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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Ultradeformable lipid vesicles can penetrate the skin and other semi-permeable barriers unfragmented. Evidence from double label CLSM experiments and direct size measurements
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Ultradeformable lipid vesicles can penetrate the skin and other semi-permeable barriers unfragmented. Evidence from double label CLSM experiments and direct size measurements

机译:超可变形的脂质囊泡可以穿透皮肤和其他半透明的屏障而不会破裂。来自双标签CLSM实验和直接尺寸测量的证据

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The stability of various aggregates in the form of lipid bilayer vesicles was tested by three different methods before and after crossing different semi-permeable barriers. First, polymer membranes with pores significantly smaller than the average aggregated diameter were used as the skin barrier model; dynamic light scattering was employed to monitor vesicle size changes after barrier passage for several lipid mixtures with different bilayer elasticities. This revealed that vesicles must adapt their size and/or shape, dependent on bilayer stability and elasto-mechanics, to overcome an otherwise confining pore. For the mixed lipid aggregates with highly flexible bilayers (Transfersomes), the change is transient and only involves vesicle shape and volume adaptation. The constancy of ultradeformable vesicle size before and after pores penetration proves this. This is remarkable in light of the very strong aggregate deformation during an enforced barrier passage. Simple phosphatidylcholine vesicles, with less flexible bilayers, lack such capability and stability. Conventionalkiposomes are therefore fractured during transport through a semip-permeable barrier; as reported by other researchers, liposomes are fragmented to the size of a narrow pore if sufficient pressure is applied across the barrier; otherwise, liposomes clog the pores. The precise outcome depends on trans-barrier flux and/or on relative vesicle vs. pore size. Lipid vescles applied on the skin behave accordingly. Mixed lipid vesicles penetrate the skin if they are sufficiently deformable. If this is the case, they cross inter-cellularconstrictions in the organ without significant composition or size modification. To prove this, we labelled vesicles with two different fluorescent markers and applied the suspension on intact murine skin without occlusion. The confocal laser scanning microscopy (CLSM) of the skin then revealed a practically indistinguishable distribution of both labels in the stratum corneum, corroborating the first assumption To confirm the second postulate, we compared vesicle size in the starting suspension and in the blood after non-invasive transcutaneous aggregate delivery. Size exclusion chromatograms of sera from the mice that received ultradeformable vesicles on the skin were undistinguishable from the results measured with the original vesicle suspension. Taken together, the results support our previous postulate that ultradeformable vesicles penetrate the skin intact, that is, without permanent disintegration.
机译:在穿过不同的半渗透性屏障之前和之后,通过三种不同的方法测试了脂质双层囊泡形式的各种聚集体的稳定性。首先,将具有明显小于平均聚集直径的孔的聚合物膜用作皮肤屏障模型。对于具有不同双层弹性的几种脂质混合物,动态光散射用于监测屏障通过后囊泡大小的变化。这表明,取决于双层的稳定性和弹性力学,囊泡必须适应其大小和/或形状,以克服否则会局限的孔。对于具有高度柔性双层的混合脂质聚集体(Transfersomes),变化是短暂的,仅涉及囊泡形状和体积适应性。孔穿透之前和之后超可变形囊泡大小的恒定性证明了这一点。鉴于在强制性屏障通过过程中非常强烈的聚集体变形,这是非常明显的。具有较少柔性双层的简单磷脂酰胆碱囊泡缺乏这种能力和稳定性。因此,传统的脂质体在通过半渗透性屏障的运输过程中破裂。正如其他研究人员所报道的那样,如果对屏障施加足够的压力,脂质体会破碎成狭窄的孔。否则,脂质体会堵塞毛孔。精确的结果取决于反渗透通量和/或相对囊泡与孔径的关系。涂在皮肤上的脂质囊相应地起作用。如果混合脂质囊泡充分可变形,它们会穿透皮肤。如果是这种情况,它们会穿过器官中的细胞间收缩而没有明显的组成或大小改变。为了证明这一点,我们用两种不同的荧光标记物标记了囊泡,并将其悬浮在完整的鼠科动物皮肤上而没有阻塞。皮肤的共聚焦激光扫描显微镜(CLSM)随后揭示了角质层中两种标记物的分布几乎没有区别,证实了第一个假设。为确认第二个假设,我们比较了起始悬浮液和非悬浮液后血液中的囊泡大小。有创经皮聚集输送。来自在皮肤上接受超可变形囊泡的小鼠的血清的尺寸排阻色谱图与用原始囊泡悬浮液测得的结果没有区别。两者合计,这些结果支持了我们先前的假设,即超可变形囊泡完好无损地穿透皮肤,也就是说,不会永久崩解。

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