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 (3/3 displayed)

  • 2024Exploring Barmah Forest virus pathogenesis: molecular tools to investigate non-structural protein 3 nuclear localization and viral genomic determinants of replication2citations
  • 2022A combination of soft X-ray and laser light sources offer 3D high content information on the native state of the cellular environmentcitations
  • 2016Modelling bispecific monoclonal antibody interaction with two cell membrane targets indicates the importance of surface diffusion23citations

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Merits, Andres
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David, Cassandra T.
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Freitas, Joseph R.
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Vaher, Mihkel
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Mutso, Margit
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Omler, Ailar
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Liu, Xiang
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Nahas, Kamal L.
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Jadhav, Archana C.
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Harkiolaki, Maria
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Fish, Thomas M.
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Vyas, Nina
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Okolo, Chidinma Adanna
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Sepp, Armin
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Argungu, Maryam
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Hawkins, Emma
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Hadji, Aymen
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Weber, Andrew
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Sengers, Bram G.
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Nouri, Fatma Z.
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Mcginty, Sean
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Co-Authors (by relevance)

  • Merits, Andres
  • David, Cassandra T.
  • Freitas, Joseph R.
  • Vaher, Mihkel
  • Mutso, Margit
  • Omler, Ailar
  • Liu, Xiang
  • Nahas, Kamal L.
  • Jadhav, Archana C.
  • Harkiolaki, Maria
  • Fish, Thomas M.
  • Vyas, Nina
  • Okolo, Chidinma Adanna
  • Sepp, Armin
  • Argungu, Maryam
  • Hawkins, Emma
  • Hadji, Aymen
  • Weber, Andrew
  • Sengers, Bram G.
  • Nouri, Fatma Z.
  • Mcginty, Sean
OrganizationsLocationPeople

article

Modelling bispecific monoclonal antibody interaction with two cell membrane targets indicates the importance of surface diffusion

  • Sepp, Armin
  • Argungu, Maryam
  • Hawkins, Emma
  • Hadji, Aymen
  • Weber, Andrew
  • Taylor, Adam
  • Sengers, Bram G.
  • Nouri, Fatma Z.
  • Mcginty, Sean
Abstract

We have developed a mathematical framework for describing a bispecific monoclonal antibody interaction with two independent membrane-bound targets that are expressed on the same cell surface. The bispecific antibody in solution binds either of the two targets first, and then cross-links with the second one whilst on the cell surface, subject to rate-limiting lateral diffusion step within the lifetime of the monovalently engaged antibody-antigen complex. At experimental densities, only a small fraction of the free targets is expected to lie within the reach of the antibody binding sites at any time. Using ordinary differential equation and Monte Carlo simulation-based models, we validated this approach against an independently published anti-CD4/CD70 DuetMab experimental data set. As a result of dimensional reduction, the cell surface reaction is expected to be so rapid that, in agreement with the experimental data, no monovalently bound bispecific antibody binary complexes accumulate until cross-linking is complete. The dissociation of the bispecific antibody from the ternary cross-linked complex is expected to be significantly slower than that from either of the monovalently bound variants. We estimate that the effective affinity of the bivalently bound bispecific antibody is enhanced for about four orders of magnitude over that of the monovalently bound species. This avidity enhancement allows for the highly specific binding of anti-CD4/CD70 DuetMab to the cells that are positive for both target antigens over those that express only one or the other We suggest that the lateral diffusion of target antigens in the cell membrane also plays a key role in the avidity effect of natural antibodies and other bivalent ligands in their interactions with their respective cell surface receptors.

Topics
  • impedance spectroscopy
  • surface
  • simulation