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通过多示踪剂范式同步实现的小鼠骨骼肌超极化功能磁共振成像

Hyperpolarized functional magnetic resonance of murine skeletal muscle enabled by multiple tracer-paradigm synchronizations.

作者信息

Leftin Avigdor, Roussel Tangi, Frydman Lucio

机构信息

Department of Chemical Physics, Weizmann Institute of Science, Rehovot, Israel.

出版信息

PLoS One. 2014 Apr 25;9(4):e96399. doi: 10.1371/journal.pone.0096399. eCollection 2014.

Abstract

Measuring metabolism's time- and space-dependent responses upon stimulation lies at the core of functional magnetic resonance imaging. While focusing on water's sole resonance, further insight could arise from monitoring the temporal responses arising from the metabolites themselves, in what is known as functional magnetic resonance spectroscopy. Performing these measurements in real time, however, is severely challenged by the short functional timescales and low concentrations of natural metabolites. Dissolution dynamic nuclear polarization is an emerging technique that can potentially alleviate this, as it provides a massive sensitivity enhancement allowing one to probe low-concentration tracers and products in a single-scan. Still, conventional implementations of this hyperpolarization approach are not immediately amenable to the repeated acquisitions needed in real-time functional settings. This work proposes a strategy for functional magnetic resonance of hyperpolarized metabolites that bypasses this limitation, and enables the observation of real-time metabolic changes through the synchronization of stimuli-triggered, multiple-bolus injections of the metabolic tracer 13C1-pyruvate. This new approach is demonstrated with paradigms tailored to reveal in vivo thresholds of murine hind-limb skeletal muscle activation, involving the conversion of 13C1-pyruvate to 13C1-lactate and 13C1-alanine. These functional hind-limb studies revealed that graded skeletal muscle stimulation causes commensurate increases in glycolytic metabolism in a frequency- and amplitude-dependent fashion, that can be monitored on the seconds/minutes timescale using dissolution dynamic nuclear polarization. Spectroscopic imaging further allowed the in vivo visualization of uptake, transformation and distribution of the tracer and products, in fast-twitch glycolytic and in slow-twitch oxidative muscle fiber groups. While these studies open vistas in time and sensitivity for metabolic functional magnetic resonance studies in muscle, the simplicity of our approach makes this technique amenable to a wide range of functional metabolic tracer studies.

摘要

测量刺激后新陈代谢的时间和空间依赖性反应是功能磁共振成像的核心。在聚焦于水的单一共振时,通过监测代谢物自身产生的时间反应(即功能磁共振波谱),可能会获得更多见解。然而,由于功能时间尺度短且天然代谢物浓度低,实时进行这些测量面临严峻挑战。溶解动态核极化是一种新兴技术,它有可能缓解这一问题,因为它能大幅提高灵敏度,使人们能够在单次扫描中探测低浓度示踪剂和产物。尽管如此,这种超极化方法的传统实施方式并不直接适用于实时功能设置所需的重复采集。这项工作提出了一种用于超极化代谢物功能磁共振的策略,该策略绕过了这一限制,并通过同步刺激触发的多剂量注射代谢示踪剂13C1 - 丙酮酸,实现了对实时代谢变化的观察。通过专门设计的范例来揭示小鼠后肢骨骼肌激活的体内阈值,展示了这种新方法,该范例涉及13C1 - 丙酮酸向13C1 - 乳酸和13C1 - 丙氨酸的转化。这些后肢功能研究表明,分级骨骼肌刺激会以频率和幅度依赖性方式导致糖酵解代谢相应增加,使用溶解动态核极化可以在秒/分钟时间尺度上进行监测。光谱成像进一步实现了在快速糖酵解和慢速氧化肌纤维组中对示踪剂及其产物的摄取、转化和分布进行体内可视化。虽然这些研究为肌肉代谢功能磁共振研究在时间和灵敏度方面开辟了新前景,但我们方法的简单性使该技术适用于广泛的功能代谢示踪剂研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a917/4000219/740b22252fa1/pone.0096399.g001.jpg

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