Design of oxidation-sensitive polymer micelles for inflammation targeting

Hu, Ping

January 2012

The research presented in this thesis focuses on the molecular design of an oxidation-sensitive nanocarrier and its enzyme conjugate with a view of their application in the field of biomaterials. I have polarised our attention on a specific class of polymers, the polysulfides, for their environmental responsiveness (towards oxidising substances, a condition often associated with inflammatory reactions), interesting physico-chemical properties, ease of the preparation and multiple possibilities for further modifications and bioconjugations, which are perfectly suitable for the development as systems for drug delivery applications. In this work we firstly have focused on the synthesis of amphiphilic poly(propylene sulfide)-poly(ethylene glycol) (PPS-PEG) block copolymers by employing vinyl sulfone as the functional group to link the blocks and modify the end of the PEG. This study was followed by an investigation of the macromolecular interchange and payload exchange of the formed polymeric micelles to understand the 'co-formulation' events, employing fluorophores (dansyl groups) and quenchers (dabsyl groups) either as terminal groups in macroamphiphiles or as encapsulated hydrophobic payloads. In another part of the work, I have developed a micellar system with which simultaneously to two of the most important ROS: superoxide and hydrogen peroxide, for inflammation-responsive drug release. The system is composed of superoxide dismutase (SOD) conjugated to oxidation-sensitive amphiphilic polysulfide/PEG block copolymers; the conjugate combines the SOD reactivity towards superoxide with that of hydrophobic thioethers towards hydrogen peroxide. Specifically, here we have demonstrated how this hybrid system can efficiently convert superoxide into hydrogen peroxide, which is then 'mopped-up' by the polysulfides. This mode of operation is functionally analogous to the SOD/catalase combination, with the advantage of being based on a single and more stable system.

617.22

Block Copolymer Solutions: Transport and Dynamics, Targeted Cargo Delivery, and Molecular Partitioning and Exchange

Li, Xiuli

23 January 2020

Block copolymers have been extensively applied in diverse fields including packaging, electrolytes, delivery devices, and biosensors. Multiple investigations have been carried out on polymeric materials for cargo delivery purpose to understand how they behave over time. Block copolymer micelles (BCMs) have demonstrated superiority to deliver cargo, especially in drug delivery due to their encapsulation of hydrophobic agents. This dissertation will mainly study BCMs for potential applications in cargo delivery. Methods to study BCMs, including NMR spectroscopy, relaxometry and diffusometry, can provide valuable molecular information, such as chemical structure, translational motion, inter- or intramolecular interaction, dynamics, and exchange kinetics. Therefore, this dissertation describes applications of versatile NMR methods to reveal the fundamental behaviors of block copolymer self-assemblies, such as their dynamic stability, cargo partitioning, polymer chain exchange, and chain distribution in solution. We have investigated two BCM systems. Poly(ethylene oxide)-b-(ε-caprolactone) (PEO-PCL) is a model system to study BCM dynamic stability. PEO-PCL can self-assemble into spherical micelles at 1% w/v in D2O-THF-d8 mixed solvents. We used NMR diffusometry to quantify diffusion coefficients and populations of micelles and unimers (i.e. free polymer chains in solution) over a range of temperature (21 – 50 °C) and solvent composition (10 – 100 vol % THF-d8). By mapping the micelle-unimer coexistence phase diagrams, we are able to enhance our ability to understand and design micelle structure and dynamics. Moreover, we can also probe the chain exchange kinetics between micelles using a new technique we developed – time-resolved NMR spin-lattice relaxation (T1) or TR-NMR. This technique is an analog to time-resolved small-angle neutron scattering (TR-SANS), which can monitor specific signal intensity changes caused after mixing of isotope-labeled micelle solutions. A second system, Pluronic® F127 (PEO99PPO69PEO99) is a test system to study BCM structure and dynamic changes upon drug uptake. Pluronic® F127 is a commercial copolymer that can solubilize different hydrophobic drugs in micelles. We successfully encapsulated three model drugs into Pluronic® F127 BCMs and investigated the effects of polymer concentration and drug composition on drug partitioning fractions. Also, we proposed to design and synthesize a series of block copolymers with varied glass transition temperatures in core-forming blocks. Using NMR diffusometry, we have measured the existing unimer concentrations in micellar solutions and correlated these results with chain mobility and internal chemical composition. Lastly, we have extended our expertise in NMR and polymers into the study of ion-containing polymer systems (polyelectrolytes). A critical problem in polymer science is the inability to reliably measure the molecular weight of polyelectrolytes. We are developing methods to solve this problem by using NMR diffusometry, rheology, scattering, and scaling theories to accomplish general molecular weight measurements for polyelectrolytes. In short, this dissertation describes studies to provide more perspectives on structural and dynamic properties at various time and length scales for polymeric materials. NMR measurements, in combination with many other advanced techniques, have given us a better picture of soft matter behaviors and provided guidance for synthesis and processing efforts, especially in block copolymer micelles for delivery purposes. / Doctor of Philosophy / Block copolymers have been extensively applied in diverse fields in packaging, electrolytes and nano-scale drug delivery carriers. In the area of cancer treatment, only a limited number of drug nanocarriers have been approved for clinical applications. Therefore, it is very important to understand the principles behind drug delivery for targeted purposes. There have been many studies on polymeric delivery carriers but their behaviors have not been completely understood. Therefore, we have tremendous interest in unraveling the mysteries in those polymeric systems. Among a multitude of techniques to study block copolymer materials, the NMR method serves as a potent tool for its non-destructive, chemical-specific and isotope-selective merits. NMR can provide basic information about block copolymer self-assembly and other polymeric properties, such as chemical structure, molecular interactions and diffusion coefficients of species of interests. Chapters 3, 4, 5, 6, and 7 have investigated different classes of polymeric materials, mainly block copolymer micelles, for their structure and stability, exchange kinetics of polymer chains or cargo, and translational properties. Greater understanding about the fundamental properties of these polymeric systems, is essential for enabling new applications and new research areas.

Block Copolymer Micelles (BCMs)

Free Unimer Chains

Exchange Kinetics

NMR Diffusometry

Molecular Structure and Interaction

Drug Loading

DYNAMICS OF POLYMER SELF-ASSEMBLY BY COMPUTER SIMULATION

LI, ZHENLONG

21 March 2011

No description available.

Polymers

self-assembly dynamics

block copolymer micelles

supramolecular polymer

computer simulation

DPD simulation

Molecular Dynamics simulation

micelle dynamics

viscosity

Probing diffusion and molecular dynamics to study self-assembly and intermolecular interactions in macromolecular and colloidal systems using NMR diffusometry and spectroscopy

Uppala, Veera Venkata Shravan

13 January 2025

The growing demand for technological advancements in energy storage and pharmaceuticals, driven by population growth and climate change, has created an urgent need for the development of novel materials with finely tuned and targeted properties. Polymers, with their inherent versatility, have emerged as key players in modulating the functionality of such advanced materials. However, achieving precise control over the performance of the materials requires a deep understanding of the molecular interactions, self-assembly processes, and transport phenomena that govern their behavior at the nanoscale. This dissertation focuses on the application of advanced nuclear magnetic resonance (NMR) techniques to probe the molecular dynamics and diffusion behavior in complex macromolecular and colloidal systems. Two key NMR techniques – NMR diffusometry and dynamic NMR spectroscopy – are employed to probe the motion and exchange process of molecules within these systems. By providing insights into the dynamics of the constituents, these methods are particularly powerful in unraveling the intermolecular interactions that govern material functionality. The materials under investigation include block copolymer micelles (BCMs), ligand-capped quantum dots (QDs), and linear polyelectrolyte chains – each with unique structural characteristics and promising applications. Block copolymer micelles are of particular interest for drug delivery applications due to their ability to encapsulate and release therapeutic agents in controlled manner. Colloidal quantum dots, with their size-tunable electronic properties, have great potential in photovoltaics and biosensing. Linear polyelectrolytes, characterized by their charged backbones, are crucial for energy storage and biomedical applications. Through a detailed analysis of the translational motion of molecules, this work reveals key molecular insights, including intermolecular interactions, the coexistence of molecules in distinct chemical environments, and their exchange mechanism between these environments. These findings establish critical structure-property relationships in each material system, providing a foundation for rational design and optimization of their functional performance. The results obtained in this research not only contribute to our fundamental understanding of the molecular behavior of these complex systems but also have practical implications for design of next-generation materials. By leveraging the power of NMR-based techniques, this dissertation offers a pathway for enhancing material properties in the desired applications. The findings emphasize the critical role of molecular characterization techniques in advancing the field of material science and facilitating the development of more efficient, high-performance materials tailored to meet the demands for modern technology. / Doctor of Philosophy / Rising global challenges, such as energy storage and healthcare, demand innovations for new technologies. At the core of many of these innovations are advanced materials, which must be meticulously designed to meet specific performance requirements. Polymers, in particular, play a key role in these developments due to their versatile properties. To create materials with precise functionality, a deeper understanding of the chemistry and molecular interactions that govern their behavior is essential. This dissertation focuses on using nuclear magnetic resonance (NMR), a powerful analytical tool, to probe molecular motions and interactions in advanced materials. Specifically, this research has developed NMR methodologies to investigate polymer-based micelles (surfactants) for drug-delivery applications, semiconductor nanoparticles for solar cells and sensor applications, and molecular weight determination of charged polymer chains. The research aims to reveal new insights into the behavior of these materials and how such knowledge can be harnessed to design more effective systems for applications in medicine and energy. By studying molecular motions and interactions, this work aspires to contribute to the development of next-generation materials capable of addressing some of the world's most pressing challenges.

Energy storage

pharmaceuticals

polymers

self-assembly

transport

NMR diffusometry

NMR spectroscopy

block copolymer micelles

quantum dots

polyelectrolytes

structure-property relationships

Srovnání polymerních nanoléčiv odpovídajících a neodpovídajících na vnější podněty pro biomedicinální aplikace / Responsive and non-responsive soft matter nanomedicines for biomedical applications

Jäger, Eliézer

January 2015

The thesis outlines possible medical applications of soft matter assemblies as nanotechnology based systems as well as their potential in the emerging field of nanomedicine. Nanomedicine can be defined as the investigation area encompassing the design of diagnostics and therapeutics at the nanoscale, including nanobots, nanobiosensors, nanoparticles and other nanodevices, for the remediation, prevention and diagnosis of a variety of illnesses. The ultimate goal of nanomedicine is to improve patient quality-of-life. Because nanomedicine includes the rational design of an enormous number of nanotechnology-based products focused on miscellaneous diseases, a variety of nanomaterials can be employed. Therefore, the thesis is driven by a focus on recent advances in the manufacture of soft matter-based nanomedicines specifically designed to improve cancer diagnostics and chemotherapy efficacy. It will in particular highlight liposomes, polymer-drug conjugates, drug- loaded block copolymer micelles and biodegradable polymeric nanoparticles, emphasizing the current investigations and potential novel approaches towards overcoming the remaining challenges in the field as well as a brief overview of formulations that are in clinical trials and marketed products. Based on vehicle-related and...