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胆固醇作为聚乙二醇化和叶酸受体靶向脂质体中靶向配体的双层锚定物。

Cholesterol as a bilayer anchor for PEGylation and targeting ligand in folate-receptor-targeted liposomes.

作者信息

Zhao Xiaobin B, Muthusamy Natarajan, Byrd John C, Lee Robert J

机构信息

Division of Pharmaceutics, NCI OSU Comprehensive Cancer Center, NSF Nanoscales Science and Engineering Center (NSEC), College of Pharmacy, The Ohio State University, 542 LM Parks Hall, 500 W. 12th Ave, Columbus, Ohio 43210, USA.

出版信息

J Pharm Sci. 2007 Sep;96(9):2424-35. doi: 10.1002/jps.20885.

Abstract

Phospholipids have been extensively evaluated as an anchor for both PEGylation and receptor-targeting in liposomal formulations. However, cholesterol, another important component in biomembranes, has not been fully investigated as an alternative anchor. In this study, the potential role of cholesterol for anchoring PEG and folate was investigated. Cholesterol derivatives were synthesized for PEGylation (mPEG-cholesterol) and folate receptor (FR) targeting (folate-PEG-cholesterol) and incorporated into the bilayer of FR-targeted liposomal doxorubicin. The colloidal stability of these cholesterol derivative-containing liposomes was superior to non-PEGylated liposomes, indicating that steric barrier provided by mPEG-cholesterol can efficiently inhibit aggregation of liposomes. FR-targeting activity of these liposomes was demonstrated by in vitro cell-binding studies on FR-overexpressing KB cells. In addition, in vivo circulation of cholesterol-anchored liposomes was prolonged compared to non-PEGylated liposomes. These studies suggest that cholesterol is a viable bilayer anchor for synthesis of PEGylated and FR-targeted liposomes.

摘要

磷脂作为脂质体制剂中聚乙二醇化和受体靶向的锚定物已得到广泛评估。然而,生物膜中的另一个重要成分胆固醇作为替代锚定物尚未得到充分研究。在本研究中,研究了胆固醇在锚定聚乙二醇(PEG)和叶酸方面的潜在作用。合成了用于聚乙二醇化的胆固醇衍生物(甲氧基聚乙二醇胆固醇,mPEG-胆固醇)和靶向叶酸受体(FR)的衍生物(叶酸-聚乙二醇-胆固醇),并将其掺入靶向FR的阿霉素脂质体双层中。这些含胆固醇衍生物的脂质体的胶体稳定性优于未聚乙二醇化的脂质体,表明mPEG-胆固醇提供的空间位阻屏障可有效抑制脂质体聚集。通过对FR过表达的KB细胞进行体外细胞结合研究,证实了这些脂质体的FR靶向活性。此外,与未聚乙二醇化的脂质体相比,胆固醇锚定脂质体的体内循环时间延长。这些研究表明,胆固醇是合成聚乙二醇化和靶向FR脂质体的可行双层锚定物。

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