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新型脂质多层囊泡的生物分布及胃肠道给药

Biodistribution and gastrointestinal drug delivery of new lipidic multilamellar vesicles.

作者信息

Freund O

机构信息

Laboratoire LEMI Technopole Montesquieu, Martillac, France.

出版信息

Drug Deliv. 2001 Oct-Dec;8(4):239-44. doi: 10.1080/107175401317245921.

Abstract

Encapsulation of therapeutic molecules in a new noncationic multilamellar vector (Spherulites), composed of phosphatidylcholine, cholesterol, and polyoxyethylene alcohol, is described here. Spherulites with entrapped drugs were prepared by shearing a phospholipidic lyotropic lamellar phase using a recently discovered method. The average size of these vesicles is approximately 300 nm. Our formulation did not show cytotoxicity to human cells and could be used as a drug delivery system. Our previous experiments showed that this new multilamellar vector is stable in many different buffers such as serum, acidic or basic buffers, and enzymatic buffers and may deliver drugs in vivo. We describe two ways of administration for drug delivery. The tissue biodistribution of radiolabeled Spherulites entrapping 125I protein A was studied after intravenous injection in Wistar rats using the major organs of the body. Approximately 70% of the radioactivity was found in the spleen 60 min after injection and about half this percentage was found in the liver. By 6 hr, only 52% remained in the spleen. The other tissues accumulated <30% of the dose throughout the duration of the study. On the other hand, oral administration of Spherulites, entrapping111 In-NTA, in fasting rats showed a significant increase of radioactivity in blood.

摘要

本文描述了一种由磷脂酰胆碱、胆固醇和聚氧乙烯醇组成的新型非阳离子多层载体(球晶)对治疗性分子的包封。采用最近发现的方法,通过剪切磷脂溶致层状相制备了载药球晶。这些囊泡的平均大小约为300nm。我们的制剂对人类细胞没有细胞毒性,可作为药物递送系统。我们之前的实验表明,这种新型多层载体在许多不同的缓冲液中都很稳定,如血清、酸性或碱性缓冲液以及酶缓冲液,并且可能在体内递送药物。我们描述了两种药物递送的给药方式。在Wistar大鼠静脉注射后,使用身体的主要器官研究了包载125I蛋白A的放射性标记球晶的组织生物分布。注射后60分钟,约70%的放射性出现在脾脏中,肝脏中的放射性约为该百分比的一半。到6小时时,脾脏中仅保留52%的放射性。在整个研究过程中,其他组织累积的剂量<30%。另一方面,在禁食大鼠中口服包载111In-NTA的球晶后,血液中的放射性显著增加。

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