Gadolinium-based contrast agents

钆造影剂
  • 文章类型: Journal Article
    背景:当使用基于钆的造影剂(GBCA)时,超敏反应(HSR)可能会意外发生并危及生命。钆沉积病(GDD)和与钆暴露相关的症状(SAGE)长期以来一直存在争议。然而,类似的研究目前还不完整或过时。因此,使用最新的上市后安全性数据比较不同GBCA在HSR和GDD/SAGE方面的安全性,应该会对安全使用GBCA产生进一步的见解.
    方法:本研究使用世界卫生组织数据库VigiBase和FDA不良事件报告系统(FAERS)数据库,对所有GBCA与GDD之间的安全性差异和GBCA相关的HSR谱进行了比较和分析。还使用FAERS数据对SAGE进行了进一步分析。报告比值比(ROR)95%置信区间的下限用于信号检测。此外,HSR的频率是通过将VigiBase中的报告数量除以2008年至2022年IQVIA跨国集成数据分析系统中的总销售量(以百万为单位)来计算的。所有不良事件均使用药物监管活动医学词典(MedDRA)26.0进行标准化。
    结果:这项研究表明,所有GBCA都具有诱导HSR的潜力,非离子线性GBCA表现出相对较低的信号。根据标准化MedDRA查询进行分层分析,gadobutrol对血管性水肿的ROR025更大。对于过敏性/过敏性休克条件,g二烯酸二甲胺和gadoteridol的ROR025较大。关于严重的皮肤不良反应,只有gadoverseamide和gadidiamide在FAERS和VigiBase中显示信号。地区之间的HSR频率也存在差异。关于GDD,Gadoterate葡甲胺,gadoteridol的ROR025较低。对与SAGE相关的29个首选术语的分析表明,应特别考虑与gadoverseamide相关的皮肤硬结的风险,gadopentetate二甲葡胺,gadobenatedimeglumine,gadodiamide,还有Gadoteridol.此外,与其他GBCA相比,gadodiamide和gadoteridol的皮肤紧绷风险更大。
    结论:本研究使用来自多个来源的数据比较了GBCA之间的风险差异。然而,作为一种假设生成方法,明确的因果关系需要进一步研究和验证.
    BACKGROUND: Hypersensitivity reactions (HSRs) can occur unexpectedly and be life-threatening when gadolinium-based contrast agents (GBCAs) are used. Gadolinium deposition disease (GDD) and symptoms associated with gadolinium exposure (SAGE) have been controversial for a long time. However, similar studies are currently incomplete or outdated. Therefore, comparing the safety of different GBCAs in terms of HSRs and GDD/SAGE using the latest post-marketing safety data should yield further insights into safely using GBCAs.
    METHODS: The safety differences between all GBCAs to GDD and the spectrum of GBCA-related HSRs were all compared and analyzed by using the World Health Organization database VigiBase and the FDA Adverse Event Reporting System (FAERS) database in this study. A further analysis of SAGE was also conducted using FAERS data. The lower limit of the reporting odds ratio (ROR) 95% confidence interval was used for signal detection. Moreover, the frequency of HSRs was calculated by dividing the number of reports in VigiBase by the total sales volume (measured in millions) from 2008 to 2022 in the IQVIA Multinational Integrated Data Analysis System. All adverse events were standardized using the Medical Dictionary for Drug Regulatory Activities (MedDRA) 26.0.
    RESULTS: This study shows that all GBCAs have the potential to induce HSRs, with nonionic linear GBCAs exhibiting a comparatively lower signal. According to standardized MedDRA query stratification analysis, gadobutrol had a greater ROR025 for angioedema. The ROR025 of gadobenate dimeglumine and gadoteridol is larger for anaphylactic/anaphylactoid shock conditions. Regarding severe cutaneous adverse reactions, only gadoversetamide and gadodiamide showed signals in FAERS and VigiBase. There were also differences in the frequency of HSRs between regions. Regarding GDD, gadoterate meglumine, and gadoteridol had a lower ROR025. An analysis of the 29 preferred terms linked to SAGE indicated that special consideration should be given to the risk of skin induration associated with gadoversetamide, gadopentetate dimeglumine, gadobenate dimeglumine, gadodiamide, and gadoteridol. Additionally, gadodiamide and gadoteridol pose a greater risk of skin tightness compared to other GBCAs.
    CONCLUSIONS: The risk differences among GBCAs using data from several sources were compared in this study. However, as a hypothesis-generating method, a clear causal relationship would require further research and validation.
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  • 文章类型: Journal Article
    灌注动力学在向组织输送必需营养素和氧气同时去除代谢废物中起着至关重要的作用。成像技术,如磁共振成像(MRI),计算机断层扫描(CT),和正电子发射断层扫描(PET)使用造影剂来可视化灌注和清除模式;然而,每种技术都有特定的局限性。混合PET/MRI将PET的定量功率和灵敏度与MRI的高功能和解剖学细节相结合,并在分子成像中具有很好的精度。然而,具有挑战性的合成和放射性标记阻碍了双PET/MRI探针的开发。这里,我们提出了一种新型的PET/MRI探头,[18F][Gd(FL1)],与临床实践中使用的大环MRI造影剂相比,具有出色的稳定性。[18F][Gd(FL1)]的独特分子设计允许在最终合成步骤中选择性和迅速地放射性标记钆螯合物。利用MRI和PET信号的优势,该探针能够通过创新的基于体素的分析定量体内灌注和排泄动力学作图。在对健康小鼠的初步研究中证明了[18F][Gd(FL1)]的诊断能力,成功发现早期单侧肾功能不全病例。这项研究为PET/MRI引入了一种新方法,并强调了简化的探头设计,以提高诊断准确性。
    Perfusion dynamics play a vital role in delivering essential nutrients and oxygen to tissues while removing metabolic waste products. Imaging techniques such as magnetic resonance imaging (MRI), computed tomography (CT), and positron emission tomography (PET) use contrast agents to visualize perfusion and clearance patterns; however, each technique has specific limitations. Hybrid PET/MRI combines the quantitative power and sensitivity of PET with the high functional and anatomical detail of MRI and holds great promise for precision in molecular imaging. However, the development of dual PET/MRI probes has been hampered by challenging synthesis and radiolabeling. Here, we present a novel PET/MRI probe, [18F][Gd(FL1)], which exhibits excellent stability comparable to macrocyclic MRI contrast agents used in clinical practice. The unique molecular design of [18F][Gd(FL1)] allows selective and expeditious radiolabeling of the gadolinium chelate in the final synthetic step. Leveraging the strengths of MRI and PET signals, the probe enables quantitative in vivo mapping of perfusion and excretion dynamics through an innovative voxel-based analysis. The diagnostic capabilities of [18F][Gd(FL1)] were demonstrated in a pilot study on healthy mice, successfully detecting early cases of unilateral renal dysfunction. This study introduces a new approach for PET/MRI and emphasizes a streamlined probe design for improved diagnostic accuracy.
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  • 文章类型: Journal Article
    基于钆的造影剂(GBCA)是钆金属中心和线性或大环的聚氨基-羧酸螯合剂的络合物。这些试剂用于通过MRI技术增强深层异常的可见性。了解各种GBCA的精确尺寸是了解其体内和药物动力学行为的关键参数。它们的扩散性,以及他们的放松。然而,传统的尺寸表征技术在处理这些微小分子(≤1nm)时不足。在这项工作中,我们建议使用泰勒色散分析(TDA)确定基于钆的造影剂的大小和扩散系数。TDA提供了流体动力学直径和扩散系数的可靠测量。将获得的结果与DOSYNMR(扩散有序核磁共振谱)和DFT(密度泛函理论)进行比较。
    Gadolinium-based contrast agents (GBCA) are complexes of a Gadolinium metal center and a linear or macrocyclic polyamino-carboxylic acid chelating agent. These agents are employed to enhance the visibility of deep abnormalities through MRI techniques. Knowing the precise dimensions of various GBCA is key parameter for understanding their in-vivo and pharmaco-kinetic behaviors, their diffusivity, as well as their relaxivity. However, conventional size characterization techniques fall short when dealing with these tiny molecules (≤1 nm). In this work, we propose to determine the size and diffusivity of gadolinium-based contrast agents using Taylor dispersion analysis (TDA). TDA provided a reliable measurement of the hydrodynamic diameter and the diffusion coefficient. The obtained results were compared to DOSY NMR (Diffusion-ordered Nuclear Magnetic Resonance Spectroscopy) and DFT (Density Functional Theory).
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  • 文章类型: Journal Article
    钆(Gd)是广泛用于工业和医学应用的稀土元素之一。后一种应用似乎有助于水生生态系统中Gd水平的上升,因为它是通过接受MRI扫描的患者的尿液排出的,并且通常不会被废水处理系统捕获。钆暴露造成的潜在环境和生物危害仍在调查中。这项研究旨在评估a螯合物对淡水刺胞动物Hydra的致畸风险。实验设计评估了纯Gadidiamide(25μg/l,50μg/l,100μg/l,500μg/l)及其商业对应化合物(Omniscan®;100μg/l,500μg/l,使用致畸风险指数(TRI)在不同浓度下)。在这里,我们显示了在暴露于浓度≥100μg/l的两种测试制剂后的中等风险(TRI的III类)。考虑到水生环境中浓度相似的可能性,特别是在废水排放点附近,使用Hydra再生试验对从三条河流收集的环境样品进行了致畸风险评估(台伯河,Almone,和萨科)在意大利中部。此外,使用ICP-MS进行现场样品的化学分析。淡水样品分析显示Gd浓度低(≤0.1μg/l),尽管在家庭和/或工业废水排放点附近局部增加。尽管环境样本中的致畸风险范围从高(TRI的IV类)到可忽略不计(TRI的I类),低Gd浓度,特别是与砷和重金属等其他污染物的含量相比,排除在环境样品中Gd与观察到的致畸风险之间建立直接的因果关系。然而,在实验室测试中观察到的致畸风险值得进一步调查。
    Gadolinium (Gd) is among the rare earth elements extensively utilized in both industrial and medical applications. The latter application appears to contribute to the rise in Gd levels in aquatic ecosystems, as it is excreted via urine from patients undergoing MRI scans and often not captured by wastewater treatment systems. The potential environmental and biological hazards posed by gadolinium exposure are still under investigation. This study aimed to assess the teratogenic risk posed by a gadolinium chelate on the freshwater cnidarian Hydra vulgaris. The experimental design evaluated the impact of pure Gadodiamide (25 μg/l, 50 μg/l, 100 μg/l, 500 μg/l) and its commercial counterpart compound (Omniscan®; 100 μg/l, 500 μg/l, 782.7 mg/l) at varying concentrations using the Teratogenic Risk Index (TRI). Here we showed a moderate risk (Class III of TRI) following exposure to both tested formulations at concentrations ≥ 100 μg/l. Given the potential for similar concentrations in aquatic environments, particularly near wastewater discharge points, a teratogenic risk assessment using the Hydra regeneration assay was conducted on environmental samples collected from three rivers (Tiber, Almone, and Sacco) in Central Italy. Additionally, chemical analysis of field samples was performed using ICP-MS. Analysis of freshwater samples revealed low Gd concentrations (≤ 0.1 μg/l), despite localized increases near domestic and/or industrial wastewater discharge sites. Although teratogenic risk in environmental samples ranged from high (Class IV of TRI) to negligible (Class I of TRI), the low Gd concentrations, particularly when compared to higher levels of other contaminants like arsenic and heavy metals, preclude establishing a direct cause-effect relationship between Gd and observed teratogenic risks in environmental samples. Nevertheless, the teratogenic risks observed in laboratory tests warrant further investigation.
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  • 文章类型: Journal Article
    这项研究的目的是研究在不同组织中引起的生化和组织学变化,作为在CD-1小鼠品系中皮下施用Gd纳米水凝胶(GdDOTACS-TPP/HA)的结果。纳米水凝胶是通过离子凝胶化过程将造影剂(GdDOTA)封装在由壳聚糖(CS)和透明质酸(HA)组成的生物相容性聚合物基质中获得的。通过测量抗氧化酶过氧化氢酶(CAT)的比活性来评估Gd纳米水凝胶对氧化还原状态的影响,谷胱甘肽过氧化物酶(GPx),和超氧化物歧化酶(SOD),以及氧化应激标志物,如还原型谷胱甘肽(GSH),丙二醛(MDA),高级氧化蛋白产品(AOPP),和蛋白质反应性羰基(PRCG),在肝脏中,肾,和心脏组织。用WesternBlot分析亚硝基化蛋白的表达,用分光光度法测定血清生化指标。此外,研究了CD-1小鼠组织的组织学分析。这些结果表明Gd纳米水凝胶由于其体内低毒性而可能是当前MRI造影剂的替代品。
    The aim of this study was the investigation of biochemical and histological changes induced in different tissues, as a result of the subcutaneous administration of Gd nanohydrogels (GdDOTA⸦CS-TPP/HA) in a CD-1 mouse strain. The nanohydrogels were obtained by encapsulating contrast agents (GdDOTA) in a biocompatible polymer matrix composed of chitosan (CS) and hyaluronic acid (HA) through the ionic gelation process. The effects of Gd nanohydrogels on the redox status were evaluated by measuring specific activities of the antioxidant enzymes catalase (CAT), glutathione peroxidase (GPx), and superoxide dismutase (SOD), as well as oxidative stress markers, such as reduced glutathione (GSH), malondialdehyde (MDA), advanced oxidation protein products (AOPP), and protein-reactive carbonyl groups (PRCG), in the liver, kidney, and heart tissues. The nitrosylated proteins expression were analyzed with Western Blot and the serum biochemical markers were measured with spectrophotometric methods. Also, a histological analysis of CD-1 mouse tissues was investigated. These results indicated that Gd nanohydrogels could potentially be an alternative to current MRI contrast agents thanks to their low toxicity in vivo.
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  • 文章类型: Journal Article
    目的:为避免在自发性低颅压(SIH)中使用对比剂,一些研究表明,接受非对比液衰减反转恢复(FLAIR)的弥漫性厚膜高强度(DPMH)作为对比增强T1WI(T1ce)的弥漫性厚膜增强(DPME)的等效信号,尽管缺乏全面的性能指标。本研究旨在全面探讨其可行性。
    方法:在这项单中心回顾性研究中,在2021年4月至2023年11月之间,使用1.5和3.0TeslaMRI扫描仪评估了43例临床诊断为SIH的患者的脑部MRI检查。两名放射科医生独立评估FLAIR上是否存在DPMH,T1ce上是否存在DPME,T1ce作为厚膜增厚的金标准。通过定量测量研究了硬膜下液体收集对DPMH的贡献。使用科恩的卡帕统计数据,评估了观察员之间的协议。
    结果:在43例患者中,有39例(90.7%),T1ce观察到厚膜增厚。FLAIR序列产生了准确性,灵敏度,特异性,正预测值,阴性预测值为72.1%,71.8%,75.0%,96.6%,和21.4%,用于确定厚膜增厚。FLAIR发现28例厚膜增厚;然而,其中,21例(75%)显示硬脑膜高信号受硬膜下积液的影响。FLAIR的假阴性率为28.2%(11/39)。
    结论:FLAIR和T1ce在识别厚膜增厚方面缺乏完全的相关性,突出了在从SIH患者的MRI方案中去除造影剂给药方面需要谨慎,因为它揭示了一个主要标准(即,厚膜增强)伯尔尼评分。
    OBJECTIVE: To avoid contrast administration in spontaneous intracranial hypotension (SIH), some studies suggest accepting diffuse pachymeningeal hyperintensity (DPMH) on non-contrast fluid-attenuated inversion recovery (FLAIR) as an equivalent sign to diffuse pachymeningeal enhancement (DPME) on contrast-enhanced T1WI (T1ce), despite lacking thorough performance metrics. This study aimed to comprehensively explore its feasibility.
    METHODS: In this single-center retrospective study, between April 2021 and November 2023, brain MRI examinations of 43 patients clinically diagnosed with SIH were assessed using 1.5 and 3.0 Tesla MRI scanners. Two radiologists independently assessed the presence or absence of DPMH on FLAIR and DPME on T1ce, with T1ce serving as a gold-standard for pachymeningeal thickening. The contribution of the subdural fluid collections to DPMH was investigated with quantitative measurements. Using Cohen\'s kappa statistics, interobserver agreement was assessed.
    RESULTS: In 39 out of 43 patients (90.7%), pachymeningeal thickening was observed on T1ce. FLAIR sequence produced an accuracy, sensitivity, specificity, positive predictive value, and negative predictive value of 72.1%, 71.8%, 75.0%, 96.6%, and 21.4% respectively, for determining pachymeningeal thickening. FLAIR identified pachymeningeal thickening in 28 cases; however, among these, 21 cases (75%) revealed that the pachymeningeal hyperintense signal was influenced by subdural fluid collections. False-negative rate for FLAIR was 28.2% (11/39).
    CONCLUSIONS: The lack of complete correlation between FLAIR and T1ce in identifying pachymeningeal thickening highlights the need for caution in removing contrast agent administration from the MRI protocol of SIH patients, as it reveals a major criterion (i.e., pachymeningeal enhancement) of Bern score.
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  • 文章类型: Journal Article
    钆基造影剂(GBCA)已经使用了30多年,以改善磁共振成像,跨多个临床环境的医疗诊断和治疗监测的重要工具。研究表明,暴露于GBCA与钆的释放和组织沉积有关,这可能会导致几种器官的短期和长期毒性,包括肾脏,大多数GBCA的主要排泄器官。考虑到全球范围内慢性肾脏病的患病率不断增加,并且GBCA暴露后的大多数并发症与肾功能不全有关,GBCA毒性的潜在机制,尤其是肾毒性,尤为重要。更好地了解钆的毒性机制可能有助于澄清与使用GBCA相关的安全性和/或潜在风险。在这项工作中,对最近有关钆和GBCA毒性机制的文献进行了综述.
    Gadolinium-based contrast agents (GBCAs) have been used for more than 30 years to improve magnetic resonance imaging, a crucial tool for medical diagnosis and treatment monitoring across multiple clinical settings. Studies have shown that exposure to GBCAs is associated with gadolinium release and tissue deposition that may cause short- and long-term toxicity in several organs, including the kidney, the main excretion organ of most GBCAs. Considering the increasing prevalence of chronic kidney disease worldwide and that most of the complications following GBCA exposure are associated with renal dysfunction, the mechanisms underlying GBCA toxicity, especially renal toxicity, are particularly important. A better understanding of the gadolinium mechanisms of toxicity may contribute to clarify the safety and/or potential risks associated with the use of GBCAs. In this work, a review of the recent literature concerning gadolinium and GBCA mechanisms of toxicity was performed.
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  • 文章类型: Journal Article
    多发性硬化(MS)是一种神经体系的慢性炎症性疾病。MR成像发现在初步诊断和评估疾病状态期间建立疾病的诊断标志中起着不可或缺的作用。各种专家组结合了大脑和脊柱的成像,提出了多次迭代的诊断标准和共识指南。并努力使MS的成像协议标准化。新兴的辅助影像学发现也吸引了越来越多的兴趣,应在放射学检查中寻求。在本文中,作者回顾了MS和相关疾病的临床指南和影像学方法,专注于临床有影响的图像解释和MR成像报告。
    Multiple sclerosis (MS) is a chronic inflammatory disease of the nervous system. MR imaging findings play an integral part in establishing diagnostic hallmarks of the disease during initial diagnosis and evaluating disease status. Multiple iterations of diagnostic criteria and consensus guidelines are put forth by various expert groups incorporating imaging of the brain and spine, and efforts have been made to standardize imaging protocols for MS. Emerging ancillary imaging findings have also attracted increasing interests and should be sought for on radiologic examination. In this paper, the authors review the clinical guidelines and approach to imaging of MS and related disorders, focusing on clinically impactful image interpretation and MR imaging reporting.
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  • 文章类型: Journal Article
    钆造影剂(GBCA)对于诊断性MRI检查至关重要。GBCA仅在每个患者的基础上少量使用;然而,全球范围内获得对比增强MRI检查导致每年使用数千升GBCA。数据显示,这些GBCA存在于污水中,地表水,和世界上许多地区的饮用水。因此,由于GBCA在水生环境中无处不在,因此人们越来越关注GBCA的环境影响。为了解决GBCA在整个水系统中的问题,所有利益相关者之间的合作是必要的,包括GBCA的生产商,医疗专业人员,重要的是,饮用水的消费者,即病人。本文旨在使医疗保健专业人员意识到有机会带头就GBCA的使用做出明智的决定,并概述了不同的行动选择。在本文中,我们首先对GBCA的代谢和临床应用进行了综述,然后是GBCA的环境命运和观察,其次是减少GBCA使用的措施。GBCA对环境的影响可以通过(1)通过基于重量的对比体积减少来关注GBCA的应用的措施来减少,每mmolGd具有较高弛豫率的GBCA,对比增强序列,和后处理;(2)减少GBCA浪费的措施,包括使用散装包装和在应用点收集GBCA的残留物。关键相关性声明本综述旨在使医疗保健专业人员意识到GBCA对环境的影响,以及他们有机会率先就GBCA的使用和减轻其环境负担的不同选择做出明智的决定。关键点•在饮用水源中发现基于钆的造影剂并构成环境风险。•放射科医生有广泛的选择,以减少GBCA的使用,而不影响诊断质量。•通过在临床实践中采用此类措施,放射学可以变得更加可持续。
    Gadolinium-based contrast agents (GBCA) are essential for diagnostic MRI examinations. GBCA are only used in small quantities on a per-patient basis; however, the acquisition of contrast-enhanced MRI examinations worldwide results in the use of many thousands of litres of GBCA per year. Data shows that these GBCA are present in sewage water, surface water, and drinking water in many regions of the world. Therefore, there is growing concern regarding the environmental impact of GBCA because of their ubiquitous presence in the aquatic environment. To address the problem of GBCA in the water system as a whole, collaboration is necessary between all stakeholders, including the producers of GBCA, medical professionals and importantly, the consumers of drinking water, i.e. the patients. This paper aims to make healthcare professionals aware of the opportunity to take the lead in making informed decisions about the use of GBCA and provides an overview of the different options for action.In this paper, we first provide a summary on the metabolism and clinical use of GBCA, then the environmental fate and observations of GBCA, followed by measures to reduce the use of GBCA. The environmental impact of GBCA can be reduced by (1) measures focusing on the application of GBCA by means of weight-based contrast volume reduction, GBCA with higher relaxivity per mmol of Gd, contrast-enhancing sequences, and post-processing; and (2) measures that reduce the waste of GBCA, including the use of bulk packaging and collecting residues of GBCA at the point of application.Critical relevance statement This review aims to make healthcare professionals aware of the environmental impact of GBCA and the opportunity for them to take the lead in making informed decisions about GBCA use and the different options to reduce its environmental burden.Key points• Gadolinium-based contrast agents are found in sources of drinking water and constitute an environmental risk.• Radiologists have a wide spectrum of options to reduce GBCA use without compromising diagnostic quality.• Radiology can become more sustainable by adopting such measures in clinical practice.
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  • 文章类型: Journal Article
    背景:基于钆(Gd)的造影剂(GBCA)滞留在2型糖尿病(T2DM)患者脑中的神经毒性潜力尚不清楚。
    目的:探讨GBCA在T2DM大鼠体内的沉积和清除以及Gd增强核苷酸结合寡聚化结构域-3(NLRP3)炎性体激活的机制。
    方法:横截面,前瞻性。
    104只T2DM雄性Wistar大鼠。
    9.4-T,T1加权快速自旋回波序列。
    结果:T2DM(雄性Wistar大鼠,n=52)和对照组(健康,雄性Wistar大鼠,n=52)大鼠接受生理盐水,gadodiamide,Gd-二亚乙基三胺五乙酸,和gadoterate葡甲胺,每周连续四天,共7周。通过MRI评估Gd在某些大脑中的分布和清除(T1信号强度和松弛率R1,在每周的最后一天),电感耦合等离子体质谱,超高效液相色谱质谱,和透射电子显微镜。行为测试,组织病理学特征,并分析了GBCAs对神经炎症的影响。
    方法:单向方差分析,bonferroni方法,和不成对t检验。P值<0.05被认为具有统计学意义。
    结果:gadodiamide组T2DM大鼠在开放视野试验中的运动距离和出现时间明显短于其他组。此外,NLRP3、Caspase-1、白细胞介素-1β(IL-1β)的表达,神经元中含有CARD蛋白的凋亡相关斑点样蛋白在gadodiamide组明显高于盐水组,如Westernblot所示。加多二酰胺还诱导小胶质细胞分化为M1型,降低了神经元线粒体膜电位,流式细胞术显示神经元凋亡显著增加。
    结论:T2DM可能影响脑内GBCA的沉积和清除。由T2DM模型通知,gadiamide可以通过激活NLRP3炎性体介导神经炎症反应。
    方法:1技术效果:第一阶段。
    BACKGROUND: The neurotoxic potential of gadolinium (Gd)-based contrast agents (GBCAs) retention in the brains of patients with type 2 diabetes mellitus (T2DM) is unclear.
    OBJECTIVE: To determine the deposition and clearance of GBCAs in T2DM rats and the mechanism by which Gd enhances nucleotide-binding oligomerization domain-3 (NLRP3) inflammasome activation.
    METHODS: Cross-sectional, prospective.
    UNASSIGNED: 104 T2DM male Wistar rats.
    UNASSIGNED: 9.4-T, T1-weighted fast spin echo sequence.
    RESULTS: T2DM (male Wistar rats, n = 52) and control group (healthy, male Wistar rats, n = 52) rats received saline, gadodiamide, Gd-diethylenetriaminepentaacetic acid, and gadoterate meglumine for four consecutive days per week for 7 weeks. The distribution and clearance of Gd in the certain brain were assessed by MRI (T1 signal intensity and relaxation rate R1, on the last day of each week), inductively coupled plasma mass-spectroscopy, ultraperformance liquid chromatography mass spectrometry, and transmission electron microscopy. Behavioral tests, histopathological features, and the effects of GBCAs on neuroinflammation were also analyzed.
    METHODS: One-way analysis of variance, bonferroni method, and unpaired t-test. A P-value <0.05 was considered statistically significant.
    RESULTS: The movement distance and appearance time in the open field test of the T2DM rats in the gadodiamide group were significantly shorter than in the other groups. Furthermore, the expression of NLRP3, Pro-Caspase-1, interleukin-1β (IL-1β), and apoptosis-associated speck-like protein containing a CARD protein in neurons was significantly higher in the gadodiamide group than in the saline group, as shown by Western blot. Gadodiamide also induced differentiation of microglia into M1 type, decreased the neuronal mitochondrial membrane potential, and significantly increased neuronal apoptosis from flow cytometry.
    CONCLUSIONS: T2DM may affect both the deposition and clearance of GBCAs in the brain. Informed by the T2DM model, gadodiamide could mediate the neuroinflammatory response by NLRP3 inflammasome activation.
    METHODS: 1 TECHNICAL EFFICACY: Stage 1.
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