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超极化(13)C-丙酮酸临床成像定量方法的比较

A comparison of quantitative methods for clinical imaging with hyperpolarized (13)C-pyruvate.

作者信息

Daniels Charlie J, McLean Mary A, Schulte Rolf F, Robb Fraser J, Gill Andrew B, McGlashan Nicholas, Graves Martin J, Schwaiger Markus, Lomas David J, Brindle Kevin M, Gallagher Ferdia A

机构信息

Department of Radiology, University of Cambridge, Addenbrooke's Hospital, Cambridge, UK.

Cancer Research UK Cambridge Institute, University of Cambridge, Li Ka Shing Centre, Cambridge, UK.

出版信息

NMR Biomed. 2016 Apr;29(4):387-99. doi: 10.1002/nbm.3468. Epub 2016 Jan 18.

Abstract

Dissolution dynamic nuclear polarization (DNP) enables the metabolism of hyperpolarized (13)C-labelled molecules, such as the conversion of [1-(13)C]pyruvate to [1-(13)C]lactate, to be dynamically and non-invasively imaged in tissue. Imaging of this exchange reaction in animal models has been shown to detect early treatment response and correlate with tumour grade. The first human DNP study has recently been completed, and, for widespread clinical translation, simple and reliable methods are necessary to accurately probe the reaction in patients. However, there is currently no consensus on the most appropriate method to quantify this exchange reaction. In this study, an in vitro system was used to compare several kinetic models, as well as simple model-free methods. Experiments were performed using a clinical hyperpolarizer, a human 3 T MR system, and spectroscopic imaging sequences. The quantitative methods were compared in vivo by using subcutaneous breast tumours in rats to examine the effect of pyruvate inflow. The two-way kinetic model was the most accurate method for characterizing the exchange reaction in vitro, and the incorporation of a Heaviside step inflow profile was best able to describe the in vivo data. The lactate time-to-peak and the lactate-to-pyruvate area under the curve ratio were simple model-free approaches that accurately represented the full reaction, with the time-to-peak method performing indistinguishably from the best kinetic model. Finally, extracting data from a single pixel was a robust and reliable surrogate of the whole region of interest. This work has identified appropriate quantitative methods for future work in the analysis of human hyperpolarized (13)C data.

摘要

溶解动态核极化(DNP)能够对超极化(13)C标记分子的代谢过程进行动态且非侵入性的组织成像,比如[1-(13)C]丙酮酸向[1-(13)C]乳酸的转化。在动物模型中对这种交换反应进行成像已被证明可以检测早期治疗反应,并与肿瘤分级相关。最近完成了首例人体DNP研究,为了实现广泛的临床转化,需要简单可靠的方法来准确探测患者体内的反应。然而,目前对于量化这种交换反应的最合适方法尚无共识。在本研究中,使用体外系统比较了几种动力学模型以及简单的无模型方法。实验采用临床超极化仪、人体3T磁共振系统和光谱成像序列进行。通过使用大鼠皮下乳腺肿瘤来研究丙酮酸流入的影响,在体内比较了定量方法。双向动力学模型是体外表征交换反应最准确的方法,纳入阶跃流入曲线能最好地描述体内数据。乳酸峰时间和曲线下乳酸与丙酮酸面积比是能够准确反映整个反应的简单无模型方法,峰时间法与最佳动力学模型的表现无明显差异。最后,从单个像素提取数据是整个感兴趣区域的一种稳健且可靠的替代方法。这项工作为未来分析人体超极化(13)C数据确定了合适的定量方法。

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