使用水溶性脂聚合物进行瘤内递送p2CMVmIL-12。
Intratumoral delivery of p2CMVmIL-12 using water-soluble lipopolymers.
作者信息
Mahato R I, Lee M, Han S, Maheshwari A, Kim S W
机构信息
Center for Controlled Chemical Delivery, Department of Pharmaceutics and Pharmaceutical Chemistry, University of Utah, Salt Lake City, Utah 84112, USA.
出版信息
Mol Ther. 2001 Aug;4(2):130-8. doi: 10.1006/mthe.2001.0425.
Our objective was to design a water-soluble lipopolymer (WSLP) and an interleukin-12 (IL-12) expression plasmid for enhanced delivery of the IL-12 gene. We synthesized WSLP using branched polyethylenimine (PEI) of 1800 Da and cholesteryl chloroformate, and constructed p2CMVmIL-12, encoding the IL-12 subunits p35 and p40, each under the transcriptional control of a separate cytomegalovirus (CMV) promoter. The percentage of cholesterol conjugated to PEI was about 47% and the average molecular weight of WSLP was approximately 2000 Da. The mean particle size of WSLP/p2CMVmIL-12 complexes formulated in 5% glucose was 26 to 62 nm and xi potential was 8 to 60 mV. The WSLP/p2CMVmIL-12 complexes were nontoxic to CT-26 colon carcinoma cells at the N/P ratio (nitrogen atoms of WSLP/phosphate of plasmid DNA) of 20 and below; PEI25000/pDNA complexes were highly toxic. WSLP/p2CMVmIL-12 complexes demonstrated higher transfection in CT-26 cells compared with the DNA formulations prepared using PEI of molecular weights 1800, 10,000 and 25,000 Da. Transfection efficiency increased with an increase in N/P ratios from 5 to 15, then there was no significant increase in transfection up to the N/P ratio of 30/1. There was an increase in the level of IL-12 when free or complexed p2CMVmIL-12 was compared with free or complexed pIRESmIL-12 in which the p35 and p40 subunits were linked to the internal ribosome entry sites (IRES). At 48 hours post-injection of WSLP/p2CMVmIL-12 complexes into BALB/c mice bearing CT-26 subcutaneous tumors, the levels of IL-12, IFN-gamma, and nitric oxide (NO) in the supernatant of the cultured tumors were higher for the WSLP/p2CMVmIL-12 complexes than for the naked p2CMVmIL-12, WSLP, and 5% glucose injected groups. There was a significant improvement in the survival rate and the inhibition of tumor growth after a single injection of WSLP/p2CMVmIL-12 complexes. We have designed an effective, nontoxic WSLP and an IL-12 expression plasmid with two CMV promoters.
我们的目标是设计一种水溶性脂聚合物(WSLP)和一种白细胞介素-12(IL-12)表达质粒,以增强IL-12基因的递送。我们使用1800 Da的支链聚乙烯亚胺(PEI)和胆固醇氯甲酸酯合成了WSLP,并构建了p2CMVmIL-12,其编码IL-12亚基p35和p40,每个亚基都在单独的巨细胞病毒(CMV)启动子的转录控制下。与PEI缀合的胆固醇百分比约为47%,WSLP的平均分子量约为2000 Da。在5%葡萄糖中配制的WSLP/p2CMVmIL-12复合物的平均粒径为26至62 nm,ζ电位为8至60 mV。WSLP/p2CMVmIL-12复合物在N/P比(WSLP的氮原子/质粒DNA的磷酸根)为20及以下时对CT-26结肠癌细胞无毒;PEI25000/pDNA复合物具有高毒性。与使用分子量为1800、10000和25000 Da的PEI制备的DNA制剂相比,WSLP/p2CMVmIL-12复合物在CT-26细胞中表现出更高的转染率。转染效率随着N/P比从5增加到15而增加,然后直到N/P比为30/1时转染率没有显著增加。当将游离或复合的p2CMVmIL-12与游离或复合的pIRESmIL-12(其中p35和p40亚基与内部核糖体进入位点(IRES)相连)进行比较时,IL-12水平有所增加。将WSLP/p2CMVmIL-12复合物注射到携带CT-26皮下肿瘤的BALB/c小鼠中48小时后,培养的肿瘤上清液中WSLP/p2CMVmIL-12复合物的IL-12、干扰素-γ和一氧化氮(NO)水平高于裸p2CMVmIL-12、WSLP和5%葡萄糖注射组。单次注射WSLP/p2CMVmIL-12复合物后,存活率和肿瘤生长抑制有显著改善。我们设计了一种有效的、无毒的WSLP和一种带有两个CMV启动子的IL-12表达质粒。
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