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Literature DB >> 24519400

Quantitative single-molecule localization microscopy combined with rule-based modeling reveals ligand-induced TNF-R1 reorganization toward higher-order oligomers.

Franziska Fricke¹, Sebastian Malkusch, Gaby Wangorsch, Johannes F Greiner, Barbara Kaltschmidt, Christian Kaltschmidt, Darius Widera, Thomas Dandekar, Mike Heilemann.

Abstract

We report on the assembly of tumor necrosis factor receptor 1 (TNF-R1) prior to ligand activation and its ligand-induced reorganization at the cell membrane. We apply single-molecule localization microscopy to obtain quantitative information on receptor cluster sizes and copy numbers. Our data suggest a dimeric pre-assembly of TNF-R1, as well as receptor reorganization toward higher oligomeric states with stable populations comprising three to six TNF-R1. Our experimental results directly serve as input parameters for computational modeling of the ligand-receptor interaction. Simulations corroborate the experimental finding of higher-order oligomeric states. This work is a first demonstration how quantitative, super-resolution and advanced microscopy can be used for systems biology approaches at the single-molecule and single-cell level.

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Year: 2014 PMID： 24519400 DOI： 10.1007/s00418-014-1195-0

Source DB: PubMed Journal: Histochem Cell Biol ISSN： 0948-6143 Impact factor: 4.304

54 in total

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10. Cell type-specific nuclear pores: a case in point for context-dependent stoichiometry of molecular machines.

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20 in total

Quantitative single-molecule localization microscopy combined with rule-based modeling reveals ligand-induced TNF-R1 reorganization toward higher-order oligomers.

1. The structure of tumor necrosis factor-alpha at 2.6 A resolution. Implications for receptor binding.

2. A mathematical model of receptor-mediated apoptosis: dying to know why fasl is a trimer.

Review 3. Optical nanoscopy: from acquisition to analysis.

Review 4. Molecular mechanisms of necroptosis: an ordered cellular explosion.

5. Two different cell types have different major receptors for human tumor necrosis factor (TNF alpha).

6. Control of receptor-induced signaling complex formation by the kinetics of ligand/receptor interaction.

7. Binding efficiency of protein-protein complexes.

8. Multi-parameter analysis of the kinetics of NF-kappaB signalling and transcription in single living cells.

9. Counting molecules in single organelles with superresolution microscopy allows tracking of the endosome maturation trajectory.

10. Cell type-specific nuclear pores: a case in point for context-dependent stoichiometry of molecular machines.

Review 1. Piecing it together: Unraveling the elusive structure-function relationship in single-pass membrane receptors.

2. Noncompetitive inhibitors of TNFR1 probe conformational activation states.

3. Artifacts in single-molecule localization microscopy.

Review 4. The Histochemistry and Cell Biology pandect: the year 2014 in review.

5. Polarization of excitation light influences molecule counting in single-molecule localization microscopy.

6. In this special issue.

7. Noncompetitive Allosteric Antagonism of Death Receptor 5 by a Synthetic Affibody Ligand.

8. Death Receptor 5 Activation Is Energetically Coupled to Opening of the Transmembrane Domain Dimer.

9. Death Receptor 5 Networks Require Membrane Cholesterol for Proper Structure and Function.

10. Computational simulations of TNF receptor oligomerization on plasma membrane.