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在活体动物中对作为报告基因的多巴胺D2受体进行重复、非侵入性成像。

Repetitive, non-invasive imaging of the dopamine D2 receptor as a reporter gene in living animals.

作者信息

MacLaren D C, Gambhir S S, Satyamurthy N, Barrio J R, Sharfstein S, Toyokuni T, Wu L, Berk A J, Cherry S R, Phelps M E, Herschman H R

机构信息

Crump Institute for Biological Imaging, UCLA School of Medicine, USA.

出版信息

Gene Ther. 1999 May;6(5):785-91. doi: 10.1038/sj.gt.3300877.

Abstract

Reporter genes (e.g. beta-galactosidase, chloramphenicol-acetyltransferase, green fluorescent protein, luciferase) play critical roles in investigating mechanisms of gene expression in transgenic animals and in developing gene delivery systems for gene therapy. However, measuring expression of these reporter genes requires biopsy or death. We now report a procedure to image reporter gene expression repetitively and non-invasively in living animals with positron emission tomography (PET), using the dopamine type 2 receptor (D2R) as a reporter gene and 3-(2'-[18F]fluoroethyl)spiperone (FESP) as a reporter probe. We use a viral delivery system to demonstrate the ability of this PET reporter gene/PET reporter probe system to image reporter gene expression following somatic gene transfer. In mice injected intravenously with replication-deficient adenovirus carrying a D2R reporter gene, PET in vivo measures of hepatic [18F] retention are proportional to in vitro measures of hepatic FESP retention, D2R ligand binding and D2R mRNA. We use tumor-forming cells carrying a stably transfected D2R gene to demonstrate imaging of this PET reporter gene/PET reporter probe system in 'tissues'. Tumors expressing the transfected D2R reporter gene retain substantially more FESP than control tumors. The D2R/FESP reporter gene/reporter probe system should be a valuable technique to monitor, in vivo, expression from both gene therapy vectors and transgenes.

摘要

报告基因(如β-半乳糖苷酶、氯霉素乙酰转移酶、绿色荧光蛋白、荧光素酶)在研究转基因动物的基因表达机制以及开发用于基因治疗的基因递送系统中发挥着关键作用。然而,测量这些报告基因的表达需要进行活检或导致动物死亡。我们现在报告一种程序,使用多巴胺2型受体(D2R)作为报告基因,3-(2'-[18F]氟乙基)螺哌隆(FESP)作为报告探针,通过正电子发射断层扫描(PET)在活体动物中对报告基因的表达进行重复且非侵入性的成像。我们使用病毒递送系统来证明这种PET报告基因/PET报告探针系统在体细胞基因转移后对报告基因表达进行成像的能力。在静脉注射携带D2R报告基因的复制缺陷型腺病毒的小鼠中,肝脏[18F]保留的PET体内测量值与肝脏FESP保留、D2R配体结合和D2R mRNA的体外测量值成正比。我们使用携带稳定转染D2R基因的肿瘤形成细胞来证明这种PET报告基因/PET报告探针系统在“组织”中的成像。表达转染的D2R报告基因的肿瘤比对照肿瘤保留更多的FESP。D2R/FESP报告基因/报告探针系统应该是一种有价值的技术,用于在体内监测基因治疗载体和转基因的表达。

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