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Query: UNIPROT:P05412 (
c-Jun
)
11,453
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The biological function of
CD30
in the thymus has been only partially elucidated, although recent data indicate that it may be involved in negative selection. Because
CD30
is expressed only by a small subpopulation of medullary thymocytes, we generated transgenic (Tg) mice overexpressing
CD30
in T lymphocytes to further address its role in T cell development.
CD30
Tg mice have normal thymic size with a normal number and subset distribution of thymocytes. In vitro, in the absence of
CD30
ligation, thymocytes of
CD30
Tg mice have normal survival and responses to apoptotic stimuli such as radiation, dexamethasone, and Fas. However, in contrast to controls,
CD30
Tg thymocytes are induced to undergo programmed cell death (PCD) upon cross-linking of
CD30
, and the simultaneous engagement of TCR and
CD30
results in a synergistic increase in thymic PCD.
CD30
-mediated PCD requires caspase 1 and caspase 3, is not associated with the activation of NF-kappaB or
c-Jun
, but is totally prevented by Bcl-2. Furthermore,
CD30
overexpression enhances the deletion of CD4+/CD8+ thymocytes induced by staphylococcal enterotoxin B superantigen and specific peptide. These findings suggest that
CD30
may act as a costimulatory molecule in thymic negative selection.
...
PMID:CD30 overexpression enhances negative selection in the thymus and mediates programmed cell death via a Bcl-2-sensitive pathway. 1038 16
TRAF5 [tumor necrosis factor (TNF) receptor-associated factor 5] is implicated in NF-kappaB and
c-Jun
NH(2)-terminal kinase/stress-activated protein kinase activation by members of the TNF receptor superfamily, including CD27,
CD30
, CD40, and lymphotoxin-beta receptor. To investigate the functional role of TRAF5 in vivo, we generated TRAF5-deficient mice by gene targeting. Activation of either NF-kappaB or
c-Jun
NH(2)-terminal kinase/stress-activated protein kinase by tumor necrosis factor, CD27, and CD40 was not abrogated in traf5(-/-) mice. However, traf5(-/-) B cells showed defects in proliferation and up-regulation of various surface molecules, including CD23, CD54, CD80, CD86, and Fas in response to CD40 stimulation. Moreover, in vitro Ig production of traf5(-/-) B cells stimulated with anti-CD40 plus IL-4 was reduced substantially. CD27-mediated costimulatory signal also was impaired in traf5(-/-) T cells. Collectively, these results demonstrate that TRAF5 is involved in CD40- and CD27-mediated signaling.
...
PMID:Targeted disruption of Traf5 gene causes defects in CD40- and CD27-mediated lymphocyte activation. 1044 75
Animal models are essential for elucidating the molecular mechanisms of carcinogenesis. Hodgkin's and many diverse non-Hodgkin's lymphomas overexpress the Hodgkin's disease antigen
CD30
(
CD30
(hi)), a tumor necrosis factor receptor II family member. Here we show that chicken Marek's disease (MD) lymphoma cells are also
CD30
(hi) and are a unique natural model for
CD30
(hi) lymphoma. Chicken
CD30
resembles an ancestral form, and we identify a previously undescribed potential cytoplasmic signaling domain conserved in chicken, human, and mouse
CD30
. Our phylogeneic analysis defines a relationship between the structures of human and mouse
CD30
and confirms that mouse
CD30
represents the ancestral mammalian gene structure.
CD30
expression by MD virus (MDV)-transformed lymphocytes correlates with expression of the MDV Meq putative oncogene (a
c-Jun
homologue) in vivo. The chicken
CD30
promoter has 15 predicted high-stringency Meq-binding transcription factor recognition motifs, and Meq enhances transcription from the
CD30
promoter in vitro. Plasma proteomics identified a soluble form of
CD30
.
CD30
overexpression is evolutionarily conserved and defines one class of neoplastic transformation events, regardless of etiology. We propose that
CD30
is a component of a critical intracellular signaling pathway perturbed in neoplastic transformation. Specific anti-
CD30
Igs occurred after infection of genetically MD-resistant chickens with oncogenic MDV, suggesting immunity to
CD30
could play a role in MD lymphoma regression.
...
PMID:Marek's disease is a natural model for lymphomas overexpressing Hodgkin's disease antigen (CD30). 1535 38
Activator protein 1
(
AP-1
) consists of a group of transcription factors including the JUN and FOS family proteins with diverse biological functions. This study assessed the genomic and expression status of the
AP-1
transcription factors in primary cutaneous T-cell lymphoma (CTCL) by using immunohistochemistry (IHC), Affymetrix expression microarray, real-time reverse transcriptase-polymerase chain reaction (RT-PCR) and fluorescent in situ hybridization (FISH). IHC showed JUNB protein expression in tumor cells from 17 of 33 cases of Sezary syndrome (SS) and JUND protein expression in 16 of 23 mycosis fungoides cases. There was no correlation between JUNB and
CD30
expression. However, 7 of 12 JUNB-positive SS cases expressed both phosphorylated and total extracellular signal-regulated kinase (ERK) 1/2 mitogen-activated protein kinase (MAPK) proteins. Expression microarray showed over threefold increased expression of JUNB in three of six SS patients and similar findings were also noted after re-analysis of previously published data. Real-time RT-PCR confirmed the overexpression of JUNB in four SS cases and of JUND in three of four cases. FISH showed increased JUNB copy number in four of seven SS cases. These findings suggest that deregulation of
AP-1
expression in CTCL is the result of aberrant expression of JUNB and possible JUND resulting from genomic amplification and constitutive activation of ERK1/2 MAPK in this type of lymphoma.
...
PMID:A genomic and expression study of AP-1 in primary cutaneous T-cell lymphoma: evidence for dysregulated expression of JUNB and JUND in MF and SS. 1849 16
We analyzed the expression of Jun family in relation to
CD30
expression, cell proliferation and B-cell differentiation immunophenotypes [Germinal Center and non-Germinal Center] in diffuse large B-cell lymphomas (DLBCL). Expression and high expression of phosphorylated-
c-Jun
(p-c-Jun), JunB, JunD and
CD30
(cut-off scores 20% and 50%, respectively) was found in 18/103, 49/103, 72/101 and 26/102 cases, respectively, and in 6/103, 27/103, 60/101 and 21/102 cases, respectively. The following significant positive correlations were observed: (a) JunB with cyclin A (p = 0.046), cyclin B1 (p = 0.033), cyclin E (p = 0.003), MUM-1 (p = 0.002) and
CD30
(p < 0.001), (b) JunD with Ki67 (p = 0.002) and cyclin E (p = 0.014), (c) p-
c-Jun
with
CD30
(p = 0.015), and (d) high p-
c-Jun
with cyclin A (p = 0.034). The positive correlation between expression of JunB, JunD and p-
c-Jun
and tumor cell proliferation in DLBCL, suggests that increased JunB, JunD and p-
c-Jun
expression may be involved in the pathogenesis of DLBCL by increasing tumor cell proliferation.
...
PMID:The expression levels of JunB, JunD and p-c-Jun are positively correlated with tumor cell proliferation in diffuse large B-cell lymphomas. 2581 3
Classical Hodgkin Lymphoma (cHL) is primarily a B cell lymphoid neoplasm and a member of the
CD30
-positive lymphomas. cHL and the other
CD30
-positive lymphomas are characterized by the elevated expression and/or constitutive activation of the activator protein-1 (AP-1) family transcription factors,
c-Jun
and JunB; however, the specific roles they play in the pathobiology of cHL are unclear. In this report we show that reducing either
c-Jun
or JunB expression with short-hairpin RNAs (shRNAs) reduced the growth of cHL cell lines in vitro and in vivo, primarily through impairing cell cycle transition through G
1
. We further investigated the effect of
c-Jun
and JunB knock-down on proliferation in another
CD30
-positive lymphoma, anaplastic lymphoma kinase-positive, anaplastic large cell lymphoma (ALK+ ALCL). We found that JunB knock-down in most ALK+ ALCL cell lines examined also resulted in reduced proliferation that was associated with a G
0
/G
1
cell cycle defect. In contrast,
c-Jun
knock-down in multiple ALK+ ALCL cell lines had no effect on proliferation. In summary, this study directly establishes that both
c-Jun
and JunB play roles in promoting HRS cell proliferation. Furthermore, we demonstrate there are similarities and differences in
c-Jun
and JunB function between cHL and ALK+ ALCL.
...
PMID:The c-Jun and JunB transcription factors facilitate the transit of classical Hodgkin lymphoma tumour cells through G
1
. 3037 7
