HHMI, Department of Cardiology, Boston Children's Hospital, Boston, Massachusetts 02115, USA.
Nat Commun. 2012;3:990. doi: 10.1038/ncomms1999.
Bacterial mechanosensitive channels are some of the largest pores in nature. In particular, MscL, with a pore diameter >25 Å, allows passage of large organic ions and small proteins. Functional MscL reconstitution into lipids has been proposed for applications in vesicular-based drug release. Here we show that these channels can be functionally expressed in mammalian cells to afford rapid controlled uptake of membrane-impermeable molecules. We first demonstrate that MscL gating in response to increased membrane tension is preserved in mammalian cell membranes. Molecular delivery is controlled by adopting an established method of MscL charge-induced activation. We then determine pore size limitations using fluorescently labelled model cargoes. Finally, we activate MscL to introduce the cell-impermeable bi-cyclic peptide phalloidin, a specific marker for actin filaments, into cells. We propose that MscL will be a useful tool for gated and controlled delivery of bioactive molecules into cells.
细菌机械敏感通道是自然界中最大的孔之一。特别是,MscL 的孔径>25Å,允许大有机离子和小蛋白质通过。将功能性 MscL 重新组装到脂质中,已被提议用于基于囊泡的药物释放应用。在这里,我们展示了这些通道可以在哺乳动物细胞中功能性表达,从而快速控制膜不可渗透分子的摄取。我们首先证明,MscL 对增加的膜张力的门控反应在哺乳动物细胞膜中得以保留。分子传递通过采用已建立的 MscL 电荷诱导激活方法来控制。然后,我们使用荧光标记的模型货物来确定孔径限制。最后,我们激活 MscL 将不透细胞膜的双环肽鬼笔环肽(肌动蛋白丝的特异性标记物)引入细胞。我们提出 MscL 将成为将生物活性分子门控和受控递送入细胞的有用工具。
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