Your search keyword '"Growth factors -- Influence"' showing total 9 results

1. A vascular endothelial growth factor mimetic accelerates gastric ulcer healing in an iNOS-dependent manner

Author

Dudar, Genevieve K., D'Andrea, Luca D., Di Stasi, Rossella, Pedone, Carlo, and Wallace, John L.

Subjects

Stomach ulcer -- Physiological aspects, Growth factors -- Influence, Neovascularization -- Evaluation, Biological sciences

Abstract

Angiogenesis is crucial to all types of wound healing, including gastric ulcer healing. The most potent promoter of angiogenesis is vascular endothelial growth factor (VEGF). We hypothesized that a 15-amino acid peptide designed to mimic the angiogenic action of VEGF would accelerate gastric ulcer healing. Gastric ulcers were induced in mice by serosal application of acetic acid. Treatment with the VEGF mimetic accelerated gastric ulcer healing when administered orally or intraperitoneally, at a dose of 50 ng/kg or greater. Such healing was not observed when the reverse sequence pentadecapeptide or the full-length VEGF protein was administered. Contrary to our hypothesis, the VEGF mimetic did not significantly increase angiogenesis in the ulcerated stomach. The enhancement of ulcer healing by the VEGF mimetic occurred independently of cyclooxygenase-2 (COX-2) activity but was blocked by inhibitors of inducible nitric oxide synthase (iNOS). These results demonstrate that a VEGF mimetic is a potent stimulus for gastric ulcer healing, even when given orally. The effects of the mimetic were independent of stimulatory effects on angiogenesis and COX-2 activity but were dependent on iNOS-derived NO production. stomach; nitric oxide; cyclooxygenase; angiogenesis; prostaglandin; gastric mucosa

Published

2008

2. GDNF is a fast-acting potent inhibitor of alcohol consumption and relapse

Author

Carnicella, Sebastien, Kharazia, Viktor, Jeanblanc, Jerome, Janak, Patricia H., and Ron, Dorit

Subjects

Growth factors -- Properties, Growth factors -- Influence, Drinking of alcoholic beverages -- Control, Glial cell line-derived neurotrophic factor -- Properties, Glial cell line-derived neurotrophic factor -- Influence, Science and technology

Abstract

Previously, we demonstrated that the action of the natural alkaloid, ibogaine, to reduce alcohol (ethanol) consumption is mediated by the glial cell line-derived neurotrophic factor (GDNF) in the ventral tegmental area (VTA). Here we set out to test the actions of GDNF in the VTA on ethanol-drinking behaviors. We found that GDNF infusion very rapidly and dose-dependently reduced rat ethanol, but not sucrose, operant self-administration. A GDNF-mediated decrease in ethanol consumption was also observed in rats with a history of high voluntary ethanol intake. We found that the action of GDNF on ethanol consumption was specific to the VTA as infusion of the growth factor into the neighboring substantia nigra did not affect operant responses for ethanol. We further show that intra-VTA GDNF administration rapidly activated the MAPK signaling pathway in the VTA and that inhibition of the MAPK pathway in the VTA blocked the reduction of ethanol self-administration by GDNF. Importantly, we demonstrate that GDNF infused into the VTA alters rats' responses in a model of relapse. Specifically, GDNF application blocked reacquisition of ethanol self-administration after extinction. Together, these results suggest that GDNF, via activation of the MAPK pathway, is a fast-acting selective agent to reduce the motivation to consume and seek alcohol. addiction | growth factor | self-administration

Published

2008

3. Insulin-like growth factor I and II regulate the life cycle of trophoblast in the developing human placenta

Author

Forbes, Karen, Westwood, Melissa, Baker, Philip N., and Aplin, John D.

Subjects

Trophoblast -- Growth, Apoptosis -- Evaluation, Cell proliferation -- Evaluation, Growth factors -- Influence, Company growth, Biological sciences

Abstract

The main disorders of human pregnancy are rooted in defective placentation. Normal placental development depends on proliferation, differentiation, and fusion of cytotrophoblasts to form and maintain an overlying syncytiotrophoblast. There is indirect evidence that the insulin-like growth factors (IGFs), which are aberrant in pregnancy disorders, are involved in regulating trophoblast turnover, but the processes that control human placental growth are poorly understood. Using an explant model of human first-trimester placental villus in which the spatial and ontological relationships between cell populations are maintained, we demonstrate that cytotrophoblast proliferation is enhanced by IGF-I/IGF-II and that both factors can rescue cytotrophoblast from apoptosis. Baseline cytotrophoblast proliferation ceases in the absence of syncytiotrophoblast, although denuded cytotrophoblasts can proliferate when exposed to IGF and the rate of cytotrophoblast differentiation/fusion and, consequently, syncytial regeneration, increases. Use of signaling inhibitors suggests that IGFs mediate their effect on cytotrophoblast proliferation/syncytial formation through the MAPK pathway, whereas effects on survival are regulated by the phosphoinositide 3-kinase pathway. These results show that directional contact between cytotrophoblast and syncytium is important in regulating the relative amounts of the two cell populations. However, IGFs can exert an exogenous regulatory influence on placental growth/development, suggesting that manipulation of the placental IGF axis may offer a potential therapeutic route to the correction of inadequate placental growth. proliferation; apoptosis; signaling

Published

2008

4. A model for neuronal competition during development

Author

Deppmann, Christopher D., Mihalas, Stefan, Sharma, Nikhil, Lonze, Bonnie E., Niebur, Ernst, and Ginty, David D.

Subjects

Gene expression -- Physiological aspects, Neurons -- Properties, Neurons -- Models, Growth factors -- Influence, Growth factors -- Genetic aspects, Apoptosis -- Research

Published

2008

5. A central role for hepatocyte growth factor in adipose tissue angiogenesis

Author

Bell, Lauren N., Cai, Liying, Johnstone, Brian H., Traktuev, Dmitry O., March, Keith L., and Considine, Robert V.

Subjects

Neovascularization -- Research, Adipose tissues -- Properties, Growth factors -- Properties, Growth factors -- Influence, Liver cells -- Properties, Biological sciences

Abstract

Hepatocyte growth factor (HGF) is a potent mitogenic and angiogenic factor produced in human adipose tissue. In this study, we use 3T3-F442A preadipocytes to study the contribution of HGF to angiogenesis in an in vivo fat pad development model. As observed for human adipocytes, HGF is synthesized and secreted by 3T3-F442A preadipocytes and mature adipocytes. HGF knockdown with small-interfering RNA reduced HGF mRNA expression 82.3 [+ or -] 4.2% and protein secretion 82.9 [+ or -] 1.4% from 3T3-F442A preadipocytes. Silencing of HGF resulted in a 70.5 [+ or -] 19.0% reduction in endothelial progenitor cell migration to 3T3-F442A-conditioned medium in vitro. 3T3-F442A preadipocytes injected under the skin of mice form a fat pad containing mature, lipid-filled adipocytes and a functional vasculature. At 72 h postinjection, expression of the endothelial cell genes TIE-1 and platelet endothelial cell adhesion molecule (PECAM)-1 was decreased 94.4 [+ or -] 2.2 and 91.5 [+ or -] 2.5%, respectively, in 3T3-F442A fat pads with HGF silencing. Knockdown of HGF had no effect on differentiation of 3T3-F442A preadipocytes to mature adipocytes in vitro or in vivo. In developing fat pads under the skin of HGF overexpressing transgenic mice, TIE-1 and PECAM-1 mRNA was increased 16.5- and 21.4-fold, respectively, at 72 h postinjection. The increase in gene expression correlated with immunohistochemical evidence of endothelial cell migration in the developing fat pad. These data suggest that HGF has a central role in regulating angiogenesis in adipose tissue. obesity; neovascularization; 3T3-F442A; tie-1; platelet endothelial cell adhesion molecule-1

Published

2008

6. Keratinocyte growth factor protects against elastase-induced pulmonary emphysema in mice

Author

Plantier, Laurent, Marchand-Adam, Sylvain, Antico, Valeria G., Boyer, Laurent, De Coster, Cecile, Marchal, Joelle, Bachoual, Rafik, Mailleux, Arnaud, Boczkowski, Jorge, and Crestani, Bruno

Subjects

Keratinocytes -- Properties, Growth factors -- Influence, Emphysema, Pulmonary -- Physiological aspects, Mice -- Physiological aspects, Biological sciences

Abstract

Pulmonary emphysema is characterized by persistent inflammation and progressive alveolar destruction. The keratinocyte growth factor (KGF) favorably influences alveolar maintenance and repair and possesses anti-inflammatory properties. We aimed to determine whether exogenous KGF prevented or corrected elastase-induced pulmonary emphysema in vivo. Treatment with 5 mg x [kg.sup.-1] x [day.sup.-1] KGF before elastase instillation prevented pulmonary emphysema. This effect was associated with 1) a sharp reduction in bronchoalveolar lavage fluid total protein and inflammatory cell recruitment, 2) a reduction in the pulmonary expression of the chemokines CCL2 (or monocyte chemoattractant protein-l) and CXCL2 (or macrophage inflammatory protein-2[alpha]) and of the adhesion molecules ICAM-1 and VCAM-1, 3) a reduction in matrix metalloproteinase (MMP)-2 and MMP-9 activity at day 3, and 4) a major reduction in DNA damage detected by terminal deoxynucleotidyltransferase-mediated dUTP nick end labeling (TUNEL) in alveolar cells at day 7. Treatment with KGF after elastase instillation had no effect on elastase-induced emphysema despite the conserved expression of the KGF receptor in the lungs of elastase-instilled animals as determined by immunohistochemistry. In vitro, KGF abolished the elastase-induced increase in CCL2, CXCL2, and ICAM-1 mRNA in the MLE-12 murine alveolar epithelial cell line. We conclude that KGF pretreatment protected against elastase-induced pulmonary inflammation, activation of MMPs, alveolar cell DNA damage, and subsequent emphysema in mice. inflammation; chronic obstructive pulmonary disease

Published

2007

7. Involvement of insulin-like growth factor-1 in the effect of caloric restriction: regulation of plasma adiponectin and leptin

Author

Yamaza, Haruyoshi, Komatsu, Toshimitsu, To, Kazuo, Toyama, Hiroaki, Chiba, Takuya, Higami, Yoshikazu, and Shimokawa, Isao

Subjects

Growth factors -- Properties, Growth factors -- Influence, Longevity -- Research, Lectins -- Properties, Lectins -- Control, Bioenergetics -- Control, Bioenergetics -- Influence, Energy metabolism -- Control, Energy metabolism -- Influence, Blood plasma -- Properties, Adipose tissues -- Properties, Health, Seniors

Abstract

Insulin-like growth factor (IGF)-1 signaling might partly mediate effects of caloric restriction (CR), an experimental intervention for increasing longevity in mammals. The present study evaluated effects of recombinant human (rh)IGF-1 infusion on adipokine levels in CR and transgenic (Tg) dwarf rats with the reduced growth hormone--IGF-1 axis, which shared similar body weight and food intake. At 9 months of age, each rat received a continuous infusion of rhIGF-1 for 14 days, and rats received an injection of glucose after overnight fasting. Infusion of rhlGF-1 had metabolic effects in all rat groups although it did not affect insulin sensitivity in any of the groups. In addition, plasma adiponectin was decreased to the control group levels and plasma leptin was further reduced in CR and Tg rats. The similarity of phenotypes and adipokine responses to rhlGF-1 between CR and Tg rats supports a role for reduced IGF-1 signaling in the CR effect.

Published

2007

8. Effect of connective tissue growth factor on hypoxia-inducible factor 1[alpha] degradation and tumor angiogenesis

Author

Chang, Cheng-Chi, Lin, Ming-Tsai, Lin, Been-Ren, Jeng, Yung-Ming, Chen, Szu-Ta, Chu, Chia-Yu, Chen, Robert J., Chang, King-Jen, Yang, Pan-Chyr, and Kuo, Min-Liang

Subjects

Metastasis -- Case studies, Metastasis -- Control, Growth factors -- Influence, Growth factors -- Case studies, Lung cancer -- Control, Lung cancer -- Case studies, Health

Abstract

Background: Connective tissue growth factor (CTGF) inhibits the metastatic activity of human lung cancer cells in a mouse model; however, the mechanism of this modulation is unclear. We investigated the role of angiogenesis in this process. Methods: CL1-5 and A549 human lung adenocarcinoma cells were stably transfected with vectors containing CTGF or hypoxia-inducible factor (HIF) 1[alpha] of with vector controls. Transfected cells were injected into nude mice (n = 10 per group), and tumor growth, metastasis, and mouse survival were measured. Excised xenograft tumors and primary human lung adenocarcinomas (n = 24) were subjected to immunohistochemistry with antibodies to the endothelial cell marker CD31 and to CTGF. Expression of HIF-1[alpha] and vascular endothelial growth factor (VEGF) A was assessed in vitro by using reporter gene assays. Ceils were transiently transfected with HIF-1[alpha] mutant and antisense arrest-defective 1 protein (ARD-1), and HIF-1[alpha] acetylation was assayed by immunoprecipitation. All statistical tests were two-sided. Results: Xenograft tumors derived from CTGF transfectants grew more slowly than those from control-transfected cells and had reduced expression of HIF-1[alpha] and VEGF-A, vascularization (as assessed by CD31 expression), and metastasis (all P

Published

2006

9. BMP induction if Id proteins suppresses differentiation and sustains embryonic stem cell self-renewal in collaboration with STAT3

Author

Ying, Qi-Long, Nichols, Jennifer, Chambers, Ian, and Smith, Austin

Subjects

Growth factors -- Influence, Growth factors -- Physiological aspects, Cell differentiation -- Physiological aspects, Bone morphogenetic proteins -- Physiological aspects, Bone morphogenetic proteins -- Influence, Stem cells -- Physiological aspects, Biological sciences

Abstract

Research indicates that serum growth factors produced by mouse embryonic stem cells can promote self renewal of the stem cells as shown by culturing stem cells in the absence of serum, in which neural differentiation is partially inhibited by leukemia inhibitory factor, in combination with bone morphogenetic proteins, attenuating self renewal.

Published

2003