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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The unique property of stem cells to self-renew suggests specific mechanisms that regulate their cell-cycle progression. In the present study, we identify a novel protein,
nucleostemin
, found in the nucleoli of CNS stem cells, embryonic stem cells, and several cancer cell lines and preferentially expressed by other stem cell-enriched populations. It contains an N-terminal basic domain and two GTP-binding motifs. When stem cells differentiate,
nucleostemin
expression decreases rapidly prior to cell-cycle exit both in vitro and in vivo. Depletion or overexpression of
nucleostemin
reduces cell proliferation in CNS stem cells and transformed cells. Mutation analysis indicates that excessive
nucleostemin
, particularly mutants that lack the GTP-regulatory domain, prevents cells from entering mitosis and causes apoptosis in a
p53
-dependent manner. The N-terminal basic domain specifies nucleolar localization, the
p53
interaction, and is required for the cell death caused by overexpression. This work describes a novel nucleolar mechanism that controls the cell-cycle progression in CNS stem cells and cancer cells.
...
PMID:A nucleolar mechanism controlling cell proliferation in stem cells and cancer cells. 1246 30
Nucleostemin is a
p53
-interactive cell cycle progression factor that shuttles between the nucleolus and nucleoplasm, but it has no known involvement in ribosome synthesis. We found the dynamic properties of
nucleostemin
differed strikingly from fibrillarin (a protein directly involved in rRNA processing) both in response to rRNA transcription inhibition and in the schedule of reentry into daughter nuclei and the nucleolus during late telophase/early G1. Furthermore,
nucleostemin
was excluded from the nucleolar domains in which ribosomes are born--the fibrillar centers and dense fibrillar component. Instead it was concentrated in rRNA-deficient sites within the nucleolar granular component. This finding suggests that the nucleolus may be more subcompartmentalized than previously thought. In support of this concept, electron spectroscopic imaging studies of the nitrogen and phosphorus distribution in the nucleolar granular component revealed regions that are very rich in protein and yet devoid of nucleic acid. Together, these results suggest that the ultrastructural texture of the nucleolar granular component represents not only ribosomal particles but also RNA-free zones populated by proteins or protein complexes that likely serve other functions.
...
PMID:A nonribosomal landscape in the nucleolus revealed by the stem cell protein nucleostemin. 1585 56
Inosine monophosphate dehydrogenase (IMPDH) is a pivotal enzyme in the de novo pathway of guanine nucleotide biosynthesis. Inhibitors of this enzyme decrease intracellular guanine nucleotide levels by 50-80% and have potential as anti-neoplastic agents. Both mycophenolic acid (MPA) and AVN-944 are highly specific inhibitors of IMPDH that cause cell cycle arrest or apoptosis in lymphocytes and leukemic cell lines. We have examined the mechanisms by which these two agents cause cytotoxicity. Both MPA and AVN-944 inhibit the growth of K562 cells, and induce apoptosis in Raji B and CCRF-CEM T cells. Both compounds strikingly inhibit RNA synthesis within 2 h of exposure. Depletion of guanine nucleotides by MPA and AVN-944 also causes an early and near-complete reduction in levels of the 45S precursor rRNA synthesis and the concomitant translocation of nucleolar proteins including nucleolin, nucleophosmin, and
nucleostemin
from the nucleolus to the nucleoplasm. This efflux correlates temporally with the sustained induction of
p53
in cell lines with wild-type
p53
. We conclude that inhibition of IMPDH causes a primary reduction in rRNA synthesis and secondary nucleolar disruption and efflux of nucleolar proteins that most likely mediate cell cycle arrest or apoptosis. The ability of AVN-944 to induce apoptosis in a number of leukemic cell lines supports its potential utility in the treatment of hematologic malignancies.
...
PMID:Guanine nucleotide depletion inhibits pre-ribosomal RNA synthesis and causes nucleolar disruption. 1746 31
The nucleolar protein
nucleostemin
(NS) is essential for cell proliferation and early embryogenesis. Both depletion and overexpression of NS reduce cell proliferation. However, the mechanisms underlying this regulation are still unclear. Here, we show that NS regulates
p53
activity through the inhibition of MDM2. NS binds to the central acidic domain of MDM2 and inhibits MDM2-mediated
p53
ubiquitylation and degradation. Consequently, ectopic overexpression of NS activates
p53
, induces G(1) cell cycle arrest, and inhibits cell proliferation. Interestingly, the knockdown of NS by small interfering RNA also activates
p53
and induces G(1) arrest. These effects require the ribosomal proteins L5 and L11, since the depletion of NS enhanced their interactions with MDM2 and the knockdown of L5 or L11 abrogated the NS depletion-induced
p53
activation and cell cycle arrest. These results suggest that a
p53
-dependent cell cycle checkpoint monitors changes of cellular NS levels via the impediment of MDM2 function.
...
PMID:Aberrant expression of nucleostemin activates p53 and induces cell cycle arrest via inhibition of MDM2. 1842 7
Nucleostemin (NS) is expressed in the nucleoli of adult and embryonic stem cells and in many tumors and tumor-derived cell lines. In coimmunoprecipitation experiments,
nucleostemin
is recovered with the
tumor suppressor p53
, and more recently we have demonstrated that
nucleostemin
exerts its role in cell cycle progression via a
p53
-dependent pathway. Here, we report that in human osteosarcoma cells,
nucleostemin
interacts with nucleophosmin, a nucleolar protein believed to possess oncogenic potential. Nucleostemin (NS) and nucleophosmin (NPM) displayed an extremely high degree of colocalization in the granular component of the nucleolus during interphase, and both proteins associated with prenucleolar bodies in late mitosis before the reformation of nucleoli. Coimmunoprecipitation experiments revealed that NS and NPM co-reside in complexes, and yeast two-hybrid experiments confirmed that they are interactive proteins, revealing the NPM-interactive region to be the 46-amino acid N-terminal domain of NS. In bimolecular fluorescence complementation studies, bright nucleolar signals were observed, indicating that these two proteins directly interact in the nucleolus in vivo. These results support the notion that cell cycle regulatory proteins congress and interact in the nucleolus, adding to the emerging concept that this nuclear domain has functions beyond ribosome production.
...
PMID:Nucleophosmin is a binding partner of nucleostemin in human osteosarcoma cells. 1844 70
Nucleolar disassembly occurs during mitosis and nucleolar stress, releasing several MDM2-interactive proteins residing in the nucleolus that share the common activity of
p53
stabilization. Here, we demonstrate that mobilization of
nucleostemin
, a nucleolar protein enriched in cancer and stem cells, has the opposite role of stabilizing MDM2 and suppressing
p53
functions. Our results show that
nucleostemin
increases the protein stability and nucleoplasmic retention of MDM2, and competes with L23 for MDM2 binding. These activities were significantly elevated when
nucleostemin
is released into the nucleoplasm by mutations that abolish its nucleolar localization or by chemotherapeutic agents that disassemble the nucleoli. Nucleostemin depletion decreases MDM2 protein, increases transcription activity without affecting the level of
p53 protein
, and triggers G2-M arrest and cell death in U2OS cells but not in H1299 cells. This work reveals that nucleoplasmic relocation of
nucleostemin
during nucleolar disassembly safeguards the G2-M transit and survival of continuously dividing cells by MDM2 stabilization and
p53
inhibition.
...
PMID:Nucleoplasmic mobilization of nucleostemin stabilizes MDM2 and promotes G2-M progression and cell survival. 1903 82
Nucleostemin is a nucleolar protein widely expressed in proliferating cells. Nucleostemin is involved in the regulation of cell proliferation, and both depletion and overexpression of
nucleostemin
induce cell cycle arrest through the
p53
signaling pathway. Although the presence of
p53
-independent functions of
nucleostemin
has been previously suggested, the identities of these additional functions remained to be investigated. Here, we show that
nucleostemin
has a novel role as an integrated component of ribosome biogenesis, particularly pre-rRNA processing. Nucleostemin forms a large protein complex (>700 kDa) that co-fractionates with the pre-60 S ribosomal subunit in a sucrose gradient. This complex contains proteins related to pre-rRNA processing, such as Pes1, DDX21, and EBP2, in addition to several ribosomal proteins. We show that the nucleolar retention of DDX21 and EBP2 is dependent on the presence of
nucleostemin
in the nucleolus. Furthermore, the knockdown of
nucleostemin
delays the processing of 32 S pre-rRNA into 28 S rRNA. This is accompanied by a substantial decrease of protein synthesis as well as the levels of rRNAs and some mRNAs. In addition, overexpressed
nucleostemin
significantly promotes the processing of 32 S pre-rRNA. Collectively, these biochemical and functional studies demonstrate a novel role of
nucleostemin
in ribosome biogenesis. This is a key aspect of the role of
nucleostemin
in regulating cell proliferation.
...
PMID:Critical role of nucleostemin in pre-rRNA processing. 1910 11
Nucleostemin is a positive regulator of cell proliferation and is highly expressed in a variety of stem cells, tumors, and tumor cell lines. The protein shuttles between the nucleolus and the nucleus in a GTP-dependent fashion. Selective depletion of intracellular guanine nucleotides by AVN-944, an inhibitor of the de novo purine synthetic enzyme, IMP dehydrogenase, leads to the rapid disappearance of
nucleostemin
protein in tumor cell lines, an effect that does not occur with two other nucleolar proteins, nucleophosmin or nucleolin. Endogenous
nucleostemin
protein is completely stabilized by MG132, an inhibitor of the 26S proteasome, as are the levels of expressed enhanced green fluorescent protein-tagged
nucleostemin
, both wild-type protein and protein containing mutations at the G(1) GTP binding site. Nutlin-3a, a small molecule that disrupts the binding of the E3 ubiquitin ligase, Mdm2, to
p53
, stabilizes
nucleostemin
protein in the face of guanine nucleotide depletion, as does siRNA-mediated knockdown of Mdm2 expression and overexpression of a dominant-negative form of Mdm2. Neither Doxorubicin nor Actinomycin D, which cause the release of
nucleostemin
from the nucleolus, results in
nucleostemin
degradation. We conclude that
nucleostemin
is a target for Mdm2-mediated ubiquitination and degradation when not bound to GTP. Because this effect does not occur with other chemotherapeutic agents, the induction of
nucleostemin
protein degradation in tumor cells by IMP dehydrogenase inhibition or by other small molecules that disrupt GTP binding may offer a new approach to the treatment of certain neoplastic diseases.
...
PMID:Depletion of guanine nucleotides leads to the Mdm2-dependent proteasomal degradation of nucleostemin. 1931 67
Stem cells have the remarkable ability to self-renew and to generate multiple cell types. Nucleostemin is one of proteins that are enriched in many types of stem cells. Targeted deletion of
nucleostemin
in the mouse results in developmental arrest at the implantation stage, indicating that
nucleostemin
is crucial for early embryogenesis. However, the molecular basis of
nucleostemin
function in early mouse embryos remains largely unknown, and the role of
nucleostemin
in tissue stem cells has not been examined by gene targeting analyses due to the early embryonic lethality of
nucleostemin
null animals. To address these questions, we generated inducible
nucleostemin
null embryonic stem (ES) cells in which both alleles of
nucleostemin
are disrupted, but
nucleostemin
cDNA under the control of a tetracycline-responsive transcriptional activator is introduced into the Rosa26 locus. We show that loss of
nucleostemin
results in reduced cell proliferation and increased apoptosis in both ES cells and ES cell-derived neural stem/progenitor cells. The reduction in cell viability is much more profound in ES cells than in neural stem/progenitor cells, an effect that is mediated at least in part by increased induction and accumulation of
p53
and/or activated caspase-3 in ES cells than in neural stem/progenitor cells.
...
PMID:Differential requirement for nucleostemin in embryonic stem cell and neural stem cell viability. 1941 58
Several nucleolar proteins, such as ARF, ribosomal protein (RP) L5, L11, L23 and S7, have been shown to induce
p53
activation by inhibiting MDM2 E3 ligase activity and consequently to trigger cell cycle arrest and/or apoptosis. Our recent study revealed another nucleolar protein called
nucleostemin
(NS), a nucleolar GTP binding protein, as a novel regulator of the
p53
-MDM2 feedback loop. However, unlike other known nucleolar regulators of this loop, NS surprisingly plays a dual role, as both up and downregulations of its levels could turn on
p53
activity. Here, we try to offer some prospective views for this unusual phenomenon by reconciling previously and recently published studies in the field in hoping to better depict the role of NS in linking the
p53
pathway with ribosomal biogenesis during cell growth and proliferation as well as to propose NS as another potential molecular target for anti-cancer drug development.
...
PMID:Nucleostemin: Another nucleolar "Twister" of the p53-MDM2 loop. 2070 89
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