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内源性大量可移动蛋白质的双频照射CEST-MRI

Dual-frequency irradiation CEST-MRI of endogenous bulk mobile proteins.

作者信息

Goerke Steffen, Breitling Johannes, Zaiss Moritz, Windschuh Johannes, Kunz Patrick, Schuenke Patrick, Paech Daniel, Longo Dario L, Klika Karel D, Ladd Mark E, Bachert Peter

机构信息

Division of Medical Physics in Radiology, German Cancer Research Center (DKFZ), Heidelberg, Germany.

Department of High-field Magnetic Resonance, Max-Planck-Institute for Biological Cybernetics, Tübingen, Germany.

出版信息

NMR Biomed. 2018 Jun;31(6):e3920. doi: 10.1002/nbm.3920. Epub 2018 Apr 19.

Abstract

A novel MRI contrast is proposed which enables the selective detection of endogenous bulk mobile proteins in vivo. Such a non-invasive imaging technique may be of particular interest for many diseases associated with pathological alterations of protein expression, such as cancer and neurodegenerative disorders. Specificity to mobile proteins was achieved by the selective measurement of intramolecular spin diffusion and the removal of semi-solid macromolecular signal components by a correction procedure. For this purpose, the approach of chemical exchange saturation transfer (CEST) was extended to a radiofrequency (RF) irradiation scheme at two different frequency offsets (dualCEST). Using protein model solutions, it was demonstrated that the dualCEST technique allows the calculation of an image contrast which is exclusively sensitive to changes in concentration, molecular size and the folding state of mobile proteins. With respect to application in humans, dualCEST overcomes the selectivity limitations at relatively low magnetic field strengths, and thus enables examinations on clinical MR scanners. The feasibility of dualCEST examinations in humans was verified by a proof-of-principle examination of a brain tumor patient at 3 T. With its specificity for the mobile fraction of the proteome, its comparable sensitivity to conventional water proton MRI and its applicability to clinical MR scanners, this technique represents a further step towards the non-invasive imaging of proteomic changes in humans.

摘要

提出了一种新型磁共振成像(MRI)造影剂,它能够在体内选择性检测内源性大量可移动蛋白质。这种非侵入性成像技术对于许多与蛋白质表达病理改变相关的疾病,如癌症和神经退行性疾病,可能特别有意义。通过选择性测量分子内自旋扩散以及通过校正程序去除半固体大分子信号成分,实现了对可移动蛋白质的特异性检测。为此,将化学交换饱和转移(CEST)方法扩展到在两个不同频率偏移下的射频(RF)照射方案(双CEST)。使用蛋白质模型溶液证明,双CEST技术允许计算一种图像对比度,该对比度仅对可移动蛋白质的浓度、分子大小和折叠状态的变化敏感。关于在人体中的应用,双CEST克服了在相对低磁场强度下的选择性限制,从而能够在临床MR扫描仪上进行检查。通过对一名3T脑肿瘤患者的原理验证检查,证实了双CEST检查在人体中的可行性。由于其对蛋白质组可移动部分的特异性、与传统水质子MRI相当的灵敏度以及对临床MR扫描仪的适用性,该技术代表了朝着人体蛋白质组学变化的非侵入性成像迈出的又一步。

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