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AAV GCG-EGFP,一种鉴定胰高血糖素分泌α细胞的新工具。

AAV GCG-EGFP, a new tool to identify glucagon-secreting α-cells.

机构信息

Department of Cellular and Physiological Sciences, Life Sciences Institute, University of British Columbia, Vancouver, British Columbia, Canada.

Centro de Investigación Biomédica en Red de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), Madrid, Spain.

出版信息

Sci Rep. 2019 Jul 25;9(1):10829. doi: 10.1038/s41598-019-46735-2.

Abstract

The study of primary glucagon-secreting α-cells is hampered by their low abundance and scattered distribution in rodent pancreatic islets. We have designed a double-stranded adeno-associated virus containing a rat proglucagon promoter (700 bp) driving enhanced green fluorescent protein (AAV GCG-EGFP), to specifically identify α-cells. The administration of AAV GCG-EGFP by intraperitoneal or intraductal injection led to EGFP expression selectively in the α-cell population. AAV GCG-EGFP delivery to mice followed by islet isolation, dispersion and separation by FACS for EGFP resulted in an 86% pure population of α-cells. Furthermore, the administration of AAV GCG-EGFP at various doses to adult wild type mice did not significantly alter body weight, blood glucose, plasma insulin or glucagon levels, glucose tolerance or arginine tolerance. In vitro experiments in transgene positive α-cells demonstrated that EGFP expression did not alter the intracellular Ca pattern in response to glucose or adrenaline. This approach may be useful for studying purified primary α-cells and for the in vivo delivery of other genes selectively to α-cells to further probe their function or to manipulate them for therapeutic purposes.

摘要

研究原发性胰高血糖素分泌细胞(α细胞)受到其在啮齿动物胰岛中含量低和分布分散的限制。我们设计了一种包含大鼠前胰高血糖素启动子(700bp)驱动增强型绿色荧光蛋白(AAV GCG-EGFP)的双链腺相关病毒,以特异性识别α细胞。通过腹腔内或胰管内注射 AAV GCG-EGFP,可使 EGFP 选择性地在α细胞群体中表达。将 AAV GCG-EGFP 递送至小鼠,然后通过 FACS 对胰岛进行分离、分散和分离,可获得 86%纯度的α细胞。此外,以不同剂量向成年野生型小鼠给予 AAV GCG-EGFP 并不会显著改变体重、血糖、血浆胰岛素或胰高血糖素水平、葡萄糖耐量或精氨酸耐量。在转基因阳性α细胞的体外实验中,发现 EGFP 表达不会改变细胞内 Ca2+对葡萄糖或肾上腺素的反应模式。这种方法可能有助于研究纯化的原发性α细胞,并可用于体内选择性地将其他基因递送至α细胞,以进一步探究其功能或用于治疗目的对其进行操作。

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