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Self-reinforced Hybrid Polyethylene/MCM-41 Nanocomposites: In-situ Polymerisation and Effect of MCM-41 Content on Rigidity

机译:自增强杂化聚乙烯/ MCM-41纳米复合材料:原位聚合和MCM-41含量对刚性的影响

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摘要

Dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI) is a widely used technique for assessing tissue physiology. Spoiled gradient echo (SPGR) pulse sequences are one of the most common methods for acquisition of DCE-MRI data, providing high temporal and spatial resolution with strong T(1)-weighting. Conversion of SPGR signal to concentration is briefly reviewed, and a new closed-form expression for concentration measurement uncertainty for finite signal-to-noise ratio (SNR) and baseline scan time is derived. This result is applicable to arbitrary concentration-dependent relaxation rate and is valid over the same domain as the theoretical SPGR signal equation. Expressions for the lower and upper bounds on measurable concentration are also derived. The existence of a concentration- and tissue-dependent optimal flip angle that minimizes concentration uncertainty is demonstrated and it is shown that, for clinically relevant pulse sequence parameters, this optimal flip angle is significantly larger than the corresponding Ernst angle. Analysis of three pulse sequences from the DCE-MRI literature shows that optimization of flip angle using the methods discussed here leads to potential improvements of 10-1166% in effective SNR over the 0.5-5.0 mM concentration range with minimal or no loss of measurement accuracy down to 0.1 mM. In vivo data from three study patients provide further support for our theoretical expression for concentration measurement uncertainty, with predicted and experimental estimates agreeing to within +/- 30%. Equations for concentration bias resulting from biases in flip angle and from pre-contrast relaxation time and contrast relaxivity (both longitudinal and transverse) are also derived in closed-form. The resulting equations show the potential for significant contributions to bias in concentration measurement arising from even relatively small mis-specification of flip angle and/or pre-contrast longitudinal relaxation time, particularly at high contrast concentrations.
机译:动态对比增强磁共振成像(DCE-MRI)是一种广泛用于评估组织生理的技术。损坏的梯度回波(SPGR)脉冲序列是DCE-MRI数据采集的最常用方法之一,可提供高时间和空间分辨率以及强大的T(1)加权。简要回顾了SPGR信号到浓度的转换,并导出了一个新的闭式表达式,用于表示有限信噪比(SNR)和基线扫描时间的浓度测量不确定度。该结果适用于任意浓度依赖性弛豫率,并且在与理论SPGR信号方程相同的域中有效。还导出了可测量浓度的上下限表达式。证明了最小化浓度不确定性的依赖于浓度和组织的最佳翻转角的存在,并且表明,对于临床相关的脉冲序列参数,该最佳翻转角明显大于对应的恩斯特角。对DCE-MRI文献中的三个脉冲序列的分析表明,使用此处讨论的方法优化翻转角可以在0.5-5.0 mM的浓度范围内将有效SNR潜在提高10-1166%,而测量精度的损失很小或没有损失低至0.1 mM。来自三名研究患者的体内数据为浓度测量不确定度的理论表达提供了进一步的支持,预测和实验估计值均在+/- 30%之内。还可以以封闭形式导出由翻转角的偏差以及预对比弛豫时间和对比度弛豫率(纵向和横向)引起的浓度偏差方程。所得方程式表明,即使翻转角和/或预对比的纵向弛豫时间相对较小(特别是在高对比度浓度下),也会因错误指定错误而对浓度测量产生重大影响。

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