Materials Map

Discover the materials research landscape. Find experts, partners, networks.

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The Materials Map is an open tool for improving networking and interdisciplinary exchange within materials research. It enables cross-database search for cooperation and network partners and discovering of the research landscape.

The dashboard provides detailed information about the selected scientist, e.g. publications. The dashboard can be filtered and shows the relationship to co-authors in different diagrams. In addition, a link is provided to find contact information.

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Materials Map under construction

The Materials Map is still under development. In its current state, it is only based on one single data source and, thus, incomplete and contains duplicates. We are working on incorporating new open data sources like ORCID to improve the quality and the timeliness of our data. We will update Materials Map as soon as possible and kindly ask for your patience.

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in Cooperation with on an Cooperation-Score of 37%

Topics

Publications (2/2 displayed)

  • 2022Developing Pd(ii) based amphiphilic polymeric nanoparticles for pro-drug activation in complex media21citations
  • 2019Stereocomplexes of discrete, isotactic lactic acid oligomers conjugated with oligodimethylsiloxanes41citations

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Palmans, Ara Anja
2 / 36 shared
Croke, Stephen
1 / 2 shared
Sathyan, Anjana
1 / 3 shared
Pérez-López, Ana M.
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Unciti-Broceta, Asier
1 / 3 shared
Lamers, Brigitte A. G.
1 / 8 shared
Van Genabeek, Bas
1 / 1 shared
Hennissen, J.
1 / 1 shared
Meijer, Ew Bert
1 / 48 shared
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2022
2019

Co-Authors (by relevance)

  • Palmans, Ara Anja
  • Croke, Stephen
  • Sathyan, Anjana
  • Pérez-López, Ana M.
  • Unciti-Broceta, Asier
  • Lamers, Brigitte A. G.
  • Van Genabeek, Bas
  • Hennissen, J.
  • Meijer, Ew Bert
OrganizationsLocationPeople

article

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

  • Palmans, Ara Anja
  • Croke, Stephen
  • Sathyan, Anjana
  • Pérez-López, Ana M.
  • Unciti-Broceta, Asier
  • Waal, Bas F. M. De
Abstract

<p>Novel approaches to targeted cancer therapy that combine improved efficacy of current chemotherapies while minimising side effects are highly sought after. The development of single-chain polymeric nanoparticles (SCPNs) as bio-orthogonal catalysts for targeted site-specific pro-drug activation is a promising avenue to achieve this. Currently, the application of SCPNs as bio-orthogonal catalysts is in its early stages due to reduced performance when increasing the medium's complexity. Herein, we present a systematic approach to identify the various aspects of SCPN-based catalytic systems, to improve their efficiency in future in vitro/in vivo studies. We developed amphiphilic polymers with a polyacrylamide backbone and functionalised with the Pd(ii)-binding ligands triphenylphosphine and bipyridine. The resulting polymers collapse into small-sized nanoparticles (5-6 nm) with an inner hydrophobic domain that comprises the Pd(ii) catalyst. We systematically evaluated the effect of polymer microstructure, ligand-metal complex, and substrate hydrophobicity on the catalytic activity of the nanoparticles for depropargylation reactions in water, PBS or DMEM. The results show that the catalytic activity of nanoparticles is primarily impacted by the ligand-metal complex while polymer microstructure has a minor influence. Moreover, the rate of reaction is increased for hydrophobic substrates. In addition, Pd(ii) leaching studies confirmed little to no loss of Pd(ii) from the hydrophobic interior which 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 cell culture medium while not in water. Finally, we activated anti-cancer pro-drugs based on 5-FU, paclitaxel, and doxorubicin using the best-performing catalytic SCPNs. We found that the rate of pro-drug activation in water was accelerated efficiently by catalytic SCPNs, whereas in cell culture medium the results depended on the type of protecting group and hydrophobicity of the prodrug. We believe our findings will aid in the development of suitable catalytic systems and pro-drugs for future in vivo applications.</p>

Topics
  • nanoparticle
  • impedance spectroscopy
  • microstructure
  • polymer
  • leaching
  • activation