Osman Eyman, Evans Vanessa, Graham Ian R, Athanasopoulos Takis, McIntosh Jenny, Nathwani Amit C, Simons J Paul, Dickson George, Owen James S
Department of Medicine, Royal Free & University College Medical School, London, UK.
Atherosclerosis. 2009 May;204(1):121-6. doi: 10.1016/j.atherosclerosis.2008.08.043. Epub 2008 Sep 11.
Hepatic gene transfer of atheroprotective human apoE by recombinant viral vectors can reverse hypercholesterolaemia and inhibit atherogenesis in apoE-deficient (apoE(-/-)) mice. Here, in preliminary studies we assess the effectiveness of a recently developed self-complementary adeno-associated virus (scAAV) serotype 8 vector, driven by a hepatocyte-specific promoter (LP1), for liver-directed gene delivery of human apoE3. Vector viability was validated by transducing cultured HepG2 cells and measuring secretion of apoE3 protein. Male and female apoE(-/-) mice, 6-month old and fed on normal chow, were intravenously injected with 1x10(11) vg (vector genomes) of scAAV2/8.LP1.apoE3; age-matched untreated mice served as controls. In male mice, plasma apoE3 levels were sufficiently high (up to 17 microg/ml) to normalize plasma total cholesterol and ameliorate their proatherogenic lipoprotein profile, by reducing VLDL/LDL and increasing HDL 5-fold. At termination (12 weeks) development of aortic atherosclerosis was significantly retarded by 58% (aortic lesion area 8.2+/-1.4% vs. 19.3+/-2.4% in control males; P<0.001). Qualitatively similar anti-atherogenic effects were noted when female mice were treated, but the benefits were less marked and aortic lesions, for example, were reduced by only 33% (15.7+/-3.7% vs. 23.6+/-6.9%). Although group numbers were small (n=4/5), this gender-specific difference reflected two to three times less apoE3 in plasma of female mice at weeks 3 and 6, implying that gene transfer to female liver using scAAV vectors may require additional optimization, despite their established superior potency to conventional single-stranded (ssAAV) vectors.
通过重组病毒载体将具有抗动脉粥样硬化作用的人载脂蛋白E(apoE)进行肝脏基因转移,可逆转高胆固醇血症并抑制载脂蛋白E缺陷(apoE(-/-))小鼠的动脉粥样硬化形成。在此,在初步研究中,我们评估了一种最近开发的由肝细胞特异性启动子(LP1)驱动的自我互补腺相关病毒(scAAV)血清型8载体用于人apoE3肝脏定向基因递送的有效性。通过转导培养的HepG2细胞并测量apoE3蛋白的分泌来验证载体的活力。给6个月大、喂食普通饲料的雄性和雌性apoE(-/-)小鼠静脉注射1×10(11) vg(载体基因组)的scAAV2/8.LP1.apoE3;年龄匹配的未处理小鼠作为对照。在雄性小鼠中,血浆apoE3水平足够高(高达17μg/ml),通过降低极低密度脂蛋白/低密度脂蛋白(VLDL/LDL)并使高密度脂蛋白(HDL)增加5倍,使血浆总胆固醇正常化并改善其促动脉粥样硬化脂蛋白谱。在实验结束时(12周),主动脉粥样硬化的发展显著延缓了58%(主动脉病变面积在对照雄性小鼠中为19.3±2.4%,而处理组为8.2±1.4%;P<0.001)。当处理雌性小鼠时,观察到了定性相似的抗动脉粥样硬化作用,但益处不太明显,例如主动脉病变仅减少了33%(15.7±3.7%对23.6±6.9%)。尽管每组数量较少(n = 4/5),但这种性别特异性差异反映出在第3周和第6周时雌性小鼠血浆中的apoE3比雄性小鼠少两到三倍,这意味着尽管scAAV载体相对于传统单链(ssAAV)载体已确立具有更高的效力,但使用scAAV载体将基因转移到雌性肝脏可能需要进一步优化。
