Developing Pd(II) based amphiphilic polymeric nanoparticles for pro-drug activation in complex media

Transition-metal-mediated bio-orthogonal reactions for synthesizing drugs in situ that target tumor cells can help to develop side-effect-free cancer therapies. THERACAT Project is designing a catalytic nanoparticles-based system to activate several prodrugs for application in cancer treatments.
Published in Chemistry
Developing Pd(II) based amphiphilic polymeric nanoparticles for pro-drug activation in complex media
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The challenge

Approaches to targeted cancer therapies that combine improved efficacy of current chemotherapies while minimizing side effects for patients are highly sought after. A team of researchers within the European Marie Skłodowska-Curie European Training Network THERACAT1 proposed solutions to this problem by developing new strategies to specifically deliver drugs only to the tumor site. The idea was that bio-orthogonal transition metal based catalysts (TMCs) could activate prodrugs — drugs made inactive by a chemical protecting group— at the site of interest because of a highly selective activation reaction that does not occur in living cells. At the UCRA-2022 conference in Leamington Spa 21-23/9/2022 dedicated to catalysis in unconventional environments, exciting state-of-the-art contributions on this challenging topic were disseminated by i.a. Jesús Santamaria, Peter Sadler and Ana Pérez-López, who have been using transition metal complexes (TMCs) to either directly attack tumor cells2 or to induce a bio-orthogonal reaction that activates a drug from an inactive prodrug in situ.3  The latter approach has attracted a lot of attention the past decade4 and Unciti-Broceta and coworkers elegantly showed that by using Pd(0)-based polystyrene microspheres such prodrug activation works in in vivo systems such as zebra fish embryos and rats.5,6 These microspheres are implanted via syringe techniques at the tumor location where they should be active. But, how can one get TMC-based catalysts at inaccessible tumor locations or when one does not exactly know where the tumor cells are?

Our approach

To address the challenge to guide TMC-based catalysts to the target location, high catalyst stability and activity is required, as well as good biocompatibility and the ability to attach recognition units for targeted delivery of the catalyst. Hereto, we applied single-chain polymeric nanoparticles (SCPNs) as carrier materials for the TMCs. SCPNs are amphiphilic polymers that fold in water into compartmentalized, nanometer-sized structures with size varying between 5-20 nm, which have a hydrophilic, biocompatible exterior and a hydrophobic interior.7,8 In many ways, the folding of the amphiphilic polymer into an SCPN is reminiscent of protein folding into functional 3D structures.9 By embedding the TMC of choice into the SCPN’s hydrophobic interior, we anticipated that we could prevent the TMC from undesired interactions with constituents in complex media that deactivate the catalyst, but also to sequester substrates around catalytic sites to enhance catalytic rates. The poster we presented at UCRA-2022 showed that the combination of molecular design of the polymer’s microstructure, optimization of ligand-Pd(II) combination, and engineering of the hydrophobicity of the substrate via logP all matter to obtain SCPNs that convert substrates in complex media.

The results

We started synthesizing a range of amphiphilic polymers with a polyacrylamide backbone, Jeffamine-based water soluble grafts, hydrophobic dodecyl grafts in combination with hydrogen-bonding benzene-1,3,5-tricarboxamide grafts to induce folding, and Pd(II)-binding ligands triphenylphosphine and bipyridine. The resulting polymers collapsed/folded into 5-6 nm sized nanoparticles, with an inner hydrophobic domain that comprised the Pd(II) catalyst. We first focused on Pd(II)-catalysed depropargylation reactions to activate a range of prodyes in water, PBS or the cell culture medium DMEM and assess the relation between polymer microstructure, ligand and logP of the substrate. Our results showed that the catalytic activity of nanoparticles is primarily impacted by the ligand-metal complex, the polymer microstructure has an influence as well, but a minor one. The rate of the reaction increased for hydrophobic substrates, corroborating our predictions that substrate sequestration enhances reaction rates because of high local concentrations. Pd(II) leaching studies confirmed little to no loss of Pd(II) from the hydrophobic interior which is important as it can reduce off-target toxicities in future applications. Careful deconstruction of the catalytic system revealed that covalent attachment of the ligand to the polymer backbone is necessary to retain its catalytic activity in DMEM, a confirmation of the usefulness of the SCPN approach for deprotection reactions in complex media. With the best performing system, we tested the activation of a range of prodrugs in collaboration with the Unciti-Broceta group in Edinburgh. We found that the rate of pro-drug activation in water accelerated efficiently by catalytic SCPNs, whereas in DMEM the results depended on the type of protecting group and the logP of the prodrug. So, further engineering of the prodrug’s logP will allow to further optimize the catalyst’s results.

A) Structure of amphiphilic polymers with Pd(II) binding ligands B) Structure of pro-dyes that can be activated using catalytic SCPNs C) Cartoon representation for the formation of SCPNs in water and activation of pro-drugs/dyes D) Comparison of catalytic activity of SCPNs vs free Pd(II) salt for activating pro-dyes.
Design of the catalytic polymeric nanoparticle system. A) Structure of amphiphilic polymers with Pd(II) binding ligands B) Structure of pro-dyes that can be activated using catalytic SCPNs C) Cartoon representation for the formation of SCPNs in water and activation of pro-drugs/dyes D) Comparison of catalytic activity of SCPNs vs free Pd(II) salt for activating pro-dyes. 

What’s next?

Given our recent promising results where the nature of the ligand – Pd(II) complex and the logP of the substrate collaborate to get activity in complex media, the next step is the further optimize the system and equip the SCPNs with suitable recognition units that target specific cancer cells.

 

References

  1. THERACAT (THERApeutic CATalysts) European Project: https://theracat.eu/
  2. Rijt, S. H. Van & Sadler, P. J. Current applications and future potential for bioinorganic chemistry in the development of anticancer drugs. Drug Discov. Today 14, 1089–1097 (2010).
  3. Pérez-López, A. M. et al. Gold-Triggered Uncaging Chemistry in Living Systems. Angew. Chem. Int. Ed. 56, 12548–12552 (2017).
  4. van de L’Isle, M. O. N., Ortega-Liebana, M. C. & Unciti-Broceta, A. Transition metal catalysts for the bioorthogonal synthesis of bioactive agents. Curr. Opin. Chem. Biol. 61, 32–42 (2021).
  5. Bray, T. L. et al. Bright insights into palladium-triggered local chemotherapy. Chem. Sci. 9, 7354–7361 (2018).
  6. Weiss, J. T. et al. Extracellular palladium-catalysed dealkylation of 5-fluoro-1-propargyl-uracil as a bioorthogonally activated prodrug approach. Nat. Commun. 2014 51 5, 1–9 (2014).
  7. Deng, L., Albertazzi, L. & Palmans, A. R. A. Elucidating the Stability of Single-Chain Polymeric Nanoparticles in Biological Media and Living Cells. Biomacromolecules acs.biomac.1c01291 (2021) doi:10.1021/acs.biomac.1c01291.
  8. ter Huurne, G. M. et al. Improving the Folding of Supramolecular Copolymers by Controlling the Assembly Pathway Complexity. Macromolecules 50, 8562–8569 (2017).
  9. Huurne, G. M. ter, Palmans, A. R. A. & Meijer, E. W. Supramolecular Single-Chain Polymeric Nanoparticles. CCS Chem. 1, 64–82 (2019).

Poster image created with BioRender.com.

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