Lauritzen Hans P M M, Reynet Christine, Schjerling Peter, Ralston Evelyn, Thomas Stephen, Galbo Henrik, Ploug Thorkil
Copenhagen Muscle Research Centre, Department of Medical Physiology 12.4, The Panum Institute, University of Copenhagen, Blegdamsvej 3C, 2200 Copenhagen N, Denmark.
Pflugers Arch. 2002 Sep;444(6):710-21. doi: 10.1007/s00424-002-0862-5. Epub 2002 Jul 27.
Cellular protein trafficking has been studied to date only in vitro or with techniques that are invasive and have a low time resolution. To establish a gentle method for analysis of glucose transporter-4 (GLUT4) trafficking in vivo in fully differentiated rat skeletal muscle fibres we combined the enhanced green fluorescent protein (EGFP) labelling technique with physical transfection methods in vivo: intramuscular plasmid injection or gene gun bombardment. During optimisation experiments with plasmid coding for the EGFP reporter alone EGFP-positive muscle fibres were counted after collagenase treatment of in vivo transfected flexor digitorum brevis (FDB) muscles. In contrast to gene gun bombardment, intramuscular injection produced EGFP expression in only a few fibres. Regardless of the transfection technique, EGFP expression was higher in muscles from 2-week-old rats than in those from 6-week-old rats and peaked around 1 week after transfection. The gene gun was used subsequently with a plasmid coding for EGFP linked to the C-terminus of GLUT4 (GLUT4-EGFP). Rats were anaesthetised 5 days after transfection and insulin given i.v. with or without accompanying electrical hindleg muscle stimulation. After stimulation, the hindlegs were fixed by perfusion. GLUT4-EGFP-positive FDB fibres were isolated and analysed by confocal microscopy. The intracellular distribution of GLUT4-EGFP under basal conditions as well as after translocation to the plasma membrane in response to insulin, contractions, or both, was in accordance with previous studies of endogenous GLUT4. Finally, GLUT4-EGFP trafficking in quadriceps muscle in vivo was studied using time-lapse microscopy analysis in anaesthetised mice and the first detailed time-lapse recordings of GLUT4-EGFP translocation in fully differentiated skeletal muscle in vivo were obtained.
迄今为止,细胞蛋白质运输仅在体外进行了研究,或者采用的是侵入性技术,且时间分辨率较低。为了建立一种温和的方法来分析完全分化的大鼠骨骼肌纤维中葡萄糖转运蛋白4(GLUT4)的体内运输情况,我们将增强型绿色荧光蛋白(EGFP)标记技术与体内物理转染方法相结合:肌肉内注射质粒或基因枪轰击。在用仅编码EGFP报告基因的质粒进行优化实验期间,在对体内转染的趾短屈肌(FDB)进行胶原酶处理后,对EGFP阳性肌纤维进行计数。与基因枪轰击相比,肌肉内注射仅在少数纤维中产生EGFP表达。无论采用何种转染技术,2周龄大鼠肌肉中的EGFP表达均高于6周龄大鼠,且在转染后约1周达到峰值。随后使用基因枪,将编码与GLUT4 C末端相连的EGFP的质粒(GLUT4-EGFP)进行转染。转染5天后对大鼠进行麻醉,并静脉注射胰岛素,同时或不同时伴有后肢肌肉电刺激。刺激后,通过灌注固定后肢。分离出GLUT4-EGFP阳性的FDB纤维,并通过共聚焦显微镜进行分析。基础条件下以及响应胰岛素、收缩或两者刺激后GLUT4-EGFP向质膜转位后的细胞内分布,与先前对内源性GLUT4的研究结果一致。最后,在麻醉小鼠中使用延时显微镜分析研究了股四头肌中GLUT4-EGFP的体内运输情况,并获得了完全分化的骨骼肌中GLUT4-EGFP转位的首个详细延时记录。