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疏水性药物的脂质体制剂

Liposome Formulations of Hydrophobic Drugs.

作者信息

Schwendener Reto A, Schott Herbert

机构信息

Laboratory of Liposome Research, Institute of Molecular Cancer Research, University of Zürich, Winterthurerstrasse 190, 8057, Zurich, Switzerland.

Institute of Organic Chemistry, Eberhard-Karls University, Auf der Morgenstelle 18, 72076, Tübingen, Germany.

出版信息

Methods Mol Biol. 2017;1522:73-82. doi: 10.1007/978-1-4939-6591-5_6.

Abstract

Here we report methods of preparation for liposome formulations containing lipophilic drugs. In contrast to the encapsulation of water soluble compounds into the entrapped aqueous volume of a liposome, drugs with lipophilic properties are incorporated into the phospholipid bilayer membrane. Water-soluble molecules, for example cytotoxic or antiviral nucleosides can be transformed into lipophilic compounds by attachment of long alkyl chains, allowing their stable incorporation into liposome membranes and taking advantage of the high loading capacity lipid bilayers provide for lipophilic molecules. We created a new class of cytotoxic drugs by chemical transformation of the hydrophilic drugs cytosine-arabinoside (ara-C), 5-fluoro-deoxyuridine (5-FdU), and ethinylcytidine (ETC) into lipophilic compounds and their formulation in liposomes.The concept of chemical modification of water-soluble molecules by attachment of long alkyl chains and their stable incorporation into liposome bilayer membranes represent a very promising method for the development of new drugs not only for the treatment of tumors or infections but also for many other diseases.

摘要

在此,我们报告了含有亲脂性药物的脂质体制剂的制备方法。与将水溶性化合物包封到脂质体截留的水相中不同,具有亲脂性的药物被掺入磷脂双分子层膜中。水溶性分子,例如细胞毒性或抗病毒核苷,可以通过连接长烷基链转化为亲脂性化合物,从而使其稳定地掺入脂质体膜中,并利用脂质双分子层为亲脂性分子提供的高负载能力。我们通过将亲水性药物阿糖胞苷(ara-C)、5-氟脱氧尿苷(5-FdU)和乙炔基胞苷(ETC)化学转化为亲脂性化合物并将其制成脂质体制剂,创造了一类新的细胞毒性药物。通过连接长烷基链对水溶性分子进行化学修饰并将其稳定地掺入脂质体双分子层膜的概念,不仅对于开发用于治疗肿瘤或感染的新药,而且对于许多其他疾病来说,都是一种非常有前景的方法。

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