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连续 20 多剂钆特酸葡胺(大环类 GBCA)注射后无临床小脑综合征:单中心回顾性研究。

Absence of clinical cerebellar syndrome after serial injections of more than 20 doses of gadoterate, a macrocyclic GBCA: a monocenter retrospective study.

机构信息

Service de Neurologie, ULB-Hôpital Erasme, Route de Lennik, Brussels, Belgium.

Service de Neuroimagerie, ULB-Hôpital Erasme, Route de Lennik, Brussels, Belgium.

出版信息

J Neurol. 2017 Nov;264(11):2277-2283. doi: 10.1007/s00415-017-8631-8. Epub 2017 Sep 27.

Abstract

Sound evidence of gadolinium accumulation in brain has been recently provided after repeated administrations of linear gadolinium-based contrast agents (GBCAs), especially at the cerebellum level. Although data regarding brain accumulation of macrocyclic GBCAs are more reassuring, there is now a genuine concern ("gadolinium-phobia") about possible long-term consequences of gadolinium deposits, especially in terms of cerebellar sequelae. We, therefore, questioned about the clinical impact of serial administration of gadoterate meglumine, a macrocyclic GBCA. In this retrospective study (2000-2016) of medical files of patients who received more than 20 administrations of gadoterate, we searched for cerebellar symptoms and signs developing during the regular follow-up. We reviewed medical files of ten patients (mean age 34.4 ± 20.8 years; 4 males, 6 females) who received 28.2 ± 5.3 doses of gadoterate (average total dose of GBCA 518 ± 226 ml; range 185-785 ml). Patients were examined by at least two medical specialists depending on initial diagnosis, and at least once by a neurosurgeon. Mean follow-up time was 91 months (range 49-168) and six out of ten patients experienced new symptoms or signs. No clinician reported the appearance of a rising cerebellar syndrome, nor newly appeared symptoms or signs suggested cerebellar toxicity. This retrospective clinical study shows no de novo clinical cerebellar syndrome following repeated administrations of gadoterate. Our results argue against a cerebellar toxicity of this macrocyclic agent. Still, confirmation in a larger number of subjects is required, as well as clinical studies concerning linear GBCAs whose structure and in vivo stability are distinct.

摘要

最近,在重复使用线性钆基造影剂(GBCA),尤其是在小脑水平时,已经提供了关于脑内钆积累的有力证据。尽管关于大环 GBCA 脑内积累的数据更为令人放心,但现在确实存在对钆沉积可能产生长期后果的担忧(“钆恐惧症”),特别是在小脑后遗症方面。因此,我们对连续使用大环 GBCA 钆特酸葡胺的临床影响提出了质疑。在这项对接受超过 20 次钆特酸葡胺给药的患者病历的回顾性研究(2000-2016 年)中,我们在常规随访期间搜索了小脑症状和体征的发展情况。我们回顾了 10 名患者(平均年龄 34.4 ± 20.8 岁;4 名男性,6 名女性)的病历,他们接受了 28.2 ± 5.3 次钆特酸葡胺治疗(平均 GBCA 总剂量为 518 ± 226 ml;范围为 185-785 ml)。根据初始诊断,患者至少由两名医学专家进行检查,至少由一名神经外科医生进行一次检查。平均随访时间为 91 个月(范围 49-168),其中 6 名患者出现新的症状或体征。没有临床医生报告出现逐渐加重的小脑综合征,也没有新出现的症状或体征提示小脑毒性。这项回顾性临床研究表明,在重复使用钆特酸葡胺后,没有新出现的临床小脑综合征。我们的结果表明,这种大环造影剂没有小脑毒性。然而,需要在更多的受试者中得到证实,并且需要进行关于线性 GBCA 的临床研究,因为它们的结构和体内稳定性不同。

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