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3-T临床扫描仪上的超短TE(UTE)MRI序列能否直接检测来自胶原蛋白质子的信号:皮质骨和跟腱标本的冻干及D2O交换研究

Can ultrashort-TE (UTE) MRI sequences on a 3-T clinical scanner detect signal directly from collagen protons: freeze-dry and D2 O exchange studies of cortical bone and Achilles tendon specimens.

作者信息

Ma Ya-Jun, Chang Eric Y, Bydder Graeme M, Du Jiang

机构信息

Department of Radiology, University of California, San Diego, CA, USA.

Radiology Service, VA San Diego Healthcare System, San Diego, CA, USA.

出版信息

NMR Biomed. 2016 Jul;29(7):912-7. doi: 10.1002/nbm.3547. Epub 2016 May 5.

Abstract

Ultrashort-TE (UTE) sequences can obtain signal directly from short-T2 , collagen-rich tissues. It is generally accepted that bound and free water can be detected with UTE techniques, but the ability to detect protons directly on the collagen molecule remains controversial. In this study, we investigated the potential of UTE sequences on a 3-T clinical scanner to detect collagen protons via freeze-drying and D2 O-H2 O exchange studies. Experiments were performed on bovine cortical bone and human Achilles tendon specimens, which were either subject to freeze-drying for over 66 h or D2 O-H2 O exchange for 6 days. Specimens were imaged using two- and three-dimensional UTE with Cones trajectory techniques with a minimum TE of 8 μs at 3 T. UTE images before treatment showed high signal from all specimens with bi-component T2 * behavior. Bovine cortical bone showed a shorter T2 * component of 0.36 ms and a longer T2 * component of 2.30 ms with fractions of 78.2% and 21.8% by volume, respectively. Achilles tendon showed a shorter T2 * component of 1.22 ms and a longer T2 * component of 15.1 ms with fractions of 81.1% and 18.9% by volume, respectively. Imaging after freeze-drying or D2 O-H2 O exchange resulted in either the absence or near-absence of signal. These results indicate that bound and free water are the sole sources of UTE signal in bovine cortical bone and human Achilles tendon samples on a clinical 3-T scanner. Protons on the native collagen molecule are not directly visible when imaged using UTE sequences. Copyright © 2016 John Wiley & Sons, Ltd.

摘要

超短回波时间(UTE)序列可直接从短T2、富含胶原蛋白的组织中获取信号。人们普遍认为,UTE技术能够检测结合水和自由水,但直接在胶原蛋白分子上检测质子的能力仍存在争议。在本研究中,我们通过冷冻干燥和D2O-H2O交换研究,探讨了3-T临床扫描仪上UTE序列检测胶原蛋白质子的潜力。实验在牛皮质骨和人跟腱标本上进行,标本要么经过超过66小时的冷冻干燥,要么进行6天的D2O-H2O交换。使用具有圆锥轨迹技术的二维和三维UTE对标本进行成像,在3-T时最小回波时间为8μs。处理前的UTE图像显示所有标本均有高信号,呈现双组分T2行为。牛皮质骨显示较短的T2组分为0.36ms,较长的T2组分为2.30ms,体积分数分别为78.2%和21.8%。跟腱显示较短的T2组分为1.22ms,较长的T2*组分为15.1ms,体积分数分别为81.1%和18.9%。冷冻干燥或D2O-H2O交换后的成像导致信号缺失或几乎缺失。这些结果表明,在临床3-T扫描仪上,结合水和自由水是牛皮质骨和人跟腱样本中UTE信号的唯一来源。使用UTE序列成像时,天然胶原蛋白分子上的质子不可直接见。版权所有©2016约翰·威利父子有限公司。

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