巯基化透明质酸包封的仿生交联基因微载体的构建

采用超分子组装技术,通过巯基化透明质酸(HA-SH)与聚乙烯亚胺(PEI)/DNA缔合体的界面静电组装,构建了壳层二硫键仿生交联的基因超分子组装体(PEI/DNA/HA-SH).凝胶电泳结果表明,该组装体有很好的DNA缔合特性.壳层的仿生交联使基因超分子组装体在生理盐溶液中的稳定性得到有效改善,细胞毒性显著降低,并能有效转染细胞,为非病毒基因传递体系的设计提供了新途径.     

小分子共价DNA的组装及生物医学应用

DNA,由于其精确的碱基互补配对、良好的生物相容性、稳定的物理化学性质,不仅可用于组装各种形状和尺寸的纳米结构,而且可以设计动态的纳米器件。为了进一步拓展DNA的应用,可通过化学修饰引入功能分子或基团,从而实现二者功能的集成。目前,DNA与高分子、树状分子、多肽和蛋白等共价有机杂化体的合成、组装及在药物运输和控释等领域的应用已研究得比较成熟,而结构和功能多样的小分子与DNA共价杂化体,由于疏水小分子体积小,其组装受到限制,近年来科研者通过结构衍生或增多芳香环等研究其组装行为及应用。本文主要综述了疏水小分子共价连接DNA后的组装行为及其在生物医药领域的潜在应用,并对这类杂化体纳米材料的研究前景进行了展望。     

基于芳香分子-糖类手性超分子组装体及功能

手性超分子组装体广泛存在于自然界中,因其在材料、化学和生物学等领域广阔的应用前景,引起了科学家们极大的兴趣。其中以糖类分子作为手性源,经分子自组装构筑手性超分子组装体的研究已成为超分子化学领域的研究热点之一。本文综述了基于糖类修饰的苝酰亚胺分子、偶氮苯分子、联苯类分子和卟啉类分子等芳香分子化合物经自组装构筑的手性超分子组装体,介绍了其在有机溶剂和水的混合溶剂、水中的凝胶性质,超分子手性特征和功能,糖分子类型与超分子组装体手性间的关系等,并对基于糖类的手性超分子组装体的前景进行了展望。     

自组装共混制备PEG化基因载体

通过含PEG链段的两亲聚合物的自组装共混, 制备了基于疏水作用力的新型PEG化非病毒基因载体. 分别选用胆固醇-聚乙二醇和聚乙二醇-聚丙二醇-聚乙二醇作为共混改性剂, 研究两亲聚合物的种类对组装体在生理盐溶液中的稳定性及基因转染效率的影响. 结果表明, 疏水驱动力的大小是获得稳定的PEG化基因超分子组装体的关键. 通过对两亲聚合物中疏水链段的选择调控, 可制备稳定的PEG化基因超分子组装体, 提高基因传递体系在生理盐溶液中的稳定性及基因转染效率. 通过自组装共混, 为新型PEG化基因超分子组装体的制备提供了切实可行的新方法.     

分子组装理论基础的探究——现状与机遇

分子组装是在分子以上层次创造新物质、产生新功能的重要手段.提升分子组装过程的可控性和组装体功能性是该领域的核心目标,但由于研究复杂分子组装体系的手段和理论的匮乏,迄今绝大部分研究只能限于了解组装过程始末的“黑箱”模式,这成为该领域的发展瓶颈之一.本文围绕分子到亚细胞层次的分子组装体系及其理论方法与模型,尝试将物质、能量与信息作为度量分子组装研究复杂性的三个维度,从简单到复杂地逐级剖析探讨分子组装的理论研究现状、机遇和突破口.首先,在物质维度上揭示分子组装过程呈现多路径、多阶段和多尺度等复杂性;进而在物质基础上引入能量维度,阐明熵驱动或熵焓互补现象普遍存在于分子组装体系中,并探讨远离平衡态的分子组装体系如何产生时空有序的功能耗散结构;继而在物质与能量基础上引入信息维度,探讨分子组装信息网络中的正、负反馈协同,以及如何促使系统涌现出复杂的生理功能.为了突破分子组装理论研究的瓶颈,似乎亟需建立更大的框架.从物质、能量和信息的三个维度协同研究,有望系统深入认知组装规律,进而建立新理论,发展高效精准的调控手段,提升分子组装体系的复杂性和功能性,并可能为生命科学和软物质科学提供新视角和新方法.     

环糊精超分子组装体与核酸的相互作用

环糊精是一类由6～8个D-型葡萄糖连接而成的环聚多糖分子,目前已广泛应用于化学和生物学的许多领域.综述了一些生物活性的环糊精超分子组装体,如环糊精假聚轮烷、环糊精/金纳米粒子组装体、环糊精/富勒烯组装体、环糊精/碳纳米管组装体等的构筑及其与核酸的相互作用,如对核酸的切割、凝聚、传递作用和对核酸酶的抑制作用等方面的研究进展.     

DNA薄膜的制备及性质研究进展

从化学的角度概述了近年来用分子组装技术对DNA分子的组装，DNA薄膜化及其性质研究的进展。     

肽超分子自组装:结构调控和功能化

生物分子自组装对生物体有重要意义,利用生物分子构筑具有功能性的有序组装体一直是人们关注的焦点.肽分子是一类重要的组装基元,肽的超分子自组装可形成多种纳米或微米尺度的结构,并可应用于能源、医药等领域.如何实现肽自组装结构的精准调控以及精准调控肽自组装实现功能化,是目前该领域面临的新挑战.肽的自组装是基于非共价键力的协同作用实现的,通过各种因素调节这些非共价键力的作用,是实现自组装结构调控和功能化的关键.虽然自组装结构调控可以通过改变外部环境调控,但是通过精确分子设计、组装基元分子间的相互作用调控可以更好地实现结构的精准调控;并有利于进一步通过引入功能性分子作为组装基元,实现自组装体的功能化.本文将针对肽自组装体的结构调控以及功能化两个方面对相关研究进行综述.     

DNA在氨基功能化偶氮苯自组装膜表面的固定

采用简单快速的方法制备出将DNA固定在其表面的单分子层敏感膜.首先采用表面自组装技术将硅氧烷基偶氮苯衍生物H2NAzoCONHC3Si(OCH3)3(APDA-N-TMSPBA)组装在硅表面,在详细考察单分子层薄膜的化学结构、表面浸润性和分子表面形貌之后,又通过紫外吸收光谱(UV)在位考察了硅氧烷基偶氮苯衍生物的光学异构特性.在DNA在自组装薄膜固定后,X光电子能谱仪(XPS)结果显示出现了明显的磷元素信号,表明DNA分子可以成功固定在自组装膜表面.     

基于冠醚衍生物的超分子聚合物

自组装现象是生命科学最本质的内容之一,生物体系可以精确地利用非共价键相互作用形成高度有序的功能组装体.受到大自然的启发,近年来利用分子自组装构筑包括超分子聚合物在内的有序聚集体是超分子科学的研究热点.此类组装体不仅在拓扑学上具有重要的意义,而且可以用来制备动态的超分子功能材料.冠醚作为第一代超分子主体化合物,由于其结构...     

A Study on Organized Assemblies in the Aqueous Systems of Alkylammonium Chlorides

Various types of organized assemblies, including micelle, planar multi-bilayer, bent multi-bilayer, fingerprint-like multi-bilayer, and multilamellar vesicles, were found in the aqueous system prepared by only one simple surfactant—alkylammonium chloride with a hydrocarbon chain length of 10 or 12. Electron microscopic images of the assemblies are provided. The properties of the system were characterized by DSC, fluorescence, and absorption probing techniques. It was found that the structure and shape of molecular assemblies in this system can be adjusted by very simple physico-chemical measures, such as pH adjustment and alcohol or salt addition. The mechanisms of formation and transformation of various molecular assemblies were discussed based on the mixing effect of the cationic amphiphile and the nonionic amphiphile which is only a hydrolysis product of the former.     

Moment equations for partial filling capillary electrophoresis

Moment equations were developed for partial filling CE systems, in which solute dissolution phenomena by spherical molecular assemblies or intermolecular interactions take place. Because experimental conditions of partial filling CE are divided into five categories on the basis of the magnitude relationship between the migration velocity of solute molecules and that of molecular assemblies or ligand molecules, the moment equations were systematically developed for each case by using the Einstein equation for diffusion and the random walk model. In order to demonstrate the effectiveness of the moment equations, they were applied to the analysis of partial filling CE behavior, which is correlated with dissolution phenomena of small solute molecules into spherical molecular assemblies as specific examples. Simulation results only in the case that the migration velocity of solute molecules is faster than that of molecular assemblies were represented in this paper. Detailed explanations about the derivation procedure of the moment equations and the simulation results in other cases can be found in the Supporting Information. The moment equations are theoretical bases for applying partial filling CE to the study on solute permeation kinetics at the interface of spherical molecular assemblies and on reaction kinetics of intermolecular interactions.     

Molecular Architectonics-guided Design of Biomaterials

The quest for mastering the controlled engineering of dynamic molecular assemblies is the basis of molecular architectonics. The rational use of noncovalent interactions to programme the molecular assemblies allow the construction of diverse molecular and material architectures with novel functional properties and applications. Understanding and controlling the assembly of molecular systems are daunting tasks owing to the complex factors that govern at the molecular level. Molecular architectures depend on the design of functional molecular modules through the judicious selection of functional core and auxiliary units to guide the precise molecular assembly and co-assembly patterns. Biomolecules with built-in information for molecular recognition are the ultimate examples of evolutionary guided molecular recognition systems that define the structure and functions of living organisms. Explicit use of biomolecules as auxiliary units to command the molecular assemblies of functional molecules is an intriguing exercise in the scheme of molecular architectonics. In this minireview, we discuss the implementation of the principles of molecular architectonics for the development of novel biomaterials with functional properties and applications ranging from sensing, drug delivery to neurogeneration and tissue engineering. We present the molecular designs pioneered by our group owing to the requirement and scope of the article while acknowledging the designs pursued by several research groups that befit the concept.     

Thermal or Mechanical Stimuli‐Induced Photoluminescence Color Change of a Molecular Assembly Composed of an Amphiphilic Anthracene Derivative in Water

Molecular assemblies that change photoluminescence color in response to thermal or mechanical stimulation without dissociation into the monomeric states in water are described herein. A dumbbell‐shaped amphiphilic compound forms micellar molecular assemblies in water and exhibits yellow photoluminescence derived from excimer formation of the luminescent core, which contains a 2,6‐diethynylanthracene moiety. Annealing of the aqueous solution induces a photoluminescence color change from yellow to green (λ_{em, max}=558→525 nm). The same photoluminescence color change is also achieved by rubbing the yellow‐photoluminescence‐emitting molecular assemblies adsorbed on glass substrates with cotton wool in water. The observed green photoluminescence is ascribed to micelles that are distinct from the yellow‐photoluminescence‐emitting micelles, on the basis of transmission electron microscopy observations, atomic force microscopy observations, and dynamic light scattering measurements. We examined the relationship between the structure of the molecular assemblies and the photophysical properties of the anthracene derivative in water before and after thermal or mechanical stimulation and concluded that thermal or mechanical stimuli‐induced slight changes of the molecular‐assembled structures in the micelles result in the change in the photoluminescence color from yellow to green in water.     

烷基氯化铵体系中分子有序组合体的转化

采用动态光散射、吸收光谱、粘度及电镜透射等方法研究了烷基氯化铵在弱碱性条件下溶液浓度变化对分子有序组合体结构的影响.当表面活性剂浓度大于cmc时,分子有序组合体的形态随表面活性剂浓度的增加出现胶团-囊泡-球状胶团的转化过程,这与水解产生的极性有机物烷基胺量的变化密切相关.     

手性超分子组装研究进展

介绍了超分子手性的基本构筑方式及其特点,分别从手性分子组装、手性分子诱导非手性分子及非手性分子组装等3个方面对最近几年来在手性超分子组装领域内的重要成果及最新进展进行了综述,并对这一领域的发展前景作了展望。     

A label-free fluorescence sensor for probing the interaction of oligonucleotides with target molecules

This paper describes a universal, label-free fluorescence sensor that gauges the interaction of oligonucleotides with their targets. The sensor is based on supramolecular assemblies formed by oligonucleotides (polyanions) and small molecule cation surfactant in aqueous solution. The environmentally dependent dye pyrene, encapsulated in the apolar interiors of the assemblies via hydrophobic interactions works as the fluorescence probe. Target binding causes the conformational change of the oligonucleotides, which results in disorganization of supramolecular assemblies, release of pyrene into the aqueous solution and subsequent quenching of its fluorescence. The kinetic processes (including the formation of supramolecular assemblies and the release of pyrenes after adding the targets) were investigated. The fluorescence decreases of pyrenes are proportional to the concentrations of targets within the linear ranges. This label-free fluorescence system is simple, convenient, low cost, and can serve as an alternative tool for interaction studies of oligonucleotides with their targets, especially with small molecular targets.     

Two Orthogonal Halogen-Bonding Interactions Directed 2D Crystalline Supramolecular J-Dimer Lamellae

Dye assemblies exhibit fascinating properties and performances, both of which depend critically on the mutual packing arrangement of dyes and on the supramolecular architecture. Herein, we engineered, for the first time, an intriguing chlorosome-mimetic 2D crystalline J-dimer lamellar structure based on halogenated dyes in aqueous media by employing two distinct orthogonal halogen-bonding (XB) interactions. As the only building motif, antiparallel J-dimer was formed and stabilized by single π-stacking and dual halogen⋅⋅⋅π interactions. With two substituted halogen atoms acting as XB donors and the other two acting as acceptors, the constituent J-dimer units were linked by quadruple highly-directional halogen⋅⋅⋅halogen interactions in a staggered manner, resulting in unique 2D lamellar dye assemblies. This work champions and advances halogen-bonding as a remarkably potent tool for engineering dye aggregates with a controlled molecular packing arrangement and supramolecular architecture.     

Precise Macroscopic Supramolecular Assemblies: Strategies and Applications

Macroscopic supramolecular assembly (MSA) is a new concept in supramolecular science with a focus on interfacial assembly of macroscopic building blocks, which has largely extended the applicable materials of supramolecular assembly and provided new solutions to fabricating tissue scaffolds, soft devices, etc. The precision of the assembled structures is of great interest; unlike molecular assemblies, MSA precision is highly dependent on the matching degree of assembled surfaces because of the large interactive area and group number, which result in remarkably increased kinetic possibilities and metastable assemblies. This Concept introduces the principle, history, and development of MSA, elaborates the low-precision challenge in MSA, summarizes the strategies for precise MSA based on the different thermodynamic stability of precise/imprecise structures and control over assembly kinetics, and finally demonstrates the applications of precise MSA structures in advanced manufacture such as tissue scaffolds.     

非水溶剂中囊泡等分子有序组合体的形成

总结了各类表面活性剂在乙醇等非水及混合溶剂中的囊泡、胶束等聚集体的形成规律,着重讨论了非水体系中介电常数改变对正负离子表面活性剂混合体系中聚集体形成的影响.对反胶束等不同分子有序组合体在非水体系中的形成情况也进行了概述.