Potential Use of Common Administration of Emulsion for Parenteral Nutrition and Vinpocetine: Compatibility Study and Prospect

IF 3.4 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Metabolites Pub Date : 2024-08-07 DOI:10.3390/metabo14080439

Szymon Tomczak, Kornelia Kaszuba, Jagoda Szkudlarek, Ludwika Piwowarczyk, Anna Jelińska

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引用次数: 0

Abstract

Vinpocetine (VP) is distributed after oral and intravenous administration, and its uptake in the thalamus, basal ganglia, and visual cortex. Due to poor bioavailability (~7%) and marked first-pass effect (~75%), including a short half-life (2–3 h), oral administration of VP is limited. It requires frequent administration of the drug to obtain a therapeutic effect. Attempts to overcome these difficulties include the use of new drug delivery systems and/or alternative routes of drug administration. One possibility is the common administration of lipid emulsion and drug using the same catheter. However, this procedure is not recommended due to potential interaction and lack of safety data. For this purpose, we checked the compatibility of VP solutions with eight commercially available parenteral nutrition admixtures, i.e., Lipoflex special, Omegaflex special, Lipoflex peri, Omegaflex peri, Kabiven, SmofKabiven, Kabiven Peripheral, and Olimel Peri N4E. Coadministration is only possible if the stability of the drug and the lipid emulsion is confirmed. The available data are scarce and only concern the incompatibility of VP with ibuprofen. Compatibility tests were carried out in simulated administration through a Y-site connector using clinical flow rates. The stability of the drug and lipid emulsion was assessed by visual inspection and measurement of pH, osmolality, particle size as mean droplet diameter (MDD) and percentage of lipids residing in globules larger than 5 µm (PFAT5), zeta potential, polydispersity index, and lipid-free parenteral nutrition admixture(PNA) turbidity. The results of the compatibility of VP with eight commercial PN admixtures showed that all lipid emulsions show different signs of destabilization. In the studied samples, particles larger than 1000 nm, a significant increase in MDD, zeta potential, and loss of homogeneity visible as an increase in the polydispersity index were observed. Most of the samples had PFAT5 above the USP limit (0.05%). Taking into account the obtained data, VP should not be administered with the studied lipid emulsions for parenteral nutrition.

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肠外营养乳剂和长春西汀的共同使用潜力：兼容性研究与展望

长春西汀（VP）经口服和静脉注射后分布于丘脑、基底神经节和视觉皮层。由于生物利用度低（约 7%）和明显的首过效应（约 75%），包括半衰期短（2-3 小时），VP 的口服给药受到限制。需要频繁给药才能获得治疗效果。克服这些困难的尝试包括使用新的给药系统和/或替代给药途径。一种可能的方法是使用同一导管共同给药脂质乳剂和药物。然而，由于潜在的相互作用和缺乏安全数据，这种方法并不推荐。为此，我们检查了 VP 溶液与八种市售肠外营养剂（即 Lipoflex special、Omegaflex special、Lipoflex peri、Omegaflex peri、Kabiven、SmofKabiven、Kabiven Peripheral 和 Olimel Peri N4E）的兼容性。只有在药物和脂质乳剂的稳定性得到确认的情况下，才能同时给药。现有数据很少，仅涉及 VP 与布洛芬的不相容性。我们使用临床流速通过 Y 型接头进行了模拟给药的兼容性测试。通过目测和测量 pH 值、渗透压、以平均液滴直径（MDD）表示的粒度和大于 5 µm 的球状脂质百分比（PFAT5）、ZETA 电位、多分散指数和无脂肠外营养混合物（PNA）浊度来评估药物和脂质乳剂的稳定性。VP 与八种商用肠外营养混合物的相容性研究结果表明，所有脂质乳剂都表现出不同的不稳定迹象。在所研究的样品中，大于 1000 nm 的颗粒的 MDD、zeta 电位显著增加，多分散指数增加，均一性丧失。大多数样品中的 PFAT5 超过了美国药典的限值（0.05%）。考虑到所获得的数据，VP 不应与所研究的脂质乳剂一起用于肠外营养。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Metabolites Biochemistry, Genetics and Molecular Biology-Molecular Biology

CiteScore

5.70

自引率

7.30%

发文量

1070

审稿时长

17.17 days

期刊介绍： Metabolites (ISSN 2218-1989) is an international, peer-reviewed open access journal of metabolism and metabolomics. Metabolites publishes original research articles and review articles in all molecular aspects of metabolism relevant to the fields of metabolomics, metabolic biochemistry, computational and systems biology, biotechnology and medicine, with a particular focus on the biological roles of metabolites and small molecule biomarkers. Metabolites encourages scientists to publish their experimental and theoretical results in as much detail as possible. Therefore, there is no restriction on article length. Sufficient experimental details must be provided to enable the results to be accurately reproduced. Electronic material representing additional figures, materials and methods explanation, or supporting results and evidence can be submitted with the main manuscript as supplementary material.