Patent Application
20240132727
The invention relates to a molecular assembly of amphiphilic molecules having a structural formation and to the use of the molecular assembly for providing anti-adhesive surface coatings. The invention also relates to a method for coating a solid surface with the molecular assembly.
Various mechanisms for influencing the adhesion of surfaces are known from the plant and animal kingdoms. These include, for example, the lotus effect, which has already been transferred successfully to technical applications. While the molecular and structural properties defining interfacial phenomena in nature have been studied extensively, it has not been possible so far to explain fully the physical mechanisms underlying the control of the adhesion. The subject matter of current studies includes, for example, the anti-adhesive cuticle of Collembola, which has honeycomb-like structures with overhanging cross-sectional profiles. It was found that the lipid-rich envelope of the Collembola cuticle contains aliphatic hydrocarbons, in particular steroids, fatty acids and wax esters. While it can be assumed that wax esters promote the wetting-resistant properties of the cuticle, it was not possible to explain the role of components such as steroids and fatty acids. However, it is presumed that in particular physical properties of different molecules are responsible for adhesive and anti-adhesive effects.
The object of the invention consists in providing a possible way of utilising anti-adhesive properties, based on physical-chemical processes, of amphiphilic molecules.
The object is achieved by a molecular assembly having the features according to claim 1 and a method according to claim 11. Developments are specified in the dependent claims.
The essence of the invention is a molecular assembly of selected amphiphilic molecules which are structured in layers and are subject to spontaneous reorientation processes and thus form an entropic barrier to adhesion when in contact with an aqueous environment.
Proposed is a molecular assembly having a structural formation of amphiphilic molecules, characterised in that the amphiphilic molecules are selected from a group containing amphiphilic molecules which
The interfacial layer is understood to mean a layer of the layer structure of the molecular assembly which is in contact with the aqueous environment. The surface of the interfacial layer forms an interface.
Within the meaning of the invention, contact with an aqueous environment means complete wetting of one side of the formed structure of the molecular assembly according to the invention with water. The wetted side forms an interface.
For the molecular assembly according to the invention, amphiphilic molecules having the features according to a), b) and c) are considered.
The molecular assembly according to the invention is based on the ability of the selected amphiphilic molecules to form layer structures by self-organisation. Accordingly, the molecular assembly is preferably a layer structure of amphiphilic molecules, wherein the amphiphilic molecules are oriented perpendicularly to an interface. This layer structure consisting of one or more layers can also be referred to as an assemblage.
It was found that the formation of molecular assemblies of the selected amphiphilic molecules in the structures of molecular layers or molecular interfacial layers brings about an amphiphilia-induced, spontaneous reorientation process of the amphiphilic molecules in the molecular interfacial layer of corresponding interfacial layer structures on contact with an aqueous environment, which results in an anti-adhesive effect on proteins and micro-organisms, in particular bacteria, present in the aqueous environment.
The spontaneous reorientation processes of individual molecules causing the anti-adhesive properties of the molecular assembly are based on the tendency of individual amphiphilic molecules to autogenic orientation.
The selection of the amphiphilic molecules can preferably comprise amphiphilic molecules in which the hydrophobic moiety accounts for at least 95%, preferably more than 95% of the molecular weight of the amphiphilic molecules. This applies in particular to cholesterol molecules.
The desired effect of the spontaneous reorientation processes within the molecular assembly has also been found in amphiphilic molecules of the type in question which have a molecular weight in the range of 300 g/mol to 2000 g/mol, preferably in the range of 300 g/mol to 413 g/mol. Preferably, the molecular assembly according to the invention can have amphiphilic molecules with a molecular weight in the range of 300 g/mol bis 413 g/mol. Molecular assemblies having amphiphilic molecules of the type in question with a molecular weight greater than 2000 g/mol are conceivable. Therefore, in particular synthetically produced amphiphilic molecules can have a higher molecular weight, that is, a molecular weight greater than 2000 g/mol and meet the requirements of a), b) and c).
The molecular assembly according to the invention can also have amphiphilic molecules, the molecular orientation of which within formed interfacial layers of the layer structure is based on the polarity of the environment such that a change in the polarity of the environment causes a change in the molecular orientation of the interfacial layer of the formed layer structure.
According to one embodiment of the molecular assembly according to the invention, the amphiphilic molecules can be polycyclic alcohols, in particular sterols.
It can also be provided for the molecular assembly to have a mass percentage of at least 1 weight % (abbreviated to wt % below), preferably at least 10 wt % cholesterol molecules and/or dehydrocholesterol molecules. That is, at least 1 wt %, preferably at least 10 wt % of the selected amphiphilic molecules can be cholesterol molecules and/or dehydrocholesterol molecules. The proportion of cholesterol molecules and/or dehydrocholesterol molecules has a positive influence on the anti-adhesive effect of the molecular assembly in the form of an interfacial layer structure on contact with an aqueous environment.
According to a further embodiment of the molecular assembly according to the invention, it can be provided for the amphiphilic molecules to be stigmasterol, cholecalciferol and/or retinol. It was found that stigmasterol molecules, cholecalciferol molecules and retinol molecules in the molecular assembly reorient comparatively rapidly on contact with an aqueous environment and have hardly any spontaneous reorientation processes, which is associated with a worsening of the anti-adhesive properties of the molecular assembly. However, the anti-adhesive effect is significantly better than for molecular assemblies of similar, non-amphiphilic molecules. If stigmasterol molecules, cholecalciferol molecules and retinol molecules are used, it is therefore advantageous if additionally at least 1 wt %, preferably at least 10 wt % cholesterol molecules and/or dehydrocholesterol molecules are used to provide the molecular assembly.
Furthermore, cholesterol molecules, dehydrocholesterol molecules, stigmasterol molecules, cholecalciferol molecules and retinol molecules can be used as amphiphilic molecules to form the molecular assembly. Different ratios of cholesterol molecules, dehydrocholesterol molecules, stigmasterol molecules, cholecalciferol molecules and retinol molecules can be used.
It is assumed that cholesterol molecules form triclinic crystals, which results in a comparatively “loose” arrangement in corresponding layers of the molecular assembly. This favours the mobility of the molecules in the layer. In contrast to this, stearic and palmitic acid molecules, which are constituents of the Collembola cuticle, form monoclinic crystals and accumulate in tightly packed layers, as a result of which possible amphiphilia-induced spontaneous reorientation processes of the molecules are prevented when the polarity of the surrounding medium changes.
The molecular assembly according to the invention has the following further properties:
A change in the polarity of the surrounding/contacting medium leads to an amphiphilia-induced reorientation of the amphiphilic molecules in the molecular interfacial layer of corresponding assemblages (layer structures). This reorientation can be detected macroscopically by means of dynamic contact angle measurements or microscopically by means of atomic force microscopy-based force spectroscopy. The spontaneous reorientation processes of amphiphilic molecules in the molecular interfacial layer of corresponding assemblages of the molecular assembly form, on contact with aqueous solutions, the basis for entropy-induced anti-adhesive properties, which can be detected by means of spatially resolved and time-resolved atomic force microscopy-based force spectroscopy.
The molecular assembly according to the invention can be designed structurally in the form of multilayers of cholesterol molecules. Such cholesterol multilayers exhibit very characteristic behaviour during dynamic contact angle measurement. In dynamic contact angle measurement, a water droplet is applied to the molecular assembly under examination and the shape of the droplet is observed. The droplet is then sucked up again and the droplet shape is again observed in the process. This procedure is repeated with different application times. With molecular assemblies in the structure of cholesterol multilayers, the shape of the droplet on application indicates a moderately hydrophobic interface. If the droplet is sucked up again immediately after application, its shape remains unchanged, which again indicates hydrophobic properties of the interface of the molecular assembly. With a longer application time of 20 seconds, for example, a different picture emerges. The droplet collapses, which indicates a very hydrophilic interface of the molecular assembly. Similar behaviour was observed for molecular assemblies of cholesterol analogues.
The molecular assembly according to the invention can therefore have a mixture of different proportions of amphiphilic molecules, in particular cholesterol analogues having the properties a), b) and c). Preferably, the molecular assembly according to the invention has at least 1 wt % cholesterol molecules. The molecular assembly according to the invention can also have non-amphiphilic molecules which are suitable for integrating within the structure of the molecular assembly. The proportion of non-amphiphilic molecules of the molecular assembly can have a mass percentage of up to 99 wt %. The non-amphiphilic molecules used can be stearyl palmitate molecules, for example. According to one embodiment of the molecular assembly according to the invention, stearyl palmitate molecules can be present in a proportion of 99 wt %. In this case, cholesterol molecules are preferably used as the amphiphilic molecules.
The layer structures of the molecular assembly according to the invention can have a thickness of 15 nm.
Preferably, the molecular assembly is deposited in the form of a layer structure of cholesterol molecules arranged perpendicularly to an interface on a solid surface by means of spin coating. In the process, the interface of the layer structure facing away from the solid surface is in contact with an aqueous solution, preferably pure water.
The molecular assembly according to the invention serves in particular for use as anti-adhesive agents for solid surfaces.
The subject matter of the invention is also a method for coating a solid surface with the molecular assembly according to the invention, wherein the amphiphilic molecules are first dissolved in a polar aprotic solvent, and the solution thus produced is then applied to a solid surface by means of spin coating. The amphiphilic molecules are applied to the solid surface by the spin coating. As a result of the application and subsequent removal of the polar aprotic solvent, the amphiphilic molecules assemble to form layer structures, which, after removal of the polar aprotic solvent, can be brought into contact with an aqueous environment in order to form the anti-adhesive properties.
Chloroform can be used as the polar aprotic solvent. The solvent evaporates after application to the solid surface. An air stream or a vacuum can be used to assist the evaporation of the solvent.
Conceivable further solvents are acetone, benzene, ethanol, ether, hexane or methanol.
Further details, features and advantages of embodiments of the invention can be found in the description of exemplary embodiments below with reference to the associated drawings. In the drawings:
The invention is based on the finding that the combination of selected amphiphilic molecules, in particular cholesterol molecules, and the effective self-organisation of the selected molecules in molecular assemblies in the form of multilayer structures, which produces a slow, adaptive, cooperative interface mobility of the molecular assembly, results in a pronounced entropic repulsion of proteins and micro-organisms.
Furthermore,
The method for coating a solid surface 5 with the molecular assembly 1 is explained in more detail below.
The molecular assembly 1 can be applied to a solid surface 5 by spin coating, wherein layer structures 3 of the molecular assembly 1 are formed. Such layer structures 3 of selected amphiphilic molecules are referred to below as SCLs (spin-coated lipid multilayers).
SCLs are produced on silicon wafers as the substrate. The substrates, which can have a size of 10×15 mm2, are cleaned by immersion in a solution of deionised water, ammonia and hydrogen peroxide (volume ratio 5/1/1) for 15 min at 70° C., repeatedly rinsed in Milli-Q water and then dried in a nitrogen stream. The cleaned substrates are immediately used for producing SCLs by spin coating. For the spin coating, cholesterol molecules 2 are dissolved in chloroform (concentration 2 wt %). The solution thus produced is applied to the solid surface 5 by spin coating (LabSpin6, SÜSS MicroTec) at a rotation speed of 3000 revolutions per minute and an acceleration of 3000 revolutions per minute/second for 30 seconds. The anti-adhesive properties form as soon as the formed layer structures 3 are brought into contact with an aqueous solution.
Cholesterol SCLs Adapt Dynamically to the Polarity of their Environment
The reorientation ability of the cholesterol molecules 2 within molecular assemblies 1 of layer structures 3, depending on the polarity of the surrounding medium, was detected by means of dynamic contact angle measurements and atomic force microscopy-based force spectroscopy.
Force-spectroscopic measurements were carried out with hydrophobic colloidal probes or individual Escherichia coli cells immobilised on the tip of the colloidal probes. Both types of probe were pressed for different time intervals onto the surface of cholesterol SCLs, which were immersed in aqueous solutions. The resulting interaction forces were quantified and it was found that they increase continuously with contact time, which proves the reorientation of the cholesterol molecules with the non-polar moiety of the molecule in the direction of the interface (to maximise the hydrophobic interactions). When contact was interrupted, the initial state of the interface was restored in contact with water, i.e., the reorientation process was repeatable multiple times.
Dynamic contact angle measurements on cholesterol SCLs in air produced similarly high advancing and receding water contact angles when the droplet was removed again immediately after application. These results indicate that the non-polar moiety of the cholesterol molecules at the interfacial layer is initially oriented towards the interface, while the polar moiety is directed inwards. However, if the droplet is kept on the surface for approximately 20 seconds after application, before it is removed, strong pinning of the three-phase contact line was observed, which indicates an interface with hydrophilic properties. Within the 20-second waiting time, a reorientation of the cholesterol molecules therefore occurred, which now point with the polar moiety in the direction of the interface. This process was also reversible.
It was demonstrated that the anti-adhesive properties of cholesterol-containing SCLs correlate with their dynamic adaptation as a reaction to changes in the polarity of the environment. It can be assumed that entropically driven orientation fluctuations of cholesterol molecules at the interface link these features mechanistically. Any adsorption of biomolecules or accumulation of (bacterial) cells requires an adaptation of the orientation (polarity) of the SCL interface, which constrains the orientation states of cholesterol and thereby reduces the entropy of the system. It was observed that protein adsorption to cholesterol SCLs decreased when the temperature was raised from 15° C. to 40° C.
The discovered entropic bioadhesion barrier which results from reorientation processes at the interface of cholesterol-containing SCLs allows numerous technical applications.
The results show that cholesterol organises itself in molecular assemblies which can limit bioadhesion via entropic effects. The combination of the amphiphilia of the cholesterol molecules and their effective assembly in layer structures, which produces a slowly adaptive, cooperative interface mobility of the assemblies, was identified as a precondition for a pronounced entropic repulsion.
| Number | Date | Country | Kind |
|---|---|---|---|
| 10 2021 104 706.4 | Feb 2021 | DE | national |
| 10 2022 104 237.5 | Feb 2022 | DE | national |
| Filing Document | Filing Date | Country | Kind |
|---|---|---|---|
| PCT/DE2022/100147 | 2/23/2022 | WO |
