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聚酰胺-胺-碱性蓝树枝状大分子用于紫杉醇递送的淋巴暴露增强及渗透压对淋巴靶向影响的研究

Study on enhanced lymphatic exposure of polyamidoamin-alkali blue dendrimer for paclitaxel delivery and influence of the osmotic pressure on the lymphatic targeting.

作者信息

Yang Rui, Mao Yuling, Ye Tiantian, Xia Suxia, Wang Shujun, Wang Siling

机构信息

a Department of Pharmaceutics , Shenyang Pharmaceutical University , Shenyang , P.R. China and.

b Laboratory of Clinical Pharmacology, Academe of Traditional Chinese Medicine of Liaoning Province , Shenyang , P.R. China.

出版信息

Drug Deliv. 2016 Sep;23(7):2617-2629. doi: 10.3109/10717544.2015.1041577. Epub 2015 May 28.

DOI:10.3109/10717544.2015.1041577
PMID:26017243
Abstract

In this study, paclitaxel (PTX)-loaded polyamidoamin-alkali blue (PTX-P-AB) was prepared in order to investigate the intralymphatic targeting ability and anti-cancer effect after subcutaneous (s.c.) administration. The physicochemical properties and in vitro drug release were evaluated. The lymphatic drainage and lymph nodes (LNs) uptake were examined by pharmacokinetics and distribution recovery of PTX in plasma, LNs, injection site (IS) and tissues after s.c. injection in healthy mice and in tumor-bearing mice. The osmotic pressure of PTX-P-AB affecting the lymphatic targeting was studied. The anti-tumor activity of PTX-P-AB was investigated in mice bearing S180 metastatic tumors. Results showed that PTX-P-AB with suitable and stable physicochemical properties could be used for in vivo lymphatic studies, and displayed the more rapid lymphatic absorption, the higher AUC value in LNs, the longer LNs residence time and the higher metastasis-inhibiting rate compared with Taxol®. Enhanced lymphatic drainage from the IS and uptake into lymph by increasing the osmotic pressure of PTX-P-AB indicated that PTX-P-AB possesses the double function of lymphatic tracing and lymphatic targeting, and suggested the potential for the development of lymphatic targeting vectors and the lymphatic tracer for treatment and diagnosis.

摘要

在本研究中,制备了负载紫杉醇(PTX)的聚酰胺胺-碱性蓝(PTX-P-AB),以研究皮下(s.c.)给药后的淋巴内靶向能力和抗癌效果。评估了其理化性质和体外药物释放情况。通过健康小鼠和荷瘤小鼠皮下注射后血浆、淋巴结(LNs)、注射部位(IS)和组织中PTX 的药代动力学和分布回收情况,检测了淋巴引流和淋巴结摄取。研究了PTX-P-AB 的渗透压对淋巴靶向的影响。在荷S180 转移性肿瘤的小鼠中研究了PTX-P-AB 的抗肿瘤活性。结果表明,具有合适且稳定理化性质的PTX-P-AB 可用于体内淋巴研究,与紫杉醇相比,其淋巴吸收更快,淋巴结中的AUC 值更高,淋巴结停留时间更长,转移抑制率更高。通过增加PTX-P-AB 的渗透压增强了从注射部位的淋巴引流和对淋巴的摄取,表明PTX-P-AB 具有淋巴示踪和淋巴靶向双重功能,并提示了开发用于治疗和诊断的淋巴靶向载体和淋巴示踪剂的潜力。

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