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Query: UMLS:C0027819 (
neuroblastoma
)
27,800
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Brain-derived neurotrophic factor
(
BDNF
) has recently been shown to enhance the survival of dopamine neurons in cultures derived from the embryonic rat mesencephalon. We now extend this study by demonstrating that, in addition to the effect of sustaining survival of dopaminergic neurons,
BDNF
also confers protection against the neurotoxic effects of 6-hydroxydopamine (6-OHDA) and N-methyl-4-phenylpyridinium ion (MPP+). Exposure of mesencephalic cultures to either 6-OHDA or MPP+ resulted in a loss of 70-80% of dopaminergic neurons, as determined by tyrosine hydroxylase (TH) immunocytochemistry. In
BDNF
-treated cultures, loss of TH-positive cells after exposure to either toxin was reduced to only 30%. To facilitate biochemical measurements, we studied SH-SY5Y dopaminergic
neuroblastoma
cells.
BDNF
was found to protect these cells from the dopaminergic neurotoxins, 6-OHDA and MPP+. Indicative of oxidative stress, treatment of SH-SY5Y cells with 10 microM 6-OHDA for 24 h caused a fivefold increase in the levels of oxidized glutathione (GSSG). Pretreatment with
BDNF
for 24 h completely prevented the rise in GSSG. Further examination revealed that
BDNF
increased the activity of the protective enzyme, glutathione reductase, by 100%. In contrast,
BDNF
had no effect on the activity of catalase. These results add further impetus to exploring the therapeutic potential of
BDNF
in animal models of Parkinson's disease.
...
PMID:Brain-derived neurotrophic factor protects dopamine neurons against 6-hydroxydopamine and N-methyl-4-phenylpyridinium ion toxicity: involvement of the glutathione system. 845 44
Brain-derived neurotrophic factor
(
BDNF
) and its receptors are necessary for the survival and development of many neuronal cells. Because
BDNF
and TrkB are expressed in many poor-prognosis
neuroblastoma
(NB) tumors, we evaluated the role of
BDNF
in affecting sensitivity to chemotherapeutic agents. We investigated the effects of activation of the
BDNF
-TrkB signal transduction pathway in two NB cell lines, 15N and SY5Y. 15N cells lack the high-affinity receptor p145TrkB and express
BDNF
; 15N cells were used along with 15N-TrkB cells, a subline transfected with a TrkB expression vector. In cytotoxicity assays, 15N-TrkB cells were consistently 1.4-2 fold more resistant to vinblastine than 15N cells. Drug accumulation assays showed a 50% reduction in[3H]vinblastine accumulation in 15N-TrkB cells compared with control 15N cells. Addition of 30 ng/ml
BDNF
resulted in a reduction to 46% of control in 15N cells and a reduction to 28% of control in 15N-TrkB cells. SY5Y cells were chosen as a second model because they lack both endogenous
BDNF
and TrkB expression. p145TrkB expression is induced by 1 nM retinoic acid. Vinblastine accumulation was not significantly affected by 1 nM retinoic acid in SY5Y cells. Addition of 30 ng/ml
BDNF
decreased [3H]vinblastine accumulation to 58% of control in SY5Y cells and decreased [3H]vinblastine accumulation to 62% of control in TrkB-expressing SY5Y cells. Although an increase in
BDNF
expression in seen in multidrug-resistant sublines of SY5Y and BE(2)-C NB cells, the protective effect of
BDNF
in vinblastine toxicity may be unrelated to mdr-1, because the activity of other agents transported by P-glycoprotein was not affected. There was no increase in mdr-1 expression in 1 nM RA SY5Y cells and 15N-TrkB cells, as assessed by Northern blot analysis. In addition to the effects of
BDNF
on vinblastine cytotoxicity and accumulation, there was an inhibition in the ability of vinblastine to depolymerize tubulin in
BDNF
-treated cells. Thus,
BDNF
and TrkB may partially rescue NB cells from vinblastine toxicity and thereby may contribute to a more chemoresistant phenotype.
...
PMID:Brain-derived neurotrophic factor protects neuroblastoma cells from vinblastine toxicity. 870 17
Brain-derived neurotrophic factor
(
BDNF
) promotes neuronal survival. Gaining an understanding of how
BDNF
, via the tropomyosin-related kinase B (TRKB) receptor, elicits specific cellular responses is of contemporary interest. Expression of mutant TrkB in fibroblasts, where tyrosine 484 was changed to phenylalanine, abrogated Shc association with TrkB, but only attenuated and did not block
BDNF
-induced phosphorylation of mitogen-activated protein kinase (MAPK). This suggests there is another
BDNF
-induced signaling mechanism for activating MAPK, which compelled a search for other TrkB substrates.
BDNF
induces phosphorylation of fibroblast growth factor receptor substrate 2 (FRS2) in both fibroblasts engineered to express TrkB and human
neuroblastoma
(NB) cells that naturally express TrkB. Additionally,
BDNF
induces phosphorylation of FRS2 in primary cultures of cortical neurons, thus showing that FRS2 is a physiologically relevant substrate of TrkB. Data are presented demonstrating that
BDNF
induces association of FRS2 with growth factor receptor-binding protein 2 (GRB2) in cortical neurons, fibroblasts, and NB cells, which in turn could activate the RAS/MAPK pathway. This is not dependent on Shc, since
BDNF
does not induce association of Shc and FRS2. Finally, the experiments suggest that FRS2 and suc-associated neurotrophic factor-induced tyrosine-phosphorylated target are the same protein.
...
PMID:Brain-derived neurotrophic factor induces phosphorylation of fibroblast growth factor receptor substrate 2. 1019 22
Brain-derived neurotrophic factor
(
BDNF
) promotes neuronal survival and protection against neuronal damage. We addressed whether
BDNF
might promote survival and chemoprotection in
neuroblastoma
(NB) using a drug-sensitive human NB cell line. All-trans-retinoic acid (ATRA) induces a striking phenotypic differentiation of NB1643 cells, and exogenous
BDNF
treatment promotes survival of these differentiated cells. ATRA induces TRKB expression, and exogenous
BDNF
stimulates both autophosphorylation of TRKB and induction of the immediate early gene, FOS, in these cells.
BDNF
mRNA is expressed in NB1643 cells. Because the time course of TRKB induction closely parallels phenotypic differentiation of these cells, it seems probable that ATRA induces differentiation of NB1643 cells by establishing an autocrine loop involving
BDNF
and TRKB. Exogenous
BDNF
treatment resulted in a further increase in neurite outgrowth, which again suggests that an autocrine loop is involved in differentiation of NB1643 cells in response to ATRA. We then tested whether
BDNF
might afford drug resistance in NB and found that
BDNF
does indeed protect in this NB model against cisplatin, a DNA-damaging agent actually used in the treatment of NB.
...
PMID:Brain-derived neurotrophic factor promotes survival and chemoprotection of human neuroblastoma cells. 1034 7
Brain-derived neurotrophic factor
(
BDNF
) is a major neurotrophin in the brain and abnormal regulation of
BDNF
may contribute to the pathophysiology of mood disorders. In the present study, we examined if alterations in the activity of glycogen synthase kinase-3-beta (GSK3beta) or treatment with mood stabilizers modulated
BDNF
-mediated signal transduction pathways in differentiated human
neuroblastoma
SH-SY5Y cells.
BDNF
increased the phosphorylation of the forkhead transcription factor FKHRL1 through activation of the phosphatidylinositol 3-kinase (PI3K)/Akt signaling pathway, and the phosphorylation of the cyclic AMP response element binding protein (CREB) through activation of extracellular signal-regulated kinase1/2 (ERK1/2).
BDNF
also increased serine(9) -phosphorylation of GSK3beta, which inhibits GSK3beta activity. Overexpression of GSK3beta did not affect
BDNF
-induced phosphorylation of Akt, ERK1/2, or FKHRL1, but abolished CREB phosphorylation induced by
BDNF
. This inhibition of
BDNF
-induced CREB phosphorylation in GSK3beta-overexpressing SH-SY5Y cells was blocked by treatment with lithium. In contrast to lithium, sodium valproate and lamotrigine did not affect
BDNF
-mediated signaling, whereas carbamazepine induced a rapid and prolonged phosphorylation of ERK1/2 and CREB in the absence or the presence of
BDNF
. Therefore, increased GSK3beta selectively attenuates
BDNF
-induced CREB phosphorylation, and lithium and carbamazepine can facilitate activation of CREB.
...
PMID:BDNF-mediated signal transduction is modulated by GSK3beta and mood stabilizing agents. 1209 67
Brain-derived neurotrophic factor
(
BDNF
) signaling through its receptor TRKB modulates survival, differentiation, and activity of neurons.
BDNF
activates TRKB on the cell surface, which leads to the initiation of intracellular signaling cascades and different biological responses in neurons. Neuronal activity has been shown to regulate TRKB levels on the plasma membrane of neurons, but little is known about other factors affecting TRKB surface expression levels. We report here that
BDNF
regulates the cell surface levels of transfected or endogenously expressed full-length TRKB, depending on the exposure time in
neuroblastoma
cells and primary hippocampal neurons.
BDNF
rapidly increases TRKB surface expression levels in seconds, whereas treatment of cells with
BDNF
for a longer time (minutes to hours) leads to decreased TRKB surface levels. Coexpression of the full-length TRKB together with the truncated TRKB.T1 isoform results in decreased levels of full-length TRKB on the cell surface. This effect is specific to the T1 isoform, because coexpression of a kinase-dead TRKB mutant or another kinase domain-lacking TRKB form, truncated T-Shc, leads to increased TRKB surface levels. Our results suggest that regulation of TRKB surface expression levels by different factors is tightly controlled by complex mechanisms in active neurons.
...
PMID:Regulation of TRKB surface expression by brain-derived neurotrophic factor and truncated TRKB isoforms. 1220 82
To understand the functional interactions between the TrkA and p75 nerve growth factor (NGF) receptors, we stably transfected LAN5
neuroblastoma
cells with an expression vector for ET-R, a chimeric receptor with the extracellular domain of the epidermal growth factor receptor (EGFR), and the TrkA transmembrane and intracellular domains. EGF activated the ET-R kinase and induced partial differentiation. NGF, which can bind to endogenous p75, did not induce differentiation but enhanced the EGF-induced response, leading to differentiation of almost all cells. A mutated NGF, 3T-NGF, that binds to TrkA but not to p75 did not synergize with EGF. Enhancement of EGF-induced differentiation required at least nanomolar concentrations of NGF, consistent with the low-affinity p75 binding site. EGF may induce a limited number of neuronal cells because it also enhanced apoptosis. Both NGF and a caspase inhibitor reduced apoptosis and, thereby, enhanced differentiation. NGF seems to enhance survival through the phosphatidylinositol-3 kinase (PI3K) pathway. Consistent with this hypothesis, Akt, a downstream effector of the PI3K pathway, was hyperphosphorylated in the presence of EGF+NGF. These results demonstrate that TrkA kinase initiates differentiation, and p75 enhances differentiation by rescuing differentiating cells from apoptosis via the PI3K pathway. Even though both EGF and NGF are required for differentiation of LAN5/ET-R cells, only NGF is required for survival of the differentiated cells. In the absence of NGF, the cells die by an apoptotic mechanism, involving caspase-3. An anti-p75 antibody blocked the survival effect of NGF.
Brain-derived neurotrophic factor
also enhanced cell survival, indicating that in differentiated cells, NGF acts through the p75 receptor to prevent apoptosis.
...
PMID:Novel functional interactions between Trk kinase and p75 neurotrophin receptor in neuroblastoma cells. 1250 79
The amyloid precursor protein (APP) belongs to a conserved gene family, also including the amyloid precursor-like proteins, APLP1 and APLP2. We have previously shown that all members of the APP protein family are up-regulated upon retinoic acid (RA)-induced neuronal differentiation of SH-SY5Y
neuroblastoma
cells. Here, we demonstrate that RA also affects the processing of APLP2 and APP, as shown by increased shedding of both sAPLP2 and sAPPalpha, as well as elevated levels of the APP intracellular domains (AICDs).
Brain-derived neurotrophic factor
(
BDNF
) has been reported to induce APP promoter activity and RA induces expression of the tyrosine kinase receptor B (TrkB) in
neuroblastoma
cells. We show that the increase in shedding of both APLP2 and APP in response to RA is not mediated through the TrkB receptor. However,
BDNF
concomitant with RA increased the expression of APP even further. In addition, the secretion of sAPLP2 and sAPPalpha as well as the levels of AICDs were increased in response to
BDNF
. In contrast, the levels of membrane-bound APP C-terminal fragment C99 significantly decreased. Our results suggest that RA and
BDNF
shifts APP processing towards the alpha-secretase pathway. In addition, we show that RA and
BDNF
regulate N-linked glycosylation of APLP1.
...
PMID:Increased processing of APLP2 and APP with concomitant formation of APP intracellular domains in BDNF and retinoic acid-differentiated human neuroblastoma cells. 1615 56
Alzheimer's disease (AD) is a senile dementia characterized by amyloid plaques, neurofibrillary tangles, and synaptic and cell loss. The "amyloid cascade" hypothesis suggests that amyloid-beta (Abeta), the peptide deposited as amyloid plaques, is the primary insult in AD. However, debate continues over the mechanism of Abeta toxicity and whether fibrillar or oligomeric Abeta is the active species of the peptide that ultimately causes the synaptic loss and dementia associated with AD.
Brain-derived neurotrophic factor
(
BDNF
) is required for survival and function of cells compromised in AD. Decreased
BDNF
causes defects in long-term potentiation and memory and correlates with cognitive decline. We previously demonstrated that
BDNF
reduction occurs early in the course of AD, suggesting that decreased
BDNF
may promote neuronal dysfunction in AD. We also demonstrated that three of seven human
BDNF
transcripts are specifically downregulated in AD. What pathological feature(s) of AD leads to the decreased
BDNF
is unknown. In this study, we administered both fibrillar and oligomeric conformations of Abeta(1-42) to differentiated SH-SY5Y, a human
neuroblastoma
cell line, and measured both phosphorylated cAMP response element-binding protein (CREB), a regulator of
BDNF
transcription, and
BDNF
total mRNA. We found that oligomeric but not fibrillar preparations of Abeta(1-42) significantly decrease both phosphorylated CREB and total
BDNF
mRNA. Furthermore, oligomeric Abeta(1-42) decreases
BDNF
transcripts IV and V in these cells, demonstrating that Abeta(1-42) downregulates the major
BDNF
transcript decreased in vivo in the AD brain. Thus, oligomeric Abeta(1-42) could compromise neuronal function, causing memory loss and cognitive dysfunction by downregulation of
BDNF
in AD.
...
PMID:Oligomeric amyloid decreases basal levels of brain-derived neurotrophic factor (BDNF) mRNA via specific downregulation of BDNF transcripts IV and V in differentiated human neuroblastoma cells. 1734
Chemokine receptors, and in particular CXCR4 and CCR5 play a key role in the neuropathogenesis of Human Immunodeficiency Virus-1 (HIV)4 associated dementia (HAD). Thus, new insight into the expression of CXCR4 in the central nervous system may help develop therapeutic compounds against HAD.
Brain-derived neurotrophic factor
(
BDNF
) is neuroprotective in vitro against two strains of the HIV envelope protein gp120 that binds to CXCR4 or CCR5. Therefore, we examined whether
BDNF
modulates chemokine receptor expression in vivo. The content of CXCR4 mRNA and proteins was determined in the cerebral cortex and hippocampus of 6-month-old
BDNF
heterozygous mice and wild type littermates by using polymerase chain reaction and immunohistochemistry, respectively.
BDNF
heterozygous mice exhibited an increase in CXCR4 mRNA compared to wild type. Histological analyses revealed an up-regulation of CXCR4 immunoreactivity mainly in neurons. Most of these neurons were positive for TrkB, the
BDNF
receptor with a tyrosine kinase activity. Increases in CXCR4 mRNA levels were observed in 18-month-old
BDNF
heterozygous mice but not in 7-day-old mice, suggesting that the modulatory role of
BDNF
occurs only in mature animals. To determine whether
BDNF
affects also CXCR4 internalization, SH-SY5Y
neuroblastoma
cells were exposed to
BDNF
and cell surface CXCR4 levels were measured at various times.
BDNF
induced CXCR4 internalization within minutes. Lastly,
BDNF
heterozygous mice showed higher levels of CCR5 and CXCR3 mRNA than wild type in the cerebral cortex, hippocampus and striatum. Our data indicate that
BDNF
may modulate the availability of chemokine receptors implicated in HIV infection.
...
PMID:Brain-derived neurotrophic factor modulates expression of chemokine receptors in the brain. 1858 60
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