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超顺磁氧化铁纳米颗粒(SPIONs)调节 hERG 离子通道活性。

Superparamagnetic iron oxide nanoparticles (SPIONs) modulate hERG ion channel activity.

机构信息

Dipartimento di Chimica "Ugo Schiff", Università di Firenze , Sesto Fiorentino , Italy.

Institute of Neuroscience, Laboratory of Cell Physiology, Université Catholique de Louvain , Brussels , Belgium.

出版信息

Nanotoxicology. 2019 Nov;13(9):1197-1209. doi: 10.1080/17435390.2019.1650969. Epub 2019 Aug 22.

Abstract

Superparamagnetic iron oxide nanoparticles (SPIONs) are widely used in various biomedical applications, such as diagnostic agents in magnetic resonance imaging (MRI), for drug delivery vehicles and in hyperthermia treatment of tumors. Although the potential benefits of SPIONs are considerable, there is a distinct need to identify any potential cellular damage associated with their use. Since human ether à go-go-related gene (hERG) channel, a protein involved in the repolarization phase of cardiac action potential, is considered one of the main targets in the drug discovery process, we decided to evaluate the effects of SPIONs on hERG channel activity and to determine whether the oxidation state, the dimensions and the coating of nanoparticles (NPs) can influence the interaction with hERG channel. Using patch clamp recordings, we found that SPIONs inhibit hERG current and this effect depends on the coating of NPs. In particular, SPIONs with covalent coating aminopropylphosphonic acid (APPA) have a milder effect on hERG activity. We observed that the time-course of hERG channel modulation by SPIONs is biphasic, with a transient increase (∼20% of the amplitude) occurring within the first 1-3 min of perfusion of NPs, followed by a slower inhibition. Moreover, in the presence of SPIONs, deactivation kinetics accelerated and the activation and inactivation I-V curves were right-shifted, similarly to the effect described for the binding of other divalent metal ions (e.g. Cd and Zn). Finally, our data show that a bigger size and the complete oxidation of SPIONs can significantly decrease hERG channel inhibition. Taken together, these results support the view that Fe ions released from magnetite NPs may represent a cardiac risk factor, since they alter hERG gating and these alterations could compromise the cardiac action potential.

摘要

超顺磁性氧化铁纳米粒子(SPIONs)广泛应用于各种生物医学领域,例如磁共振成像(MRI)中的诊断剂、药物输送载体和肿瘤的热疗。尽管 SPIONs 具有很大的潜在益处,但明确需要识别与其使用相关的任何潜在细胞损伤。由于人类 ether à go-go 相关基因(hERG)通道是参与心脏动作电位复极化阶段的一种蛋白质,被认为是药物发现过程中的主要靶标之一,因此我们决定评估 SPIONs 对 hERG 通道活性的影响,并确定氧化状态、尺寸和纳米粒子(NPs)的涂层是否会影响与 hERG 通道的相互作用。使用膜片钳记录,我们发现 SPIONs 抑制 hERG 电流,并且这种效应取决于 NPs 的涂层。特别是,具有共价涂层氨丙基膦酸(APPA)的 SPIONs 对 hERG 活性的影响较轻。我们观察到,SPIONs 对 hERG 通道调制的时程是双相的,在 NP 灌注的最初 1-3 分钟内会出现短暂的增加(幅度约为 20%),随后抑制作用减慢。此外,在 SPIONs 的存在下,失活动力学加速,激活和失活 I-V 曲线向右移位,类似于描述其他二价金属离子(例如 Cd 和 Zn)结合的效果。最后,我们的数据表明,更大的尺寸和 SPIONs 的完全氧化可以显著降低 hERG 通道抑制作用。总之,这些结果支持了这样的观点,即从磁铁矿 NPs 释放的 Fe 离子可能代表心脏危险因素,因为它们改变了 hERG 门控,并且这些改变可能会损害心脏动作电位。

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