Structural and Functional Analyses of the Shedding Protease ADAM17 in HoxB8-Immortalized Macrophages and Dendritic-like Cells
Cabron AS, El Azzouzi K, Boss M, Arnold P, Schwarz J, Rosas M, Dobert JP, Pavlenko E, Schumacher N, Renne T, Taylor PR, Linder S, Rose-John S, Zunke F (2018)
Publication Type: Journal article
Publication year: 2018
Journal
Book Volume: 201
Pages Range: 3106-3118
Journal Issue: 10
Abstract
A disintegrin and metalloproteinase (ADAM) 17 has been implicated in many shedding processes. Major substrates of ADAM17 are TNF-a, IL-6R, and ligands of the epidermal growth factor receptor. The essential role of the protease is emphasized by the fact that ADAM17 deficiency is lethal in mice. To study ADAM17 function in vivo, we generated viable hypomorphic ADAM17 mice called ADAM17ex/ex mice. Recent studies indicated regulation of proteolytic ADAM17 activity by cellular processes such as cytoplasmic phosphorylation and removal of the prodomain by furin cleavage. Maturation and thus activation of ADAM17 is not fully understood. So far, studies of ADAM17 maturation have been mainly limited to mouse embryonic fibroblasts or transfected cell lines relying on nonphysiologic stimuli such as phorbol esters, thus making interpretation of the results difficult in a physiologic context. In this article, we present a robust cell system to study ADAM17 maturation and function in primary cells of the immune system. To this end, HoxB8 conditionally immortalized macrophage precursor cell lines were derived from bone marrow of wild-type and hypomorphic ADAM17ex/ex mice, which are devoid of measurable ADAM17 activity. ADAM17 mutants were stably expressed in macrophage precursor cells, differentiated to macrophages under different growth factor conditions (M-CSF versus GM-CSF), and analyzed for cellular localization, proteolytic activity, and podosome disassembly. Our study reveals maturation and activity of ADAM17 in a more physiological-immune cell system. We show that this cell system can be further exploited for genetic modifications of ADAM17 and for studying its function in immune cells. The Journal of Immunology, 2018, 201: 3106-3118.
Authors with CRIS profile
Involved external institutions
Universitätsklinikum Hamburg-Eppendorf (UKE)
Germany (DE)
Christian-Albrechts-Universität zu Kiel
Germany (DE)
Cardiff University
United Kingdom (GB)
Karolinska Institute
Sweden (SE)
Germany (DE)
Christian-Albrechts-Universität zu Kiel
Germany (DE)
Cardiff University
United Kingdom (GB)
Karolinska Institute
Sweden (SE)
How to cite
APA:
Cabron, A.-S., El Azzouzi, K., Boss, M., Arnold, P., Schwarz, J., Rosas, M.,... Zunke, F. (2018). Structural and Functional Analyses of the Shedding Protease ADAM17 in HoxB8-Immortalized Macrophages and Dendritic-like Cells. Journal of Immunology, 201(10), 3106-3118. https://doi.org/10.4049/jimmunol.1701556
MLA:
Cabron, Anne-Sophie, et al. "Structural and Functional Analyses of the Shedding Protease ADAM17 in HoxB8-Immortalized Macrophages and Dendritic-like Cells." Journal of Immunology 201.10 (2018): 3106-3118.
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