Article

RNF41 (Nrdp1) controls type 1 cytokine receptor degradation and ectodomain shedding.

Department of Medical Protein Research, Flanders Interuniversity Institute for Biotechnology (VIB), Ghent University, Albert Baertsoenkaai 3, B-9000 Ghent, Belgium.
Journal of Cell Science (impact factor: 6.11). 03/2011; 124(Pt 6):921-32. DOI:10.1242/jcs.078055 pp.921-32
Source: PubMed

ABSTRACT Cytokines, such as interferons, erythropoietin, leptin and most interleukins, signal through type 1 cytokine receptors and activate the canonical JAK-STAT pathway. Aberrant cytokine signalling underlies numerous pathologies and adequate, temporary receptor activation is therefore under tight control. Negative-feedback mechanisms are very well studied, but cellular sensitivity also depends on the number of receptors exposed at the cell surface. This is determined by the equilibrium between receptor synthesis and transport to the plasma membrane, internalisation and recycling, degradation and ectodomain shedding, but the molecular basis of how cells establish steady state receptor levels is poorly understood. Here, we report that ring finger protein 41 (RNF41, also known as E3 ubiquitin-protein ligase Nrdp1) interacts with JAK2-associated cytokine receptor complexes and modulates their cell surface exposure and signalling. Moreover, ectopic expression of RNF41 affected turnover of leptin, leukaemia inhibitory factor and interleukin-6 receptor in a dual way: it blocked intracellular cathepsin-L-dependent receptor cleavage and concomitantly enhanced receptor shedding by metalloproteases of the ADAM family. Receptor degradation and shedding are thus interconnected phenomena with a single protein, RNF41, determining the balance.

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    Article: Novel regulatory mechanisms for generation of the soluble leptin receptor: implications for leptin action.
    Michael Schaab, Henriette Kausch, Juergen Klammt, Marcin Nowicki, Ulf Anderegg, Rolf Gebhardt, Stefan Rose-John, Juergen Scheller, Joachim Thiery, Juergen Kratzsch
    [show abstract] [hide abstract]
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    PLoS ONE 01/2012; 7(4):e34787. · 4.09 Impact Factor
Data provided are for informational purposes only. Although carefully collected, accuracy cannot be guaranteed. The impact factor represents a rough estimation of the journal's impact factor and does not reflect the actual current impact factor. Publisher conditions are provided by RoMEO. Differing provisions from the publisher's actual policy or licence agreement may be applicable.

Keywords

Aberrant cytokine signalling underlies numerous pathologies
 
activate
 
ADAM family
 
canonical JAK-STAT pathway
 
cell surface
 
cell surface exposure
 
cellular sensitivity
 
concomitantly
 
dual way
 
E3 ubiquitin-protein ligase Nrdp1
 
ectopic expression
 
intracellular cathepsin-L-dependent receptor cleavage
 
JAK2-associated cytokine receptor complexes
 
leptin
 
leukaemia inhibitory factor
 
Negative-feedback mechanisms
 
plasma membrane
 
ring finger protein 41
 
steady state receptor levels
 
type 1 cytokine receptors