CIC (capicua transcriptional repressor)

2015-07-01 Marlo Firme , Marco Marra Affiliation

Identity

HGNC

CIC

LOCATION

19q13.2

LOCUSID

23152

ALIAS

MRD45

FUSION GENES

Show Gene Fusions

Abstract

CIC is a tissue-specific transcriptional repressor that is highly conserved between metazoan organisms and is required for the normal development of multiple adult structures. CIC functions to transduce receptor tyrosine kinase (RTK) signalling into gene expression changes through a mechanism termed default repression, wherein CIC is bound to target gene promoters or enhancers and inhibits transcription in the absence of signal. This CIC-DNA interaction can be inhibited through activation of the RTK core signalling molecule mitogen-activated protein kinase (MAPK), which then allows for the transcription of CIC targets through this RTK-MAPK signalling axis. Components of RTK signalling are commonly dysregulated in cancers, possibly implying that CIC alterations observed in specific cancer types (e.g. oligodendroglioma and Ewing-like sarcomas) are a form of RTK signalling dysregulation that drives oncogenesis. CIC is also specifically expressed in cells of the developing central nervous system and its dysfunction is associated with the neurodegenerative disorder spinocerebellar ataxia type 1, implicating CIC in neuronal cell development and\/or homeostasis. Other possible cellular and physiological roles for CIC include cell cycle control, ATP-citrate lyase phosphorylation, reactive oxygen species homeostasis, and bile acid homeostasis.

DNA/RNA

Figure 1. Exon structure of 2 main CIC isoforms in humans: CIC short (CIC-S) and long (CIC-L). The highly conserved DNA-binding high mobility group (HMG) box domain is encoded mostly by exon 5 and partially by exon 6 while the highly conserved C1 motif is encoded within exon 20. Figure was obtained from Chittaranjan et al. 2014 with labels added.

Description

CIC is located on the positive strand and spans approximately 27 kilobases. It has 21 exons. According to Entrez-Gene, CIC maps to NC_000019.10 of the assembly GRCh38.p2.

Transcription

There are two known isoforms of CIC: short (CIC-S) and long (CIC-L). CIC-S and CIC-L have alternative transcription start sites at exon 1 and exon 0, respectively, and share exons 2-20 (Figure 1).

Pseudogene

According to Entrez-Gene, CIC has 28 related pseudogenes.

Proteins

Figure 2. Functional domains of CIC short (CIC-S) and long (CIC-L) isoforms in humans. N1: Conserved CIC-L N-terminal domain of unknown function. Ataxin-1 BD: Binding domain that directly interacts with Ataxin-1 (Lam et al. 2006; Kim et al. 2013). 14-3-3 BD: binding domain that directly interacts with 14-3-3 proteins. This domain harbours a serine residue that is phosphorylated by p90RSK to mediate 14-3-3 binding and consequent inhibition of DNA binding upon MAPK activation. An additional 14-3-3 BD flanking the other end of the HMG domain may also be required for 14-3-3 dimer recognition (Dissanayake et al. 2011). HMG: DNA-binding high mobility group box domain (Jimenez et al. 2000; Lee et al. 2002). NLS: Nuclear localisation signal recognized by the nuclear importer KPNA3. Phosphorylation of two nearby serine residues may mask the NLS and potentially interferes with nuclear shuttling upon MAPK activation. Other NLS sequence(s) may be encoded within the HMG domain (Dissanayake et al. 2011). C1: Highly conserved c-terminal motif that may be essential for CIC-mediated transcriptional repression in some contexts (Astigarraga et al. 2007). C2: Motif that mediates direct binding with MAPK (Futran et al. 2015).

Expression

In Drosophila and zebrafish, CIC mRNA is maternally provided to the egg (Jimenez et al. 2000; Chen et al. 2014). In zebrafish and mice, CIC mRNA is detected at various developmental stages, especially in the developing central nervous system (Lee et al. 2002; Chen et al. 2014). In adult mice, CIC mRNA is relatively highly expressed in the brain, spleen, testis, and kidney. CIC mRNA may also be expressed in the heart, lung, mammary tissue, thymus, and lymph nodes in adult mice (Lee et al. 2002).

Localisation

CIC-S and CIC-L localize to both the cytoplasm and the nucleus in multiple human cell lines. CIC may also accumulate close to the mitochondria (Chittaranjan et al. 2014).

Function

CIC has invariably been observed to act as a repressor of transcription through its DNA-binding activity. CIC has a high mobility group (HMG) box domain that confers binding to an octameric DNA motif T(G/C)AATG(A/G)A within the promoters or enhancers of its target genes (Jimenez et al. 2012). In Drosophila, presence of this octameric motif at the regulatory region of a reporter gene was necessary to confer CIC-mediated transcriptional repression, although recruitment of a corepressor protein such as Groucho may be necessary to confer repression (Ajuria et al. 2011). CICs DNA-binding activity can be inhibited through the activation (phosphorylation) of mitogen-activated protein kinase (MAPK), a core signaling molecule of receptor tyrosine kinase (RTK) pathways (Jimenez et al. 2002; Dissanayake et al. 2011). This provides a mechanism for allowing CIC target gene transcription upon RTK signaling. MAPK potentially regulates CICs transcriptionally repressive activity in three ways: through direct binding with CIC (Astigarraga et al. 2007, Futran et al. 2015), through the activation of the downstream signaling molecule p90RSK (Figure 2) to inhibit CICs DNA-binding activity (Dissanayake et al. 2011), or through influencing CICs nucleocytoplasmic shuttling (Dissanayake et al. 2011, Grimm et al. 2012). CIC levels in turn also positively regulate MAPK phosphorylation in vivo in Drosophila by protecting MAPK from phosphatases (Kim et al. 2011).
CIC functions in multiple developmental contexts in both Drosophila and mammals. For example, in Drosophila, CIC can regulate proper embryonic patterning, cell differentiation to form wing vein cells, and cell proliferation in the developing eye. In all these contexts, CIC functions in cells by restricting the expression of specific target genes when an extracellular growth signaling molecule is absent (Jimenez et al. 2002; Roch et al. 2002; Tseng et al. 2007). CIC has also been reported to function in reactive oxygen species homeostasis (Krivy et al. 2013), ATP-citrate lyase phosphorylation (Chittaranjan et al. 2014), and bile acid homeostasis (Kim et al. 2015).

Homology

CIC has homologs in mice, zebrafish, Drosophila, and C. elegans (Jimenez et al. 2000; Lee et al. 2002). Amino acid sequence identity of CICs N1 domain, HMG box domain, and C1 motif (Figure 2) is highly conserved between species (Jimenez et al 2012). This indicates that at least some of CICs biochemical functions are evolutionary conserved between animals.

Implicated in

Entity name

CIC-rearranged Ewing-like sarcomas

Note

The overwhelming majority of Ewing sarcoma/primitive neuroectodermal family of tumours (EFTs) harbour rearrangements of the EWSR1 gene with an ETS family member (Delattre et al. 1994; Mariño-Enrèquez & Fletcher 2014). However, up to 2/3 of EWSR1 fusion-negative EFTs may harbour rearrangements of CIC with a copy of DUX4 on either 4q35 or 10q26. CIC-DUX4. EFTs are aggressive and typically share characteristics such as geographical necrosis and greater heterogeneity in nuclear shape and size than classical EFTs (Italiano et al. 2012). CIC-DUX4 proteins have oncogenic transforming potential in vitro and may drive oncogenesis by strongly activating transcription of CICs oncogenic target genes ETV1, ETV4, and ETV5 instead of normally repressing them (Kawamura-Saito et al. 2006). Consistent with this, EWSR1-ETV1 and EWSR1-ETV4 fusions, which presumably function as aberrant versions of the transcription factors ETV1 and ETV4, respectively, have been observed in EFTs (Jeon et al. 1995; Kaneko et al. 1996). EFTs with CIC-FOXO4 fusions have also been reported (Sugita et al. 2014; Solomon et al. 2014).

Entity name

Oligodendroglioma

Note

CIC mutations are detected in about 70% of "classical" oligodendrogliomas (ODGs, i.e. gliomas harbouring deletions of the chromosomal arms 1p and 19q) (Bettegowda et al. 2011; Yip et al. 2012). Classical ODGs also present with a characteristic set of other somatic mutations, namely in IDH1 or IDH2 (in 100% of cases), in the TERT promoter (about 90% of cases), and in FUBP1 (about 25-40% of cases) (Bettegowda et al. 2011; Sahm et al. 2012; Jiao et al. 2012; Labussire et al. 2014). This indicates potential synergistic interactions between these mutations to promote ODG progression. Different types of detected CIC mutations seem to converge on conferring a CIC loss-of-function phenotype, indicating CIC mutations may inactivate a tumour suppressive activity (Gleize et al. 2015). A CIC mutation in a 1p/19q co-deleted background may also be compatible with the notion of a tumour suppressive role for CIC, since one allele is lost as a consequence of 19q loss while the other allele is mutated. However, there is an enrichment of CIC mutations that affect a single amino acid residue and may preserve CICs structure (Figure 3). Such "hotspots" are often detected in oncogenes (Liu et al. 2011; Stehr et al. 2011). Multiple distinct CIC mutations can arise within different areas of a single ODG lesion (Suzuki et al. 2015), possibly implicating the importance of CIC mutations in driving clonal expansion but not necessarily tumour initiation.

Figure 3. CIC-S: short isoform of CIC. HMG: high-mobility group. C1 motif: highly conserved c-terminal domain. Recurrently detected mutations are indicated in stacked symbols. Frequencies of different mutation types are given in parentheses. Mutational data were gathered from multiple sources (Bettegowda et al. 2011; Jiao et al. 2012; Sahm et al. 2012; Yip et al. 2012) and the cbioportal database (Gao et al. 2013; Chan et al. 2014). The results shown here are in part based upon data generated by the TCGA Research Network: http://cancergenome.nih.gov/.

Entity name

Other cancers

Note

Recurrent somatic CIC mutations, deletions, and amplifications have been detected in a number of other cancer types (Figure 4). Loss of CIC expression is also implicated in prostate cancer progression (Choi et al. 2015). CIC alterations may therefore promote oncogenesis in various cancers.

Figure 4. Frequency of CIC alterations detected in non-glioma cancers. Figure was obtained and modified from the cbioportal database (Cerami et al. 2012; Gao et al. 2013). The results shown here are in whole or part based upon data generated by the TCGA Research Network: http://cancergenome.nih.gov/. Cancer types with 2 or more detected CIC alterations are shown. CNA: copy number alteration.

Entity name

Spinocerebellar ataxia type 1

Note

Spinocerebellar ataxia type 1 (SCA1) is an inherited neurodegenerative disorder that is caused by the production of a toxic form of the Ataxin-1 protein harbouring an expanded tract of glutamine residues (polyQ Ataxin-1) (Orr et al. 1993). SCA1 pathogenesis is associated with a direct physical interaction of polyQ Ataxin-1 with CIC in a large (about 1.8 MDa) complex, as well as with a decrease in wild type Ataxin-1-CIC complex formation. Modulation of CICs transcriptionally repressive activity by polyQ Ataxin-1 provides a possible mechanistic basis for SCA1 pathogenesis (Lam et al. 2006; Bowman et al. 2007). SCA1 pathogenesis may also result from the preferential accumulation of another polyQ Ataxin-1 complex that includes the RBM17 protein and excludes CIC (Lim et al. 2008). In a mouse model of SCA1, a modest exercise regimen extends longevity by reducing CIC levels in the brainstem. CIC loss through genetic perturbation also mitigates multiple SCA1 phenotypes in this model (Fryer et al. 2011).

Bibliography

Pubmed ID	Last Year	Title	Authors
21270056	2011	Capicua DNA-binding sites are general response elements for RTK signaling in Drosophila.	Ajuria L et al
17255944	2007	A MAPK docking site is critical for downregulation of Capicua by Torso and EGFR RTK signaling.	Astigarraga S et al
21817013	2011	Mutations in CIC and FUBP1 contribute to human oligodendroglioma.	Bettegowda C et al
17322884	2007	Duplication of Atxn1l suppresses SCA1 neuropathology by decreasing incorporation of polyglutamine-expanded ataxin-1 into native complexes.	Bowman AB et al
24030748	2014	Loss of CIC and FUBP1 expressions are potential markers of shorter time to recurrence in oligodendroglial tumors.	Chan AK et al
25079045	2014	Characterization of Bbx, a member of a novel subfamily of the HMG-box superfamily together with Cic.	Chen T et al
25277207	2014	Mutations in CIC and IDH1 cooperatively regulate 2-hydroxyglutarate levels and cell clonogenicity.	Chittaranjan S et al
26124181	2015	miR-93/miR-106b/miR-375-CIC-CRABP1: a novel regulatory axis in prostate cancer progression.	Choi N et al
15510215	2004	Capicua integrates input from two maternal systems in Drosophila terminal patterning.	Cinnamon E et al
8022439	1994	The Ewing family of tumors--a subgroup of small-round-cell tumors defined by specific chimeric transcripts.	Delattre O et al
21087211	2011	ERK/p90(RSK)/14-3-3 signalling has an impact on expression of PEA3 Ets transcription factors via the transcriptional repressor capicúa.	Dissanayake K et al
22053053	2011	Exercise and genetic rescue of SCA1 via the transcriptional repressor Capicua.	Fryer JD et al
26124095	2015	Mapping the binding interface of ERK and transcriptional repressor Capicua using photocrosslinking.	Futran AS et al
26017892	2015	CIC inactivating mutations identify aggressive subset of 1p19q codeleted gliomas.	Gleize V et al
23048183	2012	Torso RTK controls Capicua degradation by changing its subcellular localization.	Grimm O et al
22072439	2012	High prevalence of CIC fusion with double-homeobox (DUX4) transcription factors in EWSR1-negative undifferentiated small blue round cell sarcomas.	Italiano A et al
7700648	1995	A variant Ewing's sarcoma translocation (7;22) fuses the EWS gene to the ETS gene ETV1.	Jeon IS et al
22869205	2012	Frequent ATRX, CIC, FUBP1 and IDH1 mutations refine the classification of malignant gliomas.	Jiao Y et al
10652276	2000	Relief of gene repression by torso RTK signaling: role of capicua in Drosophila terminal and dorsoventral patterning.	Jiménez G et al
8834175	1996	Fusion of an ETS-family gene, EIAF, to EWS by t(17;22)(q12;q12) chromosome translocation in an undifferentiated sarcoma of infancy.	Kaneko Y et al
16717057	2006	Fusion between CIC and DUX4 up-regulates PEA3 family genes in Ewing-like sarcomas with t(4;19)(q35;q13) translocation.	Kawamura-Saito M et al
23512657	2013	Structural basis of protein complex formation and reconfiguration by polyglutamine disease protein Ataxin-1 and Capicua.	Kim E et al
25653040	2015	Deficiency of Capicua disrupts bile acid homeostasis.	Kim E et al
21283143	2011	Substrate-dependent control of MAPK phosphorylation in vivo.	Kim Y et al
23429853	2013	Capicua regulates proliferation and survival of RB-deficient cells in Drosophila.	Krivy K et al
25314060	2014	TERT promoter mutations in gliomas, genetic associations and clinico-pathological correlations.	Labussière M et al
17190598	2006	ATAXIN-1 interacts with the repressor Capicua in its native complex to cause SCA1 neuropathology.	Lam YC et al
12393275	2002	CIC, a member of a novel subfamily of the HMG-box superfamily, is transiently expressed in developing granule neurons.	Lee CJ et al
22014525	2011	ATXN1 protein family and CIC regulate extracellular matrix remodeling and lung alveolarization.	Lee Y et al
18337722	2008	Opposing effects of polyglutamine expansion on native protein complexes contribute to SCA1.	Lim J et al
21887471	2011	Remarkable difference of somatic mutation patterns between oncogenes and tumor suppressor genes.	Liu H et al
24801613	2014	Round cell sarcomas - biologically important refinements in subclassification.	Mariño-Enríquez A et al
8358429	1993	Expansion of an unstable trinucleotide CAG repeat in spinocerebellar ataxia type 1.	Orr HT et al
11861482	2002	EGFR signalling inhibits Capicua-dependent repression during specification of Drosophila wing veins.	Roch F et al
22588899	2012	CIC and FUBP1 mutations in oligodendrogliomas, oligoastrocytomas and astrocytomas.	Sahm F et al
25321332	2014	Clinicopathologic features of a second patient with Ewing-like sarcoma harboring CIC-FOXO4 gene fusion.	Solomon DA et al
21575214	2011	The structural impact of cancer-associated missense mutations in oncogenes and tumor suppressors.	Stehr H et al
25007147	2014	A novel CIC-FOXO4 gene fusion in undifferentiated small round cell sarcoma: a genetically distinct variant of Ewing-like sarcoma.	Sugita S et al
25848751	2015	Mutational landscape and clonal architecture in grade II and III gliomas.	Suzuki H et al
17398096	2007	Capicua regulates cell proliferation downstream of the receptor tyrosine kinase/ras signaling pathway.	Tseng AS et al
22072542	2012	Concurrent CIC mutations, IDH mutations, and 1p/19q loss distinguish oligodendrogliomas from other cancers.	Yip S et al

Other Information

Locus ID:

NCBI: 23152
MIM: 612082
HGNC: 14214
Ensembl: ENSG00000079432

Variants:

dbSNP: 23152
ClinVar: 23152
TCGA: ENSG00000079432
COSMIC: CIC

RNA/Proteins

Gene ID	Transcript ID	Uniprot
ENSG00000079432	ENST00000160740	A0A0A0MQR4
ENSG00000079432	ENST00000571942	I3L2I4
ENSG00000079432	ENST00000572681	I3L2J0
ENSG00000079432	ENST00000573349	I3L135
ENSG00000079432	ENST00000575287	I3L373
ENSG00000079432	ENST00000575354	Q96RK0
ENSG00000079432	ENST00000576505	I3L1Q4

Expression (GTEx)

100

150

Adipose - Subcutaneous

Adipose - Visceral

Adrenal Gland

Artery - Aorta

Artery - Tibial

Bladder

Brain - Amygdala

Brain - Anterior cingulate cortex

Brain - Caudate

Brain - Cerebellar Hemisphere

Brain - Cerebellum

Brain - Cortex

Brain - Frontal Cortex

Brain - Hippocampus

Brain - Hypothalamus

Brain - Nucleus accumbens

Brain - Putamen

Brain - Spinal cord

Brain - Substantia nigra

Breast - Mammary Tissue

Cells - Cultured fibroblasts

Cells - EBV - transformed lymphocytes

Cervix - Ectocervix

Cervix - Endocervix

Colon - Sigmoid

Colon - Transverse

Esophagus - Gastroesophageal Junction

Esophagus - Mucosa

Esophagus - Muscularis

Fallopian Tube

Heart - Atrial Appendage

Heart - Left Ventricle

Kidney - Cortex

Kidney - Medulla

Liver

Lung

Minor Salivary Gland

Muscle - Skeletal

Nerve - Tibial

Ovary

Pancreas

Pituitary

Prostate

Skin - Not Sun Exposed

Skin - Sun Exposed

Small Intestine - Terminal Ileum

Spleen

Stomach

Testis

Thyroid

Uterus

Vagina

Whole Blood

Protein levels (Protein atlas)

Not detected

Low

Medium

High

References

Pubmed ID	Year	Title	Citations
22869205	2012	Frequent ATRX, CIC, FUBP1 and IDH1 mutations refine the classification of malignant gliomas.	196
21817013	2011	Mutations in CIC and FUBP1 contribute to human oligodendroglioma.	177
22072542	2012	Concurrent CIC mutations, IDH mutations, and 1p/19q loss distinguish oligodendrogliomas from other cancers.	91
19913121	2009	Gene-centric association signals for lipids and apolipoproteins identified via the HumanCVD BeadChip.	85
22588899	2012	CIC and FUBP1 mutations in oligodendrogliomas, oligoastrocytomas and astrocytomas.	48
21087211	2011	ERK/p90(RSK)/14-3-3 signalling has an impact on expression of PEA3 Ets transcription factors via the transcriptional repressor capicúa.	46
27869830	2017	Inactivation of Capicua drives cancer metastasis.	37
24723486	2014	Distinct transcriptional signature and immunoprofile of CIC-DUX4 fusion-positive round cell tumors compared to EWSR1-rearranged Ewing sarcomas: further evidence toward distinct pathologic entities.	36
28178529	2017	ATXN1L, CIC, and ETS Transcription Factors Modulate Sensitivity to MAPK Pathway Inhibition.	28
26017892	2015	CIC inactivating mutations identify aggressive subset of 1p19q codeleted gliomas.	26

Citation

Marlo Firme ; Marco Marra

CIC (capicua transcriptional repressor)

Atlas Genet Cytogenet Oncol Haematol. 2015-07-01

Online version: http://atlasgeneticsoncology.org/gene/46558/cic-(capicua-transcriptional-repressor)