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超短回波时间化学位移成像(UTE-CSI)。

Ultrashort TE chemical shift imaging (UTE-CSI).

作者信息

Robson Matthew D, Tyler Damian J, Neubauer Stefan

机构信息

University of Oxford Centre for Clinical Magnetic Resonance Research, MRS Unit, John Radcliffe Hospital, Oxford, UK.

出版信息

Magn Reson Med. 2005 Feb;53(2):267-74. doi: 10.1002/mrm.20344.

Abstract

A fundamental modification to the conventional chemical shift imaging (CSI) method is described that improves the imaging of species with short T2's (i.e., less than approximately 2 ms). This approach minimizes the delay before each k-space point is collected. This results in different time delays, T(d), for different free induction decay (FID) acquisitions in k-space. On a clinical 1.5 T system this yields an effective delay due to transmit/receive switching of 70 micros and an echo time (TE) from the center of the excitation pulse to the center of k-space of 170 micros, as compared with 1-2 ms for conventional CSI techniques. Using this method, the signal decay before acquisition is greatly reduced, thus enabling imaging of species with very short T2)(e.g., 200 micros) and increasing the signal-to-noise ratio (SNR) of species with intermediate T2. Increases in the SNR of the short T2 components of 23Na in the heart, and 31P acquisitions of bone are about 27% and 400%, respectively, compared to an optimized conventional CSI approach. The imperfections of this approach are also described, and the magnitude of the resultant image artifacts is quantified for different practical imaging situations. These artifacts were not found to be significant in the described applications. This new method allows us to obtain information on short T2 components without degrading the image quality from long T2 components.

摘要

本文描述了对传统化学位移成像(CSI)方法的一种根本性改进,该改进提高了对具有短T2值(即小于约2毫秒)物质的成像能力。这种方法将采集每个k空间点之前的延迟减至最小。这导致在k空间中不同的自由感应衰减(FID)采集具有不同的时间延迟T(d)。在临床1.5T系统上,由于发射/接收切换产生的有效延迟为70微秒,从激发脉冲中心到k空间中心的回波时间(TE)为170微秒,而传统CSI技术的这两个值为1 - 2毫秒。使用这种方法,采集前的信号衰减大大降低,从而能够对具有非常短T2值(例如200微秒)的物质进行成像,并提高了具有中等T2值物质的信噪比(SNR)。与优化后的传统CSI方法相比,心脏中23Na短T2成分的SNR增加约27%,骨骼的31P采集的SNR增加约400%。本文还描述了这种方法的不足之处,并针对不同的实际成像情况对所产生图像伪影的大小进行了量化。在所描述的应用中,这些伪影并不显著。这种新方法使我们能够获取关于短T2成分的信息,而不会降低长T2成分的图像质量。

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