Macrophage migration inhibitory factor (MIF) modulates trophic signaling through interaction with serine protease HTRA1

Åsa Fex Svenningsen*, Svenja Loering, Anna Lahn Sørensen, Ha Uyen Buu Huynh, Simone Hjæresen, Nellie Anne Martin, Jesper Bonnet Møller, Maria Louise Elkjær, Uffe Holmskov, Zsolt Illés, Malin Andersson, Solveig Beck Nielsen, Eirikur Benedikz

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Abstract

Macrophage migration inhibitory factor (MIF), a small conserved protein, is abundant in the immune- and central nervous system (CNS). MIF has several receptors and binding partners that can modulate its action on a cel-lular level. It is upregulated in neurodegenerative diseases and cancer although its function is far from clear. Here, we report the finding of a new binding partner to MIF, the ser-ine protease HTRA1. This enzyme cleaves several growth factors, extracellular matrix molecules and is implicated in some of the same diseases as MIF. We show that the func-tion of the binding between MIF and HTRA1 is to inhibit the proteolytic activity of HTRA1, modulating the availability of molecules that can change cell growth and differentiation. MIF is therefore the first endogenous inhibitor ever found for HTRA1. It was found that both molecules were present in astrocytes and that the functional binding has the ability to modulate astrocytic activities important in development and disease of the CNS.
OriginalsprogEngelsk
TidsskriftCellular and Molecular Life Sciences
Vol/bind74
Udgave nummer24
Sider (fra-til)4561–4572
ISSN1420-682X
DOI
StatusUdgivet - 2017

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