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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Cargo delivery kinetics of cell-penetrating peptides
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Cargo delivery kinetics of cell-penetrating peptides

机译:细胞穿透肽的货运动力学

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摘要

A diversity of cell-penetrating peptides (CPPs), is known, but so far the only common denominator for these peptides is the ability to gain cell entry in an energy-independent manner. The mechanism used by CPPs for cell entry is largely unknown, and data comparing the different peptides are lacking. In order to gain more information about the cell-penetrating process. As well as to quantitatively compare the uptake efficiency of different CPPs, we have studied the cellular uptake and cargo delivery kinetics of penetration, transportan, Tat (48-60) and MAP (KLAL). The respective CPPs (labelled with the fluorescence quencher, 3-nitrotyrosine) are coupled to small a pentapeptide cargo (labelled with the 2-amino benzoic acid fluorophore) via a disulfide bond. The cellular uptake of the cargo is registered as an increase in fluorescence intensity when the disulfide bond of the CPP-S-S-cargo construct is reduced in the intracellular milieu. Our data show that MAP has the fastest uptake, followed by transportan, Tat(48-60) and, last, penetration. Similarly, MAP has the highest cargo delivery efficiency, followed by transportan, Tat(48-60) and, last, penetration. Since some CPPs have been found to be toxic at high concentration, we characterized the influence of CPPs on cellular 2-[~3H]deoxyglucose-6-phosphate leakage. Measurements on this system show that the membrane-disturbing potential appears to be correlated with the hydrophobic moment of the peptides. In summary, the yield and kinetics of cellular cargo delivery for four different CPPs has been quantitatively characterized.
机译:已知多种细胞穿透肽(CPP),但是到目前为止,这些肽的唯一共同点是以能量独立的方式获得细胞进入的能力。 CPP用于细胞进入的机制很大程度上未知,并且缺乏比较不同肽的数据。为了获得有关细胞穿透过程的更多信息。除了定量比较不同CPP的吸收效率外,我们还研究了渗透,转运蛋白,Tat(48-60)和MAP(KLAL)的细胞吸收和货物输送动力学。各自的CPP(用荧光猝灭剂3-硝基酪氨酸标记)通过二硫键与小的五肽货物(用2-氨基苯甲酸荧光团标记)偶联。当CPP-S-S-货物构建体的二硫键在细胞内环境中减少时,货物对细胞的细胞摄取被记录为荧光强度的增加。我们的数据表明,MAP吸收最快,其次是转运蛋白,Tat(48-60),最后是渗透率。同样,MAP的货物交付效率最高,其次是运输,Tat(48-60),最后是渗透。由于已发现某些CPP在高浓度下是有毒的,因此我们表征了CPP对细胞2- [〜3H]脱氧葡萄糖-6-磷酸泄漏的影响。在该系统上的测量表明,干扰膜的电位似乎与肽的疏水力矩有关。总之,已经定量表征了四种不同的CPP的细胞货物递送的产率和动力学。

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