Hepatocyte-directed MR contrast agents. Can we take advantage of bile acids?

Acta radiologica. Supplementum Pub Date : 1997-01-01
P L Anelli, L Calabi, C de Haën, L Lattuada, V Lorusso, A Maiocchi, P Morosini, F Uggeri
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Abstract

A series of gadolinium complexes conjugated to bile acids was prepared and investigated as possible hepatospecific MR imaging contrast agents. In the design of such compounds, features such as the nature of the bile acid, the site of conjugation on the bile acid skeleton, and the global charge of the conjugate were taken into account. Relaxivity measurements carried out in human serum indicate interaction of the conjugates with human serum proteins; even small structural variations significantly affect relaxivity in human serum. Pharmacokinetic data (biliary elimination in the range of 18.4-45.6%) show that bile acids can be used as address moieties to transport gadolinium complexes through hepatocytes. For a homogeneous series of compounds, differing only in the bile acid residue conjugated, it was unexpectedly found that cholic acid is twice as efficient an address moiety as cholylglycine or cholyltaurine. Preliminary results show that none of the conjugates is transported through the basolateral membrane of hepatocytes by the Na+/taurocholate carrier.

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肝细胞定向MR造影剂。我们能利用胆汁酸吗?
制备了一系列与胆汁酸缀合的钆配合物,并对其作为肝特异性磁共振成像造影剂的可能性进行了研究。在这类化合物的设计中,考虑了胆汁酸的性质、胆汁酸骨架上的偶联位点以及偶联物的整体电荷等特征。在人血清中进行的弛豫测量表明偶联物与人血清蛋白的相互作用;即使是很小的结构变化也会显著影响人血清的松弛性。药代动力学数据(胆道消除范围为18.4-45.6%)表明胆汁酸可以作为寻址基团通过肝细胞运输钆复合物。对于同质系列的化合物,不同的只是在胆汁酸残基偶联,它出乎意料地发现,胆酸是有效的两倍的寻址部分的胆酰甘氨酸或胆酰牛磺酸。初步结果表明,没有一种缀合物是通过Na+/牛磺胆酸载体通过肝细胞基底外膜运输的。
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