School of Chemistry , University of Birmingham , Edgbaston , Birmingham B15 2TT , United Kingdom.
Department of Chemistry , University of Warwick , Gibbet Hill Road , Coventry CV4 7AL , United Kingdom.
J Am Chem Soc. 2019 Dec 26;141(51):20234-20248. doi: 10.1021/jacs.9b10152. Epub 2019 Dec 12.
The dynamic interactions of membranes, particularly their fusion and fission, are critical for the transmission of chemical information between cells. Fusion is primarily driven by membrane tension built up through membrane deformation. For artificial polymersomes, fusion is commonly induced via the external application of a force field. Herein, fusion-promoted development of anisotropic tubular polymersomes (tubesomes) was achieved in the absence of an external force by exploiting the unique features of aqueous ring-opening metathesis polymerization-induced self-assembly (ROMPISA). The out-of-equilibrium tubesome morphology was found to arise spontaneously during polymerization, and the composition of each tubesome sample (purity and length distribution) could be manipulated simply by targeting different core-block degrees of polymerization (DPs). The evolution of tubesomes was shown to occur via fusion of "monomeric" spherical polymersomes, evidenced most notably by a step-growth-like relationship between the fraction of tubular to spherical nano-objects and the average number of fused particles per tubesome (analogous to monomer conversion and DP, respectively). Fusion was also confirmed by Förster resonance energy transfer (FRET) studies to show membrane blending and confocal microscopy imaging to show mixing of the polymersome lumens. We term this unique phenomenon polymerization-induced polymersome fusion, which operates via the buildup of membrane tension exerted by the growing polymer chains. Given the growing body of evidence demonstrating the importance of nanoparticle shape on biological activity, our methodology provides a facile route to reproducibly obtain samples containing mixtures of spherical and tubular polymersomes, or pure samples of tubesomes, of programmed length. Moreover, the capability to mix the interior aqueous compartments of polymersomes during polymerization-induced fusion also presents opportunities for its application in catalysis, small molecule trafficking, and drug delivery.
膜的动态相互作用,特别是它们的融合和裂变,对于细胞间化学信息的传递至关重要。融合主要是通过膜变形产生的膜张力驱动的。对于人工聚合物囊泡,融合通常通过施加外力来诱导。在此,通过利用水相开环复分解聚合诱导自组装(ROMPISA)的独特特性,在没有外力的情况下,实现了各向异性管状聚合物囊泡(管囊泡)的融合促进发展。在聚合过程中,发现非平衡管囊泡形态会自发出现,并且每个管囊泡样品的组成(纯度和长度分布)可以通过靶向不同的核嵌段聚合度(DP)来简单地控制。管囊泡的演化被证明是通过“单体”球形聚合物囊泡的融合发生的,这一点最明显的证据是管状到球形纳米物体的分数与每个管囊泡融合颗粒的平均数量之间存在类似单体转化率和 DP 的阶跃增长关系。融合也通过Förster 共振能量转移(FRET)研究得到证实,以显示膜混合,共焦显微镜成像显示聚合物囊泡腔的混合。我们将这种独特的现象称为聚合诱导聚合物囊泡融合,它通过生长聚合物链施加的膜张力来运行。鉴于越来越多的证据表明纳米颗粒形状对生物活性的重要性,我们的方法为可重复获得包含球形和管状聚合物囊泡混合物的样品或具有预定长度的纯管囊泡样品提供了简便途径。此外,在聚合诱导融合过程中混合聚合物囊泡内部水相隔间的能力也为其在催化、小分子运输和药物传递中的应用提供了机会。
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