Fibrosis and Immune Cell Infiltration Are Separate Events Regulated by Cell-Specific Receptor Notch3 Expression.

Brandt, Sabine; Ballhause, Tobias M; Bernhardt, Anja; Becker, Annika; Salaru, Delia; Le-Deffge, Hien Minh; Fehr, Alexander; Fu, Yan; Philipsen, Lars; Djudjaj, Sonja; Müller, Andreas J; Kramann, Rafael; Ibrahim, Mahmoud; Geffers, Robert; Siebel, Chris; Isermann, Berend; Heidel, Florian H; Lindquist, Jonathan A; Mertens, Peter R

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Issue Date

2020-08-28

Submitted date

2019-12-13

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Abstract

Kidney injuries that result in chronic inflammation initiate crosstalk between stressed resident cells and infiltrating immune cells. In animal models, whole-body receptor Notch3 deficiency protects from leukocyte infiltration and organ fibrosis. However, the relative contribution of Notch3 expression in tissue versus infiltrating immune cells is unknown.

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Article

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EISSN

1533-3450

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publications of the research group genomeanalytics (GMAK)

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Except where otherwise noted, this item's license is described as Attribution 4.0 International