肝细胞特异性CT造影剂。实验调查。

Acta radiologica. Supplementum Pub Date : 1997-01-01
A Bergman
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引用次数: 0

摘要

CT是肝脏影像学的一项重要技术。为了提高局灶性肝脏病变的检测,非特异性、水溶性造影剂(CM)的使用是强制性的。然而,即使使用这些CM,肿瘤检测的敏感性也很低。在肝脏特异性CM的发展中,大多数药物都针对网状内皮系统(RES)。ress特异性造影剂的临床应用一直受到频繁的不良反应的阻碍,并且一种新的概念,即CM被肝细胞吸收,已经发展成为一种替代方案。这种CM被正常的肝实质所占据,而不被肿瘤细胞所占据,增强了正常组织与病理组织之间的差异,从而提高了诊断的敏感性。本研究采用动物模型研究了两种肝细胞特异性脂质乳剂FP 736-03和FP 736-04。在正常肝实质中发现剂量依赖性增强,而在实验性肝转移和肝细胞癌的肿瘤组织中未发现增强。肿瘤组织中几乎不变的衰减意味着在观察期间肝与病变的对比稳步增加。为了建立增强与肿瘤检测之间的关系,使用了FP 736-04的累积剂量。肝转移诊断的准确性提高了30 HU。进一步的增加产生了相似的检出率,但假阳性结果的比例更高。当使用该CM时,由于图像伪影的出现,与碘己醇的比较变得困难。然而,FP 736-03在检测肝转移方面优于原生CT和碘己醇增强CT。研究了pf736 -04对病变肝实质的治疗效果。在脂肪肝浸润的情况下,与正常对照相比,FP 736-04的增强作用明显减弱。在肝硬化中观察到的增强程度与对照组没有显著差异。这些临床前研究表明,与天然和水溶性cm增强CT相比,肝细胞特异性脂质乳FP 736-03和FP 736-04提高了局灶性肝脏病变的诊断准确性。FP 736-04被病变的肝实质占据。然而,在脂肪肝和肝硬化的恶性肿瘤的检测尚未研究使用这种CM。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hepatocyte-specific contrast media for CT. An experimental investigation.

CT is an important technique in liver imaging. To improve the detection of focal liver lesions the use of non-specific, water-soluble contrast media (CM) is mandatory. However, even with use of these CM the sensitivity in tumour detection is low. In the development of liver-specific CM, the majority of the agents have been targeted to the reticuloendothelial system (RES). The clinical use of RES-specific contrast agents has been hampered by frequent adverse reactions, and a new concept whereby the CM is taken up by the hepatocytes has been developed as an alternative. Such a CM is taken up by normal liver parenchyma but not by tumour cells, enhancing the difference between normal and pathological tissue, and therefore improving the diagnostic sensitivity. In the present investigation, FP 736-03 and FP 736-04, two hepatocyte-specific lipid emulsions, have been studied using animal models. In normal liver parenchyma dose-dependent enhancement was found, whereas in tumour tissue of experimental liver metastases and hepatocellular carcinoma, no enhancement was noted. The virtually unchanged attenuation in tumour tissue meant that the liver-to-lesion contrast increased steadily during the observation period. In an attempt to establish the relationship between enhancement and tumour detection, the accumulated doses of FP 736-04 were used. Increasing accuracy in the diagnosis of liver metastases was found up to an enhancement level of 30 HU. A further increase yielded similar detection rates, but a higher proportion of false-positive results. Comparison with iohexol was rendered difficult by the occurrence of image artefacts when this CM was used. However, FP 736-03 proved superior to both native and iohexol-enhanced CT for detection of hepatic metastases. The efficacy of FP 736-04 was also studied in diseased hepatic parenchyma. In cases of fatty liver infiltration, enhancement by FP 736-04 was significantly reduced as compared with normal controls. The degree of enhancement observed in cirrhotic livers did not differ significantly from that in the controls. These preclinical investigations have shown that the hepatocyte-specific lipid emulsions FP 736-03 and FP 736-04 improve the diagnostic accuracy of focal liver lesions as compared to native and water-soluble CM-enhanced CT. FP 736-04 is taken up by diseased liver parenchyma. However, the detection of malignancy in steatotic and cirrhotic livers has not yet been studied with use of this CM.

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