In the early 2000s, hydrogen sulfide (H₂S) was added to the family of molecules known as gasotransmitters, a class of endogenously produced and freely diffusing biological signaling molecules. Since this discovery, biologists and chemists have sought to understand the physiological roles of H₂S and to elucidate the potential benefits of exogenous H₂S delivery. As a result, many synthetic small molecule donor compounds have been created to deliver H₂S in response to various biologically relevant stimuli. Furthermore, macromolecular and supramolecular H₂S donor systems have been created to protect donors in the biological milieu, extend release kinetics, or control H₂S release conditions. Thus, H₂S-donating nanostructures with precisely tuned release rates provide invaluable tools for further investigating the biological roles and therapeutic potential of H₂S.
This work describes two polymer micelle systems for the controlled delivery of H₂S. The first system is based on H2S-releasing polymer amphiphiles with varying degrees of a plasticizing comonomer incorporated into the core-forming block. The glass transition temperature of the core-forming block varied predictably with incorporation of the plasticizing comonomer. Accordingly, the half-life of H₂S release decreased from 4.2 h to 0.18 h with increasing core-forming block mobility. The second system is based on H₂S releasing polymer amphiphiles with varying degrees of crosslinking in the core-forming block. The crosslinked system was designed to achieve control over H₂S release rate with minimal dilution of donor in the core-forming block. The half-life of H₂S release increased from 117 min to 210 min with increasing crosslink density in the core-forming block, further demonstrating that H₂S release rates can be precisely controlled by tuning micelle core mobility.
Beyond control over H₂S release rate, further study of the biological roles of H₂S requires donor systems with precisely triggered release. To this end, this dissertation also discusses efforts to investigate fundamental micelle–unimer relationships. This section includes an evaluation of the impact of core-forming block mobility on micelle–unimer coexistence utilizing a model polymer amphiphile system. Unimer populations correlated with glass transition temperatures of the core-forming block, suggesting the need to consider micelle core mobility when discussing polymer chain phase behavior of amphiphilic block copolymers. Finally, this work discloses new methods for the radical polymerization of poly(olefin sulfones) with control over molecular weight. POSs are a unique class of polymers with great potential for stimuli-responsive depolymerization to generate sulfur dioxide (SO₂), a signaling gas related to H₂S. / Doctor of Philosophy / Hydrogen sulfide (H2S) is commonly known for its pungent odor and toxicity. Despite this negative stigma, H2S has been revealed as a vital signaling molecule in both plants and animals. This discovery has prompted the coordination of biologists and chemists in an effort to better understand the roles of H2S in the body. Driven by this motive, great interest has centered around the development of finely tuned molecules designed to generate H2S in the body, termed H2S donors. A variety of synthetic H2S donors have been reported with various conditions enabling release. Building on this work, the development of polymeric H2S donors with tunable release rates will enable investigation into the complex behavior of H2S in the body.
The first half of this dissertation focuses on the design and synthesis of two polymeric H2S donor systems for the controlled release of H2S. These systems take advantage of sequestering the H2S donating species inside a polymeric nanostructure in water called a micelle. Because H2S release requires a triggering molecule to enter the polymeric nanostructure, release rate can be tuned by modifying the mobility of the structure. The first system discussed demonstrates this concept by increasing the flexibility of the micelle core. As expected, H2S release rates increased with increasing flexibility. The second system discussed advances this idea by limiting mobility within the micelle core, rather than increasing flexibility. Accordingly, H2S release rates decreased with decreasing mobility within the micelle core.
The latter half of this dissertation broadly explores the development of polymeric signaling gas delivery vehicles with triggered release conditions. We first investigate the impact of polymer chain flexibility on the formation of micelles in water. Polymer chain flexibility significantly impacted the balance between micelles and unassembled polymer chains in solution, suggesting the need to consider this characteristic when designing donor systems for precise release conditions. Lastly, we discuss the development of controlled polymerization techniques for poly(olefin sulfones). We envision that poly(olefin sulfones) will be a useful class of polymers in the design of donor systems relying on triggered depolymerization for release of the signaling gas sulfur dioxide.
Identifer | oai:union.ndltd.org:VTETD/oai:vtechworks.lib.vt.edu:10919/108233 |
Date | 08 February 2022 |
Creators | Carrazzone, Ryan Joseph |
Contributors | Chemistry, Matson, John B., Davis, Richey M., Schulz, Michael, Madsen, Louis A., Tong, Rong |
Publisher | Virginia Tech |
Source Sets | Virginia Tech Theses and Dissertation |
Language | English |
Detected Language | English |
Type | Dissertation |
Format | ETD, application/pdf |
Rights | In Copyright, http://rightsstatements.org/vocab/InC/1.0/ |
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