Institute of Human Genetics, Anthropology, Jena University Hospital, Kollegiengasse 10, 07743 Jena, Germany
CSN2 activity can be regulated through phosphorylation and dephosphorylation (Kapelari et al., 2000).
Also, corepression function was identified by CSN2 short/Alien a for transcription factors involved in cell cycle regulation and DNA repair such as several members of the E2F transcription factor family (Escher et al., 2007; reviewed in: Papaioannou et al., 2007). Alien is recruited to the E2F1 gene promoter repressing endogenous E2F1 gene expression in vivo. The data also suggest that Alien inhibits transactivation of E2F1, a positive regulator of cell cycle progression. In line with this, Alien represses cell cycle progression. Remarkably, the inhibition of E2F1-mediated transactivation is independent of retinoblastoma protein pRB (Tenbaum et al., 2007). pRB represses E2F1 transcriptional activation. It is not yet known whether Alien is able to substitute pRB function during cell cycle progression (Tenbaum et al., 2007). Furthermore, a direct interaction between Alien and pRB is detected. Interestingly, a pRB-mutant lacking silencing function also lacks interaction with CSN2 short/Alien (Escher et al., 2007).
In addition, Alien interacts with the highly conserved chromatin associated tumor suppressor proteins Inhibitor of growth 1 (p33-ING1b) and 2 (p33-ING2) in vivo and both p33ING1b and p33ING2 are known to induce premature cellular senescence. It is shown that p33ING proteins enhance Alien-mediated gene silencing (Fegers et al., 2007).
The recruitment of HDAC-activity is one mechanism by which Alien realizes its corepression functions (Dressel et al., 1999). However, it is suggested that Alien exhibits both HDAC-dependent and -independent options for gene repression (reviewed in: Papaioannou et al., 2007). Moreover, CSN2 short/Alien a interacts with nucleosome assembly protein 1 (NAP1) in vivo and in vitro regulating its activity through enhancing NAP1-mediated nucleosome assembly on DNA and thereby leading to gene repression (Eckey et al., 2007).
The CSN2 long/Alien b isoform is an essential part of the COP9 signalosome (CSN) complex which is highly conserved in eukaryotes and consists of eight subunits (reviewed in: Wie et al., 2008). The CSN complex plays a central role in the regulation of degradation of multiple proteins through the ability to de-neddylate cullin, which enables the association of cullin with CAND1, a negative regulator of the cullin-based E3 ubiquitin ligases (reviewed in: von Arnim, 2003; reviewed in: Wolf et al., 2003; Chamovitz, 2009; Wu et al., 2009). A role for CSN2 long/Alien b is suggested by the interaction between CSN2 and subunits of the 26S proteasome was already shown (Huang et al., 2005). The promoter region of the Csn2 gene contains NF-kB binding sites like other CSN subunits. Accordingly, these members of the CSN complex are regulated by NF-kB. Snail, a transcription factor, which is a part of the TGF-b pathway and is involved in inflammatory-triggered migration, invasiveness and metastasis of tumor cells, is stabilized by the induction of the CSN complex via NF-kB (Wu et al., 2009). There are also COP9 subcomplexes with yet unknown functions (reviewed in: Wei et al, 2008).
Interaction of COP9 via CSN2 with p53 in tumors can raise the stability of p53, the most important protein involving in a variety of essential tumor suppressive functions and induction of cellular senescence. But in contrast to Snail, the lower turnover does not lead to an increase in transcription activity and therefore neither to an increased p21 expression nor to cell cycle arrest (Leal et al., 2008).
Moreover, CSN2 protein interacts physically with the anaphase-promoting complex (APC/C), a major regulator of the cell cycle and affects specifically its stability (Kob et al., 2008).
Originally, the name Alien was given to a gene in the Drosophila genome with an unknown function (Goubeaud et al., 1996). It shares high homologies with Thyroid hormone receptor-interacting protein 15 (TRIP15), a mammalian protein (Lee et al.,1995; Dressel et al., 1999).
NCBI: 9318 MIM: 604508 HGNC: 30747 Ensembl: ENSG00000166200
dbSNP: 9318 ClinVar: 9318 TCGA: ENSG00000166200 COSMIC: COPS2
Susanne Jennek ; Florian Kraft ; Aria Baniahmad
COPS2 (COP9 constitutive photomorphogenic homolog subunit 2 (Arabidopsis))
Atlas Genet Cytogenet Oncol Haematol. 2009-09-01
Online version: http://atlasgeneticsoncology.org/gene/47362/css/lib/gene-fusions/deep-insight-explorer/