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小动物单光子发射计算机断层扫描及其在分子成像技术体系中的地位。

Small animal SPECT and its place in the matrix of molecular imaging technologies.

作者信息

Meikle Steven R, Kench Peter, Kassiou Michael, Banati Richard B

机构信息

School of Medical Radiation Sciences, Faculty of Health Sciences, University of Sydney, PO Box 170, Lidcombe, NSW 1825, Sydney, Australia.

出版信息

Phys Med Biol. 2005 Nov 21;50(22):R45-61. doi: 10.1088/0031-9155/50/22/R01. Epub 2005 Oct 24.

Abstract

Molecular imaging refers to the use of non-invasive imaging techniques to detect signals that originate from molecules, often in the form of an injected tracer, and observe their interaction with a specific cellular target in vivo. Differences in the underlying physical principles of these measurement techniques determine the sensitivity, specificity and length of possible observation of the signal, characteristics that have to be traded off according to the biological question under study. Here, we describe the specific characteristics of single photon emission computed tomography (SPECT) relative to other molecular imaging technologies. SPECT is based on the tracer principle and external radiation detection. It is capable of measuring the biodistribution of minute (<10(-10) molar) concentrations of radio-labelled biomolecules in vivo with sub-millimetre resolution and quantifying the molecular kinetic processes in which they participate. Like some other imaging techniques, SPECT was originally developed for human use and was subsequently adapted for imaging small laboratory animals at high spatial resolution for basic and translational research. Its unique capabilities include (i) the ability to image endogenous ligands such as peptides and antibodies due to the relative ease of labelling these molecules with technetium or iodine, (ii) the ability to measure relatively slow kinetic processes (compared with positron emission tomography, for example) due to the long half-life of the commonly used isotopes and (iii) the ability to probe two or more molecular pathways simultaneously by detecting isotopes with different emission energies. In this paper, we review the technology developments and design tradeoffs that led to the current state-of-the-art in SPECT small animal scanning and describe the position SPECT occupies within the matrix of molecular imaging technologies.

摘要

分子成像指的是利用非侵入性成像技术来检测源自分子的信号,这些信号通常以注射示踪剂的形式存在,并在体内观察其与特定细胞靶点的相互作用。这些测量技术背后物理原理的差异决定了信号的灵敏度、特异性以及可能的观察时长,而这些特性必须根据所研究的生物学问题进行权衡。在此,我们描述单光子发射计算机断层扫描(SPECT)相对于其他分子成像技术的具体特性。SPECT基于示踪剂原理和外部辐射检测。它能够以亚毫米分辨率测量体内微量(<10^(-10)摩尔)放射性标记生物分子的生物分布,并对它们所参与的分子动力学过程进行定量分析。与其他一些成像技术一样,SPECT最初是为人类应用而开发的,随后被用于对小型实验动物进行高空间分辨率成像,以开展基础研究和转化研究。其独特能力包括:(i)由于用锝或碘标记这些分子相对容易,因此能够对诸如肽和抗体等内源性配体进行成像;(ii)由于常用同位素的半衰期较长,能够测量相对缓慢的动力学过程(例如,与正电子发射断层扫描相比);(iii)能够通过检测具有不同发射能量的同位素同时探测两条或更多分子途径。在本文中,我们回顾了导致SPECT小动物扫描达到当前先进水平的技术发展和设计权衡,并描述了SPECT在分子成像技术矩阵中所占据的位置。

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