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啮齿动物输入函数的测量:挑战与解决方案。

Measurement of input functions in rodents: challenges and solutions.

作者信息

Laforest Richard, Sharp Terry L, Engelbach John A, Fettig Nicole M, Herrero Pilar, Kim Joonyoung, Lewis Jason S, Rowland Douglas J, Tai Yuan-Chuan, Welch Michael J

机构信息

Division of Radiological Sciences, Mallinckrodt Institute of Radiology, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

Nucl Med Biol. 2005 Oct;32(7):679-85. doi: 10.1016/j.nucmedbio.2005.06.012.

Abstract

INTRODUCTION

Tracer kinetic modeling used in conjunction with positron emission tomography (PET) is an excellent tool for the noninvasive quantification of physiological, biological and molecular processes and their alterations due to disease. Currently, complex multi-compartment modeling approaches are being applied in a variety of clinical studies to determine myocardial perfusion, viability and glucose utilization as well as fatty acid metabolism and oxidation in the normal and diseased heart. These kinetic models require two key measurements of tracer activity over time, tracer activity in arterial blood (input function) and its corresponding activity in the organ of interest. The alteration in the time course of tracer activity as it travels from blood to the organ of interest describes the kinetics of the tracer. To be able to implement these approaches in rodent models of disease using small-animal PET (microPET), it is imperative that the input function is measured accurately.

METHODS

The blood input functions in rodent experiments were obtained by (1) direct blood sampling, (2) direct measurement of blood activity by a beta-detecting probe that counts the activity in the blood, (3) an arterial-venous bypass (A/V shunt), (4) factor analysis of dynamic structures from dynamic PET images and (5) measurement from region-of-interest (ROI) analysis of dynamic PET images. Direct blood sampling was used as the reference standard to which the results of the other techniques were compared.

RESULTS

Beta probes are difficult to operate and may not provide accurate blood input functions unless they are used intravenously, which requires complicated microsurgery. A similar limitation applies to the A/V shunt. Factor analysis successfully extracts the blood input function for mice and rats. The ROI-based method is less accurate due to limited image resolution of the PET system, which results in severe partial volume effect and spillover from myocardium.

CONCLUSION

The current reference standard, direct blood sampling, is more invasive and has limited temporal resolution. With current imaging technology, image-based extraction of blood input functions is possible by factor analysis, while forthcoming technological developments are likely to allow extraction of input function directly from the images. These techniques will reduce the level of complexity and invasiveness for animal experiments and are likely to be used more widely in the future.

摘要

引言

与正电子发射断层扫描(PET)结合使用的示踪动力学建模是一种用于对生理、生物和分子过程及其因疾病引起的改变进行无创定量分析的优秀工具。目前,复杂的多室建模方法正应用于各种临床研究中,以确定正常和患病心脏中的心肌灌注、存活能力以及葡萄糖利用情况,还有脂肪酸代谢和氧化情况。这些动力学模型需要随时间对示踪剂活性进行两项关键测量,即动脉血中的示踪剂活性(输入函数)及其在感兴趣器官中的相应活性。示踪剂活性从血液传输到感兴趣器官过程中的时间进程变化描述了示踪剂的动力学。为了能够在使用小动物PET(微型PET)的疾病啮齿动物模型中应用这些方法,准确测量输入函数至关重要。

方法

啮齿动物实验中的血液输入函数通过以下方式获得:(1)直接采血,(2)使用能对血液中的活性进行计数的β探测仪直接测量血液活性,(3)动静脉分流(A/V分流),(4)对动态PET图像进行动态结构的因子分析,以及(5)对动态PET图像进行感兴趣区域(ROI)分析测量。直接采血用作参考标准,将其他技术的结果与之进行比较。

结果

β探测仪操作困难,除非静脉内使用,否则可能无法提供准确的血液输入函数,而静脉内使用需要复杂的显微手术。类似的局限性也适用于A/V分流。因子分析成功提取了小鼠和大鼠的血液输入函数。基于ROI的方法由于PET系统图像分辨率有限而不太准确,这会导致严重的部分容积效应和心肌溢出。

结论

当前的参考标准——直接采血——具有更高的侵入性且时间分辨率有限。利用当前的成像技术,通过因子分析可以基于图像提取血液输入函数,而即将到来的技术发展可能会允许直接从图像中提取输入函数。这些技术将降低动物实验的复杂程度和侵入性,并且未来可能会得到更广泛的应用。

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