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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Effects of pyrenebutyrate on the translocation of arginine-rich cell-penetrating peptides through artificial membranes: Recruiting peptides to the membranes, dissipating liquid-ordered phases, and inducing curvature
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Effects of pyrenebutyrate on the translocation of arginine-rich cell-penetrating peptides through artificial membranes: Recruiting peptides to the membranes, dissipating liquid-ordered phases, and inducing curvature

机译:pyr酸丁丁酯对富含精氨酸的穿透细胞的肽通过人造膜的转运的影响:将肽募集到膜上,消散液相有序相,并诱导曲率

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摘要

Arginine-rich cell-penetrating peptides, including octaarginine (R8) and HIV-1 TAT peptides, have the ability to translocate through cell membranes and transport exogenous bioactive molecules into cells. Hydrophobic counteranions such as pyrenebutyrate (PyB) have been reported to markedly promote the membrane translocation of these peptides. In this study, using model membranes having liquid-ordered (Lo) and liquid-disordered (Ld) phases, we explored the effects of PyB on the promotion of R8 translocation. Confocal microscopic observations of giant unilamellar vesicles (GUVs) showed that PyB significantly accelerated the accumulation of R8 on membranes containing negatively charged lipids, leading to the internalization of R8 without collapse of the GUV structures. PyB displayed an alternative activity, increasing the fluidity of the negatively charged membranes, which diminished the distinct Lo/Ld phase separation on GUVs. This was supported by the decrease in fluorescence anisotropy of 1,6-diphenyl-1,3,5-hexatriene (DPH). Additionally, PyB induced membrane curvature, which has been suggested as a possible mechanism of membrane translocation for R8. Taken together, our results indicate that PyB may have multiple effects that promote R8 translocation through cell membranes.
机译:富含精氨酸的可穿透细胞的肽,包括八精氨酸(R8)和HIV-1 TAT肽,具有通过细胞膜转运和将外源生物活性分子转运到细胞中的能力。疏水抗衡阴离子如pyr丁酸(PyB)据报道可显着促进这些肽的膜移位。在这项研究中,我们使用具有液体有序(Lo)和液体无序(Ld)相的模型膜,我们探索了PyB对促进R8转运的影响。大单层囊泡(GUVs)的共聚焦显微镜观察显示,PyB显着加速了R8在含有带负电脂质的膜上的积累,从而导致R8内在化而没有GUV结构的崩溃。 PyB显示出另一种活性,增加了带负电荷的膜的流动性,从而减少了GUV上独特的Lo / Ld相分离。 1,6-二苯基-1,3,5-己三烯(DPH)荧光各向异性的降低支持了这一点。此外,PyB诱导的膜曲率被认为是R8膜移位的一种可能机制。两者合计,我们的结果表明PyB可能具有多种促进R8通过细胞膜转运的作用。

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