From the Department of Diagnostic, Interventional and Pediatric Radiology, Inselspital, University Hospital, University of Bern, Bern, Switzerland.
Invest Radiol. 2018 Oct;53(10):571-578. doi: 10.1097/RLI.0000000000000507.
The issue of dechelation (transmetallation) in vivo after administration of the linear gadolinium-based contrast agents, and potential safety concerns, is considered on the basis of an extensive, focused literature review. Early indications of potential problems included the high level of excess ligand used in the formulation of 2 agents (indeed the 2 least stable thermodynamically) and interference with laboratory tests when blood was drawn from patients relatively soon after administration of these same agents. The advent of nephrogenic systemic fibrosis in the late 2000s raised additional major concerns.The correlation in 2014 of dentate nucleus hyperintensity on precontrast T1-weighted scans with multiple prior injections of linear gadolinium chelates, in patients with normal renal function, has driven subsequent research concerning dechelation of these agents in vivo. Unexpectedly high levels of gadolinium in the bone, skin, and liver have been found long term after administration, in animal models and in humans, although the latter data are limited. Bone may serve as a long-term reservoir, with a residual excretion phase for gadolinium after intravenous injection of the linear agents due to a subsequent slow release from bone. Many different patient populations could be vulnerable and potentially later develop clinical symptoms, although at this stage there are only limited data and small retrospective uncontrolled studies. Possible vulnerable populations include children, menopausal women, patients with osteoporosis (who are predisposed to fractures and often slow to heal or heal poorly), those receiving multiple doses, those with proinflammatory conditions, moderate renal dysfunction, or an undefined genetic predisposition. Of particular concern would be nephrogenic systemic fibrosis-like symptoms-including particularly pain and skin/joint symptoms, or disease related to the incorporation of gadolinium in hydroxyapatite in bone, in small subgroups of patients with a not yet defined propensity and/or cofactor. These concerns have led to withdrawal of the linear agents from the largest clinical market, Europe, with the exception of the hepatobiliary agents for delayed liver imaging, an indication that cannot be fulfilled by the current macrocyclic gadolinium chelates (for which these concerns do not apply).
基于广泛而有针对性的文献回顾,讨论了给药后线性镧系造影剂的脱螯(转金属)问题及其潜在的安全隐患。早期的潜在问题迹象包括 2 种制剂配方中使用的过量配体(实际上这 2 种制剂热力学稳定性最差),以及在给这些药物后不久从患者身上抽取血液时对实验室检测的干扰。2000 年代后期出现的肾源性系统纤维化(nephrogenic systemic fibrosis,NSF)引起了更多的重大关注。2014 年,在肾功能正常的患者中,发现齿状核在预对比 T1 加权扫描中的高信号与多次线性镧系螯合物注射相关,这一发现促使人们对这些药物在体内的脱螯作用进行了后续研究。尽管这些数据有限,但在动物模型和人类中,长期以来,在给药后发现骨、皮肤和肝脏中的钆含量异常高。骨可能是一种长期的储库,由于线性药物静脉注射后骨内缓慢释放,导致静脉注射后镧系元素的排泄阶段延迟。许多不同的患者群体可能易受影响,并可能在以后出现临床症状,尽管在现阶段,只有有限的数据和小型回顾性非对照研究。可能易受影响的人群包括儿童、绝经后妇女、骨质疏松症患者(他们易骨折,且愈合缓慢或愈合不良)、接受多次剂量的患者、有炎症性疾病、中度肾功能障碍或未定义的遗传易感性的患者。特别令人担忧的是,与肾源性系统纤维化样症状相关的疾病——包括疼痛和皮肤/关节症状,或与骨中羟磷灰石中钆结合相关的疾病,在尚未确定易感性和/或辅助因子的小亚组患者中出现。这些担忧导致线性药物在最大的临床市场欧洲被撤出,除了用于延迟肝脏成像的肝胆系统药物外,而这些药物不能被目前的大环钆螯合物所取代(这些担忧不适用于大环钆螯合物)。
