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雷帕霉素对小鼠唾液腺中单个腺相关病毒载体转基因表达的调控

Rapamycin control of transgene expression from a single AAV vector in mouse salivary glands.

作者信息

Wang J, Voutetakis A, Papa M, Rivera V M, Clackson T, Lodde B M, Mineshiba F, Baum B J

机构信息

Gene Therapy and Therapeutics Branch, NIDCR, NIH, DHHS, Bethesda, MD 20892, USA.

出版信息

Gene Ther. 2006 Jan;13(2):187-90. doi: 10.1038/sj.gt.3302647.

Abstract

Salivary glands (SGs) appear to be a useful target site for gene therapeutics. The ability to control transgene expression is essential for clinical application. Previously, in a proof-of-concept study, we have shown that the rapamycin-inducible transcriptional regulation system can regulate protein expression after adenoviral-mediated gene transfer to SGs. To evaluate the potential ability to utilize this regulatory system for long-term control of transgene expression in this tissue, we employed a 'third generation', single adenoassociated serotype 2 viral (AAV2) vector encoding human erythropoietin (hEPO) under the control of a rapamycin-inducible promoter. The vector, rAAV-TF2.3-hEPO (10(10) particles/animal), was delivered to mouse SGs. No detectable increase in serum hEPO or hematocrit levels was observed in the absence of rapamycin administration. However, rapamycin induced elevation of serum hEPO levels, as well as concomitant hematocrit changes, that were dose-dependent, completely reversible, and relatively stable over the course of this study (6 months), with no appreciable change in rapamycin responsiveness. Our results suggest that the rapamycin transcriptional regulation system delivered in a single AAV2 vector to SGs may be valuable for systemic protein replacement applications.

摘要

唾液腺似乎是基因治疗的一个有用靶位点。控制转基因表达的能力对于临床应用至关重要。此前,在一项概念验证研究中,我们已表明雷帕霉素诱导的转录调控系统在腺病毒介导的基因转移至唾液腺后可调节蛋白质表达。为评估利用该调控系统对该组织中转基因表达进行长期控制的潜在能力,我们采用了一种“第三代”、单腺相关血清型2病毒(AAV2)载体,其在雷帕霉素诱导型启动子的控制下编码人促红细胞生成素(hEPO)。该载体rAAV-TF2.3-hEPO(10¹⁰颗粒/动物)被递送至小鼠唾液腺。在未给予雷帕霉素的情况下,未观察到血清hEPO或血细胞比容水平有可检测到的升高。然而,雷帕霉素诱导血清hEPO水平升高以及伴随的血细胞比容变化,这些变化呈剂量依赖性、完全可逆,且在本研究过程(6个月)中相对稳定,雷帕霉素反应性无明显变化。我们的结果表明,以单一AAV2载体递送至唾液腺的雷帕霉素转录调控系统对于全身性蛋白质替代应用可能具有重要价值。

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