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首页> 外文期刊>Journal of forensic sciences. >Characterization of Protein Alterations in Damaged Axons in the Brainstem Following Traumatic Brain Injury Using Fourier Transform Infrared Microspectroscopy: A Preliminary Study
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Characterization of Protein Alterations in Damaged Axons in the Brainstem Following Traumatic Brain Injury Using Fourier Transform Infrared Microspectroscopy: A Preliminary Study

机译:创伤性脑损伤后脑干受损轴突中蛋白质变化的特征使用傅立叶变换红外显微技术的一项初步研究

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摘要

Axonal injury contributes greatly to neurological dysfunction following traumatic brain injury (TBI), but current histological diagnostic methods are limited in identifying the pathological profiles of injured axons and unable to provide an objective and accurate quantification. Fourier transform infrared microspectroscopy (FTIRM) has the ability to offer macromolecular bioinformatics of the tissues including biochemical composition and structure by calculating band absorption intensity. In this study, axonal injury in the brainstem of rats with traumatic brain injury at 72h post-trauma, which was confirmed with beta-amyloid precursor protein (-APP) immunostaining, was detected with FTIRM technique. The lower intensity of infrared absorbance under the amide I band corresponds strongly to the area of axonal injury, and further analysis of amide I band shows significant differences in protein conformation between injured and normal axons. The findings indicate that using FTIRM technique, the amide I band has potentials to be a infrared spectral marker of axonal injury.
机译:轴突损伤在颅脑外伤(TBI)后对神经功能障碍的影响很大,但是目前的组织学诊断方法仅限于鉴定受损轴突的病理学特征,并且无法提供客观准确的定量结果。傅里叶变换红外光谱(FTIRM)能够通过计算能带吸收强度提供组织的大分子生物信息,包括生化成分和结构。在这项研究中,通过FTIRM技术检测了创伤后72小时的颅脑外伤大鼠脑干的轴突损伤,该损伤已通过β-淀粉样蛋白前体蛋白(-APP)免疫染色得到了证实。酰胺I谱带下较低的红外吸收强度强烈对应于轴突损伤区域,对酰胺I谱带的进一步分析显示,受损的和正常的轴突之间蛋白质构象存在显着差异。研究结果表明,使用FTIRM技术,酰胺I谱带有可能成为轴突损伤的红外光谱标记。

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