Quantitative mapping of keratin networks in 3D

Author:

Windoffer Reinhard1ORCID,Schwarz Nicole1,Yoon Sungjun1ORCID,Piskova Teodora12ORCID,Scholkemper Michael3ORCID,Stegmaier Johannes4ORCID,Bönsch Andrea5ORCID,Di Russo Jacopo126ORCID,Leube Rudolf E1ORCID

Affiliation:

1. Institute of Molecular and Cellular Anatomy, RWTH Aachen University

2. Interdisciplinary Centre for Clinical Research, RWTH Aachen University

3. Department of Computer Science, RWTH Aachen University

4. Institute of Imaging and Computer Vision, RWTH Aachen University

5. Visual Computing Institute, RWTH Aachen University

6. DWI – Leibniz-Institute for Interactive Materials

Abstract

Mechanobiology requires precise quantitative information on processes taking place in specific 3D microenvironments. Connecting the abundance of microscopical, molecular, biochemical, and cell mechanical data with defined topologies has turned out to be extremely difficult. Establishing such structural and functional 3D maps needed for biophysical modeling is a particular challenge for the cytoskeleton, which consists of long and interwoven filamentous polymers coordinating subcellular processes and interactions of cells with their environment. To date, useful tools are available for the segmentation and modeling of actin filaments and microtubules but comprehensive tools for the mapping of intermediate filament organization are still lacking. In this work, we describe a workflow to model and examine the complete 3D arrangement of the keratin intermediate filament cytoskeleton in canine, murine, and human epithelial cells both, in vitro and in vivo. Numerical models are derived from confocal airyscan high-resolution 3D imaging of fluorescence-tagged keratin filaments. They are interrogated and annotated at different length scales using different modes of visualization including immersive virtual reality. In this way, information is provided on network organization at the subcellular level including mesh arrangement, density and isotropic configuration as well as details on filament morphology such as bundling, curvature, and orientation. We show that the comparison of these parameters helps to identify, in quantitative terms, similarities and differences of keratin network organization in epithelial cell types defining subcellular domains, notably basal, apical, lateral, and perinuclear systems. The described approach and the presented data are pivotal for generating mechanobiological models that can be experimentally tested.

Funder

Deutsche Forschungsgemeinschaft

RWTH Aachen University

Medizinische Fakultät, RWTH Aachen University

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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