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通过低温透射电子显微镜对静脉注射铁络合物的核心尺寸测定和结构表征

Core size determination and structural characterization of intravenous iron complexes by cryogenic transmission electron microscopy.

作者信息

Wu Yong, Petrochenko Peter, Chen Lynn, Wong Sook Yee, Absar Mohammad, Choi Stephanie, Zheng Jiwen

机构信息

Division of Biology, Chemistry and Materials Science, Office of Science and Engineering Laboratories, Center for Devices and Radiological Health, Food and Drug Administration, Silver Spring, MD 20993, United States.

Division of Therapeutic Performance, Office of Research Standards, Office of Generic Drugs, Center for Drug Evaluation and Research, Food and Drug Administration, Silver Spring, MD 20993, United States.

出版信息

Int J Pharm. 2016 May 30;505(1-2):167-74. doi: 10.1016/j.ijpharm.2016.03.029. Epub 2016 Mar 18.

Abstract

Understanding physicochemical properties of intravenous (IV) iron drug products is essential to ensure the manufacturing process is consistent and streamlined. The history of physicochemical characterization of IV iron complex formulations stretches over several decades, with disparities in iron core size and particle morphology as the major source of debate. One of the main reasons for this controversy is room temperature sample preparation artifacts, which affect accurate determination of size, shape and agglomeration/aggregation of nanoscale iron particles. The present study is first to report the ultra-fine iron core structures of four IV iron complex formulations, sodium ferric gluconate, iron sucrose, low molecular weight iron dextran and ferumoxytol, using a cryogenic transmission electron microscopy (cryo-TEM) preservation technique, as opposed to the conventional room temperature (RT-TEM) technique. Our results show that room temperature preparation causes nanoparticle aggregation and deformation, while cryo-TEM preserves IV iron colloidal suspension in their native frozen-hydrated and undiluted state. In contrast to the current consensus in literature, all four IV iron colloids exhibit a similar morphology of their iron oxide cores with a spherical shape, narrow size distribution and an average size of 2nm. Moreover, out of the four tested formulations, ferumoxytol exhibits a cluster-like community of several iron carbohydrate particles which likely accounts for its large hydrodynamic size of 25nm, measured with dynamic light scattering. Our findings outline a suitable method for identifying colloidal nanoparticle core size in the native state, which is increasingly important for manufacturing and design control of complex drug formulations, such as IV iron drug products.

摘要

了解静脉注射(IV)铁剂产品的物理化学性质对于确保生产过程的一致性和简化至关重要。IV铁络合物制剂的物理化学表征历史长达数十年,铁芯尺寸和颗粒形态的差异是主要争议来源。造成这种争议的主要原因之一是室温样品制备假象,这会影响纳米级铁颗粒尺寸、形状和团聚/聚集的准确测定。本研究首次报道了四种IV铁络合物制剂(葡萄糖酸铁钠、蔗糖铁、低分子右旋糖酐铁和 ferumoxytol)的超细铁芯结构,采用低温透射电子显微镜(cryo-TEM)保存技术,而非传统的室温(RT-TEM)技术。我们的结果表明,室温制备会导致纳米颗粒聚集和变形,而 cryo-TEM 可将 IV 铁胶体悬浮液保持在其天然冷冻水合和未稀释状态。与文献中的当前共识相反,所有四种 IV 铁胶体的氧化铁核均呈现相似形态,呈球形,尺寸分布窄,平均尺寸为 2nm。此外,在四种测试制剂中,ferumoxytol 表现出由几个铁碳水化合物颗粒组成的簇状群落,这可能解释了其通过动态光散射测量的 25nm 的大流体动力学尺寸。我们的研究结果概述了一种在天然状态下识别胶体纳米颗粒核心尺寸的合适方法,这对于复杂药物制剂(如 IV 铁剂产品)的制造和设计控制越来越重要。

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