The Diverging Routes of BORIS and CTCF: An Interactomic and Phylogenomic Analysis

Jabbari, Kamel; Heger, Peter; Sharma, Ranu; Wiehe, Thomas

doi:10.3390/life8010004

Cited by 7 publications

(3 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…ZMYM3 serves as a scaffolding protein that coordinates interactions between deacetylases, demethylases, and RNase H type enzymes (including HDAC and CoREST), and the eighth and ninth zinc fingers of ZMYM2 protein can bind directly to the LSD1-CoREST-HDAC complex ( Shapson-Coe et al, 2019 ). As RNase H2 can interact with both ZMYM2 and ZMYM4, it has been suggested that ZMYM4 may also interact with the LSD1-CoREST-HDAC complex to mediate transcriptional regulation ( Jabbari et al, 2018 ; Shapson-Coe et al, 2019 ). Furthermore, ZMYM2 and ZMYM3 contain a new class of SUMO-interacting motifs (SIMs) that can interact with SUMO2 in a 1:1 stoichiometry, and recent studies show that ZMYM4 is also SUMOylated ( Anderson, 2015 ; Lamoliatte et al, 2017 ; Cibis et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

Zmym4 is required for early cranial gene expression and craniofacial cartilage formation

Jourdeuil,

Neilson,

Cousin

et al. 2023

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

Introduction: The Six1 transcription factor plays important roles in the development of cranial sensory organs, and point mutations underlie craniofacial birth defects. Because Six1’s transcriptional activity can be modulated by interacting proteins, we previously screened for candidate interactors and identified zinc-finger MYM-containing protein 4 (Zmym4) by its inclusion of a few domains with a bona fide cofactor, Sine oculis binding protein (Sobp). Although Zmym4 has been implicated in regulating early brain development and certain cancers, its role in craniofacial development has not previously been described.Methods: We used co-immunoprecipitation and luciferase-reporter assays in cultured cells to test interactions between Zmym4 and Six1. We used knock-down and overexpression of Zmym4 in embryos to test for its effects on early ectodermal gene expression, neural crest migration and craniofacial cartilage formation.Results: We found no evidence that Zmym4 physically or transcriptionally interacts with Six1 in cultured cells. Nonetheless, knockdown of endogenous Zmym4 in embryos resulted in altered early cranial gene expression, including those expressed in the neural border, neural plate, neural crest and preplacodal ectoderm. Experimentally increasing Zmym4 levels had minor effects on neural border or neural plate genes, but altered the expression of neural crest and preplacodal genes. At larval stages, genes expressed in the otic vesicle and branchial arches showed reduced expression in Zmym4 morphants. Although we did not detect defects in neural crest migration into the branchial arches, loss of Zmym4 resulted in aberrant morphology of several craniofacial cartilages.Discussion: Although Zmym4 does not appear to function as a Six1 transcriptional cofactor, it plays an important role in regulating the expression of embryonic cranial genes in tissues critical for normal craniofacial development.

show abstract

Section: Discussionmentioning

confidence: 99%

Zmym4 is required for early cranial gene expression and craniofacial cartilage formation

Jourdeuil,

Neilson,

Cousin

et al. 2023

Front. Cell Dev. Biol.

View full text Add to dashboard Cite

show abstract

“…In the 10 samples with CTCFL mutations among samples that had complete mutations and copy number alterations information in the Colorectal PanCancer Atlas cohort [15] (Table 5), all had concomitant mutations in one of the four MSI associated genes or the POLE or POLD1 genes, while only one of the 25 samples with CTCFL amplifications (used as a control) had such lesions in MSI-associated genes or POLE / POLD1 genes (in POLD1 ) (Fisher’s two-tailed exact test p < 0.0001). In the respective endometrial carcinoma TCGA PanCancer Atlas study, which included 509 cases with complete mutations and copy number alterations information [23], among the 27 cases with CTCFL mutations 22 had mutations in one of the four MSI associated genes or the POLE or POLD1 genes.…”

Section: Resultsmentioning

confidence: 99%

“…Thus, CTCFL belongs to the category of so called cancer testis antigens, alternatively termed cancer-germline antigens [14]. Although details of the interaction are not known, CTCFL has been reported to be part of the CTCF interactome [15]. Whether the two proteins interact directly or indirectly in cells where they are co-expressed remains to be confirmed experimentally.…”

Section: Introductionmentioning

confidence: 99%

Molecular Lesions of Insulator CTCF and Its Paralogue CTCFL (BORIS) in Cancer: An Analysis from Published Genomic Studies

Voutsadakis

2018

High-Throughput

View full text Add to dashboard Cite

CTCF (CCCTC-binding factor) is a transcription regulator with hundreds of binding sites in the human genome. It has a main function as an insulator protein, defining together with cohesins the boundaries of areas of the genome called topologically associating domains (TADs). TADs contain regulatory elements such as enhancers which function as regulators of the transcription of genes inside the boundaries of the TAD while they are restricted from regulating genes outside these boundaries. This paper will examine the most common genetic lesions of CTCF as well as its related protein CTCFL (CTCF-like also called BORIS) in cancer using publicly available data from published genomic studies. Cancer types where abnormalities in the two genes are more common will be examined for possible associations with underlying repair defects or other prevalent genetic lesions. The putative functional effects in CTCF and CTCFL lesions will also be explored.

show abstract

Boosting Macroevolution: Genomic Changes Triggering Qualitative Expansions of Regulatory Potential

Irimia

Maeso

2019

Old Questions and Young Approaches to Animal Evolution

View full text Add to dashboard Cite

Two main types of factors have been traditionally considered as potential driving forces underlying macroevolutionary patterns: environmental ('external') cues and genetic and/or developmental ('internal') factors. However, whereas the impact of non-gradual environmental changes has been extensively investigated, the contribution of internal causes, especially of genomic factors, has been approached in a less systematic manner, without clear definitions and classification schemes. Here, taking advantage of recent advances in comparative and functional genomics, we define three types of genomic changes that likely play important roles in macroevolutionary processes: (i) emergence of novel functional genomic properties, (ii) large-scale genome reshaping, and (iii) qualitative single amplifications of regulatory potentials (which we term quasa-regs). Their unifying theme is their ability to qualitatively expand the genomic regulatory potential of the species.We review examples in which these types of changes have likely played important roles and discuss their potential macroevolutionary implications. We conclude that, although such changes may have a minor organismal impact at the time of emergence, they are likely to often have profound long-term effects by expanding regulatory abilities and opening new highways that boost the evolutionary process.

show abstract

The Diverging Routes of BORIS and CTCF: An Interactomic and Phylogenomic Analysis

Cited by 7 publications

References 50 publications

Zmym4 is required for early cranial gene expression and craniofacial cartilage formation

Zmym4 is required for early cranial gene expression and craniofacial cartilage formation

Molecular Lesions of Insulator CTCF and Its Paralogue CTCFL (BORIS) in Cancer: An Analysis from Published Genomic Studies

Boosting Macroevolution: Genomic Changes Triggering Qualitative Expansions of Regulatory Potential

Contact Info

Product

Resources

About