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细胞穿透肽转运蛋白 10 穿越脂膜及其诱导的孔进入单个囊泡的转运。

Entry of cell-penetrating peptide transportan 10 into a single vesicle by translocating across lipid membrane and its induced pores.

机构信息

Integrated Bioscience Section, Graduate School of Science and Technology, ‡Nanomaterials Research Division, Research Institute of Electronics, and §Department of Physics, Graduate School of Science, Shizuoka University , Shizuoka 422-8529, Japan.

出版信息

Biochemistry. 2014 Jan 21;53(2):386-96. doi: 10.1021/bi401406p. Epub 2014 Jan 8.

Abstract

The cell-penetrating peptide, transportan 10 (TP10), can translocate across the plasma membrane of living cells and thus can be used for the intracellular delivery of biological cargo such as proteins. However, the mechanisms underlying its translocation and the delivery of large cargo remain unclear. In this report we investigated the entry of TP10 into a single giant unilamellar vesicle (GUV) and the TP10-induced leakage of fluorescent probes using the single GUV method. GUVs of 20% dioleoylphosphatidylglycerol (DOPG)/80% dioleoylphosphatidylcholine (DOPC) were prepared, and they contained a water-soluble fluorescent dye, Alexa Fluor 647 hydrazide (AF647), and smaller vesicles composed of 20% DOPG/80% DOPC. The interaction of carboxyfluorescein (CF)-labeled TP10 (CF-TP10) with these loaded GUVs was investigated using confocal microscopy. The fluorescence intensity of the GUV membrane increased with time to a saturated value, then the fluorescence intensity due to the membranes of the smaller vesicles inside the GUV increased prior to leakage of AF647. This result indicates that CF-TP10 entered the GUV from the outside by translocating across the lipid membrane before CF-TP10-induced pore formation. The rate constant of TP10-induced pore formation in lipid membranes increased with an increase in TP10 concentration. Large molecules such as Texas Red Dextran 40,000, and vesicles with a diameter of 1-2 μm, permeated through the TP10-induced pores or local rupture in the lipid membrane. These results provide the first direct experimental evidence that TP10 can deliver large cargo through lipid membranes, without the need for special transport mechanisms such as those found in cells.

摘要

细胞穿透肽,转运素 10(TP10),可以穿过活细胞的质膜,因此可以用于生物货物(如蛋白质)的细胞内递送。然而,其转位和大货物递送的机制尚不清楚。在本报告中,我们使用单个大单层囊泡(GUV)方法研究了 TP10 进入单个巨大的单分子层囊泡(GUV)和 TP10 诱导的荧光探针泄漏的情况。制备了 20%二油酰基磷脂酰甘油(DOPG)/80%二油酰基磷脂酰胆碱(DOPC)的 GUV,它们包含水溶性荧光染料 Alexa Fluor 647 酰肼(AF647)和由 20%DOPG/80%DOPC 组成的较小囊泡。使用共焦显微镜研究了羧基荧光素(CF)标记的 TP10(CF-TP10)与这些负载 GUV 的相互作用。GUV 膜的荧光强度随时间增加到饱和值,然后 GUV 内部较小囊泡的膜的荧光强度在 AF647 泄漏之前增加。这一结果表明,CF-TP10 在形成孔之前,通过穿过脂质膜从外部进入 GUV。脂质膜中 TP10 诱导形成孔的速率常数随 TP10 浓度的增加而增加。像 Texas Red Dextran 40,000 这样的大分子和直径为 1-2μm 的囊泡通过 TP10 诱导的孔或脂质膜的局部破裂渗透。这些结果提供了第一个直接的实验证据,证明 TP10 可以在不需要特殊运输机制(如细胞中发现的那些机制)的情况下,通过脂质膜输送大货物。

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