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Functional patient-derived organoid screenings identify MCLA-158 as a therapeutic EGFR × LGR5 bispecific antibody with efficacy in epithelial tumors

Batlle and colleagues develop an organoid platform for functional antibody screening and identify a therapeutic bispecific antibody that binds EGFR and LGR5 and that shows efficacy across epithelial tumor patient-derived xenograft models in vivo.

Bram Herpers
Berina Eppink
Mark Throsby
Research25 Apr 2022
Nature Cancer

Volume: 3, P: 418-436
Author Correction: Directing HIV-1 for degradation by non-target cells, using bi-specific single-chain llama antibodies

Jord C. Stam
Steven de Maat
C. Theo Verrips
Amendments and CorrectionsOpen Access28 Apr 2025
Scientific Reports

Volume: 15, P: 1
The architecture of EGFR’s basal complexes reveals autoinhibition mechanisms in dimers and oligomers

To prevent ligand-independent dimerisation the epidermal growth factor receptor (EGFR) is autoinhibited by an extracellular dimer interaction. Here, the authors use several imaging technologies and simulations to provide structural insights on the inactive species and on how intracellular mutations circumvent the autoinhibition of the basal state.

Laura C. Zanetti-Domingues
Dimitrios Korovesis
Marisa L. Martin-Fernandez
ResearchOpen Access18 Oct 2018
Nature Communications

Volume: 9, P: 1-17
ErbB1 dimerization is promoted by domain co-confinement and stabilized by ligand binding

Dimerization, ligand-binding and co-confinement are all expected to contribute to erbB1 signaling, but the level of their contribution has not yet been fully appreciated. Two-color quantum-dot tracking in live cells now shows that ligand-binding (two ligands with two receptors) stabilizes erbB1 dimers, whereas actin networks influence dimer mobility and promote repeated encounters between erbB1 monomers.

Shalini T Low-Nam
Keith A Lidke
Diane S Lidke
Research23 Oct 2011
Nature Structural & Molecular Biology

Volume: 18, P: 1244-1249
Directing HIV-1 for degradation by non-target cells, using bi-specific single-chain llama antibodies

Jord C. Stam
Steven de Maat
C. Theo Verrips
ResearchOpen Access04 Aug 2022
Scientific Reports

Volume: 12, P: 1-14

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Functional patient-derived organoid screenings identify MCLA-158 as a therapeutic EGFR × LGR5 bispecific antibody with efficacy in epithelial tumors

Author Correction: Directing HIV-1 for degradation by non-target cells, using bi-specific single-chain llama antibodies

The architecture of EGFR’s basal complexes reveals autoinhibition mechanisms in dimers and oligomers

ErbB1 dimerization is promoted by domain co-confinement and stabilized by ligand binding

Directing HIV-1 for degradation by non-target cells, using bi-specific single-chain llama antibodies

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