形导向线索。详细了解控制这些生物力学反应的机制对于理解神经元生长和再生的基本原理是必要的。在这里,我们展示了活皮质神经元(胚胎大鼠)作为温度函数的弹性图谱,并将这些图谱与细胞骨架内部结构成分的位置相关联。神经元在环境温度从 37°C 降至 25°C 时,平均弹性模量显著增加。我们证明了神经元弹性响应温度变化的主要机制是肌球蛋白 II 诱导的细胞骨架中肌动蛋白成分的变硬。我们还报告了随着温度的变化,神经元细胞骨架的高硬度区域的位置和组成发生可逆性变化。在 37°C 时,显示高弹性模量的细胞区域与微管密集区域重叠,而在 25°C 时,这些高硬度区域对应于细胞骨架的肌动蛋白密集区域。这些结果表明,在研究细胞骨架动力学时,考虑温度效应非常重要。

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