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非病毒基因递送载体对人补体系统的作用:基于lacZ质粒和磷脂/寡聚阳离子脂质体的脂质体复合物的低抗补体活性

Action of nonviral gene delivery vectors on human complement system: low anticomplementary activity of lipoplexes based on lacZ plasmid and phospholipid/oligocation liposomes.

作者信息

Kozlov L V, Zhdanov R I, Guzova V A, Podobed V, Sviridov Y V, Bogdanenko E V, Shvets V I, Dyabina S, Ermakov A S

机构信息

G. N. Gabrichevskii Moscow Research Institute of Epidemiology and Microbiology, Russia.

出版信息

Cytobios. 2001;106 Suppl 1:67-74.

PMID:11534830
Abstract

A simple test-system has been developed for the first time in order to detect the ability of effectors (lipoplexes) to activate the complement system in an antibody-independent manner to serve as acceptors of nascent C4b and to inhibit formation of the key enzyme of complement, C3-convertase. The effect of plasmid DNA (pCMV-SPORT-LacZ), negatively charged cardiolipin (CL), neutral phosphatidylcholine (PC) vesicles and their lipoplexes, on the complement system was studied using the method developed. It was revealed that PC vesicles did not affect the complement system, while CL vesicles manifested low activation. The influence of plasmid DNA and its lipoplex based on PC liposomes as well on the complement system was very low. PC/LacZ lipoplex (143 microg/ml) acted on the complement system like 5.36 microg/ml heat aggregated IgG (agg) (the level of no pathological ruptures), whereas CL/LacZ lipoplex (143 microg/ml) acted similar to 10.7 microg/ml IgG (agg). Thus, weak activation of the complement system with CL lipoplex, and even weaker for the PC lipoplex testified to the use of neutral and positively charged lipoplexes preferably in gene therapy protocols. The technique can also be used for testing the influence of injectable gene therapy vectors on the complement system.

摘要

首次开发了一种简单的测试系统,以检测效应物(脂质体复合物)以抗体非依赖方式激活补体系统、作为新生C4b受体以及抑制补体关键酶C3转化酶形成的能力。使用所开发的方法研究了质粒DNA(pCMV-SPORT-LacZ)、带负电荷的心磷脂(CL)、中性磷脂酰胆碱(PC)囊泡及其脂质体复合物对补体系统的影响。结果显示,PC囊泡不影响补体系统,而CL囊泡表现出低激活。质粒DNA及其基于PC脂质体的脂质体复合物对补体系统的影响也非常小。PC/LacZ脂质体复合物(143微克/毫升)对补体系统的作用类似于5.36微克/毫升热聚集IgG(agg)(无病理破裂水平),而CL/LacZ脂质体复合物(143微克/毫升)的作用类似于10.7微克/毫升IgG(agg)。因此,CL脂质体复合物对补体系统的弱激活,以及PC脂质体复合物更弱的激活,证明在基因治疗方案中最好使用中性和带正电荷的脂质体复合物。该技术也可用于测试可注射基因治疗载体对补体系统的影响。

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