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流体动力学肝脏基因转移机制涉及短暂的肝血窦血流停滞和大量肝细胞内吞小泡。

Hydrodynamic liver gene transfer mechanism involves transient sinusoidal blood stasis and massive hepatocyte endocytic vesicles.

作者信息

Crespo A, Peydró A, Dasí F, Benet M, Calvete J J, Revert F, Aliño S F

机构信息

Departamento de Farmacología, Valencia, Spain.

出版信息

Gene Ther. 2005 Jun;12(11):927-35. doi: 10.1038/sj.gt.3302469.

Abstract

The present study contributes to clarify the mechanism underlying the high efficacy of hepatocyte gene transfer mediated by hydrodynamic injection. Gene transfer experiments were performed employing the hAAT gene, and the efficacy and differential identification in mouse plasma of human transgene versus mouse gene was assessed by ELISA and proteomic procedures, respectively. By applying different experimental strategies such as cumulative dose-response efficacy, hemodynamic changes reflected by venous pressures, intravital microscopy, and morphological changes established by transmission electron microscopy, we found that: (a) cumulative multiple doses of transgene by hydrodynamic injection are efficient and well tolerated, resulting in therapeutic plasma levels of hAAT; (b) hydrodynamic injection mediates a transient inversion of intrahepatic blood flow, with circulatory stasis for a few minutes mainly in pericentral vein sinusoids; (c) transmission electron microscopy shows hydrodynamic injection to promote massive megafluid endocytic vesicles among hepatocytes around the central vein but not in hepatocytes around the periportal vein. We suggest that the mechanism of hydrodynamic liver gene transfer involves transient inversion of intrahepatic flow, sinusoidal blood stasis, and massive fluid endocytic vesicles in pericentral vein hepatocytes.

摘要

本研究有助于阐明经流体动力学注射介导的肝细胞基因转移高效性的潜在机制。采用hAAT基因进行基因转移实验,并分别通过酶联免疫吸附测定(ELISA)和蛋白质组学方法评估人转基因与小鼠基因在小鼠血浆中的功效及差异识别。通过应用不同的实验策略,如累积剂量 - 反应功效、静脉压力反映的血流动力学变化、活体显微镜检查以及透射电子显微镜确定的形态学变化,我们发现:(a)通过流体动力学注射给予累积多剂量的转基因是有效的且耐受性良好,可产生治疗性的hAAT血浆水平;(b)流体动力学注射介导肝内血流的短暂反转,主要在中央静脉窦状隙出现几分钟的循环停滞;(c)透射电子显微镜显示流体动力学注射促进中央静脉周围肝细胞中出现大量巨大流体胞饮小泡,但门周静脉周围的肝细胞中未出现。我们认为,流体动力学肝脏基因转移的机制涉及肝内血流的短暂反转、窦状隙血液停滞以及中央静脉肝细胞中的大量流体胞饮小泡。

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