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对周围动脉疾病患者的腓肠肌进行光学探测可表征肌病性生化改变,并与疾病阶段相关。

Optical probing of gastrocnemius in patients with peripheral artery disease characterizes myopathic biochemical alterations and correlates with stage of disease.

作者信息

Becker Ryan A, Cluff Kim, Duraisamy Nithyanandhi, Mehraein Hootan, Farhoud Hussam, Collins Tracie, Casale George P, Pipinos Iraklis I, Subbiah Jeyamkondan

机构信息

Biomedical Engineering Department, Wichita State University, Wichita, Kansas.

Biomedical Engineering Department, Wichita State University, Wichita, Kansas

出版信息

Physiol Rep. 2017 Mar;5(5). doi: 10.14814/phy2.13161.

Abstract

Peripheral artery disease (PAD) is a condition caused by atherosclerotic blockages in the arteries supplying the lower limbs and is characterized by ischemia of the leg, progressive myopathy, and increased risk of limb loss. The affected leg muscles undergo significant changes of their biochemistry and metabolism including variations in the levels of many key proteins, lipids, and nucleotides. The mechanisms behind these changes are poorly understood. The objective of this study was to correlate the severity of the PAD disease stage and associated hemodynamic limitation (determined by the ankle brachial index, ABI) in the legs of the patients with alterations in the biochemistry of chronically ischemic leg muscle as determined by ATR-Fourier transform infrared micro-spectroscopy. Muscle (gastrocnemius) biopsies were collected from 13 subjects including four control patients (ABI≥0.9), five claudicating patients (0.4 ≤ ABI<0.9), and four critical limb ischemia (CLI) patients (ABI<0.4). Slide mounted specimens were analyzed by ATR-Fourier transform infrared micro-spectroscopy. An analysis of variance and a partial least squares regression model were used to identify significant differences in spectral peaks and correlate them with the ABI The spectra revealed significant differences ( < 0.05) across control, claudicating, and CLI patients in the fingerprint and functional group regions. Infrared microspectroscopic probing of ischemic muscle biopsies demonstrates that PAD produces significant and unique changes to muscle biochemistry in comparison to control specimens. These distinctive biochemical profiles correlate with disease progression and may provide insight and direction for new targets in the diagnosis and therapy of muscle degeneration in PAD.

摘要

外周动脉疾病(PAD)是一种由供应下肢的动脉发生动脉粥样硬化阻塞引起的疾病,其特征为腿部缺血、进行性肌病以及肢体丧失风险增加。受影响的腿部肌肉在生物化学和代谢方面会发生显著变化,包括许多关键蛋白质、脂质和核苷酸水平的改变。这些变化背后的机制尚不清楚。本研究的目的是将患者腿部PAD疾病阶段的严重程度及相关血流动力学限制(由踝臂指数,即ABI确定)与通过衰减全反射 - 傅里叶变换红外显微光谱法测定的慢性缺血腿部肌肉生物化学变化相关联。从13名受试者身上采集了肌肉(腓肠肌)活检样本,其中包括4名对照患者(ABI≥0.9)、5名间歇性跛行患者(0.4≤ABI<0.9)和4名严重肢体缺血(CLI)患者(ABI<0.4)。对载玻片上的标本进行衰减全反射 - 傅里叶变换红外显微光谱分析。采用方差分析和偏最小二乘回归模型来识别光谱峰的显著差异,并将其与ABI相关联。光谱显示,在对照、间歇性跛行和CLI患者的指纹区和官能团区存在显著差异(P<0.05)。对缺血肌肉活检样本进行红外显微光谱探测表明,与对照样本相比,PAD会使肌肉生物化学产生显著且独特的变化。这些独特的生物化学特征与疾病进展相关,可能为PAD肌肉退化的诊断和治疗新靶点提供见解和方向。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bcbe/5350172/bf398cdfae61/PHY2-5-e13161-g001.jpg

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