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碘化酪氨酸-L-毛喉素类似物细胞穿透特性的定量评估

Quantitative evaluation of the cell penetrating properties of an iodinated Tyr-L-maurocalcine analog.

作者信息

Tisseyre Céline, Ahmadi Mitra, Bacot Sandrine, Dardevet Lucie, Perret Pascale, Ronjat Michel, Fagret Daniel, Usson Yves, Ghezzi Catherine, De Waard Michel

机构信息

INSERM, U836, Grenoble Institute of Neuroscience, LabEx Ion Channels, Science and Therapeutics, Grenoble, France; Université Joseph Fourier, Grenoble, France.

Université Joseph Fourier, Grenoble, France; INSERM, U1039, Radiopharmaceutiques Biocliniques, Grenoble, France.

出版信息

Biochim Biophys Acta. 2014 Oct;1843(10):2356-64. doi: 10.1016/j.bbamcr.2014.03.017. Epub 2014 Mar 22.

Abstract

L-Maurocalcine (L-MCa) is the first reported animal cell-penetrating toxin. Characterizing its cell penetration properties is crucial considering its potential as a vector for the intracellular delivery of drugs. Radiolabeling is a sensitive and quantitative method to follow the cell accumulation of a molecule of interest. An L-MCa analog containing an additional N-terminal tyrosine residue (Tyr-L-MCa) was synthesized, shown to fold and oxidize properly, and successfully radioiodinated to (125)I-Tyr-L-MCa. Using various microscopy techniques, the average volume of the rat line F98 glioma cells was evaluated at 8.9 to 18.9×10(-7)μl. (125)I-Tyr-L-MCa accumulates within cells with a dose-dependency similar to the one previously published using 5,6-carboxyfluorescein-L-MCa. According to subcellular fractionation of F98 cells, plasma membranes keep less than 3% of the peptide, regardless of the extracellular concentration, while the nucleus accumulates over 75% and the cytosol around 20% of the radioactive material. Taking into account both nuclear and cytosolic fractions, cells accumulate intracellular concentrations of the peptide that are equal to the extracellular concentrations. Estimation of (125)I-Tyr-L-MCa cell entry kinetics indicate a first rapid phase with a 5min time constant for the plasma membrane followed by slower processes for the cytoplasm and the nucleus. Once inside cells, the labeled material no longer escapes from the intracellular environment since 90% of the radioactivity remains 24h after washout. Dead cells were found to have a lower uptake than live ones. The quantitative information gained herein will be useful for better framing the use of L-MCa in biotechnological applications. This article is part of a Special Issue entitled: Calcium Signaling in Health and Disease. Guest Editors: Geert Bultynck, Jacques Haiech, Claus W. Heizmann, Joachim Krebs, and Marc Moreau.

摘要

L-毛喉素(L-MCa)是首个被报道的可穿透动物细胞的毒素。鉴于其作为药物细胞内递送载体的潜力,表征其细胞穿透特性至关重要。放射性标记是一种灵敏且定量的方法,可用于追踪感兴趣分子在细胞内的积累情况。合成了一种含有额外N端酪氨酸残基的L-MCa类似物(酪氨酸-L-MCa),证明其能正确折叠和氧化,并成功进行放射性碘化,得到(125)I-酪氨酸-L-MCa。使用各种显微镜技术,评估了大鼠F98胶质瘤细胞的平均体积为8.9至18.9×10(-7)微升。(125)I-酪氨酸-L-MCa在细胞内的积累具有剂量依赖性,类似于先前使用5,6-羧基荧光素-L-MCa发表的结果。根据F98细胞的亚细胞分级分离,无论细胞外浓度如何,质膜保留的肽少于3%,而细胞核积累超过75%的放射性物质,细胞质积累约20%。综合考虑细胞核和细胞质部分,细胞积累的肽的细胞内浓度与细胞外浓度相等。对(125)I-酪氨酸-L-MCa细胞进入动力学的估计表明,第一个快速阶段的质膜时间常数为5分钟,随后细胞质和细胞核的过程较慢。一旦进入细胞,标记物质不再从细胞内环境中逸出,因为洗脱后90%的放射性在24小时后仍保留。发现死细胞的摄取量低于活细胞。本文获得的定量信息将有助于更好地规划L-MCa在生物技术应用中的使用。本文是名为:健康与疾病中的钙信号的特刊的一部分。客座编辑:Geert Bultynck、Jacques Haiech、Claus W. Heizmann、Joachim Krebs和Marc Moreau。

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