Multi-omic analysis of CIC’s functional networks reveals novel interaction partners and a potential role in mitotic fidelity

Chittaranjan, Suganthi; Song, Jungeun; Chan, Sum‐Yin; Sd, Lee; St, Ahmad; Rd, Corbett; Gagliardi, Alessia; A, Lum; Moradian, Annie; Pleasance, Stephen; Coope, Robin; J, Gregory Cairncross; Yip, Sungkit; Laks, Emma; Aparicio, Samuel; Ja, Chan; Cs, Hughes; Gb, Morin; LeBlanc, VG; Ma, Marra

doi:10.1101/533323

Cited by 4 publications

(8 citation statements)

References 217 publications

(170 reference statements)

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“…This functional interaction with the SWI/SNF complex may be critical for the dynamic regulation of the epigenome during normal differentiation or contribute to epigenomic dysregulation in cancer. CIC interaction with several SWI/SNF complex members (ARID1A, ARID2, SMARCA2, SMARCC1) has also been observed during mitosis, colocalising around chromosomes during cytokinesis, suggesting that CIC may also play a role in maintaining chromosomal integrity during mitosis [55]. CIC interaction with other proteins involved in epigenomic gene silencing, such as L3MBTL3, MECP2 and UTP3, has also been observed, further supporting the notion of CIC's involvement in chromatin maintenance and/or architecture [55].…”

Section: Capicua In Cancer 533mentioning

confidence: 55%

“…In ELS, activation of CCNE1 by CIC-DUX4 fusion promotes tumour survival and proliferation [76]. Context-dependent dysregulation of cyclin genes CCND1/2, CCNE1/2, CCNA1/2 and CCNB1/2 has also been observed in several cancers with CIC aberrations [32,40,55,76]. Taken together, these studies suggest that apart from the ETS factors, CIC is a regulator of an array of context-dependent cell cycle pathways and acts as a general regulator of the cell cycle.…”

Section: The Role Of Cic Dysregulation In Cancermentioning

confidence: 99%

“…Another hallmark of cancer that CIC has been linked to is genomic instability. Loss of CIC in normal human astrocytes has been found to dysregulate several mitotic regulators (HMGA1, PLK1/3, AURKA1), resulting in mitotic defects, chromosomal instability, and aneuploidy [55]. Interestingly, chromosomal instability and aneuploidy was recently demonstrated to induce epithelial cell invasion through downregulation of CIC in a Drosophila model [77].…”

Section: The Role Of Cic Dysregulation In Cancermentioning

confidence: 99%

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Making heads or tails – the emergence of capicua (CIC) as an important multifunctional tumour suppressor

Wong

Yip

2020

The Journal of Pathology

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Capicua, encoded by the gene CIC, is an evolutionarily conserved high-mobility group-box transcription factor downstream of the receptor tyrosine kinase and mitogen-activated protein kinase pathways. It was initially discovered and studied in Drosophila. Recurrent mutations in CIC were first identified in oligodendroglioma, a subtype of low-grade glioma. Subsequent studies have identified CIC aberrations in multiple types of cancer and have established CIC as a potent tumour suppressor involved in regulating pathways related to cell growth and proliferation, invasion and treatment resistance. The most well-known and studied targets of mammalian CIC are the oncogenic E-Twenty Six transcription factors ETV1/4/5, which have been found to be elevated in cancers with CIC aberrations. Here, we review the role of CIC in normal mammalian development, oncogenesis and tumour progression, and the functional interactors that mediate them.

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Section: Capicua In Cancer 533mentioning

confidence: 55%

Section: The Role Of Cic Dysregulation In Cancermentioning

confidence: 99%

Section: The Role Of Cic Dysregulation In Cancermentioning

confidence: 99%

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Making heads or tails – the emergence of capicua (CIC) as an important multifunctional tumour suppressor

Wong

Yip

2020

The Journal of Pathology

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“…Using CIC KO cell lines with stably expressing FLAG-tagged CIC-S [ 30 ], CIC interaction with 14-3-3 regulatory proteins and the nuclear pore protein TPR was observed to increase following siRNA knockdown of ATXN1L using PLA (Additional file 5 : Figure S4A, B, C). CIC was not found to interact with many previously identified proteins involved in transcriptional regulation such as SIN3A, HDAC1/2, and members of the SWI/SNF complex in our ATXN1L KO background which may contribute to the dysregulation of CIC target genes [ 30 – 32 ]. Among the most highly enriched CIC interactors was the E3-ligase TRIM25.…”

Section: Resultsmentioning

confidence: 99%

“…Cells were harvested 24–72 h post-transfection for experiments. Stable transfection of FLAG-tagged CIC-S in CIC KO cells was performed as previously described [ 30 ].…”

Section: Methodsmentioning

confidence: 99%

TRIM25 promotes Capicua degradation independently of ERK in the absence of ATXN1L

et al. 2020

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Background Aberrations in Capicua (CIC) have recently been implicated as a negative prognostic factor in a multitude of cancer types through the derepression of targets downstream of the mitogen-activated protein kinase (MAPK) signaling cascade, such as oncogenic E26 transformation-specific (ETS) transcription factors. The Ataxin-family protein ATXN1L has previously been reported to interact with CIC in both developmental and disease contexts to facilitate the repression of CIC target genes and promote the post-translational stability of CIC. However, little is known about the mechanisms at the base of ATXN1L-mediated CIC post-translational stability. Results Functional in vitro studies utilizing ATXN1LKO human cell lines revealed that loss of ATXN1L leads to the accumulation of polyubiquitinated CIC protein, promoting its degradation through the proteasome. Although transcriptomic signatures of ATXN1LKO cell lines indicated upregulation of the mitogen-activated protein kinase pathway, ERK activity was found to contribute to CIC function but not stability. Degradation of CIC protein following loss of ATXN1L was instead observed to be mediated by the E3 ubiquitin ligase TRIM25 which was further validated using glioma-derived cell lines and the TCGA breast carcinoma and liver hepatocellular carcinoma cohorts. Conclusions The post-translational regulation of CIC through ATXN1L and TRIM25 independent of ERK activity suggests that the regulation of CIC stability and function is more intricate than previously appreciated and involves several independent pathways. As CIC status has become a prognostic factor in several cancer types, further knowledge into the mechanisms which govern CIC stability and function may prove useful for future therapeutic approaches.

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Novel CIC variants identified in individuals with neurodevelopmental phenotypes

et al. 2022

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Heterozygous pathogenic variants in CIC, which encodes a transcriptional repressor, have been identified in individuals with neurodevelopmental phenotypes. To date, 11 CIC variants have been associated with the CIC-related neurodevelopmental syndrome. Here, we describe three novel and one previously reported CIC variants in four individuals with neurodevelopmental delay. Notably, we report for the first time a de novo frameshift variant specific to the long isoform of CIC (CIC-L, NM_001304815.1:c.1100dup, p.Pro368AlafsTer16) in an individual with speech delay, intellectual disability, and autism spectrum disorder. Our investigation into the function of CIC-L reveals that partial loss of CIC-L leads to transcriptional derepression of CIC target genes. We also describe a missense variant (NM_015125.3:c.683G>A, p.Arg228Gln) in an individual with a history of speech delay and relapsed pre-B acute lymphoblastic leukemia. Functional studies of this variant suggest a partial loss of CIC transcriptional repressor activity. Our study expands the list of CIC pathogenic variants and contributes to the accumulating evidence that CIC haploinsufficiency or partial loss of function is a pathogenic mechanism causing neurodevelopmental phenotypes.

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Multi-omic analysis of CIC’s functional networks reveals novel interaction partners and a potential role in mitotic fidelity

Cited by 4 publications

References 217 publications

Making heads or tails – the emergence of capicua (CIC) as an important multifunctional tumour suppressor

Making heads or tails – the emergence of capicua (CIC) as an important multifunctional tumour suppressor

TRIM25 promotes Capicua degradation independently of ERK in the absence of ATXN1L

Novel CIC variants identified in individuals with neurodevelopmental phenotypes

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