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Query: UNIPROT:P42345 (
mTOR
)
26,049
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The autosomal dominantly inherited disease tuberous sclerosis (TSC) affects approximately 1 in 6000 individuals and is characterized by the development of tumors, named hamartomas, in different organs. TSC1, encoding hamartin, and TSC2, encoding
tuberin
are tumor suppressor genes responsible for TSC. Hamartin and
tuberin
form a complex, of which
tuberin
is assumed to be the functional component. The TSC proteins have been implicated in the control of cell cycle by activating the cyclin-dependent kinase inhibitor p27 and in cell size regulation by inhibiting the
mammalian target of rapamycin
(
mTOR
)/p70S6K cascade. Phosphorylation of S939 and T1462 by Akt downregulates
tuberin
's potential to inhibit
mTOR
/p70S6K. Here, we show that this
tuberin
phosphorylation by Akt does not affect
tuberin
-mediated control of p27 protein amounts. This demonstrates that regulating p27 protein amounts and
mTOR
/p70S6K are separable functions of
tuberin
. Furthermore, we found that phosphorylation by Akt triggers upregulation of cytoplasmic and downregulation of nuclear
tuberin
. In cycling cells with high Akt activity,
tuberin
is predominantly localized to the cytoplasm. In arrested G0 cells with downregulated Akt activity, a significant proportion of
tuberin
is localized to the nucleus. Upon re-entry into the normal ongoing cell cycle, nuclear localization of
tuberin
is downregulated parallel to the activation of Akt. Recently, the
mTOR
/p70S6K cascade has been demonstrated to exist in both the cytoplasm and nucleus. We here also found that
tuberin
harbors the potential to regulate p70S6K activity in both the cytoplasm and nucleus. This description of functional
tuberin
in the cytoplasm and the nucleus together with our observation of Akt-controlled and cell cycle-regulated
tuberin
localization are of particular interest for a further understanding of
tuberin
's function as a gate keeper of the G0 cell status as well as of Akt's activity to control cell proliferation.
...
PMID:Akt regulates nuclear/cytoplasmic localization of tuberin. 1686 80
Androgen receptor (AR) plays a central role in prostate cancer, with most tumors responding to androgen deprivation therapies, but the molecular basis for this androgen dependence has not been determined. Androgen [5alpha-dihydrotestosterone (DHT)] stimulation of LNCaP prostate cancer cells, which have constitutive phosphatidylinositol 3-kinase (PI3K)/Akt pathway activation due to PTEN loss, caused increased expression of cyclin D1, D2, and D3 proteins, retinoblastoma protein hyperphosphorylation, and cell cycle progression. However, cyclin D1 and D2 message levels were unchanged, indicating that the increases in cyclin D proteins were mediated by a post-transcriptional mechanism. This mechanism was identified as
mammalian target of rapamycin
(
mTOR
) activation. DHT treatment increased
mTOR
activity as assessed by phosphorylation of the downstream targets p70 S6 kinase and 4E-BP1, and
mTOR
inhibition with rapamycin blocked the DHT-stimulated increase in cyclin D proteins. Significantly, DHT stimulation of
mTOR
was not mediated through activation of the PI3K/Akt or mitogen-activated protein kinase/p90 ribosomal S6 kinase pathways and subsequent tuberous sclerosis complex 2/
tuberin
inactivation or by suppression of AMP-activated protein kinase. In contrast,
mTOR
activation by DHT was dependent on AR-stimulated mRNA synthesis. Oligonucleotide microarrays showed that DHT-stimulated rapid increases in multiple genes that regulate nutrient availability, including transporters for amino acids and other organic ions. These results indicate that a critical function of AR in PTEN-deficient prostate cancer cells is to support the pathologic activation of
mTOR
, possibly by increasing the expression of proteins that enhance nutrient availability and thereby prevent feedback inhibition of
mTOR
.
...
PMID:Androgens induce prostate cancer cell proliferation through mammalian target of rapamycin activation and post-transcriptional increases in cyclin D proteins. 1688 82
The Kaposi's sarcoma-associated herpesvirus (KSHV), the infectious causative agent of Kaposi's sarcoma (KS), encodes a G protein-coupled receptor (vGPCR) implicated in the initiation of KS. Here we demonstrate that Kaposi's sarcomagenesis involves stimulation of
tuberin
(TSC2) phosphorylation by vGPCR, promoting the activation of
mTOR
through both direct and paracrine mechanisms. Pharmacologic inhibition of
mTOR
with rapamycin prevented vGPCR sarcomagenesis, while overactivation of this pathway was sufficient to render endothelial cells oncogenic. Moreover, mice haploinsufficient for TSC2 are predisposed to vascular sarcomas remarkably similar to KS. Collectively, these results implicate
mTOR
in KS initiation and suggest that the sarcomagenic potential of KSHV may be a direct consequence of the profound sensitivity of endothelial cells to vGPCR dysregulation of the TSC2/
mTOR
pathway.
...
PMID:The TSC2/mTOR pathway drives endothelial cell transformation induced by the Kaposi's sarcoma-associated herpesvirus G protein-coupled receptor. 1690 12
The products of the tuberous sclerosis complex (TSC) genes, hamartin and
tuberin
(TSC1 and 2), form a heteromer, which represses the kinase
mammalian target of rapamycin
. Loss of TSC1 or 2 results in diseases characterized by loss of cell-cycle control, including TSC and lymphangioleiomyomatosis. As
tuberin
has multiple signaling inputs, including phosphatidylinositide-3-OH kinase, mitogen-activated protein kinase, and adenosine monophosphate kinase, we postulated
tuberin
would have multiple protein interactions governed by subcellular localization and cellular status and examined this in primary human airway smooth muscle cells. Using immunofluorescence and confocal microscopy,
tuberin
was detected in cytoplasm, nucleus, nucleoli, and mitochondria. Fractionation of synchronized airway smooth cells showed that
tuberin
enters the nucleus in late G(1), and passage through the cell cycle is necessary for nuclear entry. Deletion constructs showed localization sequences for the nucleus between amino acids 1351 and 1807, for mitochondria between 901 and 1350, and for cytoplasmic speckles between 1 and 450. Using fluorophore-tagged proteins, we observed fluorescence resonance energy transfer between
tuberin
and hamartin within these speckles, indicating a direct interaction between the proteins at this site. The observations that
tuberin
is localized to mitochondria and translocated to the nucleus in G(1) are novel and consistent with interactions with proteins within multiple signaling pathways. Dynamic relocalization of
tuberin
may control these interactions to integrate these pathways. As
tuberin
has potential roles in proliferation, migration, and cell phenotype, it therefore warrants further investigation in diseases categorized by abnormalities in airway smooth muscle.
...
PMID:Subcellular distribution of the TSC2 gene product tuberin in human airway smooth muscle cells is driven by multiple localization sequences and is cell-cycle dependent. 1690 38
Inhibitors of the
mammalian target of rapamycin
(
mTOR
) are currently in clinical trials for the treatment of breast cancer. The mechanisms through which
mTOR
are activated in breast cancer and the relationship of
mTOR
activation to steroid hormones, such as estrogen, that are known to influence breast cancer pathogenesis, are not yet understood. Using MCF-7 cells as a model, we found that 17-beta estradiol (E(2)) rapidly increased the phosphorylation of downstream targets of
mTOR
: p70 ribosomal protein S6 kinase, ribosomal protein S6, and eukaryotic initiation factor 4E-binding protein 1. The phosphoinositide-3-kinase inhibitor, wortmannin, and the
mTOR
inhibitor, rapamycin, blocked E(2)-induced activation of p70 ribosomal protein S6 kinase. We hypothesized that
tuberin
and the small GTPase Ras homologue enriched in brain (Rheb), regulators of the
mTOR
pathway, mediate E(2)-induced activation of
mTOR
. Consistent with this hypothesis, E(2) rapidly (within 5 minutes) stimulated
tuberin
phosphorylation at T1462, a site at which Akt phosphorylates and inactivates
tuberin
. E(2) also rapidly decreased the inactive, GDP-bound form of Rheb. Finally, we found that small interfering RNA down-regulation of endogenous Rheb blocked the E(2)-stimulated proliferation of MCF-7 cells, demonstrating that Rheb is a key determinant of E(2)-dependent cell growth. Taken together, these data reveal that the TSC/Rheb/
mTOR
pathway plays a critical role in the regulation of E(2)-induced proliferation, and highlight Rheb as a novel molecular target for breast cancer therapy.
...
PMID:Estrogen-induced activation of mammalian target of rapamycin is mediated via tuberin and the small GTPase Ras homologue enriched in brain. 1701 1
Tuberous sclerosis complex (TSC) is a multisystem disorder that affects numerous organ systems. Brain lesions that form during development, known as tubers, are highly associated with epilepsy, cognitive disability, and autism. Following the identification of two genes and their encoded proteins, TSC1 (hamartin) and TSC2 (
tuberin
), responsible for TSC, identification of several downstream protein cascades that might be affected in TSC have been discovered. Of primary importance is the
mammalian target of rapamycin
pathway that controls cell growth and protein synthesis. The mechanisms governing brain lesion growth have not been fully identified but likely altered regulation of the
mammalian target of rapamycin
cascade by hamartin and
tuberin
during development leads to aberrant cell growth. Secondary effects of TSC gene mutations might disrupt normal neuronal migration and cerebral cortical lamination. Numerous studies have identified changes in gene and protein expression in animal models of TSC and in human TSC brain specimens that contribute to altered brain cytoarchitecture. This review will provide an overview of the neurobiological aspects of TSC.
...
PMID:The neurobiology of the tuberous sclerosis complex. 1702 74
Tuberous sclerosis (TS), autosomal dominant disorder manifested by the formation of usually benign tumors in the brain, heart, kidneys and skin, results from an inactivating mutation in one of two tumor suppressor genes TSC1 or TSC2. Protein products of these genes, hamartin and
tuberin
, respectively, have been shown to participate in the
mTOR
pathway controlling translation of approx. 10-15% of all proteins. In the current paper, we aimed at verifying whether hamartin and
tuberin
may also be implicated in the control of gene transcription. Very recently it has been hypothesized that the pathway triggered by WNT, one of embryonic growth factors involved in cell differentiation and migration, could be disturbed in TS. In order to test this hypothesis we evaluated samples of four subependymal giant cell astrocytomas (SEGAs), brain tumors developing in the progress of TS. We found that beta-catenin, transcription factor and mediator of WNT pathway activity is indeed present and active in SEGAs. mRNA transcripts for c-Myc and N-Myc, proteins whose transcription is regulated by beta-catenin, were upregulated in two of four SEGAs, while cyclin D1 mRNA was significantly higher in three SEGAs. At the same time, c-Myc and N-Myc proteins were detected in the same two samples. Thus, we show for the first time that aberrant WNT signaling may contribute to the pathogenesis of TS-associated SEGAs.
...
PMID:Upregulation of the WNT pathway in tuberous sclerosis-associated subependymal giant cell astrocytomas. 1707 Oct 37
The
mammalian target of rapamycin
(
mTOR
), a critical modulator of cell growth, acts to integrate signals from hormones, nutrients, and growth-promoting stimuli to downstream effector mechanisms involved in the regulation of protein synthesis. Dexamethasone, a synthetic glucocorticoid that represses protein synthesis, acts to inhibit
mTOR
signaling as assessed by reduced phosphorylation of the downstream targets S6K1 and 4E-BP1. Dexamethasone has also been shown in one study to up-regulate the expression of REDD1 (also referred to RTP801, a novel stress-induced gene linked to repression of
mTOR
signaling) in lymphoid, but not nonlymphoid, cells. In contrast to the findings of that study, here we demonstrate that REDD1, but not REDD2, mRNA expression is dramatically induced following acute dexamethasone treatment both in rat skeletal muscle in vivo and in L6 myoblasts in culture. In L6 myoblasts, the effect of the drug on
mTOR
signaling is efficiently blunted in the presence of REDD1 RNA interference oligonucleotides. Moreover, the dexamethasone-induced assembly of the
mTOR
regulatory complex
Tuberin
. Hamartin is disrupted in L6 myoblasts following small interfering RNA-mediated repression of REDD1 expression. Finally, overexpression of Rheb, a downstream target of
Tuberin
function and a positive upstream effector of
mTOR
, reverses the effect of dexamethasone on phosphorylation of
mTOR
substrates. Overall, the data support the conclusion that REDD1 functions upstream of
Tuberin
and Rheb to down-regulate
mTOR
signaling in response to dexamethasone.
...
PMID:Dexamethasone represses signaling through the mammalian target of rapamycin in muscle cells by enhancing expression of REDD1. 1707 51
Recent work has uncovered a functional link between polycystin-1 (PC1), the protein affected in autosomal-dominant polycystic kidney disease (ADPKD) and
tuberin
, the protein affected in tuberous sclerosis complex (TSC). These data suggest that PC1 functions by inducing the formation of a complex with
tuberin
and the Ser/Thr kinase
mTOR
thereby inhibiting
mTOR
activity. In normal, adult kidney,
mTOR
is inactive. However, it is activated in response to insults and required for proliferative and hyperthrophic repair processes. We propose a model in which the PC1-
tuberin
-
mTOR
complex functions to sense renal insults, possibly by ciliary mechanotransduction, and regulates the activity of
mTOR
to trigger a formal repair program. In ADPKD, defects in PC1 would lead to constitutive activation of
mTOR
, and the affected cells would be engaged in a permanent state of futile repair leading to the formation and growth of renal cysts. The
mTOR
inhibitor rapamycin has proven highly effective in preventing and even reversing cyst growth in rodent models of polycystic kidney disease resulting in preservation of renal function.
mTOR
inhibitors, already in clinical use as immunosuppressants, may therefore be promising for future therapeutic approaches for ADPKD.
...
PMID:Regulation of mTOR by polycystin-1: is polycystic kidney disease a case of futile repair? 1710 41
The mechanisms regulating initiation of mRNA translation for the generation of protein products that mediate interferon (IFN) responses are largely unknown. We have previously shown that both Type I and II IFNs engage the
mammalian target of rapamycin
(
mTOR
), resulting in downstream phosphorylation and deactivation of the translational repressor 4E-BP1 (eIF4E-binding protein 1). In the current study, we provide direct evidence that such regulation of 4E-BP1 by IFNalpha or IFNgamma results in sequential dissociation of 4E-BP1 from eukaryotic initiation factor-4E and subsequent formation of a functional complex between eukaryotic initiation factor-4E and eukaryotic initiation factor-4G, to allow initiation of mRNA translation. We also demonstrate that the induction of key IFNalpha- or IFNgamma-inducible proteins (ISG15 (interferon-stimulated gene 15) and CXCL10) that mediate IFN responses are enhanced in 4E-BP1 (4E-BP1(-/-)) knockout MEFs, as compared with wild-type 4E-BP1(+/+) MEFs. On the other hand, IFN-dependent transcriptional regulation of the Isg15 and Cxcl10 genes is intact in the absence of 4E-BP1, as determined by real time reverse transcriptase-PCR assays and promoter assays for ISRE and GAS, establishing that 4E-BP1 plays a selective negative regulatory role in IFN-induced mRNA translation. Interestingly, the induction of expression of ISG15 and CXCL10 proteins by IFNs was also strongly enhanced in cells lacking expression of the
tuberin
(TSC2(-/-)) or hamartin (TSC1(-/-)) genes, consistent with the known negative regulatory effect of the TSC1-TSC2 complex on
mTOR
activation. In other work, we demonstrate that the induction of an IFN-dependent antiviral response is strongly enhanced in cells lacking expression of 4E-BP1 and TSC2, demonstrating that these elements of the IFN-activated
mTOR
pathway exhibit important regulatory effects in the generation of IFN responses. Taken altogether, our data suggest an important role for
mTOR
-dependent pathways in IFN signaling and identify 4E-BP1 and TSC1-TSC2 as key components in the generation of IFN-dependent biological responses.
...
PMID:Regulatory effects of mammalian target of rapamycin-activated pathways in type I and II interferon signaling. 1711 81
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