基于改进非线性拟合的核磁共振T2谱多指数反演

核磁共振T₂谱多指数反演算法是开展复杂体系样品核磁共振(NMR)弛豫研究最重要的数学工具. 常用的T₂谱多指数反演算法一般都是事先给出弛豫时间T₂分布的布点, 然后转化为线性拟合问题进行求解. 在求解的T₂谱较为分散的时候, 反演得到的T₂谱精确度不高, 分辨率较低. 非线性拟合是解决这个问题的有效办法. 本文针对分散T₂谱反演利用非线性拟合时遇到的初值依赖及运算复杂问题, 利用线性回归最小二乘方法, 改进了其中的带非负约束非线性优化模型, 将搜索的反演参数从T₂, f 减少为T₂, 加快了收敛速度, 减少了对初值的依赖, 提高了反演精度, 使算法更加稳健. 通过用改进的Levenberg-Marquardt算法和差分进化算法进行计算机模拟反演及实验数据反演, 验证了改进方法在核磁共振T₂ 谱反演中的有效性.     

油井样品NMR T2谱的影响因素及T2截止值的确定方法

T₂ 谱是核磁共振（NMR）测、录井技术应用与解释、评价的基础. 岩样T₂ 谱受仪器测量参数、样品性质（岩性、颗粒大小、样品粒度、样品干湿状态、孔隙流体含量及性质、磁化率、润湿性）及地层水矿化度等因素的影响. T₂ 截止值是T₂ 谱中最重要的参数之一,选取的科学性与准确性直接影响到核磁共振测量结果. 通过文献查询,对T2 谱的影响因素及T₂ 截止值的确定方法进行了分析.     

基于磁共振弛豫时间实现加权像和压脂技术

磁共振成像是根据生物磁性核在磁场中表现的共振特性进行成像的新技术,其中弛豫时间是实现和控制成像的重要物理量.本文使用磁共振成像实验仪,对相关样品的纵向弛豫时间T₁、横向弛豫时间T₂进行测量,并且基于不同弛豫时间采用自旋回波序列实现T₁、T₂加权像,用反转恢复成像序列实现磁共振成像对脂肪的抑制.     

磁共振成象诊断出血性胆囊炎——离体及活体研究

在离体研究的基础上,对三个出血性胆囊炎的病人术前做出诊断,出血性胆囊炎可分为混合性及非混合性.在离体实验中,如果血液未与胆汁混合,T₁加权象可发现加于10mL胆汁中的0.2mL的血液表现为高信号区;质子密度加权象可发现加于10mL,胆汁中的0.4mL血液表现为稍高信号区;T₂加权象对此不敏感.如果血液与胆汁完全混合,在所有采用的磁共振成象上均使胆汁信号增高.非混合性出血性胆囊炎的磁共振成象具有特征性:在T₁加权象及质子密度加权象胆囊内有高信号区,T₂加权象此区为等信号、低信号或其中心为低信号周围与胆汁相接的为高信号。混合性出血性胆囊炎在所采用的磁共振成象图象中,相对于肝脏,胆囊内容物表现为均匀高信号,临床资料及胆囊壁、胆囊周围渗出有助于这种出血性胆囊炎的诊断.     

玉米胚芽胚乳中油水动态行为的NMR研究

应用核磁共振时域二维弛豫相关谱分析的方法,对玉米胚芽的核磁共振弛豫特性进行了研究.对以下三种样品进行了测定:(1)胚芽不含油(用化学方法蒸馏出)但是含有不同百分含量的水;(2)胚芽不含水(真空蒸发)但是含有不同百分含量的油;(3)含有不同百分含量的水的胚乳水系统.研究表明随着水含量的增加水的纵向弛豫时间T₁减小,表明水与胚芽基质具有强烈的相互作用,而油的纵向弛豫时间T₁随着油含量的增加变化很小,表明油与胚芽基质之间没有大的相互作用,油几乎独立地处在胚芽中;对低水分(少于5%)玉米胚芽水系统,结果表明水是束缚于胚芽基质上,而油则是以油胞的形式存在于胚芽中.在玉米胚芽水系统中有两个T₁弛豫成分,长T₁弛豫成分从基质到水的交换率为57s^-1;从水到基质的交换率为113s^-1.短T₁成分从基质到水的交换率为245s^-1;从水到基质的交换率为821s^-1.在低水合状态下,胚乳水系统仅有一个T₁弛豫成分.胚乳到水的交换率高于37s^-1.     

常规T2像和组织学研究APPswe/PS1dE9转基因小鼠模型

用常规的T₂加权像研究阿尔茨海默病双转基因APPswe/PS1dE9小鼠模型,拟合了海马和顶叶皮层的T₂,并用组织学方法研究了APP/PS1小鼠在这2个感兴趣区域随年龄相关的淀粉样斑块病理的发展及铁质的沉积. T₂拟合的结果显示,较高月龄的APP/PS1小鼠相比于低月龄APP/PS1小鼠T₂有升高但不显著,各月龄组APP/PS1小鼠与同窝生非阳性小鼠之间也无明显差异;组织学的结果则显示年龄相关的淀粉样斑块的增多,铁质在16月龄的APP/PS1小鼠脑区中有明显沉积且和斑块具有“共域性”. 两方面的实验结果提示：在该模型淀粉样斑块沉积病理发展的早期,这2个脑区的T₂并不能作为特异性的病理发展的标志.     

不同能量的氦原子与同位素分子H2(D2，T2)碰撞分波截面的理论计算

用Tang-Toennies势模型和密耦近似方法计算了不同能量下惰性气体原子He与H₂及其同位素D₂,T₂替代碰撞体系的振转激发碰撞截面. 通过分析He-H₂(D₂,T₂)各碰撞体系分波截面的差异,总结出在H₂分子的对称同位素替代情形下He-H₂(D₂,T₂)碰撞体系分波截面随量子数和体系 关键词： 散射截面 密耦方法 同位素     

小白鼠肌肉组织的NMR质子自旋交换分析

本文在Zimmerman-Brittin两相质子交换核磁共振弛豫模型基础上,分析了NMR弛豫实验中检测信号与各相表现和本征弛豫多数的关系,编写了自动化处理实验数据的计算机程序,这一技术可用于复相系统中不同成分的NMR表现和本征弛豫特性研究中,本文中的样品是选用健康新鲜的小白鼠肌肉,没加任何处理,用h-h,s-h,s-s脉冲序列,反转恢复法(π-τ-π/2)在强场下(0.92T)做T₁、T₂测定实验,分析结果表明本征弛豫参数T₁=1050ms,T₂=4500μs的成分是由肌肉中的"自由水"引起的,其质子相对含量为69%;本征弛豫参数T₁=530ms,T₂=26μs的成分是由肌肉中的"束附水"引起的,其质子相对含量为9%,本征弛豫多数T₁=530ms,T₂=1250μs的成分是由肌肉中的各种大分子和有机物引起的,其质子相对含量为9%,本征弛豫参数T₁=470ms,T₂=1250μs的成分由样品中的脂肪引起的,其质子相对含量为13%,在肌肉组织中的质子与水中质子之间有强烈的交换作用,其交换率k=1000s^-1.在脂肪中的质子与其它成分之间没有交换作用。     

水/甲醇混合溶剂中PNIPAAM相变行为的NMR研究

通过液体核磁共振（NMR）谱以及动力学参数测量研究了聚N-异丙基丙烯酰胺（PNIPAAM）在水和甲醇的混合溶液中的相变行为. 通过PNIPAAM在水和甲醇混合溶剂中¹H核磁共振谱、纵向弛豫时间T₁、横向弛豫时间T₂和自扩散系数D随甲醇含量的变化发现,大分子在发生相变时,在¹H核磁共振谱中伴随有宽峰的出现和消失,同时弛豫时间和自扩散系数均有显著变化. 实验结果表明,¹H NMR谱图以及弛豫时间和自扩散系数等多种核磁共振参数可以用来灵敏表征PNIPAAM在水和甲醇混合溶液中的相变行为     

慢性电刺激海马结构诱发大鼠脑磁共振成像异常信号分析

为探讨海马结构(hippocampal formation)功能失衡与癫痫源性脑损伤的关系,本工作采用 慢性强直电刺激大鼠海马(hippocampus, HPC) CA1顶树突区（apical dendrite region, A DR）或齿状回（dentate gyrus, DG）诱发大鼠癫痫模型,一天一次,连续刺激6～8天后, 观察人工致痫灶以外的横向弛豫时间加权的核磁共振(T₂ weighted magnetic reson ance im age, T₂-WI) 绝对信号值变化（片厚1mm）,以及深部电图和原发性湿狗颤抖（pri mary wet dog shakes, WEDS）,并对被检测动物T₂-WI信号异常的相应脑区进行组织学鉴定. 结果表明：（1）电 刺激大 鼠ADR或DG的作用基本相似,引起深部电图的癫痫样电活动和侧脑室区域T₂值增强.（2）含有电极尖端痕迹的核磁共振（magnetic resonance image,MRI）脑切片出现对称性腹部侧脑室区域T₂值增强,连续向后1mm取MRI脑切片进行观察发现,对侧腹部侧脑室区域信号异常. （3）组织学切片观察到：MRI检测的侧脑室区域T₂-WI信号增强与组织切片的侧脑室扩大相吻合,可见扩大的侧脑室中脉络丛上皮细胞病理性增生现象. 提示：在大鼠癫痫点燃现象出现之前,过度激活DG或ADR均可引起相似的早期癫痫源性脑损伤.     

Cerebral ischemic injury model of rat demonstrated withT 2-weighted magnetic resonance imaging

A photochemical reaction model of focal cerebral ischemic injury of rat was demonstrated by means of enhancedT ₂-weighted magnetic resonance imaging. The cerebral ischemia model was made using vein injection of rose bengal and irradiation by a beam of a cw laser with the wave-length of 514 nm. The ischemic injury region in rat brain can be found clearly in theT ₂-weighted magnetic resonance images in one hour, this time was calculated from the beginning of the laser irradiation to the end of the NMR data acquisition. It suggests thatT ₂-weighted imaging can find cerebral ischemia earlier than several hours after the onset of ischemia given in other papers. It also confirms that theT ₂-weighted magnetic resonance imaging approach should be of great potential to be applied in studying the cerebral ischemia.     

Comparison of T2 and LASER T2dagger image contrast in a rat model of acute cerebral ischemia

Previous studies have shown that T2(dagger)-weighted magnetic resonance images acquired using localization by adiabatic selective refocusing (LASER) can provide early tissue contrast following ischemia, possibly due to alterations in microscopic susceptibility within the tissue. The purpose of this study was to make a direct in vivo comparison of T2-, T2(dagger)- and diffusion-weighted image contrast during acute ischemia. Acute middle cerebral artery (MCA) occlusion was attempted in 14 rats using a modified Tamura approach incorporating electrocoagulation of the left MCA. T2(dagger)-weighted LASER images (Echo Time [TE]=108 ms), T2-weighted Carr-Purcell-Meiboom-Gill (CPMG) images (TE=110 ms) and diffusion-weighted images (b value=105 s/mm(2)) were acquired at 4 T within 1.5 h of ischemia onset. Tissue contrast in the MCA territory was quantified for histologically verified ischemic tissue (n=6) and in sham controls (n=4). T2(dagger)-weighted LASER images demonstrated greater contrast compared to the T2-weighted CPMG images, and more focal contrast compared to the diffusion-weighted images, suggesting different contrast mechanisms were involved.     

A fast screening protocol for carotid plaques imaging using 3D multi-contrast MRI without contrast agent

PurposeTo implement a fast (~ 15 min) MRI protocol for carotid plaque screening using 3D multi-contrast MRI sequences without contrast agent on a 3 Tesla MRI scanner.Materials and methods7 healthy volunteers and 25 patients with clinically confirmed transient ischemic attack or suspected cerebrovascular ischemia were included in this study. The proposed protocol, including 3D T1-weighted and T2-weighted SPACE (variable-flip-angle 3D turbo spin echo), and T1-weighted magnetization prepared rapid acquisition gradient echo (MPRAGE) was performed first and was followed by 2D T1-weighted and T2-weighted turbo spin echo, and post-contrast T1-weighted SPACE sequences. Image quality, number of plaques, and vessel wall thicknesses measured at the intersection of the plaques were evaluated and compared between sequences.ResultsAverage examination time of the proposed protocol was 14.6 min. The average image quality scores of 3D T1-weighted, T2-weighted SPACE, and T1-weighted magnetization prepared rapid acquisition gradient echo were 3.69, 3.75, and 3.48, respectively. There was no significant difference in detecting the number of plaques and vulnerable plaques using pre-contrast 3D images with or without post-contrast T1-weighted SPACE. The 3D SPACE and 2D turbo spin echo sequences had excellent agreement (R = 0.96 for T1-weighted and 0.98 for T2-weighted, p < 0.001) regarding vessel wall thickness measurements.ConclusionThe proposed protocol demonstrated the feasibility of attaining carotid plaque screening within a 15-minute scan, which provided sufficient anatomical coverage and critical diagnostic information. This protocol offers the potential for rapid and reliable screening for carotid plaques without contrast agent.     

High-resolution ultrahigh-field MRI of stroke

BACKGROUND: Ultrahigh-field MRI at 8 T offers unprecedented resolution for imaging brain structures and microvasculature. OBJECTIVE: The aim of this study is to apply high-resolution MRI for stroke imaging and to characterize findings at 1.5 and 8 T. METHODS: Seventeen subjects with minor ischemic infarcts were studied using T2-weighted gradient echo (GE) and rapid acquisition with relaxation enhancement (RARE) images at 8 T with resolution up to 200 microm. In 10 subjects, T1- and T2-weighted fast spin echo (FSE) and fluid-attenuated inversion recovery (FLAIR) images were also acquired at 1.5-T MRI. RESULTS: The 8-T images showed infarcts as sharply demarcated areas of high-signal intensity (n=21) and revealed more infarctions than 1.5-T images (n=14) (P<.003). The low-signal intensity areas that surrounded infarctions were suggestive of hemosiderin deposits. The 8-T characteristics of microvessels terminating within the infractions were distinct from normal vasculature. The 8-T images revealed an angioma at the site of a second stroke, not apparent on 1.5-T images. CONCLUSIONS: Ultrahigh-field MRI at 8 T is feasible for stroke imaging. The 8-T MRI visualized infarcts and microvasculature with high resolution, revealing infarcts and vascular pathologies that were not apparent at 1.5 T.     

Renal-related perinephric fluid collections: MRI findings

We retrospectively reviewed MR studies on 10 patients with renal-related perinephric fluid collections who underwent MRI in three institutions between January 2001 and August 2004. All patients underwent MRI of the abdomen and T1-weighted, T2-weighted and serial contrast-enhanced images, including delayed-phase contrast-enhanced images 10-12 min after contrast injection, were obtained. Perinephric fluid collections in 5 patients revealed MRI findings of simple fluid content (i.e., hypointense on T1-weighted images and hyperintense on T2-weighted images). In another 5 patients, a complex perinephric fluid content (i.e., mixed hyper/hypointense on T1-weighted images and mixed hypo/hyperintense on T2-weighted images compatible with blood breakdown products and pus) was observed. In 5 patients, contrast extravasation on late-phase images that was compatible with urine leak was demonstrated. Our results suggest that MRI may determine the content of perinephric fluid collections on noncontrast T1-weighted and T2-weighted images and that contrast extravasation on late-phase images is associated with urine extravasation from renal collecting systems.     

Magnetic resonance imaging of burn injury in rats.

In-vivo magnetic resonance imaging (MRI) studies have been performed to follow pathological changes induced by 3-sec and 10-second burns on eleven rat tails. T1-weighted, T2-weighted, density-weighted, and water-suppressed images were acquired immediately after and four days following thermal injury. MRI results were correlated with histology. For 3-sec burns, both edema and lipids contributed significantly to the hyperintensity seen on MRI at the site of injury. For 10-sec burns, edema was the major contributor to hyperintensity. Quantitative comparisons indicated the intensity and spatial extent of the edema signal to be most indicative of the degree of injury. MRI also demonstrated potential in determining coagulation necrosis and lipid accumulation at burn sites. These studies indicate the potential of MRI in diagnosing and monitoring burn injuries and therapies.     

Sodium T2*-weighted MR imaging of acute focal cerebral ischemia in rabbits

Changes in T2*-weighted tissue sodium (23Na) signal following acute ischemia may help to identify necrotic tissue and estimate the duration of ischemia. Sodium signal was monitored in a rabbit model of acute (0-4 h) focal cerebral ischemia, using gradient echo 23Na MR images (echo time = 3.2 ms) acquired continuously in 20-min intervals on a 4-Tesla MRI. 2,3,5-Triphenyl-tetrazolium chloride staining was used to identify regions of necrosis. In necrotic tissue, average 23Na image signal intensity decreased by 11% +/- 8% during the first 40 min of ischemia followed by a linear increase (0.19%/min) to 25% +/- 14% greater than baseline after 4 h of ischemia. The time course of 23Na signal change observed in necrotic tissue following focal ischemia in this rabbit model is consistent with an initial decrease in 23Na T2* relaxation time followed by an increase in tissue sodium concentration and provides further evidence that tissue 23Na signal may offer unique information regarding tissue viability that is complementary to other MR imaging techniques.     

MR imaging of radiation osteitis in the sacroiliac joints

The purpose of this study was to analyze magnetic resonance (MR) images of radiation osteitis of sacroiliac joints, retrospectively. Seven patients with radiation osteitis, which was diagnosed by pelvic plain radiographs and CT images, underwent MRI. T(1)-weighted spin echo images and T(2)-weighted fast spin echo images were obtained in all patients. Four patients were examined after gadolinium injection. Major signal changes of radiation osteitis were distributed on the iliac side. T(1)-weighted images showed diffuse low intensity both in sacral and iliac sides. T(2)-weighted images showed very low intensity adjacent to sacroiliac joints, but mixed intensity was illustrated apart from joints, and high intensity in the peripheral areas. Radiation osteitis showed slight to mild, but irregular enhancement in four patients after gadolinium administration. MRI can illustrate abnormal bone change distribution and is useful for diagnosing this entity by characteristic intensity patterns on T(1)-weighted images with and without gadolinium and T(2)-weighted image. However, the diagnosis of accompanied insufficiency fractures in the area of radiation osteitis is occasionally difficult with conventional MRI.     

Neuroprotective effect of agmatine in rats with transient cerebral ischemia using MR imaging and histopathologic evaluation

Purpose

This study aimed to further investigate the effects of agmatine on brain edema in the rats with middle cerebral artery occlusion (MCAO) injury using magnetic resonance imaging (MRI) monitoring and biochemical and histopathologic evaluation.

Materials and methods

Following surgical induction of MCAO for 90 min, agmatine was injected 5 min after beginning of reperfusion and again once daily for the next 3 post-operative days. The events during ischemia and reperfusion were investigated by T2-weighted images (T2WI), serial diffusion-weighted images (DWI), calculated apparent diffusion coefficient (ADC) maps and contrast-enhanced T1-weighted images (CE-T1WI) during 3 h–72 h in a 1.5 T Siemens MAGNETON Avanto Scanner. Lesion volumes were analyzed in a blinded and randomized manner. Triphenyltetrazolium chloride (TTC), Nissl, and Evans Blue stainings were performed at the corresponding sections.

Results

Increased lesion volumes derived from T2WI, DWI, ADC, CE-T1WI, and TTC all were noted at 3 h and peaked at 24 h–48 h after MCAO injury. TTC-derived infarct volumes were not significantly different from the T2WI, DWI-, and CE-T1WI-derived lesion volumes at the last imaging time (72 h) point except for significantly smaller ADC lesions in the MCAO model (P < 0.05). Volumetric calculation based on TTC-derived infarct also correlated significantly stronger to volumetric calculation based on last imaging time point derived on T2WI, DWI or CE-T1WI than ADC (P < 0.05). At the last imaging time point, a significant increase in Evans Blue extravasation and a significant decrease in Nissl-positive cells numbers were noted in the vehicle-treated MCAO injured animals. The lesion volumes derived from T2WI, DWI, CE-T1WI, and Evans blue extravasation as well as the reduced numbers of Nissl-positive cells were all significantly attenuated in the agmatine-treated rats compared with the control ischemia rats (P < 0.05).

Conclusion

Our results suggest that agmatine has neuroprotective effects against brain edema on a reperfusion model after transient cerebral ischemia.     

Early and delayed neuroprotective effects of FK506 on experimental focal ischemia quantitatively assessed by diffusion-weighted MRI

The immunosuppressive drug FK506 (tacrolimus) has been reported to be a powerful neuroprotective agent in the focal ischemia of animals. However, no report has been published concerning neuroprotective effect of this compound on the morphology in superacute stage. The separate analysis between early and delayed effects of FK506 on the morphology may be helpful in the study of the compound's mechanism of action which is still unknown. The goal of this study was to determine early and delayed effects of pharmacological treatment with FK506 in permanent MCA occlusion using magnetic resonance imaging (MRI). Nineteen rats were subjected to permanent MCA occlusion, and given either intravenous injection of placebo or 1 mg/kg FK506 immediately after occlusion. DWI and T(2)-weighted MRI were performed 3 and 24 h after MCA occlusion, and postmortem histological analysis was also performed. FK506 drastically reduced the ischemic damage in 3-h apparent diffusion coefficient (ADC) map. This is the first report to demonstrate the neuroprotective effects of FK506 on focal cerebral ischemia in superacute stage. In addition, postmortem ischemic damage tended to be smaller than ischemic area indicated by 3-h ADC map in the FK506 group, whereas there was an excellent equality between them in the placebo group, suggesting the possible effect of FK506 on the later ischemic period. Our findings provide direct evidence for the neuroprotective effect of FK506 on ischemic cell damage in both early stage and possibly later stage.