The COP9 Signalosome Controls Adipocyte Differentiation by Regulating CHOP Protein Stability

doi:10.4236/eng.2012.410B050

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Engineering, 2012, 5, 192-193

doi:10.4236/eng.2012.410B050 Published Online October 2012 (http://www.SciRP.org/journal/eng)

The COP9 Signalosome Controls Adipocyte Differentiation by

Regulating CHOP Protein Stability

Xiaohua Huang, Wolfgang D u b ie l

Department of General, Visceral, Vascular and Thoracic Surgery, Division of Molecular Biology,

Charité - Universitätsmedizin Berlin, Berlin, Germany

Email: Xiaohua.huang@charite.de, Wolfgang.dubiel@charite.de

Received 2012

ABSTRACT

Obesity is a serious health problem of our time. Dysfunction of adipogenesis, the differentiation of adipocytes, is a hallmark of obes-

ity. Therefore her e we investigate the role of the COP9 signalosome and of CHOP in the differentiation of LiSa-2 preadipocytes.

Keywords: COP9 Signalosome; CHOP; Adipogenesis; Cullin-RING Ubiquitin Ligase

1. Introduction

Adipogenesis (differentiation of adipocytes) is a highly com-

plex mechanism, closely cross-linked to the induction of an-

giogenesis which in turn promotes preadipocyte differentiation.

Dysfunction of adipogenesis causes obesity. The process of

adipogenesis is regulated by an elaborate network of transcrip-

tion factors that coordinate the expression of hundreds of pro-

teins responsible for establishing fat cell phenotype. In the cen-

tre of that network are the two master regulators of adipocyte

differentiation, the peroxisome proliferator-activated receptor γ

(PPAR-γ) and CCAAT/enhancer binding protein α (C/EBPα).

Besides P PAR-γ, C/EBPα is considered a primary transcription

factor that mediates adipogenesis. Early in the differentiation

program C/EBPβ is expressed, which is the transcriptional ac-

tivator of PPAR-γ and C/EBPα. Its activity is delayed by the

C/EBP homologous protein (CHOP, also called growth ar-

rest-DNA damage-induced 153, GADD153), a dominant nega-

tive form of C/EBP family members. CHOP dimerizes with

adipogenic C/EBPs, suppresses their transactivation activity

and, therefore, blocks adipogenesis. CHOP has to be

down-regulated for the progression of the differentiation pro-

gram. Interestingly, CHOP protein is degraded by the ubiquitin

(Ub) proteasome system (UPS) and proteasome inhibitors sta-

bilize the protein and block adipocyte differentiation [1].

2. Results

he COP9 signalosome (CSN) was first discovered in 1994 as

a protein complex which negatively regulates photomorpho-

genesis in Arabidopsis [2]. It consists of 8 subunits (CSN1-8;

depending on their size) and was detected in all eukaryoti c cells .

The CSN exhibits an extensive range of biological responses

including embryonic development, cell cycle, signal transduc-

tion, apoptosis, DNA repair, homeostasis and also angiogenesis

- all together reflecting the multifunctionality of the complex.

The most important function of the CSN is the regulation of the

activity of cullin-RING E3 Ub-ligases (CRLs) [3]. These li-

gases are the prominent transducers for protein degradation

mediating the formation of a complex composed of the Ub

carrying E2 conjugating enzyme and the substrate which is to

be ubiquitinated. The CSN5 subunit of the CSN exhibits a met-

alloprotease activity, which can remove Nedd8 from CRLs,

which regulates their activity [4].

Recently we have shown that the CSN is involved in adipo-

genesis [5]. Inhibitors of CSN associated kinases such curcu-

min and curcumin-like substances block the production of

VEGF in tumor cells [6] as well as in adipocytes [5]. Inhibition

of adipocyte VEGF production is one explanation for the fact

that obesity can be downregulated by curcumin and resveratrol

[7], although t he exact mechanism remained obscure.

Here we show that the curcumin-like compound piceatannol

induces CHOP in LiSa-2 preadipocytes, which blocks the

process of adipocyte differentiation. CHOP is targeted for de-

gradation via UPS by the CSN and permanent downregulation

of the CSN in LiSa-2 cells inhibits adipogenesis by stabilizing

CHOP . Permanent overexpres sion of Flag-CHOP causes a sim-

ilar phenotype as downregulation of the CSN. The CRL re-

sponsible for CHOP Ubiquitination was identified.

3. Conclusions

CHOP is an important regulator of adipogenesis. The COP9

signalosome is essential for the differentiation of adipocytes.

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