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Query: UNIPROT:Q86TM3 (
cage
)
29,987
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
CTCF is a ubiquitous 11 zinc finger (ZF) protein with highly versatile functions: in addition to transcriptional silencing or activating in a context-dependent fashion, it organizes epigenetically controlled chromatin insulators that regulate imprinted genes in soma. Recently, we have identified a CTCF paralogue, termed
BORIS
for Brother of the Regulator of Imprinted Sites, that is expressed only in the testis.
BORIS
has the same exons encoding the 11 ZF domain as mammalian CTCF genes, and hence interacts with similar cis elements, but encodes amino and carboxy termini distinct from those in CTCF. Normally, CTCF and
BORIS
are expressed in a mutually exclusive pattern that correlates with re-setting of methylation marks during male germ cell differentiation. The antagonistic features of these two gene siblings are underscored by showing that while CTCF overexpression blocks cell proliferation, expression of
BORIS
in normally
BORIS
-negative cells promotes cell growth which can lead to transformation. The suggestion that
BORIS
directs epigenetic reprogramming at CTCF target sites impinges on the observations that human
BORIS
is not only abnormally activated in a wide range of human cancers, but also maps to the
cancer-associated
amplification region at 20q13. The sibling rivalry occasioned by aberrant expression of
BORIS
in cancer may interfere with normal functions of CTCF including growth suppression, and contribute to epigenetic dysregulation which is a common feature in human cancer.
...
PMID:The novel BORIS + CTCF gene family is uniquely involved in the epigenetics of normal biology and cancer. 1219 39
Cancer testis (CT) antigens are promising candidates for tumor vaccines due to their immunogenicity and tissue-restricted expression. Recently, we identified a novel cancer testis gene,
BORIS
, whose expression is restricted to male testis after puberty and is strictly absent in non-malignant female tissue.
BORIS
encodes a DNA-binding protein that shares 11 zing finger (ZF) with transcription factor CTCF and differs at the N- and C-termini. CTCF has been implicated in epigenetic regulation of imprinting, X chromosome inactivation, repression, and activation of cancer testis antigens.
BORIS
expression has been documented in cancers of diverse histological origin, including, but not limited to breast, prostate, ovary, gastric, liver, endometrial, glia, colon, and esophagus. Interestingly,
BORIS
induces demethylation and subsequent expression of many cancer-testis genes, including MAGE-A1 and NY-ESO-1, indicating that it is expressed very early in malignancy and might be an attractive candidate for immunotherapy. In this study we tested
BORIS
as a vaccine in a very aggressive, highly metastatic, and poorly immunogenic murine model of mammary carcinoma. Immunizations with a DNA encoding the mutant form of murine
BORIS
antigen (pmBORIS lacking DNA-binding function) significantly prolonged survival, and inhibited tumor growth in BALB/c mice inoculated with 4T1 cells. Priming with pmBORIS mixed with molecular adjuvant and boosting with adenoviral vector expressing mBORIS was generally more effective, suggesting that the vaccination protocol could be further optimized. This is the first report demonstrating the feasibility of vaccination with a
cancer associated
epigenetic regulator for the induction of tumor inhibition.
...
PMID:Antitumor efficacy of DNA vaccination to the epigenetically acting tumor promoting transcription factor BORIS and CD80 molecular adjuvant. 1674 71
Global loss of DNA methylation is frequently observed in the genome of human tumors. Although this epigenetic alteration is clearly associated with cancer progression, the way it exerts its pro-tumoral effect remains incompletely understood. A remarkable consequence of DNA hypomethylation in tumors is the aberrant activation of "cancer-germline" genes (also known as "cancer-testis" genes), which comprise a diverse group of germline-specific genes that use DNA methylation as a primary mechanism for repression in normal somatic tissues. Here we review the evidence that such cancer-germline genes contribute to key processes of tumor development. Notably, several cancer-germline genes were found to stimulate oncogenic pathways involved in cell proliferation (SSX, DDX43, MAEL, PIWIL1), angiogenesis (
DDX53
), immortality (
BORIS
/CTCFL), and metastasis (CT-GABRA3). Others appear to inhibit tumor suppressor pathways, including those controlling growth inhibition signals (MAGEA11, MAGEB2), apoptosis (MAGEA2, MAGEC2), and genome integrity (HORMAD1, NXF2). Cancer-germline genes were also implicated in the regulation of tumor metabolism (MAGEA3/MAGEA6). Together, our survey substantiates the concept that DNA hypomethylation promotes tumorigenesis via transcriptional activation of oncogenes. Importantly, considering their highly restricted pattern of expression, cancer-germline genes may represent valuable targets for the development of anti-cancer therapies with limited side effects.
...
PMID:Oncogenic roles of DNA hypomethylation through the activation of cancer-germline genes. 2834 86
High-grade serous carcinoma (HGSC) is the most aggressive and predominant form of epithelial ovarian cancer and the leading cause of gynecologic cancer-related death. We have previously shown that
CTCFL
(also known as
BORIS
,
B
rother
o
f the
R
egulator of
I
mprinted
S
ites) is expressed in most ovarian cancers, and is associated with global and promoter-specific DNA hypomethylation, advanced tumor stage, and poor prognosis. To explore its role in HGSC, we expressed
BORIS
in human fallopian tube secretory epithelial cells (FTSEC), the presumptive cells of origin for HGSC.
BORIS
-expressing cells exhibited increased motility and invasion, and
BORIS
expression was associated with alterations in several
cancer-associated gene
expression networks, including fatty acid metabolism, TNF signaling, cell migration, and ECM-receptor interactions. Importantly,
GALNT14
, a glycosyltransferase gene implicated in cancer cell migration and invasion, was highly induced by
BORIS
, and
GALNT14
knockdown significantly abrogated
BORIS
-induced cell motility and invasion. In addition,
in silico
analyses provided evidence for
BORIS
and
GALNT14
coexpression in several cancers. Finally, ChIP-seq demonstrated that expression of
BORIS
was associated with
de novo
and enhanced binding of CTCF at hundreds of loci, many of which correlated with activation of transcription at target genes, including
GALNT14
. Taken together, our data indicate that
BORIS
may promote cell motility and invasion in HGSC via upregulation of
GALNT14
, and suggests
BORIS
as a potential therapeutic target in this malignancy. IMPLICATIONS: These studies provide evidence that aberrant expression of
BORIS
may play a role in the progression to HGSC by enhancing the migratory and invasive properties of FTSEC.
...
PMID:
BORIS
Expression in Ovarian Cancer Precursor Cells Alters the CTCF Cistrome and Enhances Invasiveness through
GALNT14
. 3129 1
