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稳定剂对固体纳米晶制剂在生物相关介质中的粒径及分散行为的影响

Impact of stabilizers on particle size and dispersion behavior in biorelevant media in solid nanocrystal formulations.

作者信息

Böck Nils Christian, Sundermann Julius, Koziolek Mirko, Keller Benjamin-Luca, Mäder Karsten

机构信息

Small Molecule CMC Development Development Sciences AbbVie Deutschland GmbH & Co. KG Germany.

Small Molecule CMC Development Development Sciences AbbVie Deutschland GmbH & Co. KG Germany.

出版信息

Eur J Pharm Biopharm. 2025 Mar;208:114651. doi: 10.1016/j.ejpb.2025.114651. Epub 2025 Jan 25.

Abstract

Nanocrystalline formulations typically contain stabilizing additives to minimize the risk of particle growth or agglomeration. This risk is particularly relevant when the nanosuspension is converted into a solid drug product as the original state of the nanosuspension should be restored upon redispersion of the drug product in vivo. In this work, the behavior of different nonionic and anionic surfactants in solid nanocrystalline formulations and their effects on redispersibility under biorelevant conditions were investigated. For this purpose, nanocrystalline formulations of basic (itraconazole, ritonavir), acidic (naproxen), and neutral (fenofibrate) API containing nonionic polymers acting as steric stabilizers combined either with anionic (sodium dodecyl sulfate, deoxycholate sodium, docusate sodium) or non-ionic surfactants (polysorbate 80, vitamin E-TPGS) were manufactured by nano-milling. These formulations were turned into a solid drug product by lyophilization and their redispersibility was tested by dispersing them in biorelevant media with different pH values and by characterizing their particle size distribution (PSD) and surface charge. In the absence of an anionic surfactant, it was difficult to achieve particle sizes below 500 nm. However, formulations stabilized anionically were at risk of agglomeration in gastric media. For basic API, the agglomeration was reversible for formulations containing sodium deoxycholate after increasing the pH from acidic to neutral levels, but it was found to be irreversible for those containing sodium dodecyl sulfate and docusate sodium. In summary, the type of anionic stabilizer and its interplay with the physicochemical properties of the API (basic, acidic, or neutral) should be considered in the development of solid nanocrystal formulations.

摘要

纳米晶体制剂通常含有稳定添加剂,以将颗粒生长或团聚的风险降至最低。当纳米混悬液转化为固体药物产品时,这种风险尤为突出,因为药物产品在体内重新分散后应恢复纳米混悬液的原始状态。在这项工作中,研究了不同非离子和阴离子表面活性剂在固体纳米晶体制剂中的行为及其在生物相关条件下对再分散性的影响。为此,通过纳米研磨制备了含有作为空间稳定剂的非离子聚合物,并与阴离子(十二烷基硫酸钠、脱氧胆酸钠、多库酯钠)或非离子表面活性剂(聚山梨酯80、维生素E-TPGS)组合的碱性(伊曲康唑、利托那韦)、酸性(萘普生)和中性(非诺贝特)活性药物成分(API)的纳米晶体制剂。这些制剂通过冻干转化为固体药物产品,并通过将它们分散在具有不同pH值的生物相关介质中并表征其粒度分布(PSD)和表面电荷来测试其再分散性。在没有阴离子表面活性剂的情况下,很难获得低于500nm的粒径。然而,阴离子稳定的制剂在胃介质中有团聚的风险。对于碱性API,在将pH从酸性提高到中性水平后,含有脱氧胆酸钠的制剂的团聚是可逆的,但对于含有十二烷基硫酸钠和多库酯钠的制剂,团聚是不可逆的。总之,在固体纳米晶体制剂的开发中应考虑阴离子稳定剂的类型及其与API(碱性、酸性或中性)物理化学性质的相互作用。

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