Your search keyword '"Rahm, Johanna"' showing total 2 results

1. Biased activation of the receptor tyrosine kinase HER2.

Author

Catapano, Claudia, Rahm, Johanna V., Omer, Marjan, Teodori, Laura, Kjems, Jørgen, Dietz, Marina S., and Heilemann, Mike

Abstract

HER2 belongs to the ErbB sub-family of receptor tyrosine kinases and regulates cellular proliferation and growth. Different from other ErbB receptors, HER2 has no known ligand. Activation occurs through heterodimerization with other ErbB receptors and their cognate ligands. This suggests several possible activation paths of HER2 with ligand-specific, differential response, which has so far remained unexplored. Using single-molecule tracking and the diffusion profile of HER2 as a proxy for activity, we measured the activation strength and temporal profile in live cells. We found that HER2 is strongly activated by EGFR-targeting ligands EGF and TGFα, yet with a distinguishable temporal fingerprint. The HER4-targeting ligands EREG and NRGβ1 showed weaker activation of HER2, a preference for EREG, and a delayed response to NRGβ1. Our results indicate a selective ligand response of HER2 that may serve as a regulatory element. Our experimental approach is easily transferable to other membrane receptors targeted by multiple ligands. [ABSTRACT FROM AUTHOR]

Published

2023

2. Imaging the fibroblast growth factor receptor network on the plasma membrane with DNA-assisted single-molecule super-resolution microscopy.

Author

Schröder, Mark S., Harwardt, Marie-Lena I.E., Rahm, Johanna V., Li, Yunqing, Freund, Petra, Dietz, Marina S., and Heilemann, Mike

Subjects

*FIBROBLAST growth factor receptors, *MEMBRANE proteins, *HIGH resolution imaging, *MICROSCOPY, *STEREOLOGY, *FIBROBLAST growth factors

Abstract

[Display omitted] • DNA nanotechnology was correlated with multiplexed single-molecule super-resolution imaging. • A procedure for near-molecular visualization and analysis of membrane receptor networks was established. • This approach enabled quantitative microscopy of the FGFR1-4 receptor network at the native cellular expression level. • Information on receptor clustering and distance relationships was extracted. • The imaging and analysis pipeline can be easily adapted to other protein networks. Fibroblast growth factor receptors (FGFRs) are a subfamily of receptor tyrosine kinases and central players in health and disease. Following ligand binding and the formation of homo- and heteromeric complexes, FGFRs initiate a cellular response. Challenges in studying FGFR activation are inner-subfamily interactions and a complex heterogeneity of these in the cell membrane, which demand for observation techniques that can resolve individual protein complexes and that are compatible with endogenous protein levels. Here, we established an imaging and analysis pipeline for multiplexed single-molecule localization microscopy (SMLM) of the FGFR network at the plasma membrane. Using DNA-labeled primary antibodies, we visualize all four FGFRs in the same cell with near-molecular spatial resolution. From the super-resolution imaging data, we extract information on FGFR density, spatial distribution, and inner-subfamily colocalization. Our approach is straightforward and easily adaptable to other multiplexed SMLM data of membrane proteins. [ABSTRACT FROM AUTHOR]

Published

2021