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A major problem regarding public health is the emergence of antibiotic resistant bacterial strains, especially methicillin resistant Staphylococcus aureus (MRSA). This is mainly attributed to the unnecessary overuse of antimicrobial drugs by patients; however, one aspect that is often neglected is their untargeted mechanism of action, affecting not only the infection itself but also commensal bacteria which are often opportunistic pathogens causing many diseases as well. Therefore, our goal was to develop a bioresponsive antibiotic delivery system triggered by virulence factors. The designed system is comprised of a polymer to enhance its pharmacokinetic profile, a peptide cleavable linker, and the antibiotic agent itself. The bacterial protease aureolysin which is expressed by S. aureus during infections would cleave the linker and partially release the antibiotic which would be still attached to a remaining tetrapeptide. These would be cleaved by a group of proteases naturally present in plasma called aminopeptidases, finally releasing the compound.
In the first part of this project, we searched for a suitable sequence to serve as a cleavable linker. It should be sensitive towards the target bacterial protease but not be cleaved by any human enzymes to guarantee the specificity of the system. Therefore, we synthesized three peptide sequences via Solid Phase Peptide Synthesis and incubated them with aureolysin as well as with many human matrix Metalloproteases. The analysis and quantification of enzymatic activity was monitored chromatographically (RP-HPLC). The plasminogen originated sequence was chosen since it was not sensitive towards MMPs, but cleaved by aureolysin.
In the second part, we tried to incorporate the chosen peptide sequences as crosslinkers in hydrogel formulations. The purpose was to physically incorporate the antibiotic within the hydrogel, which would be released by the cleavage of those sequences and the consequent loosening the hydrogel net. For that purpose we used a commercially available hydrogel kit with a PVA matrix modified with maleimide, which allows a conjugation reaction with thiol functionalized crosslinkers. Three fluorophores were chosen to serve as antibiotic models and a diffusion assay was performed. Only the glomerular structured Green Fluorescent Protein (GFP) presented a low diffusion rate, thus the aureolysin release assays were performed only using this prototype. Assays showed that with a low hydrogel polymer concentration, the fluorophore either quickly diffused into the medium or was not released at all. The physical incorporation of the antibiotic within the hydrogel pores was therefore abolished as a suitable release approach. For a second attempt, we covalently bound a fluorophore to the linker, which was conjugated to the hydrogel matrix. The incubation with aureolysin and subsequent RP-HPLC analysis showed a peak with the same retention time correspondent to the fragment product after cleavage of the free linker. This is a proof that the concept of linking the peptide sequence to the antibiotic is a promising strategy for its bioresponsive release.
Within the third part of this study, we analyzed the degradation of the resulted fragment after aureolysin activity and subsequent full release of the antibiotic by human aminopeptidases. We determined the concentration of those enzymes in human plasma and synthesized the fragment by conjugating the tetrapeptide sequence to aminofluorescein via EDC/NHS reaction. By incubating the construct with the lowest aminopeptidase concentration measured in plasma, the fluorophore was completely released within two hours, showing the efficacy of these enzymes as bioresponsive agents.
The last part was the construction of the PEGylated linker-antibiotic. For this purpose we chose the tetracycline like antibiotic chelocardin (CHD) as our prototype. The conjugation of the linker- CHD to the polymer was performed by copper free click chemistry. The cleavage rate of the linker by aureolysin was very similar to the one obtained for the free peptide, indicating that the PEGylation does not interfere on the enzymatic activity. However, by trying to increase the loading ratio of chelocardin onto the polymer, we observed a very low cleavage rate for the system, indicating the formation of aggregates by those constructs.
The designed system has proved to be a smart strategy for the delivery on demand of antibiotics in which the drug is only released by the presence of S. aureus during their virulent state.
In order to mimic the extracellular matrix for tissue engineering, recent research approaches often involve 3D printing or electrospinning of fibres to scaffolds as cell carrier material. Within this thesis, a micron fibre printing process, called melt electrospinning writing (MEW), combining both additive manufacturing and electrospinning, has been investigated and improved. Thus, a unique device was developed for accurate process control and manufacturing of high quality constructs. Thereby, different studies could be conducted in order to understand the electrohydrodynamic printing behaviour of different medically relevant thermoplastics as well as to characterise the influence of MEW on the resulting scaffold performance.
For reproducible scaffold printing, a commonly occurring processing instability was investigated and defined as pulsing, or in extreme cases as long beading. Here, processing analysis could be performed with the aim to overcome those instabilities and prevent the resulting manufacturing issues. Two different biocompatible polymers were utilised for this study: poly(ε-caprolactone) (PCL) as the only material available for MEW until then and poly(2-ethyl-2-oxazoline) for the first time. A hypothesis including the dependency of pulsing regarding involved mass flows regulated by the feeding pressure and the electrical field strength could be presented. Further, a guide via fibre diameter quantification was established to assess and accomplish high quality printing of scaffolds for subsequent research tasks.
By following a combined approach including small sized spinnerets, small flow rates and high field strengths, PCL fibres with submicron-sized fibre diameters (fØ = 817 ± 165 nm) were deposited to defined scaffolds. The resulting material characteristics could be investigated regarding molecular orientation and morphological aspects. Thereby, an alignment and isotropic crystallinity was observed that can be attributed to the distinct acceleration of the solidifying jet in the electrical field and by the collector uptake. Resulting submicron fibres formed accurate but mechanically sensitive structures requiring further preparation for a suitable use in cell biology. To overcome this handling issue, a coating procedure, by using hydrophilic and cross-linkable star-shaped molecules for preparing fibre adhesive but cell repellent collector surfaces, was used.
Printing PCL fibre patterns below the critical translation speed (CTS) revealed the opportunity to manufacture sinusoidal shaped fibres analogously to those observed using purely viscous fluids falling on a moving belt. No significant influence of the high voltage field during MEW processing could be observed on the buckling phenomenon. A study on the sinusoidal geometry revealed increasing peak-to-peak values and decreasing wavelengths as a function of decreasing collector speeds sc between CTS > sc ≥ 2/3 CTS independent of feeding pressures. Resulting scaffolds printed at 100 %, 90 %, 80 % and 70 % of CTS exhibited significantly different tensile properties, foremost regarding Young’s moduli (E = 42 ± 7 MPa to 173 ± 22 MPa at 1 – 3 % strain). As known from literature, a changed morphology and mechanical environment can impact cell performance substantially leading to a new opportunity of tailoring TE scaffolds.
Further, poly(L-lactide-co-ε-caprolactone-co-acryloyl carbonate) as well as poly(ε-caprolactone-co-acryloyl carbonate) (PCLAC) copolymers could be used for MEW printing. Those exhibit the opportunity for UV-initiated radical cross-linking in a post-processing step leading to significantly increased mechanical characteristics. Here, single fibres of the polymer composed of 90 mol.% CL and 10 mol.% AC showed a considerable maximum tensile strength of σmax = 53 ± 16 MPa. Furthermore, sinusoidal meanders made of PCLAC yielded a specific tensile stress-strain characteristic mimicking the qualitative behaviour of tendons or ligaments. Cell viability by L929 murine fibroblasts and live/dead staining with human mesenchymal stem cells revealed a promising biomaterial behaviour pointing out MEW printed PCLAC scaffolds as promising choice for medical repair of load-bearing soft tissue.
Indeed, one apparent drawback, the small throughput similar to other AM methods, may still prevent MEW’s industrial application yet. However, ongoing research focusses on enlargement of manufacturing speed with the clear perspective of relevant improvement. Thereby, the utilisation of large spinneret sizes may enable printing of high volume rates, while downsizing the resulting fibre diameter via electrical field and mechanical stretching by the collector uptake. Using this approach, limitations of FDM by small nozzle sizes could be overcome. Thinking visionary, such printing devices could be placed in hospitals for patient-specific printing-on-demand therapies one day. Taking the evolved high deposition precision combined with the unique small fibre diameter sizes into account, technical processing of high performance membranes, filters or functional surface finishes also stands to reason.
Sensitivity and selectivity remain the central technical requirement for analytical devices, detectors and sensors. Especially in the gas phase, concentrations of threat substances can be very low (e.g. explosives) or have severe effects on health even at low concentrations (e.g. benzene) while it contains many potential interferents. Preconcentration, facilitated by active or passive sampling of air by an adsorbent, followed by thermal desorption, results in these substances being released in a smaller volume, effectively increasing their concentration.
Traditionally, a wide range of adsorbents, such as active carbons or porous polymers, are used for preconcentration. However, many adsorbents either show chemical reactions due to active surfaces, serious water retention or high background emission due to thermal instability. Metal-organic frameworks (MOFs) are a hybrid substance class, composed inorganic and organic building blocks, being a special case of coordination polymers containing pores. They can be tailored for specific applications such as gas storage, separation, catalysis, sensors or drug delivery.
This thesis is focused on investigating MOFs for their use in thermal preconcentration for airborne detection systems. A pre-screening method for MOF-adsorbate interactions was developed and applied, namely inverse gas chromatography (iGC). Using this pulse chromatographic method, the interaction of MOFs and molecules from the class of explosives and volatile organic compounds was studied at different temperatures and compared to thermal desorption results.
In the first part, it is shown that archetype MOFs (HKUST-1, MIL-53 and Fe-BTC) outperformed the state-of-the-art polymeric adsorbent Tenax® TA in nitromethane preconcentration for a 1000 (later 1) ppm nitromethane source. For HKUST-1, a factor of more than 2000 per g of adsorbent was achieved, about 100 times higher than for Tenax. Thereby, a nitromethane concentration of 1 ppb could be increased to 2 ppm. High enrichment is addressed to the specific interaction of the nitro group as by iGC, which was determined by comparing nitromethane’s free enthalpy of adsorption with the respective saturated alkane. Also, HKUST-1 shows a similar mode of sorption (enthalpy-entropy compensation) for nitro and saturated alkanes.
In the second part, benzene of 1 ppm of concentration was enriched with a similar setup, using 2nd generation MOFs, primarily UiO-66 and UiO-67, under dry and humid (50 %rH) conditions using constant sampling times. Not any MOF within the study did surpass the polymeric Tenax in benzene preconcentration. This is most certainly due to low sampling times – while Tenax may be highly saturated after 600 s, MOFs are not. For regular UiO-66, four differently synthesized samples showed a strongly varying behavior for dry and humid enrichment which cannot be completely explained. iGC investigations with regular alkanes and BTEX compounds revealed that confinement factors and dispersive surface energy were different for all UiO-66 samples. Using physicochemical parameters from iGC, no unified hypothesis explaining all variances could be developed.
Altogether, it was shown that MOFs can replace or add to state-of-the-art adsorbents for the enrichment of specific analytes with preconcentration being a universal sensitivity-boosting concept for detectors and sensors. Especially with iGC as a powerful screening tool, most suitable MOFs for the respective target analyte can be evaluated. iGC can be used for determining “single point” retention volumes, which translate into partition coefficients for a specific MOF × analyte × temperature combination.
Biofabrication is an advancing new research field that might, one day, lead to complex products like tissue replacements or tissue analogues for drug testing. Although great progress was made during the last years, there are still major hurdles like new types of materials and advanced processing techniques. The main focus of this thesis was to help overcoming this hurdles by challenging and improving existing fabrication processes like extrusion-based bioprinting but also by developing new techniques. Furthermore, this thesis assisted in designing and processing materials from novel building blocks like recombinant spider silk proteins or inks loaded with charged nanoparticles.
A novel 3D printing technique called Melt Electrospinning Writing (MEW) was used in Chapter 3 to create tubular constructs from thin polymer fibers (roughly 12 μm in diameter) by collecting the fibers onto rotating and translating cylinders. The main focus was put on the influence of the collector diameter and its rotation and translation on the morphology of the constructs generated by this approach. In a first step, the collector was not moving and the pattern generated by these settings was analyzed. It could be shown that the diameter of the stationary collectors had a big impact on the morphology of the constructs. The bigger the diameter of the mandrel (smallest collector diameters 0.5 mm, biggest 4.8 mm) got, the more the shape of the generated footprint converged into a circular one known from flat collectors. In a second set of experiments the mandrels were only rotated. Increasing the rotational velocity from 4.2 to 42.0 rpm transformed the morphology of the constructs from a figure-of-eight pattern to a sinusoidal and ultimately to a straight fiber morphology. It was possible to prove that the transformation of the pattern was comparable to what was known from increasing the speed using flat collectors and that at a critical speed, the so called critical translation speed, straight fibers would appear that were precisely stacking on top of each other. By combining rotation and translation of the mandrel, it was possible to print tubular constructs with defined winding angles. Using collections speeds close to the critical translation speed enabled higher control of fiber positioning and it was possible to generate precisely stacked constructs with winding angles between 5 and 60°.
In Chapter 4 a different approach was followed. It was based on extrusion-based bioprinting in combination with a hydrogel ink system. The ink was loaded with nanoparticles and the nanoparticle release was analyzed. In other words, two systems, a printable polyglycidol/hyaluronic acid ink and mesoporous silica nanoparticles (MSN), were combined to analyze charge driven release mechanism that could be fine-tuned using bioprinting. Thorough rheological evaluations proved that the charged nanoparticles, both negatively charged MSN-COOH and positively charged MSN-NH2, did not alter the shear thinning properties of the ink that revealed a negative base charge due to hyaluronic acid as one of its main components. Furthermore, it could be shown that the particles did also not have a negative effect on the recovery properties of the material after exposure to high shear. During printing, the observations made via rheological testing were supported by the fact that all materials could be printed at the same settings of the bioprinter. Using theses inks, it was possible to make constructs as big as 12x12x3 mm3 composed of 16 layers. The fiber diameters produced were about 627±31 μm and two-component constructs could be realized utilizing the two hydrogel print heads of the printer to fabricate one hybrid construct. The particle distribution within those constructs was homogeneous, both from a microscopic and a macroscopic point of view. Particle release from printed constructs was tracked over 6 weeks and revealed that the print geometry had an influence on the particle release. Printed in a geometry with direct contact between the strands containing different MSN, the positively charged particles quickly migrated into the strand previously containing only negatively charged MSN-COOH. The MSN-COOH seemed to be rather released into the surrounding liquid and also after 6 weeks no MSN-COOH signal could be detected in the strand previously only containing MSN-NH2. In case of a geometry without direct contact between the strands, the migration of the positively charged nanoparticles into the MSN-COOH containing strand was strongly delayed. This proved that the architecture of the printed construct can be used to fine-tune the particle release from nanoparticle containing printable hydrogel ink systems.
Chapter 5 discusses an approach using hydrogel inks based on recombinant spider silk proteins processed via extrusion-based bioprinting. The ink could be applied for printing at protein concentrations of 3 % w/v without the addition of thickeners or any post process crosslinking. Both, the recombinant protein eADF4(C16) and a modification introducing a RGD-sequence to the protein (eADF4(C16)-RGD), could be printed revealing a very good print fidelity. The RGD modification had positive effect on the adhesion of cells seeded onto printed constructs. Furthermore, human fibroblasts encapsulated in the ink at concentrations of 1.2 million cells per mL did not alter the print fidelity and did not interfere with the crosslinking mechanism of the ink. This enabled printing cell laden constructs with a cell survival rate of 70.1±7.6 %. Although the cell survival rate needs to be improved in further trials, the approach shown is one of the first leading towards the shift of the window of biofabrication because it is based on a new material that does not need potentially harmful post-process crosslinking and allows the direct encapsulation of cells staying viable throughout the print process.
Chemoselective poly(oxazolines) (POx) and poly[(oligo ethylene glycol) acrylates] were synthesized. An initiator was produced for the preparation of poly(oxazoline)s capable of participating in click chemistry reactions which allows the functionalization of the polymer at the α terminus which was confirmed by 1H NMR spectroscopy. The initiator was used for the polymerization of hydrophilic 2 methyl 2 oxazoline (MeOx), whereby chemoselective, alkyne functionalized polymers could be prepared for Cu-catalyzed azide–alkyne cycloaddition. The desired molecular weight could be achieved through the living, ring opening cationic polymerization and was confirmed by 1H NMR, SEC and MALDI ToF measurements. Polymers were terminated with piperidine if no further functionalization was needed, or with an ester derivate for enabling amine attachment in a subsequent step. In addition, polymers were functionalized by termination with NaN3 in order to provide the counterpart to the azide–alkyne reaction. IR spectroscopy was suitable for the azide detection. The coupling of polymers showed the reactivity and could be confirmed by SEC, 1H NMR and IR spectroscopy.
The composition of cysteine functionalized POx was completed by thiol–ene chemistry. Since the commercially available iso 2 propyl 2 oxazoline is not available for the cationic polymerization, 2 butenyl and 2 decenyl 2 oxazoline (ButenOx and DecenOx) were first prepared. The synthesis of both copolymers, based on MeOx could be confirmed by 1H NMR as well as with SEC, whereby narrow distributions with dispersities of 1.06 could be achieved. The cysteine functionalization of the copolymers was enabled by the creation of a thiazolidine component which could be synthesized by acetal and formyl protection of cysteine and subsequent functionalization with a thiol. The component enabled the reaction with a polymer by thiol–ene reaction which was started by the addition of dimethoxyphenyl-acetophenone and was catalyzed by irradiation with UV light. Both copolymers, with a shorter (polymers with BuenOx) and longer (polymers with DecenOx) hydrophobic sidechain could be functionalized. 1H NMR spectroscopic analysis showed a quantitative reaction with the thiazolidine derivate. After deprotection by acidic workup the desired, cysteine functionalized polymer could be isolated. Quantification of cysteine functions was ensured by a modified TNBSA assay, whereby the thiols were first oxidized in order to confirm an independent measurement of amine functions. Both, the TNBSA assay as well as the NMR measurement showed the desired number of cysteine residues.
The cytotoxicity of functionalized polymers with different compositions was tested by a luminescent cell viability assay (LCVA). Both, the amount of cysteine functions (5–10%) in the copolymers as well as the length of the hydrophobic side chain were varied. All polymers did not show cytotoxicity up to concentrations of 10 mg∙mL-1. The cell activity and cell numbers only decreased below 50% and 20% respectively, when copolymers with 5% cysteine and longer sidechains were measured, which was attributed to a contamination of the sample itself. The cooperation partner performed Native Chemical Ligation (NCL) with model peptides and purified the products by HPLC. A sterically non demanding peptide was synthesized, consisting of an aromatic amino acid and four glycine units. The aromatic unit was used for the quantification of the polymer–peptide conjugate in the 1H NMR spectroscopy. A polymer having five cysteine side chains has been fully implemented by NCL to a conjugate of one polymer with five peptides. A sterically more demanding peptide was additionally used and MALDI ToF measurements confirmed the successful conjugation.
Furthermore the cysteine functionalized polymer was used for nanogel synthesis. The thiol of the cysteine function was oxidized in an inverse mini-emulsion by H2O2, resulting in nanogels (~500 nm) which could be confirmed by SEM, AFM, DLS and NTA measurements.
Besides POx, oligo (ethylene glycol)acrylates (OEGA) were polymerized; by copolymerization with the reactive pentafluorophenyl acrylate (PFPA) reactive and amphiphilic polymers were obtained. The synthesis of PFPA could be confirmed spectroscopically by 1H , 19F NMR, and by FT IR. Copolymers were synthesized by RAFT polymerization with narrow dispersities. Functionalization with an amine functionalized thiazolidine led to a hydrophilic cysteine functionalized polymer after acidic deprotection. Apart from this polymer, a thioester functionalization was successfully performed by reaction of the active polymer with a cyclic amine functionalized thioester which does not release a toxic by product (such as the resulting thiol) during NCL and thus features a very high potential to replace former thioester.
The aim of this thesis was the preparation of a biomaterial ink for the fabrication of chemically crosslinked hydrogel scaffolds with low micron sized features using melt electrowriting (MEW). By developing a functional polymeric material based on 2-alkyl-2-oxazine (Ozi) and 2-alkyl-2-oxazoline (Ox) homo- and copolymers in combination with Diels-Alder (DA)-based dynamic covalent chemistry, it was possible to achieve this goal. This marks an important step for the additive manufacturing technique melt electrowriting (MEW), as soft and hydrophilic structures become available for the first time. The use of dynamic covalent chemistry is a very elegant and efficient method for consolidating covalent crosslinking with melt processing. It was shown that the high chemical versatility of the Ox and Ozi chemistry offers great potential to control the processing parameters. The established platform offers straight forward potential for modification with biological cues and fluorescent markers. This is essential for advanced biological applications. The physical properties of the material are readily controlled and the potential for 4D-printing was highlighted as well. The developed hydrogel architectures are excellent candidates for 3D cell culture applications. In particular, the low internal strength of some of the scaffolds in combination with the tendency of such constructs to collapse into thin strings could be interesting for the cultivation of muscle or nerve cells. In this context it was also possible to show that MEW printed hydrogel scaffolds can withstand the aspiration and ejection through a cannula. This allows the application as scaffolds for the minimally invasive delivery of implants or functional tissue equivalent structures to various locations in the human body.
Die vorliegende Arbeit befasste sich mit der bisher relativ unbekannten Polymerklasse der Polypeptoide, die hinsichtlich ihrer Verwendung als Biomaterial näher untersucht werden sollte. Hierbei war die Untersuchung des Polymerisationssystems ein wesentlicher Schwerpunkt. Dies beinhaltete zum einen die Synthesen verschiedener Monomere sowie deren Polymerisationskinetiken und zum anderen Studien über die Stabilität des aktiven Kettenendes. Um mehr über die Polypeptoide zu erfahren, wurden die erhaltenen Homopolymere nach der Strukturanalyse hinsichtlich ihrer physikochemischen Eigen-schaften untersucht. Im Anschluss erfolgte die Synthese von (amphiphilen) Blockco-polypeptoiden, die sich in wässrigen Lösungen zu definierten Morphologien zusammen-lagern. Die resultierenden Morphologien, sowohl mizellare als auch vesikuläre Strukturen, wurden mit verschiedenen Methoden, wie z. B. der Pyren-Fluoreszenz-Spektroskpie und der dynamischen Lichtstreuung, untersucht. Erste Erkenntnisse über die Biokompatibilität der Polypeptoide sollte die Bestimmung der Zellviabilität in verschiedenen Polymerlösungen liefern.
Die verschiedenen Studien über die Polypeptoide zeigten, dass diese Polymerklasse über eine besonders lebende Polymerisation synthetisiert werden kann. Dabei resultieren Produkte, die sich durch eine Poisson-Verteilung und eine hohe Endgruppengenauigkeit auszeichnen. Zusätzlich bestehen Polypeptoide aus einem abbaubaren Rückgrat und, im Vergleich zu den Polypeptiden, besitzen sie eine erhöhte proteolytische Stabilität. Amphiphile Blockcopolypeptoide sind zudem in der Lage, sich in Lösung zu verschiedenen Morphologien anzuordnen. Durch die Variierung der Seitenkette und des f kann sowohl die Selbstorganisation als auch das Mikroumfeld der Aggregate abgestimmt werden. Darüber hinaus können die amphiphile Blockcopolymere, die sich zu Mizellen anordnen, hydrophobe Substanzen solubilisieren.
Polypeptoide liefern all die nötige chemische Vielseitigkeit und potentielle Biokompatibilität, um bestehende sowie neuartige Probleme in biomedizinischen Anwendungen zu bewältigen. Zukünftige in vivo und in vitro Test werden das Potential, aber auch die Grenzen dieser neuen Polymerklasse als Biomaterial zeigen.
This thesis identifies how the printing conditions for a high-resolution additive manufacturing technique, melt electrowriting (MEW), needs to be adjusted to process electroactive polymers (EAPs) into microfibers. Using EAPs based on poly(vinylidene difluoride) (PVDF), their ability to be MEW-processed is studied and expands the list of processable materials for this technology.
In this work, the influence of aromatic structures on drug encapsulation, self-assembly and hydrogel formation was investigated. The physically crosslinked gelling systems were characterized and optimized for the use in biofabrication and applied in initial (bio)printing experiments.
Chapter I: The cytocompatible (first in vitro and in vivo studies) amphiphile PMeOx-b-PBzOx-b- PMeOx (A-PBzOx-A) was used for the solubilization of PTX, schizandrin A (SchA), curcumin (CUR), niraparib and HS-173.
Chapter II: Compared to the polymers A-PPheOx-A, A-PBzOx-A and A-PBzOzi-A, only the polymer A-PPheOzi-A showed a reversible temperature- and concentration-dependent inverse thermogelation, which is accompanied by a morphology change from long wormlike micelles in the gel to small spherical micelles in solution. The worm formation results from novel interactions between the hydrophilic and hydrophobic aromatic polymer blocks. Changes in the hydrophilic block significantly alter the gel system. Rheological properties can be optimized by concentration and temperature, which is why the hydrogel was used to significantly improve the printability and stability of Alg in a blend system.
Chapter III: By extending the side chain of the aromatic hydrophobic block, the inverse thermogelling polymer A-poly(2-phenethyl-2-oxazoline)-A (A-PPhenEtOx-A) is obtained. Rapid gelation upon cooling is achieved by inter-correlating spherical micelles. Based on ideal rheological properties, first cytocompatible bioprinting experiments were performed in combination with Alg. The polymers A- poly(2-benzhydryl-2-oxazoline)-A (A-PBhOx-A) and A-poly(2-benzhydryl-2-oxazine) (A-PBhOzi-A) are characterized by two aromatic benzyl units per hydrophobic repeating unit. Only the polymer A- PBhOzi-A exhibited inverse thermogelling behavior. Merging micelles could be observed by electron microscopy. The system was rheologically characterized and discussed with respect to an application in 3D printing.
Chapter IV: The thermogelling POx/POzi system, in particular the block copolymer PMeOx-b- PnPrOzi, was used in different applications in the field of biofabrication. The introduction of maleimide and furan units along the hydrophilic polymer part ensured additional stabilization by Diels-Alder crosslinking after the printing process.
Motivated by the great potential offered by the combination of additive manufacturing technology and hydrogels, especially in the field of tissue engineering and regenerative medicine, a series of novel hybrid hydrogel inks were developed based on the recently described thermogelling poly(2-oxazoline)s-block-poly(2-oxazine)s diblock copolymers, which may help to expand the platform of available hydrogel inks for this transformative 3D printing technology (Fig. 5.1).
In the present thesis, the first reported thermogelling polymer solely consisting of POx and POzi, i.e., the diblock copolymer PMeOx-b-PnPrOzi comprising a hydrophilic block (PMeOx) and a thermoresponsive block (PnPrOzi), was selected and used as a proof-of-concept for the preparation of three novel hybrid hydrogels. Therefore, three batches of the diblock copolymers with a DP of 100 were synthesized for the study of three different hybrid hydrogels with a special focus on their suitability as (bio)inks for extrusion-based 3D printing. The PMeOx-b-PnPrOzi diblock copolymer solution shows a temperature induced reversible gelation behavior above a critical polymer concentration of 20 wt%, as described for the Pluronic F127 solution but with a unique gelation mechanism, working through the formation of a bicontinuous sponge-like structure from the physically crosslinked vesicles. Specially, its intrinsic shear thinning behavior and excellent recovery property with a certain yield point make it a promising ink candidate for extrusion-based printing technology.
Increasing the polymer concentration is the most traditional approach to improve the printability of an ink material, and serve as the major strategy available to improve the printability of PMeOx-b-PnPrOzi systems prior to this work. From the analysis of rheological properties related to printability, it came a conclusion that increasing the copolymer concentration does improve the hydrogel strength and thus the printability. However, such improvement is very limited and usually leads to other problems such as more viscous systems and stringent requirements on the printers, which are not ideal for the printing process and applications especially in the cell-embedded biofabrication field.
POx-b-POzi/clay Hybrid Hydrogel
An alternative method proposed to improve the printability of this thermoresponsive hydrogel ink is through nanoclay (Laponite XLG) addition, i.e., the first hybrid hydrogel system of PMeOx-b-PnPrOzi/clay (also named shortly as POx-b-POzi/clay) in this thesis. To optimize the viscoelastic properties of the ink material, Laponite XLG acted as a reinforcement additive and a physically crosslinker was blended with the copolymers. Compared with the pristine copolymer solution of PMeOx-b-PnPrOzi, the hybrid PMeOx-b-PnPrOzi/clay solution well retained the temperature induced gelation performance of the copolymers.
The obtained hybrid hydrogels exhibited a rapid in situ reversible thermogelation at a physiological relevant Tgel of around 15 ℃ and a rapid recovery of viscoelastic properties within a few seconds. More importantly, with the addition of only a small amount of 1.2 wt% clay, it exhibited obviously enhanced shear thinning character (n = 0.02), yield stress (240 Pa) and mechanical strength (storage modulus over 5 kPa). With this novel hybrid hydrogel, real three-dimensional constructs with multiple layers and various geometries are generation with greatly enhanced shape fidelity and resolution. In this context, the thermogelling properties of the hybrid hydrogels over a copolymer concentration range of 10-20 wt% and a clay concentration of 0-4 wt% were systematically investigated, and from which a printable window was obtained from the laboratory as a reference.
In fact, the printing performance of an ink is not only determined by the intrinsic physicochemical properties of the material, but is also influenced by the external printing environments as well as the printer parameter settings. All the printing experiments in this study were conducted under a relatively optimized conditions obtained from preliminary experiments. In future work, the relationship between material rheology properties, printer parameters and printing performance could be systematically explored. Such a fundamental study will help to develop models that allows the prediction and comparison of printing results from different researches based on the parameters available through rheology, which is very beneficial for further development of more advanced ink systems.
Although the printability has been significantly improved by the addition of nanoclay Laponite XLG, the hybrid hydrogels and their printed constructs still suffer from some major limitations. For example, these materials are still thermoresponsive, which will cause the printed constructs to collapse when the environment temperature changes below their Tgel. In addition, the formed hydrogel constructs are mechanical too weak for load-bearing applications, and the allowed incubation time is very limited during media exchange/addition as it will lead to dissolution of the hydrogels due to dilution effects. Therefore, it is essential to establish a second (chemical or physical) crosslinking mechanism that allows further solidification of the gels after printing. It should be kept in mind that the second crosslinking step will eliminate the thermoresponsive behavior of the gels and thus the possibility of cell recovery. In this case, besides through the traditional approach of copolymer modification to realize further crosslinking, like one of the well-known post-polymerization modification approach Diels-Alder reaction,[430] designing of interpenetrating networks (IPN) hydrogels serves as one of the major strategy for advanced (bio)ink preparation.[311] Therefore, the second hybrid hydrogel system of PMeOx-b-PnPrOzi/PDMAA/clay (also named shortly as POx-b-POzi/PDMAA/clay) was developed in this thesis, which is a 3D printable and highly stretchable ternary organic-inorganic IPN hydrogel.
POx-b-POzi/PDMAA/clay Hybrid Hydrogel
The nanocomposite IPN hydrogel combines a thermoresponsive hydrogel with clay described above and in situ polymerized poly(N, N-dimethylacrylamide). Before in situ polymerization, the thermoresponsive hydrogel precursors exhibited thermogelling behavior (Tgel ~ 25 ℃, G' ~ 6 kPa) and shear thinning properties, making the system well-suited for extrusion-based 3D printing. After chemical curing of the 3D-printed constructs by free radical polymerization, the resulting IPN hydrogels show excellent mechanical strength with a high stretchability to a tensile strain at break exceeding 550%. The hybrid hydrogel can sustain a high stretching deformation and recover quickly due to the energy dissipation from the non-covalent interactions. With this hybrid hydrogel, integrating with the advanced 3D-printing technique, various 3D constructs can be printed and cured successfully with high shape fidelity and geometric accuracy.
In this context, we also investigated the possibility of acrylic acid (AA) and 2-hydroxyethylmethacrylate (HEMA) as alternative hydrogel precursors. However, the addition of these two monomers affected the thermogelation of POx-b-POzi in an unfavorable manner, as these monomers competed more effectively with water molecules, preventing the hydration of nPrOzi block at lower temperatures and therefore, the liquefaction of the gels. Furthermore, the influence of the printing process and direction on the mechanical properties of the hydrogel was investigated and compared with the corresponding bulk materials obtained from a mold. No significant effects from the additive manufacturing process were observed due to a homogeneously adhesion and merging between sequentially deposited layers. In the future, further studies on the specific performance differences among hydrogels fabricated at different printing directions/speeds would be of great interest to the community, as this allows for a more accurately control and better predict of the printed structures.
This newly developed hybrid IPN hydrogel is expected to expand the material toolbox available for hydrogel-based 3D printing, and may be interesting for a wide range of applications including tissue engineering, drug delivery, soft robotics, and additive manufacturing in general. However, in this case, the low toxicity from the monomer DMAA and other small molecules residuals in the polymerized hydrogels made this hybrid hydrogel not ideal for bioprinting in the field of biofabrication. For this problem, cyto-/biocompatible monomers such as polyethylene glycol diacrylate (PEGDA) can be used as an alternative, while the overall properties of the hydrogels including mechanical properties should be re-evaluated accordingly. Moreover, the swelling behavior of the hydrogels should also be taken into account, as it may most likely affect the mechanical strength and geometry size of the printed scaffold, but is often be overlooked after printing. For example, regarding the specific hybrid hydrogel POx-b-POzi/PDMAA/clay in this work, an equilibrium swelling ratio of 1100% was determined. The printed hydrogel cuboid experienced a volume increasing over 6-fold after equilibrium swelling in water, and became mechanical fragile due to the formation of a swollen hydrogel network absorbing large amount of water.
POx-b-POzi/Alg/clay Hybrid Hydrogel
In the final part of this dissertation, to enable the cell-loaded bioprinting and long-term cell culture, the third hybrid hydrogel system POx-b-POzi/Alg/clay was introduced by replacing the monomer DMAA to the natural polysaccharides alginate. Initially, detailed rheological characterization and mechanical tests were performed to evaluate their printability and mechanically properties. Subsequently, some simple patterns were printed with the optimized hydrogel precursor solutions for the preliminary filament fusion and collapse test before proceeding to more complex printings. The fibers showed a sufficient stability which allows the creation of large structures with a height of a few centimeters and a suspended filament up to centimeter. Accordingly, various 3D constructs including suspended filaments were printed successfully with high stackability and shape fidelity. The structure after extrusion was physical crosslinked easily by soaking in CaCl2 solution and, thereafter exhibited a good mechanical flexibility and long-term stability. Interestingly, the mechanical strength and geometry size of the generated scaffolds were well maintained over a culture period of weeks in water, which is of great importance for clinical applications. In addition, the post-printing ionic crosslinking of alginate could also be realized by other di/trivalent cations such as Fe3+ and Tb3+.
Subsequently, the cell-laden printing with this hybrid hydrogel and post-printing crosslinking by Ca2+ ions highlighting its feasibility for 3D bioprinting. WST-1 assay of fibroblast suggested no-dose dependent cytocompatibility of the hydrogel precursor solution. The cell distribution was uniform throughout the printed construct, and proliferated with high cell viability during the 21 days culture. The presented hybrid approach, utilizing the beneficial properties of the POx-b-POzi base material, could be interesting for a wide range of bioprinting applications and potentially enabling also other biological bioinks such as collagen, hyaluronic acid, decellularized extracellular matrix or cellulose based bioinks. Although the results look promising and the developed hydrogel is an important bioink candidate, the long-term in vitro cell studies with different cell lines and clinical model establishment are still under investigation, which remains a long road but is of great importance before realizing real clinical application.
Last but not least, the improvement to the printability of thermogelling POx/POzi-based copolymers by the clay Laponite XLG was also demonstrated in another thermogelling copolymer PEtOx-b-PnPrOzi. This suggests that the addition of clay may be a general strategy to improve the printability of such polymers. Despite these advances in this work which significantly extended the (bio)material platform of additive manufacturing technology, the competition is still fierce and more work should be done in the further to reveal the potential and limitations of this kind of new and promising candidate (bio)ink materials. It is also highly expected for further creative works based on the thermogelling POx/POzi polymers, such as crosslinking in Ca2+ solution containing monomer acrylamide to prepare printable and mechanically tough hydrogels, research on POx-based support bath material, and print of clinically more relevant sophisticated structures such as 3D microvascular networks omnidirectionally.
Motivated by the great potential which is offered by the combination of additive manufacturing and tissue engineering, a novel polymeric bioink platform based on poly(2 oxazoline)s was developed which might help to further advance the young and upcoming field of biofabrication. In the present thesis, the synthesis as well as the characteristics of several diblock copolymers consisting of POx and POzi have been investigated with a special focus on their suitability as bioinks.
In general, the copolymerization of 2-oxazolines and 2-oxazines bearing different alkyl side chains was demonstrated to yield polymers in good agreement with the degree of polymerization aimed for and moderate to low dispersities.
For every diblock copolymer synthesized during the present study, a more or less pronounced dependency of the dynamic viscosity on temperature could be demonstrated. Diblock copolymers comprising a hydrophilic PMeOx block and a thermoresponsive PnPrOzi block showed temperature induced gelation above a degree of polymerization of 50 and a polymer concentration of 20 wt%. Such a behavior has never been described before for copolymers solely consisting of poly(cyclic imino ether)s.
Physically cross linked hydrogels based on POx b POzi copolymers exhibit reverse thermal gelation properties like described for solutions of PNiPAAm and Pluronic F127. However, by applying SANS, DLS, and SLS it could be demonstrated that the underlying gel formation mechanism is different for POx b POzi based hydrogels. It appears that polymersomes with low polydispersity are formed already at very low polymer concentrations of 6 mg/L. Increasing the polymer concentration resulted in the formation of a bicontinuous sponge like structure which might be formed due to the merger of several vesicles. For longer polymer chains a phase transition into a gyroid structure was postulated and corresponds well with the observed rheological data.
Stable hydrogels with an unusually high mechanical strength (G’ ~ 4 kPa) have been formed above TGel which could be adjusted over a range of 20 °C by changing the degree of polymerization if maintaining the symmetric polymer architecture. Variations of the chain ends revealed only a minor influence on TGel whereas the influence of the solvent should not be neglected as shown by a comparison of cell culture medium and MilliQ water.
Rotationally as well as oscillatory rheological measurements revealed a high suitability for printing as POx b POzi based hydrogels exhibit strong shear thinning behavior in combination with outstanding recovery properties after high shear stress.
Cell viability assays (WST-1) of PMeOx b PnPrOzi copolymers against NIH 3T3 fibroblasts and HaCat cells indicated that the polymers were well tolerated by the cells as no dose-dependent cytotoxicity could be observed after 24 h at non-gelling concentrations up to 100 g/L.
In summary, copolymers consisting of POx and POzi significantly increased the accessible range of properties of POx based materials. In particular thermogelation of aqueous solutions of diblock copolymers comprising PMeOx and PnPrOzi was never described before for any copolymer consisting solely of POx or POzi. In combination with other characteristics, e.g. very good cytocompatibility at high polymer concentrations and comparably high mechanical strength, the formed hydrogels could be successfully used for 3D bioprinting. Although the results appear promising and the developed hydrogel is a serious bioink candidate, competition is tough and it remains an open question which system or systems will be used in the future.
Articular cartilage defects represent one of the most challenging clinical problem for orthopedic surgeons and cartilage damage after trauma can result in debilitating joint pain, functional impairment and in the long-term development of osteoarthritis. The lateral cartilage-cartilage integration is crucial for the long-term success and to prevent further tissue degeneration. Tissue adhesives and sealants are becoming increasingly more popular and can be a beneficial approach in fostering tissue integration, particularly in tissues like cartilage where alternative techniques, such as suturing, would instead introduce further damage. However, adhesive materials still require optimization regarding the maximization of adhesion strength on the one hand and long-term tissue integration on the other hand. In vitro models can be a valuable support in the investigation of potential candidates and their functional mechanisms. For the conducted experiments within this work, an in vitro disc/ring model obtained from porcine articular cartilage tissue was established. In addition to qualitative evaluation of regeneration, this model facilitates the implementation of biomechanical tests to quantify cartilage integration strength. Construct harvesting for histology and other evaluation methods could be standardized and is ethically less questionable compared to in vivo testing. The opportunity of cell culture technique application for the in vitro model allowed a better understanding of cartilage integration processes.
Tissue bonding requires chemical or physical interaction of the adhesive material and the substrate. Adhesive hydrogels can bind to the defect interface and simultaneously fill the gap of irregularly shaped defect voids. Fibrin gels are derived from the physiological blood-clot formation and are clinically applied for wound closure. Within this work, comparisons of different fibrin glue formulations with the commercial BioGlue® were assessed, which highlighted the need for good biocompatibility when applied on cartilage tissue in order to achieve satisfying long-term integration. Fibrin gel formulations can be adapted with regard to their long-term stability and when applied on cartilage disc/ring constructs improved integrative repair is observable. The kinetic of repairing processes was investigated in fibrin-treated cartilage composites as part of this work. After three days in vitro cultivation, deposited extracellular matrix (ECM) was obvious at the glued interface that increased further over time. Interfacial cell invasion from the surrounding native cartilage was detected from day ten of tissue culture. The ECM formation relies on molecular factors, e.g., as was shown representatively for ascorbic acid, and contributes to increasing integration strengths over time. The experiments performed with fibrin revealed that the treatment with a biocompatible adhesive that allows cartilage neosynthesis favors lateral cartilage integration in the long term. However, fibrin has limited immediate bonding strength, which is disadvantageous for use on articular cartilage that is subject to high mechanical stress. The continuing aim of this thesis was to further develop adhesive mechanisms and new adhesive hydrogels that retain the positive properties of fibrin but have an increased immediate bonding strength.
Two different photochemical approaches with the advantage of on-demand bonding were tested. Such treatment potentially eases the application for the professional user. First, an UV light induced crosslinking mechanism was transferred to fibrin glue to provide additional bonding strength. For this, the cartilage surface was functionalized with highly reactive light-sensitive diazirine groups, which allowed additional covalent bonds to the fibrin matrix and thus increased the adhesive strength. However, the disadvantages of this approach were the multi-step bonding reactions, the need for enzymatic pretreatment of the cartilage, expensive reagents, potential UV-light damage, and potential toxicity hazards. Due to the mentioned disadvantages, no further experiments, including long-term culture, were carried out. A second photosensitive approach focused on blue light induced crosslinking of fibrinogen (RuFib) via a photoinitiator molecule instead of using thrombin as a crosslinking mediator like in normal fibrin glue. The used ruthenium complex allowed inter- and intramolecular dityrosine binding of fibrinogen molecules. The advantage of this method is a one-step curing of fibrinogen via visible light that further achieved higher adhesive strengths than fibrin. In contrast to diazirine functionalization of cartilage, the ruthenium complex is of less toxicological concern. However, after in vitro cultivation of the disc/ring constructs, there was a decrease in integration strength. Compared to fibrin, a reduced cartilage synthesis was observed at the defect. It is also disadvantageous that a direct adjustment of the adhesive can only be made via protein concentration, since fibrinogen is a natural protein that has a fixed number of tyrosine binding sites without chemical modification.
An additional cartilage adhesive was developed that is based on a mussel-inspired adhesive mechanism in which reactivity to a variety of substrates is enabled via free DOPA amino acids. DOPA-based adhesion is known to function in moist environments, a major advantage for application on water-rich cartilage tissue surrounded by synovial liquid. Reactive DOPA groups were synthetically attached to a polymer, here POx, to allow easy chemical modifiability, e.g. insertion of hydrolyzable ester motifs for tunable degradation. The possibility of preparing an adhesive hybrid hydrogel of POx in combination with fibrinogen led to good cell compatibility as was similarly observed with fibrin, but with increased immediate adhesive strength. Degradation could be adjusted by the amount of ester linkages on the POx and a direct influence of degradation rates on the development of integration in the in vitro model could be shown.
Hydrogels are well suited to fill defect gaps and immediate integration can be achieved via adhesive properties. The results obtained show that for the success of long-term integration, a good ability of the adhesive to take up synthesized ECM components and cells to enable regeneration is required. The degradation kinetics of the adhesive must match the remodeling process to avoid intermediate loss of integration power and to allow long-term firm adhesion to the native tissue.
Hydrogels are not only important as adhesives for smaller lesions, but also for filling large defect volumes and populating them with cells to produce tissue engineered cartilage. Many different hydrogel types suitable for cartilage synthesis are reported in the literature. A long-term stable fibrin formulation was tested in this work not only as an adhesive but also as a bulk hydrogel construct. Agarose is also a material widely used in cartilage tissue engineering that has shown good cartilage neosynthesis and was included in integration assessment. In addition, a synthetic hyaluronic acid-based hydrogel (HA SH/P(AGE/G)) was used. The disc/ring construct was adapted for such experiments and the inner lumen of the cartilage ring was filled with the respective hydrogel. In contrast to agarose, fibrin and HA-SH/P(AGE/G) gels have a crosslink mechanism that led to immediate bonding upon contact with cartilage during curing. The enhanced cartilage neosynthesis in agarose compared to the other hydrogel types resulted in improved integration during in vitro culture. This shows that for the long-term success of a treatment, remodeling of the hydrogel into functional cartilage tissue is a very high priority. In order to successfully treat larger cartilage defects with hydrogels, new materials with these properties in combination with chemical modifiability and a direct adhesion mechanism are one of the most promising approaches.
Motivated by the perceived great potential of chiral polymers, the presented work aimed at the investigation of synthesis, solubility and optical activity of chiral poly(2,4-disubstituted-2-oxazoline)s. A novel polymeric carrier based on ABA-type triblock copolymers poly(2-oxazoline)s with chiral and racemic hydrophobic blocks was developed for the formulation of chiral and achiral drugs (Fig. 5.1). Poly(2-methyl-2-oxazoline) (pMeOx) was used as hydrophilic A block, and poly(2-ethyl-4-ethyl-2-oxazoline) (pEtEtOx) and poly(2-propyl-4-methyl-2-oxazoline) (pPrMeOx) were used as hydrophobic B blocks. Curcumin (CUR), paclitaxel (PTX) and chiral/racemic ibuprofen (R/S/RS-IBU) were applied as model drugs. Nanoformulations were prepared consisting of these triblock copolymers and model drugs. ...
This thesis aims to investigate the form-phase diagram of aqueous solutions of the triblock copolymer Pluronic P123 focusing on its high-temperature phases. P123 is based on polyethylene as well as polypropylene oxide blocks and shows a variety of di erent temperaturedependent micelle morphologies or even lyotropic liquid crystal phases in aqueous solutions. Besides the already well-studied spherical aggregates at intermediate temperatures, the size and internal structure of both worm-like and lamellar micelles, which appear near the cloud point, is determined using light, neutron and X-ray scattering. By combining the results of time-resolved dynamic light as well as small-angle neutron and X-ray scattering experiments, the underlying structural changes and kinetics of the sphere-to-worm transition were studied supporting the random fusion process, which is proposed in literature. For temperatures near the cloud point, it was observed that aqueous P123 solutions below the critical crystallization concentration gelate after several hours, which is linked to the presence and structure of polymeric surface layers on the sample container walls as shown by neutron re ectometry
measurements. Using a hierarchical model for the lamellar micelles including their periodicity as well as domain and overall size, it is possible to unify the existing results in literature and propose a direct connection between the near-surface and bulk properties of P123 solutions at temperatures near the cloud point.
The present work aims towards the investigation of polymer degradation under biologically relevant conditions. In order to assess a potential degradation of polymers of interest for biomedical applications in vivo and associated effects on living tissue, representatives of poly(2-oxazoline)s and polypeptoids as well as poly(ethylene glycol) and poly(N-vinylpyrrolidone) for reference purposes are examined regarding their stability under oxidative and hydrolytic conditions as well as towards enzymatic degradation.
The polymers investigated in the framework of this thesis are generally considered to be non-biodegradable. Both poly(ethylene glycol) and poly(N-vinylpyrrolidone) are or were applied intensively in vivo provoking seriously harmful side effects like fatal blood poisoning from the oxidation of poly(ethylene glycol) chain ends or poly(N-vinylpyrrolidone) storage disease. Poly(2-alkyl-2-oxazoline)s and polypeptoids, both promising polymeric biomaterials for a wide variety of in vivo applications, are not clinically applied yet but undergo thorough investigations. However, comprising amide bonds within the backbone or the appending side chain, poly(2-alkyl-2-oxazoline)s and polypeptoids potentially offer a higher susceptibility towards (bio-)degradation. Representing the three most impactful initiators of degradation in vivo, the present study is focused on polymer deterioration by oxidative species, hydrolytic conditions and enzymes.
Oxidative species are generated in a variety of processes in vivo, both on purpose and as an unintentional by-product. Previous investigations revealed the susceptibility of poly(ethylene glycol), poly(N-vinylpyrrolidone), poly(2-alkyl-2-oxazoline)s and polypeptoids to deterioration by hydroxyl radicals deriving from hydrogen peroxide and copper ions. The obtained data confirm previous results of an apparent degradation rate increasing with increasing chain length due to self-inhibitory end group effects for all investigated polymer species. Although the exact concentrations of oxidative species in vivo are very controversial, with respect to their great variety and wide distribution the investigated polymers are likely prone to oxidative deterioration to some extent, with rates, mechanisms and degradation products strongly depending on the respective reactive species, polymer structure and chain length.
Like blood, most tissues of the human body benefit from a slightly alkaline pH value. Nevertheless, specific areas like the human stomach or tumor tissues possess acidic conditions potentially capable to cleave amide bonds comprised by poly(2-alkyl-2-oxazoline)s and polypeptoids. Unlike the hydrolysis of poly(2-alkyl-2-oxazoline)s resulting in side chain cleavage, the hydrolysis of polypeptoids induces backbone scission decreasing the polymer chain length tremendously and releasing, if performed exhaustively, the respective amino acids. Hydrolysis of polysarcosine is monitored by quantification of the released sarcosine via 1H-NMR spectroscopy and determination of the residual Mw via GPC. Its cyclic dimer sarcosine anhydride is formed as an intermediate product in this process via cyclization of unstable linear dimers of sarcosine.
Modification and degradation of bio(macro)molecules is an essential part of human metabolism. Polymers bearing amide bonds and showing a great similarity to natural occurring and widely distributed polypeptides, like poly(2-alkyl-2-oxazoline)s and polypeptoids, bear the potential of an enzymatic biodegradability by (more or less specific) peptidases. Just like the acidic hydrolysis described previously, peptidase activity would result in the cleavage of polymer amide bonds. The aim of the present thesis was to evaluate the stability of poly(2-alkyl-2-oxazoline)s and polypeptoids as well as poly(ethylene glycol) for the sake of reference under circumstances resembling in vivo conditions as closely as possible. Initial experiments focused on the degradation of dye-labeled upon incubation with homogenates of freshly harvested rat liver and kidney. However, although the obtained results are promising for the most part, they are considered rather unreliable and non-reproducible for various reasons. More conclusive data are attained from the incubation of non-labeled polymers in freshly laid chicken eggs. While no evidence for an enzymatic digestion of poly(ethylene glycol) in chicken egg white is found and deterioration of poly(2-methyl-2-oxazoline) upon incubation apparently derives from non-enzymatic hydrolysis, incubated polysarcosine samples reveal distinct elugram patterns depending on the respective C- and N-terminal end groups indicating both exopeptidase and endopeptidase activity. It has to be kept in mind though, that an enzymatic digestibility of polysarcosine does not necessarily imply the digestion of polypeptoids bearing longer side chains by peptidases as well, which should be investigated in further studies.
Die vorliegende Arbeit befasst sich mit der Synthese und Charakterisierung von nanostrukturierten Mikropartikelpulvern mit einstellbarem Zerfalls- und Dispergierungsverhalten und deren Anwendung als verstärkender Füllstoff sowie deren Eignung für Sensoranwendungen. Sie ist in drei Teilbereiche gegliedert: Der erste Teil beschreibt die Synthese der nanostrukturierten Mikropartikelpulvern durch Sprühtrocknung von kolloidalen oxidischen (silicatischen und eisenoxidischen) Nanopartikeln. Es wird ausgeführt, wie durch Variation der Art und Größe der Primärpartikel und deren mengenanteiligen Kombination Mikropartikel unterschiedlichster nanostruktureller Maserung und Ausprägung erhalten wurden. Das Spektrum dieser Partikel reichte von homogen verteilten Strukturen bis hin zu Kern-Satellit-Struktur, von kontrollierter Aggregierung bis hin zur vollständigen Dispergierbarkeit. Im zweiten Teil der Arbeit wurden die Partikel im Hinblick auf ihre Eignung und Verwendung als Füllstoffe für Elastomer-Matrices untersucht. Im Fokus stand die Verstärkungswirkung und die Korrelation mit dem Dispergierverhalten in PDMS. Im dritten Teil der Arbeit wurde das Syntheseprinzip der Herstellung nanostrukturierter Mikropartikel auf Hydroxid-basierte Systeme wie LDHs erweitert. Teil I: Von Silica-NP zu nanostrukturierten Mikropartikeln mit einstellbarem Zerfallsverhalten Um nanostrukturierte Mikropartikel mit einem integrierten Zerfallsverhalten zu erzeugen, wurden zunächst kolloidale Silica-NP mit einer Größe von 20 nm abgestuft mit unterschiedlichen Mengen (0, 1/10, 1/5, 1/3, 1/2, 2/3, 1) eines hydrophobierend wirkenden Silans (Triethoxyoctylsilan, OCTEO) modifiziert. Neben den beiden Extremen der vollständigen und unmodifizierten Varianten (1 und 0) wurden teilweise modifizierte Zwischenstufen erhalten, indem die Silanmenge auf 2/3, 1/2, 1/3, 1/5 und 1/10 im Vergleich zu den vollmodifizierten Silica-NP verringert wurde. Die modifizierten Nanopartikel zeigten beim Dispergieren in verschiedenen Flüssigkeiten (Wasser, Toluol) eindeutige und graduell klar differenzierbare Unterschiede in Abhängigkeit vom Bedeckungsgrad der Partikeloberfläche mit dem Silan. Wie erwartet nahm das hydrophobe Verhalten der Nanopartikel mit zunehmendem Bedeckungs- und damit Modifizierungsgrad zu und die Nanopartikel waren in unpolaren Flüssigkeiten wie Toluol gut dispergierbar, während sie in polaren Flüssigkeiten wie Wasser zur Agglomeration und Sedimentation neigten. In einem nächsten Schritt wurden die zu unterschiedlichen Graden mit OCTEO modifizierten kolloidalen Silica-NP mittels Sprühtrocknung in mikroskalige Pulver überführt. Die nanostrukturierten Mikropartikelpulver wurden mit verschiedenen Analysemethoden wie REM-Aufnahmen, BET-, FTIR- und TG-Messungen untersucht, und die Eigenschaften der gebildeten Partikel charakterisiert. Die nanostrukturierten Mikropartikel zeigten auf den REM-Aufnahmen abhängig vom Modifizierungsgrad der Nanopartikel ein sehr unterschiedliches Aussehen. Während die Mikropartikel aus vollständig modifizierten Nanopartikeln eine eher raue Oberfläche besaßen, hatten die aus unmodifizierten Nanopartiklen gebildeten eine sehr glatte, kompakt erscheinende Oberfläche, was als Hinweis auf eine Kondensation und eine damit verbundene Aggregation der Nanopartikel gewertet wurde. Da sich diese Hypothese anhand der Aufnahmen aber nicht beweisen ließ, wurden in einer nächsten weiterführenden Testreihe Nano-Indenter-Experimente unter dem REM mit den aus voll- und unmodifizierten Nanopartikeln aufgebauten Mikropartikeln durchgeführt. Die Ergebnisse bestätigten den ersten Eindruck der REM-Aufnahmen insofern, als das sich die sehr kompakt wirkenden unmodifizierten Partikel nicht mit einer Wolfram-Spitze eindrücken ließen und damit die Hypothese mechanisch stabiler Aggregate untermauerten. Ganz anders verhielten sich die vollmodifizierten Partikel, die mithilfe der Wolfram-Spitze so eingedrückt werden konnten, dass die Nanopartikel aus dem Mikropartikelverbund herausgelöst wurden und teilweise vereinzelt vorlagen. Hier handelte es sich mit hoher Wahrscheinlichkeit um Agglomerate, die unter der Einwirkung einer Scherkraft wieder vereinzelt werden konnten. Da es mit mikroskopischen Verfahren wie REM nicht möglich war, unmittelbare Aussagen bezüglich der Wechselwirkung der Nanopartikel im Mikropartikel zu treffen, wurden zunächst die Oberflächeneigenschaften mittels BET-, FTIR- und TG-Messungen untersucht. Im Hinblick auf die spätere Anwendung war es sehr wichtig, die Oberflächeneigenschaften der Mikropartikel möglichst umfassend zu charakterisieren, da diese entscheidend zur Dispergierbarkeit der Partikel in einem Matrixsystem beitragen. Mithilfe der FTIR- und TG-Messungen konnte die Anwesenheit und Menge von Silan auf der Partikeloberfläche bestimmt werden. Es zeigte sich ein klarer Trend für die zu verschiedenen Graden mit OCTEO modifizierten Silica-NP. Mit zunehmender Silanmenge nahm sowohl die Intensität der FTIR-Bande für die CH2- und CH3-Streckschwingung als auch der Masseverlust zu. Im Gegensatz zu diesen Messungen zeigte sich bei den BET-Messungen kein klarer Trend in Abhängigkeit vom Bedeckungsgrad der Silica-NP. Die höchsten Werte für die spezifische Oberfläche hatten Mikropartikel, die aus 1/5- und 1/3-modifizierten Silica-NP bestanden. Eine schlüssige Erklärung wird darin gesehen, dass durch die Alkylgruppen auf der Oberfläche ein Kondensieren der Silica-NP weitestgehend verhindert wurde und gleichzeitig noch genügend Mikroporen vorhanden blieben, die mit den Stickstoffmolekülen wechselwirken konnten. Neben den Standard-Analysemethoden wurden Dispergierbarkeitsuntersuchungen durchgeführt sowie die Hansen-Dispergierbarkeitsparameter (HDP) und die ET (30)-Werte mit dem Reichardt-Farbstoff bestimmt. Anhand der Dispergierbarkeitsuntersuchungen konnten erste qualitative Aussagen getroffen werden, ob es sich um hydrophile oder hydrophobe Partikel handelt. Diese ersten Ergebnisse und Trends konnten anschließend mit den HDP und dem RD quantitativ untermauert werden. Die Polarität der Mikropartikel, die aus zu unterschiedlichen Graden mit OCTEO modifizierten Silica-NP aufgebaut waren, nahm mit zunehmender Oberflächenbedeckung ab. Dieser Trend korrelierte mit den aus den FTIR- und TG-Messungen erhaltenen Werten. Da es mit den Silica-basierten Mikropartikeln nicht möglich war, unmittelbare Aussagen zum Agglomerations- bzw. Aggregationsgrad der Nanopartikel im Mikropartikel zu treffen, wurde das Prinzip der Agglomerations/Aggregationssteuerung über Oberflächenmodifikation auf magnetische Nanopartikel übertragen und so ein Modell geschaffen, das die Wechselwirkung auf nanopartikulärer Ebene sichtbar und messbar macht. Diese Informationen zum Agglomerationsgrad der Nanopartikel lieferten wertvolle Hinweise im Hinblick auf die Dispergierbarkeit der Partikel in einer Matrix: Handelte es sich bei den Partikeln um lose Agglomerate, könnten diese zum Beispiel in einem Elastomer wieder auf Primärpartikelgröße dispergiert werden, während Aggregate nur in undefinierte Sekundärstrukturen zerfallen. Gleichzeitig wurde mit dieser Systemübertragung die Frage beantwortet, ob es sich bei den teilmodifizierten Partikeln um eine Mischung aus voll- und unmodifizierten Partikeln handelte oder ob das Silan statistisch über die komplette Oberfläche verteilt war. Wie auch schon beim Silica-System wurden die Nanopartikel zunächst abgestuft mit OCTEO modifiziert (0, 1/10, 1/3, 1/2, 2/3, 1) und anschließend sprühgetrocknet. Aufgrund ihrer magnetischen Eigenschaften konnten die Eisenoxid-Partikel mittels ZFC- und FC-Messungen untersucht werden. Diese spezielle Analysemethode erlaubte es, Aussagen über den Grad der magnetischen Wechselwirkung der Partikel zu treffen und somit indirekt auch über den Grad der Agglomeration/ Aggregation der Nanopartikel im Mikropartikel. Es zeigten sich klare Unterschiede in den Werten für die Blocking-Temperatur (TB) zwischen den voll- und unmodifizierten Partikeln. TB ist die Temperatur, ab welcher die Magnetisierungsrichtung der Partikel aufgrund der thermischen Energie frei fluktuieren kann. Die vollmodifizierten Partikeln hatten einen sehr niedrigen Wert für TB, was auf eine schwache Dipol-Dipol- Wechselwirkung zwischen den einzelnen Eisenoxid-NP schließen ließ, während die unmodifizierten Eisenoxid-Partikel einen hohen TB-Wert hatten, woraus zu schließen war, dass es sich um Aggregate mit einem sehr geringen Partikel-Partikel-Abstand handelte und einer deshalb höheren Wechselwirkung. Die Werte der teilmodifizierten Partikel folgten dem Trend, dass mit zunehmender Silan-Bedeckung der TB-Wert abnahm. Um die Frage der Silan-Verteilung zu beantworten, wurde zusätzlich ein Mischsystem aus voll- und unmodifizierten Eisenoxid-NP versprüht. Sollte es sich bei den teilmodifizierten Partikeln (als Beispiel 1/2) nicht um eine statistische Verteilung der Octylgruppen auf der Oberfläche handeln, müssten die beiden Messungen Übereinstimmungen aufweisen. Dies war allerdings nicht der Fall, was mithilfe der ZFC- und FC-Messungen gezeigt werden konnte. Der TB-Wert des Mischsystems lag zwischen dem der voll- und zu 2/3-modifizierten Partikel, während der Tir-Wert dem der unmodifizierten Partikel entsprach. Die Breite der Aufspaltung zwischen TB undTir konnte als breite Partikelverteilung (Mischung aus Agglomeraten und Aggregaten) interpretiert werden. Im Hinblick auf die Anwendung als Füllstoff wurden die Mikropartikel in eine PDMS-Matrix eingearbeitet und erneut ZFC- und FC-Messungen durchgeführt, wobei die gleichen Trends wie bei den reinen nanostrukturierten Mikropartikeln erhalten wurden. Das bedeutete, dass sich die vollmodifizierten Eisenoxid-NP gut im Elastomer verteilt hatten und somit eine nur sehr geringe Dipol-Dipol-Wechselwirkung vorhanden war. Mit dem entwickelten System der nanostrukturierten Mikropartikel lässt sich der Agglomerations- bzw. Aggregationsgrad der Nanopartikel mehr oder weniger gezielt einstellen, und es können zusätzlich Voraussagen über die Redispergierbarkeit des Partikelpulvers in einer geeigneten Matrix gemacht werden. Basierend auf den gewonnen Erkenntnissen, die zum Verständnis der nanostrukturierten Mikropartikel beitrugen, wurden in einem nächsten Schritt gezielt komplexe Strukturen aufgebaut. Für eine gezielte Strukturierung von Nanopartikeln in Kern-Satellit-Partikel wurde zunächst große 100 nm Silica-NP mit einem PCE funktionalisiert und anschließend mit kleinen und großen unmodifizierten Silica-NP versprüht. Wurden die geeigneten Verhältnisse (70:20:10; 100 nm Mel : 100 nm blank : 20 nm blank) der Partikel zueinander gewählt, konnten Kern-Satellit-Strukturen auf der Mikropartikeloberfläche erzeugt werden. Beim Dispergieren der Mikropartikel in einer Flüssigkeit und in einem Elastomer (PDMS) konnten vereinzelte Kern-Satellit-Strukturen erhalten werden. Um zu bestätigen, dass es sich bei den dispergierten Kern-Satellit-Partikeln nicht um durch Trocknungseffekte entstandene Strukturen handelte, wurden in-situ-Flüssigkeitszellen- TEM-Aufnahmen gemacht. Die Aufnahmen konnten zeigen, dass sich die Kern-Satellit- Partikel in Abhängigkeit zueinander bewegen und nicht jeder Nanopartikel für sich, was auf eine Bindung der Partikel untereinander hindeutete. Neben den Silica-basierten Kern-Satellit-Partikeln konnten auch welche erzeugt werden, deren Satellit-Partikel aus Eisenoxid bestanden. Mit diesem System ist es möglich, multifunktionelle Partikel mit verschiedensten Eigenschaften und Strukturen herzustellen. Teil II: Anwendungspotential nanostrukturierter Mikropartikel Im zweiten Teil der Arbeit wurde zunächst die Anwendung der nanostrukturierten Mikropartikel als Füllstoff in IR und PDMS untersucht. Dafür wurde ein weiteres Silan, Si69TM, zur abgestuften Modifizierung der Silica-NP eingesetzt. Es handelt sich um ein multifunktionelles Silan, welches sowohl an die Partikeloberfläche als auch an das Elastomer binden kann. Bei den mechanischen Untersuchungen der IR-Silica-Komposite zeigte sich, dass das Silan einen entscheidenden Einfluss auf die Verstärkung bei kleinen Deformationen hatte. Während bei dem monofunktionellen Silan (OCTEO) eine direkte Korrelation zwischen Bedeckungsgrad und mechanischer Verstärkung (G‘) bei gleichbleibendem Füllstoffgehalt beobachtet werden konnte, hatte der Bedeckungsgrad beim multifunktionellen Silan (Si69TM) keinen Einfluss. Anders als bei kleinen Deformationen zeigte sich bei großen Deformationen ein gegenteiliges Bild. Die Verschleißrate der IR-Silica-Komposite nahm bei beiden Silantypen mit zunehmendem Modifizierungsgrad ab, wobei die mit Si69TM modifizierten Partikel-Komposite wesentlich beständiger gegen Verschleiß waren als die mit OCTEO modifizierten Partikel-Komposite, was auf die zusätzliche Matrixanbindung des Si69TM zurückzuführen war. Wurden die IR-Silica- Komposite mit den PDMS-Silica-Kompositen verglichen, konnten keine übereinstimmenden Trends gefunden werden. Im PDMS-System war die mechanische Verstärkung für Mikropartikel aus 2/3 mit OCTEO modifizierten Silica-NP maximal. Diese Unterschiede könnten sowohl auf die unterschiedliche Einarbeitung als auch auf die sehr unterschiedlichen Matrices zurückgeführt werden. Als weitere Anwendung wurden die nanostrukturierten Mikropartikel als Schersensoren für den 3D-Druck untersucht. Hierfür wurden die Silica-NP mit einem PCE modifiziert und anschließend sprühgetrocknet. Um die entstandenen Mikropartikel vollständig in einer Matrix zu dispergieren, waren hohe Scherkräfte und lange Scherzeiten erforderlich, was eine mögliche Anwendung als Schersensor nur schwer realisierbar macht. Teil III: Erweiterung des Ansatzes zur Herstellung nanostrukturierter Mikropartikel auf Hydroxid-basierte Systeme Im dritten Teil dieser Arbeit wurde das System zur Modifizierung von oxidischen Silicaund Eisenoxid-Partikeln auf ein hydroxidisches Systeme übertragen. Hierfür wurden mittels Fällungsprozess LDH-Partikel hergestellt, die anschließend mit OCTEO modifiziert und abschließend sprühgetrocknet wurden. In gleicher Weise wie bei den Mikropartikeln aus Silica-NP nahm der hydrophobe Charakter der LDH-Mikropartikel mit zunehmendem Modifizierungsgrad der Ausgangspartikel zu, was sich anhand von Untersuchungen zur Dispergierbarkeit in Flüssigkeiten unterschiedlicher Polarität zeigte. Zudem ließen sich die aus vollmodifizierten LDHs aufgebauten Mikropartikel in einer PDMS-Matrix wieder in vereinzelte Partikel dispergieren. Die Verstärkung der Komposite war für die teilmodifizierten Partikel (2/3) maximal, da es sich hier, wie auch bei den anderen Partikelsystemen (Silica und Eisenoxid), um eine Mischung aus vereinzelten LDHs und kleineren Aggregate handelte, was aufgrund der starken Füllstoff-Füllstoff-Wechselwirkung zu einer mechanischen Verstärkung bei kleinen Deformationen/Dehnungen führte. Die Eigenschaften der Polymer-Partikel-Komposite ließen sich über den Modifizierungsgrad der Primärpartikel einstellen. Dies konnte für alle drei Partikelsysteme (Silica, Eisenoxid und LDH) beobachtet werden. Ausblick In der vorliegenden Arbeit konnte die Synthese von verschiedenen nanostrukturierten Mikropartikeln und deren einstellbaren Zerfall gezeigt werden. Um den Zerfall der Mikropartikel noch gezielter einstellen zu können, sollte in weiterführenden Arbeiten vor allem die Modifizierung der Nanopartikel noch eingehender untersucht werden. Mithilfe der magnetischen Messungen konnte zwar zwischen einer Mischung aus un- und vollmodifizierten Partikel im Vergleich zu teilmodifizierten Partikel unterschieden werden, es konnten jedoch keine konkreten Aussagen zur Verteilung der Silanmoleküle auf der Partikeloberfläche getroffen werden. Hierfür sollten weitere Charakterisierungsmethoden hinzugezogen werden, die die Modifizierung auf molekularer Ebene analysieren. Zusätzlich sollte die Verteilung/Anordnung der teilmodifizierten Nanopartikel im Mikropartikel untersucht werden. Gerade für Nanopartikel mit einem geringen Modifizierungsgrad (1/10, 1/5 und 1/3) sind verschiedene Anordnungen möglich. Die Nanopartikel können sich während der Sprühtrocknung so anordnen, dass sich die Alkylketten entweder nach außen oder in die Mitte des Mikropartikels orientieren/ausrichten. Die Anordnung der Nanopartikel hat einen großen Einfluss auf die Polarität der entstehenden Mikropartikel- pulver. Darüber hinaus hat sie einen Einfluss auf die Aggregation der Nanopartikel untereinander und somit auf die Bildung von komplexen Unterstrukturen wie zum Beispiel Kern-Satellit-Partikel. Neben der Modifizierung der Nanopartikel sollte die Herstellung der komplexen Strukturen/Suprapartikel weiter optimiert werden. Mit einem detaillierten Verständnis der physikalischen Prozesse während der Sprühtrocknung könnte die Anzahl der Satelliten auf den Kernpartikel kontrollierter eingestellt werden. Grundsätzlich kann das hier entwickelte System der nanostrukturierten Mikropartikel mit einstellbarem Zerfallsverhalten an eine Vielzahl von Anwendungen angepasst werden. Da das System für zahlreiche Partikeltypen (Silica-, Eisenoxid-NP und LDH) geeignet ist, könnten verschiedene Partikel ko-versprüht und so Suprapartikel mit ganz neuen Funktionalitäten und Eigenschaften erzeugt werden. Diese können als verstärkende Füllstoffe in Elastomere oder zur Stabilisierung von Dispersionen eingesetzt werden. Mischpartikel aus Silica- und Eisenoxid-Partikel hätten zum Beispiel den Vorteil, dass sie eine Dispersion stabilisieren und gleichzeitig wieder magnetisch abgetrennt werden können. Diese Mischpartikel könnten auch als Füllstoffe in komplexe Kunststoffbauteile eingearbeitet werden, in denen sie zum einen als mechanisch verstärkender Füllstoff wirken und gleichzeitig durch induktive Erwärmung das Bauteil vernetzt. Beim induktiven Erwärmen handelt es sich um eine schonende Methode Bauteile gezielt zu vernetzen, indem die Wärme im Bauteil selbst, über magnetische Verluste der Magnetpartikel in einem magnetischen Wechselfeld, erzeugt wird und nicht über seine Oberfläche eingebracht werden muss. Eine weitere interessante Anwendung für Mischpartikel ist die als magnetooptisch aktiver Marker oder Tracer in der medizinischen Diagnostik. Aufgrund von Quenching-Effekten (Auslöschungseffekte) ist es schwierig magnetische Nanopartikel mit einer Farbigkeit oder Fluoreszenz auszustatten.[385] Mischt man jedoch die magnetischen Nanopartikel mit einem weiteren Partikelsystem wie zum Beispiel Silica-NP oder LDHs, können magnetooptische Eigenschaften erhalten werden
In order to shrink the size of semiconductor devices and improve their
efficiency at the same time, silicon-based semiconductor devices have
been engineered, until the material almost reaches its performance
limits. As the candidate to be used next in semiconducting devices,
single-wall carbon nanotubes show a great potential due to their
promise of increased device efficiency and their high charge carrier
mobilities in the nanometer size active areas. However, there are
material based problems to overcome in order to imply SWNTs in the
semiconductor devices. SWNTs tend to aggregate in bundles and it is
not trivial to obtain an electronically or chirally homogeneous SWNT
dispersion and when it is done, a homogeneous thin film needs to be
produced with a technique that is practical, easy and scalable. This
work was aimed to solve both of these problems.
In the first part of this study, six different polymers, containing
fluorene or carbazole as the rigid part and bipyridine, bithiophene or
biphenyl as the accompanying copolymer unit, were used to selectively
disperse semiconducting SWNTs. With the data obtained from
absorption and photoluminescence spectroscopy of the corresponding
dispersions, it was found out that the rigid part of the copolymer plays a
primary role in determining its dispersion efficiency and electronic
sorting ability. Within the two tested units, carbazole has a higher π
electron density. Due to increased π−π interactions, carbazole
containing copolymers have higher dispersion efficiency. However, the
electronic sorting ability of fluorene containing polymers is superior.
Chiral selection of the polymers in the dispersion is not directly
foreseeable from the selection of backbone units. At the end, obtaining a monochiral dispersion is found to be highly dependent on the used raw
material in combination to the preferred polymer.
Next, one of the best performing polymers due to high chirality
enrichment and electronic sorting ability was chosen in order to
disperse SWNTs. Thin films of varying thickness between 18 ± 5 to
755o±o5 nm were prepared using vacuum filtration wet transfer method
in order to analyze them optically and electronically.
The scalability and efficiency of the integrated thin film production
method were shown using optical, topographical and electronic
measurements. The relative photoluminescence quantum yield of the
radiative decay from the SWNT thin films was found to be constant for
the thickness scale. Constant roughness on the film surface and linearly
increasing concentration of SWNTs were also supporting the scalability
of this thin film production method. Electronic measurements on bottom
gate top contact transistors have shown an increasing charge carrier
mobility for linear and saturation regimes. This was caused by the
missing normalization of the mobility for the thickness of the active
layer. This emphasizes the importance of considering this dimension for
comparison of different field effect transistor mobilities.
Dielektrische Elastomersensoren sind aus Elastomermaterialien aufgebaute Sensoren mit einem kapazitiven Messprinzip. In ihrer einfachsten Form bestehen sie aus einer dehnbaren Elastomerfolie als Dielektrikum, die beidseitig mit leitfähigen und ebenfalls dehnbaren Schichten als Elektroden bedeckt ist.
Damit entsteht ein mechanisch verformbarer elektrischer Kondensator, dessen Kapazität mit der Dehnung der Elastomerfolie stetig ansteigt. Neben solchen Dehnungssensoren lassen sich mit einem geeigneten geometrischen Aufbau auch dielektrische Elastomersensoren realisieren, bei denen eine elektrische Kapazität mit einem angelegten Druck bzw. einer Kraft auf die Oberfläche, mit einer Scherkraft oder mit der Annäherung eines elektrisch leitfähigen oder polarisierbaren Körpers wie z. B. der menschlichen Hand messbar ansteigt.
Durch ihre vielfältige Funktion, intrinsische Verformbarkeit und flächige Ausgestaltung weisen Dielektrische Elastomersensoren erhebliches Potential in der Schaffung smarter, sensitiver Oberflächen auf. Dabei sind weitgehende und individuelle Adaptionen auf den jeweiligen Anwendungszweck durch Abstimmung geometrischer, mechanischer und elektrischer Eigenschaften möglich. Die bisherige Forschung beschränkt sich jedoch auf die Analyse und Optimierung einzelner Aspekte ohne das Potential einer übergreifenden systemischen Perspektive zu nutzen.
Diese Arbeit widmet sich daher der Betrachtung der Sensorik als Gesamtsystem, sowohl horizontal - von abstrakten Modellen bis zur Fertigung und prototypischen Anwendung - als auch vertikal über die Komponenten Material, Struktur und Elektronik.
Hierbei wurden in mehreren Teilgebieten eigenständige neue Erkenntnisse und Verbesserungen erzielt, die anschließend in die übergreifende Betrachtung des Gesamtsystems integriert wurden. So wurden in den theoretischen Vorarbeiten neue Konzepte zur ortsaufgelösten Erfassung mehrerer physikalischer Größen und zur elektrischen und mechanischen Modellierung entwickelt. Die abgeleiteten Materialanforderungen wurden in eine tiefgehende Charakterisierung der verwendeten Elastomer-Kompositwerkstoffe überführt, in der neuartige analytische Methoden in Form von dynamischer elektromechanischer Testung und nanoskaliger Computertomographie zur Aufklärung der inneren Wechselwirkungen zum Einsatz kamen.
Im Bereich der automatisierten Prozessierung wurde ein für die komplexen mehrschichtigen Elektrodenstrukturen geeigneter neuer lasergestützer substraktiver Fertigungprozess etabliert, der zudem die Brücke zu elastischer Elektronik schlägt.
In der abschließenden Anwendungsevaluierung wurden mehrere ortsaufgelöste und multimodale Gesamtsysteme aufgebaut und geeignete Messelektronik und Software entwickelt. Abschließend wurden die Systeme mit einem eigens entwickelten robotischen Testsystem charakterisiert und zudem das Potential der Auswertung mittels maschinellem Lernen aufgezeigt.
After examining suitable parameters for a newly designed system, dynamic SIPGP could be developed. For the first time, SIPGP was performed while applying a constant flow of monomer solution through the reaction system. This added a new parameter: the flow rate (rfl). Accordingly, this parameter was examined, comparing dynamic to static SIPGP. It could be shown, that by applying higher rfl to the system, the contact angle increases, which indicates a slower coating. The flow patterns inside the reactor were then modelled and calculated. These calculations indicated, that, due to higher flow velocities, the contact angle on the coated samples would be lower on the sides of the sample and higher in the middle. This finding was verified by contact angle measurements. The influence of dynamic SIPGP on the temperature inside the reaction chamber during the reaction was examined by temperature sensors inside the reactor. This showed, that the constant flow of monomer solution can be utilized to decrease the warming of the reaction solution during the reaction. Finally it was shown, that dynamic SIPGP can decrease the formation of bulk polymer on the sample, which is forming during the reaction. This enables SIPGP to fabricate more homogeneous coatings by applying a constant monomer flow.
Structure-property relationships in poly(2-oxazoline)/poly(2-oxazine) based drug formulations
(2020)
According to estimates, more than 40% of all new chemical entities developed in pharmaceutical industry are practically insoluble in water. Naturally, the demand for excipients which increase the water solubility and thus, the bioavailability of such hydrophobic drugs is enormous. Poly(2-oxazoline)s (POx) are currently intensively discussed as highly versatile class of biomaterials. Although selected POx based micellar drug formulations exhibit extraordinarily high drug loadings > 50 wt.% enabling high anti-tumor efficacies in vivo, the formulation of other hydrophobic compounds has failed. This casts doubt on the general understanding in which a hydrophobic active pharmaceutical ingredient is dissolved rather unspecifically in the hydrophobic core of the micelles following the fundamental concept of “like dissolves like”. Therefore, a closer look at the interactions between all components within a formulation becomes increasingly important. To do so, a large vehicle platform was synthesized, loaded with various hydrophobic drugs of different structure, and the formulations subsequently characterized with conventional and less conventional techniques. The obtained in-depth insights helped to develop a more thorough understanding about the interaction of polymer and incorporated API finally revealing morphologies deviating from a classical core/shell structure. During these studies, the scarcely investigated polymer class of poly(2-oxazine)s (POzi) was found as promising drug-delivery vehicle for hydrophobic drugs. Apart from this fundamental research, the anti-tumor efficacy of the two APIs curcumin and atorvastatin has been studied in more detail. To increase the scope of POx and POzi based formulations designed for intravenous administration, a curcumin loaded hydrogel was developed as injectable drug-depot.