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新型吸附剂血液灌流在慢性肾脏病(CKD)啮齿动物模型中清除钆基造影剂。

Removal of a gadolinium based contrast agent by a novel sorbent hemoperfusion in a chronic kidney disease (CKD) rodent model.

机构信息

Department of Biomedical Engineering, Oregon Health and Science University (OHSU), Portland, Oregon, USA.

PDX Pharmaceuticals, LLC, Portland, Oregon, USA.

出版信息

Sci Rep. 2019 Jan 24;9(1):709. doi: 10.1038/s41598-018-37348-2.

Abstract

Gadolinium based contrast agents (GBCAs) have been linked to toxicity in patients, regardless of having impaired or normal renal function. Currently, no therapy is considered highly effective for removing gadolinium (Gd) from the body. We propose a new strategy to reduce blood Gd content that facilitates whole body removal of Gd using a hemoperfusion system consisting of a cartridge of porous silica beads (Davisil®) functionalized with 1,2-hydroxypyridinone (1,2-HOPO). Herein, we report optimization of the hemoperfusion system using an ex vivo blood and an in vivo rat model of chronic kidney disease (CKD). In our ex vivo system, 1,2-HOPO-Davisil outperformed Gambro activated charcoal (AC), which is commonly used in clinical hemoperfusion of aqueous toxins, in terms of Gd capture capacity and rate. In the CKD rat model, the 1,2-HOPO-Davisil hemoperfusion system removed Gd by 3.4 times over the Gambro AC system. 1,2-HOPO-Davisil did not change complete blood counts and common blood biochemistry. Thus, this strategy has great potential for clinical translation to manage GBCAs after magnetic resonance imaging (MRI), before Gd can deposit in the body and cause long-term toxicity. Although gadodiamide was used as a proof of concept model for GBCAs in this study, 1,2-HOPO functionalized mesoporous silica could also capture dissociated Gd and other GBCAs.

摘要

基于钆的对比剂(GBCAs)已被证实与患者的毒性有关,无论其肾功能受损还是正常。目前,尚无被认为对从体内去除钆(Gd)非常有效的疗法。我们提出了一种新的策略,通过使用由多孔硅珠(Davisil®)组成的血液灌流系统来降低血液中的 Gd 含量,该系统用 1,2-羟基吡啶酮(1,2-HOPO)进行功能化,从而促进 Gd 的全身清除。在此,我们报告了使用离体血液和慢性肾脏病(CKD)的体内大鼠模型优化血液灌流系统的情况。在我们的离体系统中,1,2-HOPO-Davisil 在 Gd 捕获容量和速率方面优于常用于临床水毒血液灌流的 Gambro 活性炭(AC)。在 CKD 大鼠模型中,1,2-HOPO-Davisil 通过血液灌流系统去除 Gd 的效率比 Gambro AC 系统高 3.4 倍。1,2-HOPO-Davisil 并未改变全血细胞计数和常见的血液生化指标。因此,该策略具有很大的临床转化潜力,可在磁共振成像(MRI)后管理 GBCAs,在 Gd 沉积并引起长期毒性之前。尽管在这项研究中,使用了钆喷酸葡胺作为 GBCAs 的概念验证模型,但 1,2-HOPO 功能化介孔硅也可以捕获游离的 Gd 和其他 GBCAs。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9ad/6345740/f1403ea46acb/41598_2018_37348_Fig1_HTML.jpg

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