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联合磁共振成像与光谱成像的前列腺癌分子成像方法。

Combined magnetic resonance imaging and spectroscopic imaging approach to molecular imaging of prostate cancer.

作者信息

Kurhanewicz John, Swanson Mark G, Nelson Sarah J, Vigneron Daniel B

机构信息

Magnetic Resonance Science Center, Department of Radiology, University of California-San Francisco, San Francisco, California 94143-1290, USA.

出版信息

J Magn Reson Imaging. 2002 Oct;16(4):451-63. doi: 10.1002/jmri.10172.

Abstract

Magnetic resonance spectroscopic imaging (MRSI) provides a noninvasive method of detecting small molecular markers (historically the metabolites choline and citrate) within the cytosol and extracellular spaces of the prostate, and is performed in conjunction with high-resolution anatomic imaging. Recent studies in pre-prostatectomy patients have indicated that the metabolic information provided by MRSI combined with the anatomical information provided by MRI can significantly improve the assessment of cancer location and extent within the prostate, extracapsular spread, and cancer aggressiveness. Additionally, pre- and post-therapy studies have demonstrated the potential of MRI/MRSI to provide a direct measure of the presence and spatial extent of prostate cancer after therapy, a measure of the time course of response, and information concerning the mechanism of therapeutic response. In addition to detecting metabolic biomarkers of disease behavior and therapeutic response, MRI/MRSI guidance can improve tissue selection for ex vivo analysis. High-resolution magic angle spinning ((1)H HR-MAS) spectroscopy provides a full chemical analysis of MRI/MRSI-targeted tissues prior to pathologic and immunohistochemical analyses of the same tissue. Preliminary (1)H HR-MAS spectroscopy studies have already identified unique spectral patterns for healthy glandular and stromal tissues and prostate cancer, determined the composition of the composite in vivo choline peak, and identified the polyamine spermine as a new metabolic marker of prostate cancer. The addition of imaging sequences that provide other functional information within the same exam (dynamic contrast uptake imaging and diffusion-weighted imaging) have also demonstrated the potential to further increase the accuracy of prostate cancer detection and characterization.

摘要

磁共振波谱成像(MRSI)提供了一种非侵入性方法,用于检测前列腺细胞溶质和细胞外空间中的小分子标志物(传统上是代谢物胆碱和柠檬酸盐),并且与高分辨率解剖成像结合进行。最近对前列腺切除术前患者的研究表明,MRSI提供的代谢信息与MRI提供的解剖信息相结合,可以显著改善对前列腺内癌症位置和范围、包膜外扩散以及癌症侵袭性的评估。此外,治疗前和治疗后的研究已经证明了MRI/MRSI在提供治疗后前列腺癌的存在和空间范围的直接测量、反应时间过程的测量以及有关治疗反应机制信息方面的潜力。除了检测疾病行为和治疗反应的代谢生物标志物外,MRI/MRSI引导还可以改善用于离体分析的组织选择。高分辨率魔角旋转((1)H HR-MAS)波谱在对同一组织进行病理和免疫组织化学分析之前,对MRI/MRSI靶向的组织进行全面的化学分析。初步的(1)H HR-MAS波谱研究已经确定了健康腺组织、基质组织和前列腺癌的独特光谱模式,确定了体内胆碱复合峰的组成,并将多胺精胺鉴定为前列腺癌的一种新的代谢标志物。在同一检查中添加提供其他功能信息的成像序列(动态对比剂摄取成像和扩散加权成像)也显示出进一步提高前列腺癌检测和特征描述准确性的潜力。

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