Your search keyword '"Olefsky JM"' showing total 80 results

1. Neuronal Sirt1 deficiency increases insulin sensitivity in both brain and peripheral tissues.

Author

Lu M, Sarruf DA, Li P, Osborn O, Sanchez-Alavez M, Talukdar S, Chen A, Bandyopadhyay G, Xu J, Morinaga H, Dines K, Watkins S, Kaiyala K, Schwartz MW, and Olefsky JM

Subjects

Animals, Cells, Cultured, Forkhead Box Protein O1, Forkhead Transcription Factors genetics, Forkhead Transcription Factors metabolism, Glucose genetics, Glucose metabolism, Hypoglycemic Agents metabolism, Hypoglycemic Agents pharmacology, Insulin genetics, Insulin pharmacology, Insulin Receptor Substrate Proteins genetics, Insulin Receptor Substrate Proteins metabolism, Mice, Mice, Knockout, Nerve Tissue Proteins genetics, Organ Specificity, Phosphatidylinositol 3-Kinases genetics, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation drug effects, Phosphorylation physiology, Proto-Oncogene Proteins c-akt genetics, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction drug effects, Signal Transduction physiology, Sirtuin 1 genetics, Energy Metabolism physiology, Hypothalamus metabolism, Insulin metabolism, Insulin Resistance physiology, Nerve Tissue Proteins metabolism, Sirtuin 1 metabolism

Abstract

Sirt1 is a NAD(+)-dependent class III deacetylase that functions as a cellular energy sensor. In addition to its well-characterized effects in peripheral tissues, emerging evidence suggests that neuronal Sirt1 activity plays a role in the central regulation of energy balance and glucose metabolism. To assess this idea, we generated Sirt1 neuron-specific knockout (SINKO) mice. On both standard chow and HFD, SINKO mice were more insulin sensitive than Sirt1(f/f) mice. Thus, SINKO mice had lower fasting insulin levels, improved glucose tolerance and insulin tolerance, and enhanced systemic insulin sensitivity during hyperinsulinemic euglycemic clamp studies. Hypothalamic insulin sensitivity of SINKO mice was also increased over controls, as assessed by hypothalamic activation of PI3K, phosphorylation of Akt and FoxO1 following systemic insulin injection. Intracerebroventricular injection of insulin led to a greater systemic effect to improve glucose tolerance and insulin sensitivity in SINKO mice compared with controls. In line with the in vivo results, insulin-induced AKT and FoxO1 phosphorylation were potentiated by inhibition of Sirt1 in a cultured hypothalamic cell line. Mechanistically, this effect was traced to a reduced effect of Sirt1 to directly deacetylate and repress IRS-1 function. The enhanced central insulin signaling in SINKO mice was accompanied by increased insulin receptor signal transduction in liver, muscle, and adipose tissue. In summary, we conclude that neuronal Sirt1 negatively regulates hypothalamic insulin signaling, leading to systemic insulin resistance. Interventions that reduce neuronal Sirt1 activity have the potential to improve systemic insulin action and limit weight gain on an obesigenic diet.

Published

2013

2. Liver-specific p70 S6 kinase depletion protects against hepatic steatosis and systemic insulin resistance.

Author

Bae EJ, Xu J, Oh DY, Bandyopadhyay G, Lagakos WS, Keshwani M, and Olefsky JM

Subjects

Animals, Male, Mice, Mice, Inbred C57BL, Fatty Liver prevention & control, Insulin Resistance, Liver metabolism, Ribosomal Protein S6 Kinases metabolism

Abstract

Obesity-associated hepatic steatosis is a manifestation of selective insulin resistance whereby lipogenesis remains sensitive to insulin but the ability of insulin to suppress glucose production is impaired. We created a mouse model of liver-specific knockdown of p70 S6 kinase (S6K) (L-S6K-KD) by systemic delivery of an adeno-associated virus carrying a shRNA for S6K and examined the effects on steatosis and insulin resistance. High fat diet (HFD) fed L-S6K-KD mice showed improved glucose tolerance and systemic insulin sensitivity compared with controls, with no changes in food intake or body weight. The induction of lipogenic gene expression was attenuated in the L-S6K-KD mice with decreased sterol regulatory element-binding protein (SREBP)-1c expression and mature SREBP-1c protein, as well as decreased steatosis on HFD. Our results demonstrate the importance of S6K: 1) as a modulator of the hepatic response to fasting/refeeding, 2) in the development of steatosis, and 3) as a key node in selective hepatic insulin resistance in obese mice.

Published

2012

3. Functional heterogeneity of CD11c-positive adipose tissue macrophages in diet-induced obese mice.

Author

Li P, Lu M, Nguyen MTA, Bae EJ, Chapman J, Feng D, Hawkins M, Pessin JE, Sears DD, Nguyen AK, Amidi A, Watkins SM, Nguyen U, and Olefsky JM

Subjects

Adipose Tissue cytology, Animals, Apoptosis, Base Sequence, DNA Primers, Glucose administration & dosage, Immunohistochemistry, Insulin Resistance, Male, Mice, Mice, Inbred C57BL, Polymerase Chain Reaction, Adipose Tissue immunology, CD11c Antigen immunology, Diet, Macrophages immunology, Obesity immunology

Abstract

Obesity represents a state of chronic, low grade inflammation and is associated with infiltration of increased numbers of adipose tissue macrophages (ATMs). Diet-induced obesity leads to an increase in non-inflammatory M1-like ATMs displaying the CD11c surface marker. We assessed the function of CD11c-positive ATMs when insulin resistant high fat diet (HFD) mice become insulin-sensitive after switching from HFD to normal chow (NC). HFD mice rapidly become insulin-sensitive in all major insulin-target tissues, including muscle, liver, and adipose tissue, after the diet switch. In adipose tissue the CD11c-positive macrophages remain constant in number despite the presence of insulin sensitivity, but these macrophages now assume a new phenotype in which they no longer exhibit increased inflammatory pathway markers. Adipose tissue markers of apoptosis and necrosis were elevated on HFD and remain high after the HFD --> NC diet switch. Furthermore, ATM accumulation preceded detectable adipocyte necrosis at the early phase of HFD. Together, these results indicate that 1) CD11c-positive M1-like ATMs can exhibit phenotypic plasticity and that the polarization of these cells between inflammatory and non-inflammatory states is well correlated to the presence of absence of insulin resistance, and 2) adipocyte necrosis and apoptosis can be dissociated from ATM accumulation.

Published

2010

4. Glucocorticoids and thiazolidinediones interfere with adipocyte-mediated macrophage chemotaxis and recruitment.

Author

Patsouris D, Neels JG, Fan W, Li PP, Nguyen MT, and Olefsky JM

Subjects

Adipocytes drug effects, Animals, Cell Line, Fatty Acids, Nonesterified immunology, Macrophages drug effects, Male, Mice, Mice, Inbred C57BL, Tumor Necrosis Factor-alpha immunology, Adipocytes immunology, Chemotaxis drug effects, Glucocorticoids pharmacology, Macrophages immunology, Thiazolidinediones pharmacology

Abstract

The link between intra-abdominal adiposity and type II diabetes has been known for decades, and adipose tissue macrophage (ATM)-associated inflammation has recently been linked to insulin resistance. However, the mechanisms associated with ATM recruitment remain ill defined. Herein, we describe in vitro chemotaxis studies, in which adipocyte conditioned medium was used to stimulate macrophage migration. We demonstrate that tumor necrosis factor alpha and free fatty acids, key inflammatory stimuli involved in obesity-associated autocrine/paracrine inflammatory signaling, stimulate adipocyte expression and secretion of macrophage chemoattractants. Pharmacological studies showed that peroxisome proliferator-activated receptor gamma agonists and glucocorticoids potently inhibit adipocyte- induced recruitment of macrophages. This latter effect was mediated by the glucocorticoid receptor, which led to decreased chemokine secretion and expression. In vivo results were quite comparable; treatment of high fat diet-fed mice with dexamethasone prevented ATM accumulation in epididymal fat. This decrease in ATM was most pronounced for the proinflammatory F4/80(+), CD11b(+), CD11c(+) M-1-like ATM subset. Overall, our results elucidate a beneficial function of peroxisome proliferator-activated receptor gamma activation and glucocorticoid receptor/glucocorticoids in adipose tissue and indicate that pharmacologic prevention of ATM accumulation could be beneficial.

Published

2009

5. FOXO1 transrepresses peroxisome proliferator-activated receptor gamma transactivation, coordinating an insulin-induced feed-forward response in adipocytes.

Author

Fan W, Imamura T, Sonoda N, Sears DD, Patsouris D, Kim JJ, and Olefsky JM

Subjects

Amino Acid Motifs physiology, Animals, Cell Line, Cell Nucleus genetics, Cell Nucleus metabolism, Forkhead Box Protein O1, Forkhead Transcription Factors genetics, Hypoglycemic Agents metabolism, Hypoglycemic Agents pharmacology, Insulin pharmacology, Insulin Resistance physiology, Male, Mice, PPAR gamma genetics, Phosphorylation drug effects, Phosphorylation physiology, Protein Binding physiology, Protein Structure, Tertiary physiology, Signal Transduction drug effects, Signal Transduction physiology, Adipocytes metabolism, Forkhead Transcription Factors metabolism, Insulin metabolism, PPAR gamma metabolism, Response Elements physiology, Transcriptional Activation physiology

Abstract

The transcriptional factor FoxO1 plays an important role in metabolic homeostasis. Herein we identify a novel transrepressional function that converts FoxO1 from an activator of transcription to a promoter-specific repressor of peroxisome proliferator-activated receptor gamma (PPARgamma) target genes that regulate adipocyte biology. FoxO1 transrepresses PPARgamma via direct protein-protein interactions; it is recruited to PPAR response elements (PPRE) on PPARgamma target genes by PPARgamma bound to PPRE and interferes with promoter DNA occupancy of the receptor. The FoxO1 transrepressional function, which is independent and dissectible from the transactivational effects, does not require a functional FoxO1 DNA binding domain, but dose require an evolutionally conserved 31 amino acids LXXLL-containing domain. Insulin induces FoxO1 phosphorylation and nuclear exportation, which prevents FoxO1-PPARgamma interactions and rescues transrepression. Adipocytes from insulin resistant mice show reduced phosphorylation and increased nuclear accumulation of FoxO1, which is coupled to lowered expression of endogenous PPARgamma target genes. Thus the innate FoxO1 transrepression function enables insulin to augment PPARgamma activity, which in turn leads to insulin sensitization, and this feed-forward cycle represents positive reinforcing connections between insulin and PPARgamma signaling.

Published

2009

6. A subpopulation of macrophages infiltrates hypertrophic adipose tissue and is activated by free fatty acids via Toll-like receptors 2 and 4 and JNK-dependent pathways.

Author

Nguyen MT, Favelyukis S, Nguyen AK, Reichart D, Scott PA, Jenn A, Liu-Bryan R, Glass CK, Neels JG, and Olefsky JM

Subjects

Animals, Bone Marrow Cells metabolism, CD11b Antigen biosynthesis, CD11c Antigen biosynthesis, Inflammation, Insulin Resistance, Male, Mice, Mice, Inbred C57BL, Models, Biological, Signal Transduction, Adipose Tissue metabolism, Fatty Acids, Nonesterified metabolism, MAP Kinase Kinase 4 metabolism, Macrophages metabolism, Toll-Like Receptor 2 metabolism, Toll-Like Receptor 4 metabolism

Abstract

Obesity and type 2 diabetes are characterized by decreased insulin sensitivity, elevated concentrations of free fatty acids (FFAs), and increased macrophage infiltration in adipose tissue (AT). Here, we show that FFAs can cause activation of RAW264.7 cells primarily via the JNK signaling cascade and that TLR2 and TLR4 are upstream of JNK and help transduce FFA proinflammatory signals. We also demonstrate that F4/80(+)CD11b(+)CD11c(+) bone marrow-derived dendritic cells (BMDCs) have heightened proinflammatory activity compared with F4/80(+)CD11b(+)CD11c(-) bone marrow-derived macrophages and that the proinflammatory activity and JNK phosphorylation of BMDCs, but not bone marrow-derived macrophages, was further increased by FFA treatment. F4/80(+)CD11b(+)CD11c(+) cells were found in AT, and the proportion and number of these cells in AT is increased in ob/ob mice and by feeding wild type mice a high fat diet for 1 and 12 weeks. AT F4/80(+)CD11b(+)CD11c(+) cells express increased inflammatory markers compared with F4/80(+)CD11b(+)CD11c(-) cells, and FFA treatment increased inflammatory responses in these cells. In addition, we found that CD11c expression is increased in skeletal muscle of high fat diet-fed mice and that conditioned medium from FFA-treated wild type BMDCs, but not TLR2/4 DKO BMDCs, can induce insulin resistance in L6 myotubes. Together our results show that FFAs can activate CD11c(+) myeloid proinflammatory cells via TLR2/4 and JNK signaling pathways, thereby promoting inflammation and subsequent cellular insulin resistance.

Published

2007

7. Tumor necrosis factor receptor-1 can function through a G alpha q/11-beta-arrestin-1 signaling complex.

Author

Kawamata Y, Imamura T, Babendure JL, Lu JC, Yoshizaki T, and Olefsky JM

Subjects

3T3-L1 Cells, Animals, Diabetes Complications metabolism, Enzyme Activation drug effects, Extracellular Signal-Regulated MAP Kinases metabolism, Glycerol metabolism, Humans, Inflammation Mediators metabolism, Insulin Resistance, Lipolysis drug effects, Mice, Obesity metabolism, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation drug effects, Tumor Necrosis Factor-alpha metabolism, beta-Arrestin 1, beta-Arrestins, Adipocytes metabolism, Arrestins metabolism, GTP-Binding Protein alpha Subunits, Gq-G11 metabolism, MAP Kinase Signaling System drug effects, Multiprotein Complexes metabolism, Receptors, Tumor Necrosis Factor, Type I metabolism, Tumor Necrosis Factor-alpha pharmacology

Abstract

Tumor necrosis factor-alpha (TNFalpha) is a proinflammatory cytokine secreted from macrophages and adipocytes. It is well known that chronic TNFalpha exposure can lead to insulin resistance both in vitro and in vivo and that elevated blood levels of TNFalpha are observed in obese and/or diabetic individuals. TNFalpha has many acute biologic effects, mediated by a complex intracellular signaling pathway. In these studies we have identified new G-protein signaling components to this pathway in 3T3-L1 adipocytes. We found that beta-arrestin-1 is associated with TRAF2 (TNF receptor-associated factor 2), an adaptor protein of TNF receptors, and that TNFalpha acutely stimulates tyrosine phosphorylation of G alpha(q/11) with an increase in G alpha(q/11) activity. Small interfering RNA-mediated knockdown of beta-arrestin-1 inhibits TNFalpha-induced tyrosine phosphorylation of G alpha(q/11) by interruption of Src kinase activation. TNFalpha stimulates lipolysis in 3T3-L1 adipocytes, and beta-arrestin-1 knockdown blocks the effects of TNFalpha to stimulate ERK activation and glycerol release. TNFalpha also led to activation of JNK with increased expression of the proinflammatory gene, monocyte chemoattractant protein-1 and matrix metalloproteinase 3, and beta-arrestin-1 knockdown inhibited both of these effects. Taken together these results reveal novel elements of TNFalpha action; 1) the trimeric G-protein component G alpha(q/11) and the adapter protein beta-arrestin-1 can function as signaling molecules in the TNFalpha action cascade; 2) beta-arrestin-1 can couple TNFalpha stimulation to ERK activation and lipolysis; 3) beta-arrestin-1 and G alpha(q/11) can mediate TNFalpha-induced phosphatidylinositol 3-kinase activation and inflammatory gene expression.

Published

2007

8. Disruption of microtubules ablates the specificity of insulin signaling to GLUT4 translocation in 3T3-L1 adipocytes.

Author

Huang J, Imamura T, Babendure JL, Lu JC, and Olefsky JM

Subjects

3T3-L1 Cells, Actins metabolism, Animals, Mice, Phosphatidylinositol 3-Kinases metabolism, Platelet-Derived Growth Factor pharmacology, Protein Transport, Proto-Oncogene Proteins c-akt metabolism, Adipocytes metabolism, Glucose Transporter Type 4 metabolism, Insulin metabolism, Microtubules metabolism, Signal Transduction

Abstract

Although the cytoskeletal network is important for insulin-induced glucose uptake, several studies have assessed the effects of microtubule disruption on glucose transport with divergent results. Here, we investigated the effects of microtubule-depolymerizing reagent, nocodazole and colchicine, on GLUT4 translocation in 3T3-L1 adipocytes. After nocodazole treatment to disrupt microtubules, GLUT4 vesicles were dispersed from the perinuclear region in the basal state, and insulin-induced GLUT4 translocation was partially inhibited by 20-30%, consistent with other reports. We found that platelet-derived growth factor (PDGF), which did not stimulate GLUT4 translocation in intact cells, was surprisingly able to enhance GLUT4 translocation to approximately 50% of the maximal insulin response, in nocodazole-treated cells with disrupted microtubules. This effect of PDGF was blocked by pretreatment with wortmannin and attenuated in cells pretreated with cytochalasin D. Using confocal microscopy, we found an increased co-localization of GLUT4 and F-actin in nocodazole-treated cells upon PDGF stimulation compared with control cells. Furthermore, microinjection of small interfering RNA targeting the actin-based motor Myo1c, but not the microtubule-based motor KIF3, significantly inhibited both insulin- and PDGF-stimulated GLUT4 translocation after nocodazole treatment. In summary, our data suggest that 1) proper perinuclear localization of GLUT4 vesicles is a requirement for insulin-specific stimulation of GLUT4 translocation, and 2) nocodazole treatment disperses GLUT4 vesicles from the perinuclear region allowing them to engage insulin and PDGF-sensitive actin filaments, which can participate in GLUT4 translocation in a phosphatidylinositol 3-kinase-dependent manner.

Published

2005

9. JNK and tumor necrosis factor-alpha mediate free fatty acid-induced insulin resistance in 3T3-L1 adipocytes.

Author

Nguyen MT, Satoh H, Favelyukis S, Babendure JL, Imamura T, Sbodio JI, Zalevsky J, Dahiyat BI, Chi NW, and Olefsky JM

Subjects

3T3-L1 Cells, Adipocytes metabolism, Adiponectin metabolism, Animals, Biological Transport, Blotting, Western, Cell Differentiation, Deoxyglucose metabolism, Down-Regulation, Enzyme Activation, Enzyme-Linked Immunosorbent Assay, Genes, Dominant, Glucose metabolism, Glucose Transporter Type 4, I-kappa B Kinase metabolism, Inflammation, Insulin metabolism, JNK Mitogen-Activated Protein Kinases metabolism, Lipids chemistry, MAP Kinase Kinase 4 metabolism, Mice, Protein Transport, RNA Interference, Signal Transduction, Suppressor of Cytokine Signaling 3 Protein, Suppressor of Cytokine Signaling Proteins metabolism, Time Factors, Tumor Necrosis Factor-alpha metabolism, Fatty Acids, Nonesterified metabolism, Insulin Resistance, MAP Kinase Kinase 4 physiology, Tumor Necrosis Factor-alpha physiology

Abstract

Lipid infusion and high fat feeding are established causes of systemic and adipose tissue insulin resistance. In this study, we treated 3T3-L1 adipocytes with a mixture of free fatty acids (FFAs) to investigate the molecular mechanisms underlying fat-induced insulin resistance. FFA treatment impaired insulin receptor-mediated signal transduction and decreased insulin-stimulated GLUT4 translocation and glucose transport. FFAs activated the stress/inflammatory kinases c-Jun N-terminal kinase (JNK) and IKKbeta, and the suppressor of cytokine signaling protein 3, increased secretion of the inflammatory cytokine tumor necrosis factor (TNF)-alpha, and decreased secretion of adiponectin into the medium. RNA interference-mediated down-regulation of JNK blocked JNK activation and prevented most of the FFA-induced defects in insulin action. Blockade of TNF-alpha signaling with neutralizing antibodies to TNF-alpha or its receptors or with a dominant negative TNF-alpha peptide had a partial effect to inhibit FFA-induced cellular insulin resistance. We found that JNK activation by FFAs was not inhibited by blocking TNF-alpha signaling, whereas the FFA-induced increase in TNF-alpha secretion was inhibited by RNA interference-mediated JNK knockdown. Together, these results indicate that 1) JNK can be activated by FFAs through TNF-alpha-independent mechanisms, 2) activated JNK is a major contributor to FFA-induced cellular insulin resistance, and 3) TNF-alpha is an autocrine/paracrine downstream effector of activated JNK that can also mediate insulin resistance.

Published

2005

10. Insulin-induced beta-arrestin1 Ser-412 phosphorylation is a mechanism for desensitization of ERK activation by Galphai-coupled receptors.

Author

Hupfeld CJ, Resnik JL, Ugi S, and Olefsky JM

Subjects

Antigens, Viral, Tumor metabolism, Arrestins metabolism, Dose-Response Relationship, Drug, Enzyme Activation, Heterotrimeric GTP-Binding Proteins metabolism, Insulin pharmacology, Insulin-Like Growth Factor I pharmacology, MAP Kinase Signaling System, Mitogen-Activated Protein Kinases metabolism, Okadaic Acid pharmacology, Phosphatidylinositol 3-Kinases metabolism, Phosphoprotein Phosphatases antagonists & inhibitors, Phosphorylation drug effects, Phosphoserine metabolism, Protein Binding, Protein Phosphatase 2, Receptor, IGF Type 1 metabolism, Receptors, Adrenergic, beta metabolism, Time Factors, beta-Arrestins, Phosphoprotein Phosphatases metabolism

Abstract

Beta-arrestin1 is an adapter/scaffold for many G protein-coupled receptors during mitogen-activated protein kinase signaling. Phosphorylation of beta-arrestin1 at position Ser-412 is a regulator of beta-arrestin1 function, and in the present study, we showed that insulin led to a time- and dose-dependent increase in beta-arrestin1 Ser-412 phosphorylation, which blocked isoproterenol- and lysophosphatidic acid-induced Ser-412 dephosphorylation and impaired ERK signaling by these G protein-coupled receptor ligands. Insulin treatment also led to accumulation of Ser-412-phosphorylated beta-arrestin1 at the insulin-like growth factor 1 receptor and prevented insulin-like growth factor 1/Src association. Insulin-induced Ser-412 phosphorylation was partially dependent on ERK as treatment with the MEK inhibitor PD98059 inhibited the insulin effect (62% reduction, p = 0.03). Inhibition of phosphatidylinositol 3-kinase by wortmannin did not have a significant effect (9% reduction, p = 0.41). We also found that the protein phosphatase 2A (PP2A) was in a molecular complex with beta-arrestin1 and that the PP2A inhibitor okadaic acid increased Ser-412 phosphorylation. Concomitant addition of insulin and okadaic acid did not produce an additive effect on Ser-412 phosphorylation, suggesting a common mechanism. Small t antigen specifically inhibited PP2A, and in HIRcB cells expressing small t antigen, beta-arrestin1 Ser-412 phosphorylation was increased, and insulin had no further effect. Insulin treatment caused increased beta-arrestin1 Ser-412 phosphorylation, which blocked mitogen-activated protein kinase signaling and internalization by beta-arrestin1-dependent receptors with no effect on beta-adrenergic receptor Gs-mediated cAMP production. These findings provide a new mechanism for insulin-induced desensitization of ERK activation by Galphai-coupled receptors.

Published

2005

11. Protein phosphatase-2C alpha as a positive regulator of insulin sensitivity through direct activation of phosphatidylinositol 3-kinase in 3T3-L1 adipocytes.

Author

Yoshizaki T, Maegawa H, Egawa K, Ugi S, Nishio Y, Imamura T, Kobayashi T, Tamura S, Olefsky JM, and Kashiwagi A

Subjects

3T3-L1 Cells, Adenoviridae genetics, Adenoviridae metabolism, Animals, Blotting, Northern, Blotting, Western, Cell Differentiation, Dose-Response Relationship, Drug, Electrophoresis, Polyacrylamide Gel, Enzyme Activation, Fibroblasts metabolism, Glucose pharmacokinetics, Glucose Transporter Type 4, Humans, Mice, Models, Biological, Monosaccharide Transport Proteins metabolism, Mutation, Phosphoprotein Phosphatases metabolism, Phosphorylation, Precipitin Tests, Protein Phosphatase 2C, Protein Transport, RNA, Small Interfering metabolism, Recombinant Proteins metabolism, Signal Transduction, Time Factors, Transfection, Adipocytes metabolism, Insulin metabolism, Muscle Proteins, Phosphatidylinositol 3-Kinases metabolism, Phosphoprotein Phosphatases physiology

Abstract

During differentiation, expression of protein phosphatase-2Calpha (PP2Calpha) is increased in 3T3-L1 adipocytes. To elucidate the role of PP2Calpha in insulin signaling, we overexpressed wild-type (WT) PP2Calpha by adenovirus-mediated gene transfer in 3T3-L1 adipocytes. Overexpression of PP2Calpha-WT enhanced the insulin sensitivity of glucose uptake without any changes in the early steps of insulin signaling. Infection with adenovirus 5 expressing PP2Calpha-WT increased phosphatidylinositol 3-kinase (PI3K) activities in the immunoprecipitate using antibody against the p85 or p110 subunit under both basal and insulin-stimulated conditions, followed by activation of downstream steps in the PI3K pathway, such as phosphorylation of Akt, glycogen synthase kinase-3, and atypical protein kinase C. In contrast, overexpression of the phosphatase-defective mutant PP2Calpha(R174G) did not produce such effects. Furthermore, overexpression of PP2Calpha-WT (but not PP2Calpha(R174G)) decreased the (32)P-labeled phosphorylation state as well as the gel mobility shift of the p85 subunit, suggesting that dephosphorylation of the p85 subunit by PP2Calpha activation might stimulate PI3K catalytic activity. Moreover, knockdown of PP2Calpha by transfection of small interfering RNA led to a significant decrease in Akt phosphorylation. In addition, microinjection of anti-PP2Calpha antibody or PP2Calpha small interfering RNA led to decreased insulin-stimulated GLUT4 translocation. In conclusion, PP2Calpha is a new positive regulator of insulin sensitivity that acts through a direct activation of PI3K in 3T3-L1 adipocytes.

Published

2004

12. Complex distribution, not absolute amount of adiponectin, correlates with thiazolidinedione-mediated improvement in insulin sensitivity.

Author

Pajvani UB, Hawkins M, Combs TP, Rajala MW, Doebber T, Berger JP, Wagner JA, Wu M, Knopps A, Xiang AH, Utzschneider KM, Kahn SE, Olefsky JM, Buchanan TA, and Scherer PE

Subjects

3T3-L1 Cells, Adiponectin, Adolescent, Adult, Aged, Aged, 80 and over, Animals, Blood Glucose metabolism, Chromatography, Gel, Diabetes, Gestational metabolism, Dose-Response Relationship, Drug, Female, Humans, Immunoblotting, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Middle Aged, Pregnancy, Proteins chemistry, Proteins metabolism, Time Factors, Hypoglycemic Agents pharmacology, Insulin metabolism, Intercellular Signaling Peptides and Proteins, Protein Biosynthesis, Thiazolidinediones pharmacology

Abstract

Adiponectin is an adipocyte-specific secretory protein that circulates in serum as a hexamer of relatively low molecular weight (LMW) and a larger multimeric structure of high molecular weight (HMW). Serum levels of the protein correlate with systemic insulin sensitivity. The full-length protein affects hepatic gluconeogenesis through improved insulin sensitivity, and a proteolytic fragment of adiponectin stimulates beta oxidation in muscle. Here, we show that the ratio, and not the absolute amounts, between these two oligomeric forms (HMW to LMW) is critical in determining insulin sensitivity. We define a new index, S(A), that can be calculated as the ratio of HMW/(HMW + LMW). db/db mice, despite similar total adiponectin levels, display decreased S(A) values compared with wild type littermates, as do type II diabetic patients compared with insulin-sensitive individuals. Furthermore, S(A) improves with peroxisome proliferator-activated receptor-gamma agonist treatment (thiazolidinedione; TZD) in mice and humans. We demonstrate that changes in S(A) in a number of type 2 diabetic cohorts serve as a quantitative indicator of improvements in insulin sensitivity obtained during TZD treatment, whereas changes in total serum adiponectin levels do not correlate well at the individual level. Acute alterations in S(A) (DeltaS(A)) are strongly correlated with improvements in hepatic insulin sensitivity and are less relevant as an indicator of improved muscle insulin sensitivity in response to TZD treatment, further underscoring the conclusions from previous clamp studies that suggested that the liver is the primary site of action for the full-length protein. These observations suggest that the HMW adiponectin complex is the active form of this protein, which we directly demonstrate in vivo by its ability to depress serum glucose levels in a dose-dependent manner.

Published

2004

13. Cdc42 is a Rho GTPase family member that can mediate insulin signaling to glucose transport in 3T3-L1 adipocytes.

Author

Usui I, Imamura T, Huang J, Satoh H, and Olefsky JM

Subjects

3T3 Cells, Animals, Biological Transport, Blotting, Western, Chromones pharmacology, Deoxyglucose pharmacokinetics, Dose-Response Relationship, Drug, GTP-Binding Protein alpha Subunits, Gq-G11, Heterotrimeric GTP-Binding Proteins metabolism, Immunoglobulin G metabolism, Isoenzymes, Mice, Microscopy, Fluorescence, Morpholines pharmacology, Phosphatidylinositol 3-Kinases metabolism, Precipitin Tests, Protein Kinase C metabolism, Protein Transport, Time Factors, cdc42 GTP-Binding Protein metabolism, Adipocytes metabolism, Glucose metabolism, Insulin metabolism, Signal Transduction, cdc42 GTP-Binding Protein physiology, rho GTP-Binding Proteins physiology

Abstract

We investigated the role of cdc42, a Rho GTPase family member, in insulin-induced glucose transport in 3T3-L1 adipocytes. Microinjection of anti-cdc42 antibody or cdc42 siRNA led to decreased insulin-induced and constitutively active G(q) (CA-G(q); Q209L)-induced GLUT4 translocation. Adenovirus-mediated expression of constitutively active cdc42 (CA-cdc42; V12) stimulated 2-deoxyglucose uptake to 56% of the maximal insulin response, and this was blocked by treatment with the phosphatidylinositol 3-kinase (PI3-kinase) inhibitor, wortmannin, or LY294002. Both insulin and CA-G(q) expression caused an increase in cdc42 activity, showing that cdc42 is activated by insulin and is downstream of G alpha(q/11) in this activation pathway. Immunoprecipitation experiments showed that insulin enhanced a direct association of cdc42 and p85, and both insulin treatment and CA-cdc42 expression stimulated PI3-kinase activity in immunoprecipitates with anti-cdc42 antibody. Furthermore, the effects of insulin, CA-G(q), and CA-cdc42 on GLUT4 translocation or 2-deoxyglucose uptake were inhibited by microinjection of anti-protein kinase C lambda (PKC lambda) antibody or overexpression of a kinase-deficient PKC lambda construct. In summary, activated cdc42 can mediate 1) insulin-stimulated GLUT4 translocation and 2) glucose transport in a PI3-kinase-dependent manner. 3) Insulin treatment and constitutively active G(q) expression can enhance the cdc42 activity state as well as the association of cdc42 with activated PI3-kinase. 4) PKC lambda inhibition blocks CA-cdc42, CA-G(q), and insulin-stimulated GLUT4 translocation. Taken together, these data indicate that cdc42 can mediate insulin signaling to GLUT4 translocation and lies downstream of G alpha(q/11) and upstream of PI3-kinase and PKC lambda in this stimulatory pathway.

Published

2003

14. Involvement of both G(q/11) and G(s) proteins in gonadotropin-releasing hormone receptor-mediated signaling in L beta T2 cells.

Author

Liu F, Usui I, Evans LG, Austin DA, Mellon PL, Olefsky JM, and Webster NJ

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Cell Line, Colforsin pharmacology, GTP-Binding Protein alpha Subunits, Gq-G11, Molecular Sequence Data, Mutagenesis, Site-Directed, Peptide Fragments chemistry, Pertussis Toxin, Pituitary Gland, Protein Serine-Threonine Kinases, Rats, Recombinant Fusion Proteins metabolism, Tetradecanoylphorbol Acetate pharmacology, Trypsin, Virulence Factors, Bordetella pharmacology, GTP-Binding Protein alpha Subunits, Gs metabolism, Heterotrimeric GTP-Binding Proteins metabolism, Mitogen-Activated Protein Kinases metabolism, Nuclear Proteins metabolism, Receptors, LHRH physiology, Signal Transduction physiology

Abstract

The hypothalamic hormone gonadotropin-releasing hormone (GnRH) stimulates the synthesis and release of the pituitary gonadotropins. GnRH acts through a plasma membrane receptor that is a member of the G protein-coupled receptor (GPCR) family. These receptors interact with heterotrimeric G proteins to initiate downstream signaling. In this study, we have investigated which G proteins are involved in GnRH receptor-mediated signaling in L beta T2 pituitary gonadotrope cells. We have shown previously that GnRH activates ERK and induces the c-fos and LH beta genes in these cells. Signaling via the G(i) subfamily of G proteins was excluded, as neither ERK activation nor c-Fos and LH beta induction was impaired by treatment with pertussis toxin or a cell-permeable peptide that sequesters G beta gamma-subunits. GnRH signaling was partially mimicked by adenoviral expression of a constitutively active mutant of G alpha(q) (Q209L) and was blocked by a cell-permeable peptide that uncouples G alpha(q) from GPCRs. Furthermore, chronic activation of G alpha(q) signaling induced a state of GnRH resistance. A cell-permeable peptide that uncouples G alpha(s) from receptors was also able to inhibit ERK, c-Fos, and LH beta, indicating that both G(q/11) and G(s) proteins are involved in signaling. Consistent with this, GnRH caused GTP loading on G(s) and G(q/11) and increased intracellular cAMP. Artificial elevation of cAMP with forskolin activated ERK and caused a partial induction of c-Fos. Finally, treatment of G alpha(q) (Q209L)-infected cells with forskolin enhanced the induction of c-Fos showing that the two pathways are independent and additive. Taken together, these results indicate that the GnRH receptor activates both G(q) and G(s) signaling to regulate gene expression in L beta T2 cells.

Published

2002

15. Phosphatidylinositol 3-kinase is required for insulin-stimulated tyrosine phosphorylation of Shc in 3T3-L1 adipocytes.

Author

Ugi S, Sharma PM, Ricketts W, Imamura T, and Olefsky JM

Subjects

3T3 Cells, Adipocytes enzymology, Animals, Epidermal Growth Factor pharmacology, GRB2 Adaptor Protein, Mice, Phosphorylation, Platelet-Derived Growth Factor pharmacology, Proteins metabolism, Adaptor Proteins, Signal Transducing, Adipocytes metabolism, Insulin pharmacology, Phosphatidylinositol 3-Kinases metabolism, Tyrosine metabolism

Abstract

The interactions between the phosphatidylinositol 3-kinase (PI 3-kinase) and Ras/MAPK kinase pathways have been the subject of considerable interest. In the current studies, we find that epidermal growth factor (EGF) and platelet-derived growth factor (PDGF) lead to rapid phosphorylation of Shc (maximum at 1-2 min), whereas insulin-mediated Shc phosphorylation is relatively delayed (maximum at 5-10 min), suggesting that an intermediary step may be necessary for insulin stimulation of Shc phosphorylation. The Src homology-2 (SH2) domain of Shc is necessary for PDGF- and EGF-mediated Shc phosphorylation, whereas the phosphotyrosine binding (PTB) domain is critical for the actions of insulin. Because the Shc PTB domain can interact with phospholipids, we postulated that PI 3-kinase might be a necessary intermediary step facilitating insulin-stimulated phosphorylation of Shc. In support of this, we found that the PI 3-kinase inhibitors, wortmannin and LY294002, blocked insulin-stimulated but not EGF- or PDGF-stimulated Shc phosphorylation. Furthermore, overexpression of a dominant negative PI 3-kinase construct (p85N-SH2) blocked insulin, but not EGF- or PDGF-induced Shc phosphorylation. All three growth factors cause localization of Shc to the plasma membrane, but only the effect of insulin was inhibited by wortmannin, supporting the view that PI 3-kinase-generated phospholipids mediate insulin-stimulated Shc phosphorylation. Consistent with this, expression of a constitutively active PI 3-kinase (p110(C)(AAX)) increased membrane localization of Shc, and this was completely blocked by wortmannin. A mutant Shc with a disrupted PTB domain (Shc S154) did not localize to the membrane in p110(C)(AAX)-expressing cells or after insulin stimulation and was not phosphorylated by insulin. In summary, 1) PI 3-kinase is a necessary early step in insulin-stimulated Shc phosphorylation, whereas the effects of EGF and PDGF on Shc phosphorylation are independent of PI 3-kinase. 2) PI 3-kinase-stimulated generation of membrane phospholipids can localize Shc to the plasma membrane through the Shc PTB domain facilitating phosphorylation by the insulin receptor.

Published

2002

16. beta -Arrestin-mediated recruitment of the Src family kinase Yes mediates endothelin-1-stimulated glucose transport.

Author

Imamura T, Huang J, Dalle S, Ugi S, Usui I, Luttrell LM, Miller WE, Lefkowitz RJ, and Olefsky JM

Subjects

3T3 Cells, Animals, Arrestins metabolism, Biological Transport, GTP-Binding Protein alpha Subunits, Gq-G11, Glucose Transporter Type 4, Heterotrimeric GTP-Binding Proteins metabolism, Mice, Microscopy, Fluorescence, Monosaccharide Transport Proteins metabolism, Proto-Oncogene Proteins c-yes, Signal Transduction, beta-Arrestin 1, beta-Arrestins, Arrestins physiology, Endothelin-1 pharmacology, Glucose metabolism, Muscle Proteins, Proto-Oncogene Proteins metabolism, src-Family Kinases metabolism

Abstract

The insulin and the endothelin type A (ETA) receptor both can couple into the heterotrimeric G protein alpha(q/11) (Galpha(q/11)), leading to Galpha(q/11) tyrosine phosphorylation, phosphatidylinositol 3-kinase activation, and subsequent stimulation of glucose transport. In this study, we assessed the potential role of Src kinase in ET-1 signaling to glucose transport in 3T3-L1 adipocytes. Src kinase inhibitor PP2 blocked ET-1-induced Src kinase activity, Galpha(q/11) tyrosine phosphorylation, and glucose transport stimulation. To determine which Src family kinase member was involved, we microinjected anti-c-Src, -c-Fyn, or -c-Yes antibody into these cells and found that only anti-c-Yes antibody blocked GLUT4 translocation (70% decreased). Overexpression or microinjection of a dominant negative mutant (K298M) of Src kinase also inhibited ET-1-induced Galpha(q/11) tyrosine phosphorylation and GLUT4 translocation. In co-immunoprecipitation experiments, we found that beta-arrestin 1 associated with the ETA receptor in an agonist-dependent manner and that beta-arrestin 1 recruited Src kinase to a molecular complex that included the ETA receptor. Microinjection of beta-arrestin 1 antibody inhibited ET-1- but not insulin-stimulated GLUT4 translocation. In conclusion, 1) the Src kinase Yes can induce tyrosine phosphorylation of Galpha(q/11) in response to ET-1 stimulation, and 2) beta-arrestin 1 and Src kinase form a molecular complex with the ETA receptor to mediate ET-1 signaling to Galpha(q/11) with subsequent glucose transport stimulation.

Published

2001

17. Nuclear receptor minireview series.

Author

Olefsky JM

Subjects

Animals, Cholesterol metabolism, DNA metabolism, Humans, Receptors, Cytoplasmic and Nuclear chemistry, Receptors, Estrogen metabolism, Sterols metabolism, Transcription Factors metabolism, Receptors, Cytoplasmic and Nuclear metabolism

Published

2001

18. Insulin and insulin-like growth factor I receptors utilize different G protein signaling components.

Author

Dalle S, Ricketts W, Imamura T, Vollenweider P, and Olefsky JM

Subjects

3T3 Cells, Animals, Antibodies pharmacology, Arrestins antagonists & inhibitors, Arrestins metabolism, Cell Division drug effects, Cell Division physiology, Cell Line, ErbB Receptors drug effects, ErbB Receptors physiology, Fibroblasts, Glutathione Transferase metabolism, Heterotrimeric GTP-Binding Proteins antagonists & inhibitors, Humans, Insulin pharmacology, Insulin-Like Growth Factor I pharmacology, Kinetics, Mice, Pertussis Toxin, Rats, Receptor, IGF Type 1 drug effects, Receptor, Insulin drug effects, Recombinant Fusion Proteins metabolism, Virulence Factors, Bordetella pharmacology, beta-Adrenergic Receptor Kinases, beta-Arrestin 1, beta-Arrestins, Cyclic AMP-Dependent Protein Kinases metabolism, Heterotrimeric GTP-Binding Proteins metabolism, Receptor, IGF Type 1 physiology, Receptor, Insulin physiology

Abstract

We examined the role of heterotrimeric G protein signaling components in insulin and insulin-like growth factor I (IGF-I) action. In HIRcB cells and in 3T3L1 adipocytes, treatment with the Galpha(i) inhibitor (pertussis toxin) or microinjection of the Gbetagamma inhibitor (glutathione S-transferase-betaARK) inhibited IGF-I and lysophosphatidic acid-stimulated mitogenesis but had no effect on epidermal growth factor (EGF) or insulin action. In basal state, Galpha(i) and Gbeta were associated with the IGF-I receptor (IGF-IR), and after ligand stimulation the association of IGF-IR with Galpha(i) increased concomitantly with a decrease in Gbeta association. No association of Galpha(i) was found with either the insulin or EGF receptor. Microinjection of anti-beta-arrestin-1 antibody specifically inhibited IGF-I mitogenic action but had no effect on EGF or insulin action. beta-Arrestin-1 was associated with the receptors for IGF-I, insulin, and EGF in a ligand-dependent manner. We demonstrated that Galpha(i), betagamma subunits, and beta-arrestin-1 all play a critical role in IGF-I mitogenic signaling. In contrast, neither metabolic, such as GLUT4 translocation, nor mitogenic signaling by insulin is dependent on these protein components. These results suggest that insulin receptors and IGF-IRs can function as G protein-coupled receptors and engage different G protein partners for downstream signaling.

Published

2001

19. Insulin signals to prenyltransferases via the Shc branch of intracellular signaling.

Author

Goalstone ML, Leitner JW, Berhanu P, Sharma PM, Olefsky JM, and Draznin B

Subjects

3T3 Cells, Adenoviridae, Animals, CHO Cells, Cricetinae, Farnesyltranstransferase, GRB2 Adaptor Protein, Humans, Insulin Receptor Substrate Proteins, Kinetics, Mice, Phosphoproteins metabolism, Phosphorylation, Protein Prenylation, Protein Subunits, Receptor, Insulin genetics, Recombinant Proteins metabolism, Shc Signaling Adaptor Proteins, Src Homology 2 Domain-Containing, Transforming Protein 1, Transfection, src Homology Domains, Adaptor Proteins, Signal Transducing, Adaptor Proteins, Vesicular Transport, Alkyl and Aryl Transferases metabolism, Insulin pharmacology, Proteins metabolism, Receptor, Insulin physiology

Abstract

We assessed the roles of insulin receptor substrate-1 (IRS-1) and Shc in insulin action on farnesyltransferase (FTase) and geranylgeranyltransferase I (GGTase I) using Chinese hamster ovary (CHO) cells that overexpress wild-type human insulin receptors (CHO-hIR-WT) or mutant insulin receptors lacking the NPEY domain (CHO-DeltaNPEY) or 3T3-L1 fibroblasts transfected with adenoviruses that express the PTB or SAIN domain of IRS-1 and Shc, the pleckstrin homology (PH) domain of IRS-1, or the Src homology 2 (SH2) domain of Shc. Insulin promoted phosphorylation of the alpha-subunit of FTase and GGTase I in CHO-hIR-WT cells, but was without effect in CHO-DeltaNPEY cells. Insulin increased FTase and GGTase I activities and the amounts of prenylated Ras and RhoA proteins in CHO-hIR-WT (but not CHO-DeltaNPEY) cells. Overexpression of the PTB or SAIN domain of IRS-1 (which blocked both IRS-1 and Shc signaling) prevented insulin-stimulated phosphorylation of the FTase and GGTase I alpha-subunit activation of FTase and GGTase I and subsequent increases in prenylated Ras and RhoA proteins. In contrast, overexpression of the IRS-1 PH domain, which impairs IRS-1 (but not Shc) signaling, did not alter insulin action on the prenyltransferases, but completely inhibited the insulin effect on the phosphorylation of IRS-1 and on the activation of phosphatidylinositol 3-kinase and Akt. Finally, overexpression of the Shc SH2 domain completely blocked the insulin effect on FTase and GGTase I activities without interfering with insulin signaling to MAPK. These data suggest that insulin signaling from its receptor to the prenyltransferases FTase and GGTase I is mediated by the Shc pathway, but not the IRS-1/phosphatidylinositol 3-kinase pathway. Shc-mediated insulin signaling to MAPK may be necessary (but not sufficient) for activation of prenyltransferase activity. An additional pathway involving the Shc SH2 domain may be necessary to mediate the insulin effect on FTase and GGTase I.

Published

2001

20. The osmotic shock-induced glucose transport pathway in 3T3-L1 adipocytes is mediated by gab-1 and requires Gab-1-associated phosphatidylinositol 3-kinase activity for full activation.

Author

Janez A, Worrall DS, Imamura T, Sharma PM, and Olefsky JM

Subjects

3T3 Cells, Adaptor Proteins, Signal Transducing, Adipocytes metabolism, Androstadienes pharmacology, Animals, Biological Transport, Enzyme Inhibitors pharmacology, Mice, Osmotic Pressure, Phosphoinositide-3 Kinase Inhibitors, Phosphorylation, Sorbitol pharmacology, Tyrosine metabolism, Wortmannin, Adipocytes drug effects, Glucose metabolism, Phosphatidylinositol 3-Kinases metabolism, Phosphoproteins physiology

Abstract

Osmotic shock treatment of 3T3-L1 adipocytes causes an increase in glucose transport activity and translocation of GLUT4 protein similar to that elicited by insulin treatment. Insulin stimulation of GLUT4 translocation and glucose transport activity was completely inhibited by wortmannin, however, activation by osmotic shock was only partially blocked. Additionally, we have found that the newly identified insulin receptor substrate Gab-1 (Grb2-associated binder-1) is tyrosine-phosphorylated following sorbitol stimulation. Treatment of cells with the tyrosine kinase inhibitor genistein inhibited osmotic shock-stimulated Gab-1 phosphorylation as well as shock-induced glucose transport. Furthermore, pretreatment with the selective Src family kinase inhibitor PP2 completely inhibited the ability of sorbitol treatment to cause tyrosine phosphorylation of Gab-1. We have also shown that microinjection of anti-Gab-1 antibody inhibits osmotic shock-induced GLUT4 translocation. Furthermore, phosphorylated Gab-1 binds and activates phosphatidylinositol 3-kinase (PI3K) in response to osmotic shock. The PI3K activity associated with Gab-1 was 82% of that associated with anti-phosphotyrosine antibodies, indicating that Gab-1 is the major site for PI3K recruitment following osmotic shock stimulation. Although wortmannin only causes a partial block of osmotic shock-stimulated glucose uptake, wortmannin completely abolishes Gab-1 associated PI3K activity. This suggests that other tyrosine kinase-dependent pathways, in addition to the Gab-1-PI3K pathway, contribute to osmotic shock-mediated glucose transport. To date, Gab-1 is the first protein identified as a member of the osmotic shock signal transduction pathway.

Published

2000

21. The tumor suppressor PTEN negatively regulates insulin signaling in 3T3-L1 adipocytes.

Author

Nakashima N, Sharma PM, Imamura T, Bookstein R, and Olefsky JM

Subjects

3T3 Cells, Adenoviridae genetics, Animals, Blotting, Western, Cell Line, DNA, Complementary metabolism, Deoxyglucose metabolism, Gene Transfer Techniques, Glucose Transporter Type 4, Green Fluorescent Proteins, Humans, Luminescent Proteins metabolism, MAP Kinase Signaling System, Mice, Microscopy, Fluorescence, Monosaccharide Transport Proteins metabolism, PTEN Phosphohydrolase, Phosphatidylinositol 3-Kinases metabolism, Phosphorylation, Adipocytes metabolism, Insulin metabolism, Muscle Proteins, Phosphoric Monoester Hydrolases physiology, Tumor Suppressor Proteins

Abstract

PTEN is a tumor suppressor with sequence homology to protein-tyrosine phosphatases and the cytoskeleton protein tensin. PTEN is capable of dephosphorylating phosphatidylinositol 3,4, 5-trisphosphate in vitro and down-regulating its levels in insulin-stimulated 293 cells. To study the role of PTEN in insulin signaling, we overexpressed PTEN in 3T3-L1 adipocytes approximately 30-fold above uninfected or control virus (green fluorescent protein)-infected cells, using an adenovirus gene transfer system. PTEN overexpression inhibited insulin-induced 2-deoxy-glucose uptake by 36%, GLUT4 translocation by 35%, and membrane ruffling by 50%, all of which are phosphatidylinositol 3-kinase-dependent processes, compared with uninfected cells or cells infected with control virus. Microinjection of an anti-PTEN antibody increased basal and insulin stimulated GLUT4 translocation, suggesting that inhibition of endogenous PTEN function led to an increase in intracellular phosphatidylinositol 3,4,5-trisphosphate levels, which stimulates GLUT4 translocation. Further, insulin-induced phosphorylation of downstream targets Akt and p70S6 kinase were also inhibited significantly by overexpression of PTEN, whereas tyrosine phosphorylation of the insulin receptor and IRS-1 or the phosphorylation of mitogen-activated protein kinase were not affected, suggesting that the Ras/mitogen-activated protein kinase pathway remains fully functional. Thus, we conclude that PTEN may regulate phosphatidylinositol 3-kinase-dependent insulin signaling pathways in 3T3-L1 adipocytes.

Published

2000

22. Endothelin-1-induced GLUT4 translocation is mediated via Galpha(q/11) protein and phosphatidylinositol 3-kinase in 3T3-L1 adipocytes.

Author

Imamura T, Ishibashi K, Dalle S, Ugi S, and Olefsky JM

Subjects

3T3 Cells, Adipocytes enzymology, Adipocytes metabolism, Animals, Biological Transport, GTP-Binding Protein alpha Subunits, Gq-G11, Glucose Transporter Type 4, Mice, Phosphatidylinositol 3-Kinases chemistry, Signal Transduction, Adipocytes drug effects, Endothelin-1 pharmacology, GTP-Binding Proteins metabolism, Monosaccharide Transport Proteins metabolism, Muscle Proteins, Phosphatidylinositol 3-Kinases metabolism

Abstract

Endothelin-1 (ET-1) can stimulate insulin-responsive glucose transporter (GLUT4) translocation in 3T3-L1 adipocytes (Wu-Wong, J. R., Berg, C. E., Wang, J., Chiou, W. J., and Fissel, B. (1999) J. Biol. Chem. 274, 8103-8110), and in the current study, we have evaluated the signaling pathway leading to this response. First, we inhibited endogenous Galpha(q/11) function by single-cell microinjection using anti-Galpha(q/11) antibody or RGS2 protein (a GTPase activating protein for Galpha(q)) followed by immunostaining to quantitate GLUT4 translocation in 3T3-L1 adipocytes. ET-1-stimulated GLUT4 translocation was markedly decreased by 70 or 75% by microinjection of Galpha(q/11) antibody or RGS2 protein, respectively. Pretreatment of cells with the Galpha(i) inhibitor (pertussis toxin) or microinjection of a Gbetagamma inhibitor (glutathione S-transferase-beta-adrenergic receptor kinase (GST-BARK)) did not inhibit ET-1-induced GLUT4 translocation, indicating that Galpha(q/11 )mediates ET-1 signaling to GLUT4 translocation. Next, we found that ET-1-induced GLUT4 translocation was inhibited by the phosphatidylinositol (PI) 3-kinase inhibitors wortmannin or LY294002, but not by the phospholipase C inhibitor U-73122. ET-1 stimulated the PI 3-kinase activity of the p110alpha subunit (5.5-fold), and microinjection of anti-p110alpha or PKC-lambda antibodies inhibited ET-stimulated GLUT4 translocation. Finally, we found that Galpha(q/11) formed immunocomplexes with the type-A endothelin receptor and the 110alpha subunit of PI 3-kinase and that ET-1 stimulation enhances tyrosine phosphorylation of Galpha(q/11). These results indicate that: 1) ET-1 signaling to GLUT4 translocation is dependent upon Galpha(q/11) and PI 3-kinase; and 2) Galpha(q/11) can transmit signals from the ET(A) receptor to the p110alpha subunit of PI 3-kinase, as does insulin, subsequently leading to GLUT4 translocation.

Published

1999

23. Membrane-targeted phosphatidylinositol 3-kinase mimics insulin actions and induces a state of cellular insulin resistance.

Author

Egawa K, Sharma PM, Nakashima N, Huang Y, Huver E, Boss GR, and Olefsky JM

Subjects

3T3 Cells, Animals, Biological Transport, Catalytic Domain, Glucose metabolism, Glycogen Synthase metabolism, Mice, Molecular Mimicry, Monosaccharide Transport Proteins, Peptide Fragments metabolism, Proto-Oncogene Proteins p21(ras) metabolism, Ribosomal Protein S6 Kinases metabolism, Signal Transduction, Swine, Insulin physiology, Insulin Resistance, Phosphatidylinositol 3-Kinases metabolism

Abstract

Phosphatidylinositol (PI) 3-kinase plays an important role in various insulin-stimulated biological responses including glucose transport, glycogen synthesis, and protein synthesis. However, the molecular link between PI 3-kinase and these biological responses is still unclear. We have investigated whether targeting of the catalytic p110 subunit of PI 3-kinase to cellular membranes is sufficient and necessary to induce PI 3-kinase dependent signaling responses, characteristic of insulin action. We overexpressed Myc-tagged, membrane-targeted p110 (p110(CAAX)), and wild-type p110 (p110(WT)) in 3T3-L1 adipocytes by adenovirus-mediated gene transfer. Overexpressed p110(CAAX) exhibited approximately 2-fold increase in basal kinase activity in p110 immunoprecipitates, that further increased to approximately 4-fold with insulin. Even at this submaximal PI 3-kinase activity, p110(CAAX) fully stimulated p70 S6 kinase, Akt, 2-deoxyglucose uptake, and Ras, whereas, p110(WT) had little or no effect on these downstream effects. Interestingly p110(CAAX) did not activate MAP kinase, despite its stimulation of p21(ras). Surprisingly, p110(CAAX) did not increase basal glycogen synthase activity, and inhibited insulin stimulated activity, indicative of cellular resistance to this action of insulin. p110(CAAX) also inhibited insulin stimulated, but not platelet-derived growth factor-stimulated mitogen-activated protein kinase phosphorylation, demonstrating that the p110(CAAX) induced inhibition of mitogen-activated protein kinase and insulin signaling is specific, and not due to some toxic or nonspecific effect on the cells. Moreover, p110(CAAX) stimulated IRS-1 Ser/Thr phosphorylation, and inhibited IRS-1 associated PI 3-kinase activity, without affecting insulin receptor tyrosine phosphorylation, suggesting that it may play an important role as a negative regulator for insulin signaling. In conclusion, our studies show that membrane-targeted PI 3-kinase can mimic a number of biologic effects normally induced by insulin. In addition, the persistent activation of PI 3-kinase induced by p110(CAAX) expression leads to desensitization of specific signaling pathways. Interestingly, the state of cellular insulin resistance is not global, in that some of insulin's actions are inhibited, whereas others are intact.

Published

1999

24. The functional role of CrkII in actin cytoskeleton organization and mitogenesis.

Author

Nakashima N, Rose DW, Xiao S, Egawa K, Martin SS, Haruta T, Saltiel AR, and Olefsky JM

Subjects

Cells, Cultured, Cytoskeleton drug effects, DNA Replication, Electroporation, Epidermal Growth Factor administration & dosage, Epidermal Growth Factor pharmacology, Humans, Insulin administration & dosage, Insulin pharmacology, Insulin-Like Growth Factor I administration & dosage, Insulin-Like Growth Factor I pharmacology, Microinjections, Mitosis, Phosphorylation, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-cbl, Proto-Oncogene Proteins c-crk, Receptor, Insulin metabolism, Recombinant Fusion Proteins metabolism, Signal Transduction, Tyrosine metabolism, Actins physiology, Cytoskeleton physiology, Protein Kinases physiology, Ubiquitin-Protein Ligases, src Homology Domains

Abstract

Crk is a member of a family of adapter proteins predominantly composed of Src homology 2 and 3 domains, whose role in signaling pathways is presently unclear. Using an in situ electroporation system which permits the introduction of glutathione S-transferase (GST) fusion proteins into cells, we found that c-CrkII bound to p130(cas), but not to paxillin in serum-starved rat-1 fibroblasts overexpressing the human insulin receptor (HIRc cells) in vivo. 17 nM insulin stimulation dissociated the binding of c-CrkII to p130(cas), whereas 13 nM insulin-like growth factor-I, 16 nM epidermal growth factor (EGF), and 10% serum each showed little or no effect. We found that stress fiber formation is consistent with a change in the p130(cas).c-CrkII interactions before and after growth factor stimulation. Microinjection of either GST-Crk-SH2 or -Crk-(N)SH3 domains, or anti-Crk antibody each inhibited stress fiber formation before and after insulin-like growth factor-I, EGF, and serum stimulation. Insulin stimulation by itself caused stress fiber breakdown and there was no additive effect of microinjection. Microinjection of anti-p130(cas) antibody also blocked stress fiber formation in quiescent cells. Microinjection of the Crk-inhibitory reagents also inhibited DNA synthesis after insulin-like growth factor-I, EGF, and serum stimulation, but not after insulin. These data suggest that the complex containing p130(cas).c-CrkII may play a crucial role in actin cytoskeleton organization and in anchorage-dependent DNA synthesis.

Published

1999

25. Insulin-stimulated glucose transport minireview series.

Author

Olefsky JM

Subjects

Animals, Biological Transport, Glucose Transporter Type 4, Humans, Mice, Monosaccharide Transport Proteins metabolism, Glucose metabolism, Insulin physiology, Muscle Proteins

Published

1999

26. Platelet-derived growth factor inhibits insulin stimulation of insulin receptor substrate-1-associated phosphatidylinositol 3-kinase in 3T3-L1 adipocytes without affecting glucose transport.

Author

Staubs PA, Nelson JG, Reichart DR, and Olefsky JM

Subjects

3T3 Cells, Adipocytes drug effects, Adipocytes enzymology, Animals, Biological Transport, Enzyme Activation, Glucose Transporter Type 4, Insulin pharmacology, Insulin Receptor Substrate Proteins, Mice, Monosaccharide Transport Proteins metabolism, Phosphorylation, Serine metabolism, Threonine metabolism, Tyrosine metabolism, Glucose metabolism, Insulin Antagonists pharmacology, Muscle Proteins, Phosphatidylinositol 3-Kinases metabolism, Phosphoproteins metabolism, Platelet-Derived Growth Factor pharmacology

Abstract

Phosphatidylinositol 3-kinase (PI3K) activation is necessary for insulin-responsive glucose transporter (GLUT4) translocation and glucose transport. Insulin and platelet-derived growth factor (PDGF) stimulate PI3K activity in 3T3-L1 adipocytes, but only insulin is capable of stimulating GLUT4 translocation and glucose transport. We found that PDGF causes serine/threonine phosphorylation of insulin receptor substrate 1 (IRS-1) in 3T3-L1 cells, measured by altered mobility on SDS-polyacrylamide gel, and this leads to a decrease in insulin-stimulated tyrosine phosphorylation of IRS-1. The PI3K inhibitors wortmannin and LY294002 inhibit the PDGF-induced phosphorylation of IRS-1, whereas the MEK inhibitor PD98059 was without a major effect. PDGF pretreatment for 60-90 min led to a marked 80-90% reduction in insulin stimulatable phosphotyrosine and IRS-1-associated PI3K activity. We examined the functional consequences of this decrease in IRS-1-associated PI3K activity. Interestingly, insulin stimulation of GLUT4 translocation and glucose transport was unaffected by 60-90 min of PDGF preincubation. Furthermore, insulin activation of Akt and p70(s6kinase), kinases downstream of PI3K, was unaffected by PDGF pretreatment. Wortmannin was capable of blocking these insulin actions following PDGF pretreatment, suggesting that PI3K was still necessary for these effects. In conclusion, 1) PDGF causes serine/threonine phosphorylation of IRS-1, and PI3K, or a kinase downstream of PI3K, mediates this phosphorylation. 2) This PDGF-induced phosphorylation of IRS-1 leads to a significant decrease in insulin-stimulated PI3K activity. 3) PDGF has no effect on insulin stimulation of Akt, p70(s6kinase), GLUT4 translocation, or glucose transport. 4) This suggests the existence of an IRS-1-independent pathway leading to the activation of PI3K, Akt, and p70(s6kinase); GLUT4 translocation; and glucose transport.

Published

1998

27. Inhibition of phosphatidylinositol 3-kinase activity by adenovirus-mediated gene transfer and its effect on insulin action.

Author

Sharma PM, Egawa K, Huang Y, Martin JL, Huvar I, Boss GR, and Olefsky JM

Subjects

3T3 Cells, Adenoviridae, Adipocytes enzymology, Animals, Biological Transport, Calcium-Calmodulin-Dependent Protein Kinases metabolism, DNA Replication, Deoxyglucose metabolism, Fibroblasts metabolism, Genetic Vectors, Guanosine Triphosphate metabolism, Humans, Insulin Receptor Substrate Proteins, Mice, Phosphatidylinositol 3-Kinases metabolism, Phosphoproteins metabolism, Proto-Oncogene Proteins p21(ras) metabolism, RNA, Messenger metabolism, Swine, Gene Transfer Techniques, Insulin physiology, Phosphatidylinositol 3-Kinases genetics, Phosphoinositide-3 Kinase Inhibitors

Abstract

Phosphatidylinositol 3-kinase (PI 3-K) is implicated in cellular events including glucose transport, glycogen synthesis, and protein synthesis. It is activated in insulin-stimulated cells by binding of the Src homology 2 (SH2) domains in its 85-kDa regulatory subunit to insulin receptor substrate-1 (IRS-1), and, others. We have previously shown that IRS-1-associated PI 3-kinase activity is not essential for insulin-stimulated glucose transport in 3T3-L1 adipocytes, and that alternate pathways exist in these cells. We now show that adenovirus-mediated overexpression of the p85N-SH2 domain in these cells behaves in a dominant-negative manner, interfering with complex formation between endogenous PI 3-K and its SH2 binding targets. This not only inhibited insulin-stimulated IRS-1-associated PI 3-kinase activity, but also completely blocked anti-phosphotyrosine-associated PI 3-kinase activity, which would include the non-IRS-1-associated activity. This resulted in inhibition of insulin-stimulated glucose transport, glycogen synthase activity and DNA synthesis. Further, Ser/Thr phosphorylation of downstream molecules Akt and p70 S6 kinase was inhibited. However, co-expression of a membrane-targeted p110(C) with the p85N-SH2 protein rescued glucose transport, supporting our argument that the p85N-SH2 protein specifically blocks insulin-mediated PI 3-kinase activity, and, that the signaling pathways downstream of PI 3-kinase are intact. Unexpectedly, GTP-bound Ras was elevated in the basal state. Since p85 is known to interact with GTPase-activating protein in 3T3-L1 adipocytes, the overexpressed p85N-SH2 peptide could titrate out cellular GTPase-activating protein by direct association, such that it is unavailable to hydrolyze GTP-bound Ras. However, insulin-induced mitogen-activated protein kinase phosphorylation was inhibited. Thus, PI 3-kinase may be required for this action at a step independent of and downstream of Ras. We conclude that, in 3T3-L1 adipocytes, non-IRS-1-associated PI 3-kinase activity is crucial for insulin's metabolic signaling, and that overexpressed p85N-SH2 protein inhibits a variety of insulin's ultimate biological effects.

Published

1998

28. Association of the insulin receptor with phospholipase C-gamma (PLCgamma) in 3T3-L1 adipocytes suggests a role for PLCgamma in metabolic signaling by insulin.

Author

Kayali AG, Eichhorn J, Haruta T, Morris AJ, Nelson JG, Vollenweider P, Olefsky JM, and Webster NJ

Subjects

3T3 Cells, Adipocytes enzymology, Animals, Deoxyglucose metabolism, Enzyme Inhibitors pharmacology, Estrenes pharmacology, Glucose Transporter Type 4, Isoenzymes antagonists & inhibitors, Lipolysis, Male, Mice, Microinjections, Monosaccharide Transport Proteins metabolism, Phospholipase C gamma, Pyrrolidinones pharmacology, Rats, Rats, Sprague-Dawley, Recombinant Fusion Proteins metabolism, Type C Phospholipases antagonists & inhibitors, src Homology Domains, Adipocytes metabolism, Insulin metabolism, Isoenzymes metabolism, Muscle Proteins, Receptor, Insulin metabolism, Signal Transduction, Type C Phospholipases metabolism

Abstract

Phospholipase C-gamma (PLCgamma) is the isozyme of PLC phosphorylated by multiple tyrosine kinases including epidermal growth factor, platelet-derived growth factor, nerve growth factor receptors, and nonreceptor tyrosine kinases. In this paper, we present evidence for the association of the insulin receptor (IR) with PLCgamma. Precipitation of the IR with glutathione S-transferase fusion proteins derived from PLCgamma and coimmunoprecipitation of the IR and PLCgamma were observed in 3T3-L1 adipocytes. To determine the functional significance of the interaction of PLCgamma and the IR, we used a specific inhibitor of PLC, U73122, or microinjection of SH2 domain glutathione S-transferase fusion proteins derived from PLCgamma to block insulin-stimulated GLUT4 translocation. We demonstrate inhibition of 2-deoxyglucose uptake in isolated primary rat adipocytes and 3T3-L1 adipocytes pretreated with U73122. Antilipolytic effect of insulin in 3T3-L1 adipocytes is unaffected by U73122. U73122 selectively inhibits mitogen-activated protein kinase, leaving the Akt and p70 S6 kinase pathways unperturbed. We conclude that PLCgamma is an active participant in metabolic and perhaps mitogenic signaling by the insulin receptor in 3T3-L1 adipocytes.

Published

1998

29. Grb10 interacts differentially with the insulin receptor, insulin-like growth factor I receptor, and epidermal growth factor receptor via the Grb10 Src homology 2 (SH2) domain and a second novel domain located between the pleckstrin homology and SH2 domains.

Author

He W, Rose DW, Olefsky JM, and Gustafson TA

Subjects

Amino Acid Sequence, Animals, Blood Proteins chemistry, CHO Cells, Cricetinae, GRB10 Adaptor Protein, Humans, Insulin-Like Growth Factor I metabolism, Microinjections, Mitosis drug effects, Molecular Sequence Data, Protein Binding, Proteins chemistry, Blood Proteins metabolism, ErbB Receptors metabolism, Phosphoproteins, Proteins metabolism, Receptor, IGF Type 1 metabolism, Receptor, Insulin metabolism, src Homology Domains

Abstract

The Grb10 protein appears to be an adapter protein of unknown function that has been implicated in insulin receptor (IR) signaling. The interaction of this protein with the IR has been shown to be mediated in part by the Src homology 2 (SH2) domain of Grb10. Here we demonstrate the existence of a second novel domain within Grb10 that interacts with the IR and insulin-like growth factor receptor in a kinase-dependent manner. This domain was localized to a region of approximately 50 amino acids, and we term it the BPS domain to denote its location between the PH and SH2 domains. The BPS domain does not bear any obvious resemblance to other known protein interaction domains but is highly conserved among the Grb10-related proteins Grb7 and Grb14. We show that the BPS domain interaction is dependent upon receptor tyrosine kinase activity. Furthermore, interaction of the BPS domain requires the kinase domain of the IR, since mutation of the paired tyrosine residues (Y1150F/Y1151F) within the IR activation loop dramatically reduced the interaction. Last, our data suggest that the presence of two distinct protein interaction domains may help to determine the specificity by which Grb10 interacts with different receptors. Specifically, the IR, which appears to interact most strongly with Grb10, interacts well with both the SH2 and BPS domains. Conversely, the insulin-like growth factor receptor and EGFR, which interact less avidly with Grb10, interact well only with the BPS domain or the SH2 domain, respectively. In summary, our findings demonstrate the existence of a previously unidentified tyrosine kinase activity-dependent binding domain located between the Pleckstrin homology and SH2 domains of Grb10.

Published

1998

30. The proto-oncogene product p120(cbl) links c-Src and phosphatidylinositol 3'-kinase to the integrin signaling pathway.

Author

Ojaniemi M, Martin SS, Dolfi F, Olefsky JM, and Vuori K

Subjects

Animals, Cell Adhesion, Cytoskeletal Proteins metabolism, Mice, Microfilament Proteins metabolism, Paxillin, Phosphatidylinositol 3-Kinases, Phosphoproteins metabolism, Phosphorylation, Proto-Oncogene Proteins c-cbl, Tensins, Tyrosine metabolism, src Homology Domains, Genes, src, Integrins physiology, Phosphotransferases (Alcohol Group Acceptor) metabolism, Proto-Oncogene Proteins metabolism, Signal Transduction, Ubiquitin-Protein Ligases

Abstract

Integrin-mediated cell adhesion triggers intracellular signaling cascades, including tyrosine phosphorylation of intracellular proteins. We show in this report that p120(cbl) (Cbl), the 120-kDa c-cbl proto-oncogene product, becomes tyrosine-phosphorylated during integrin-mediated macrophage cell adhesion to extracellular matrix substrata and anti-integrin antibodies. This tyrosine phosphorylation does not occur when cells attach to polylysine, to which cells adhere in a nonspecific fashion. It also does not take place when adhesion-induced reorganization of the cytoskeleton is inhibited with cytochalasin D. In contrast to the rapid and transient tyrosine phosphorylation of Cbl by CSF-1 stimulation, tyrosine phosphorylation of Cbl by cell attachment was gradual and persistent. Tyrosine-phosphorylated Cbl was found to form complexes with the SH2 domain-containing signaling proteins Src and phosphatidylinositol 3-kinase; in vitro kinase assays demonstrated that these kinases were active in the Cbl complexes following integrin ligand binding. Furthermore, Cbl was found to translocate to the plasma membrane in response to cell adhesion to fibronectin. These observations suggest that Cbl serves as a docking protein and may transduce signals to downstream signaling pathways following integrin-mediated cell adhesion in macrophages.

Published

1997

31. Functional roles of the Shc phosphotyrosine binding and Src homology 2 domains in insulin and epidermal growth factor signaling.

Author

Ricketts WA, Rose DW, Shoelson S, and Olefsky JM

Subjects

Animals, Cell Cycle, Cell Line, Cricetinae, Cricetulus, Fibroblasts metabolism, Glutathione Transferase metabolism, Microinjections, Recombinant Fusion Proteins metabolism, ErbB Receptors metabolism, Phosphotyrosine metabolism, Proteins metabolism, Receptor, Insulin metabolism, Signal Transduction, src Homology Domains

Abstract

Shc is involved in the activation of Ras in response to many growth factors. Shc contains two phosphotyrosine binding domains, an Src homology 2 (SH2) domain in the carboxyl terminus of the protein and a phosphotyrosine binding (PTB) domain in the amino terminus. Since functional roles for these two domains have not been established, we microinjected glutathione S-transferase fusion proteins of either the Shc PTB or SH2 domains into fibroblasts expressing insulin and epidermal growth factor receptors and measured their effects on DNA synthesis. We found that the Shc PTB was necessary for insulin-induced mitogenic signaling, whereas the SH2 domain was not. In contrast, for epidermal growth factor signaling, the Shc SH2 was functionally more important. These differential modes of signal transduction may be an important factor in determining the specificity of the response of a cell to external stimuli.

Published

1996

32. Interaction of a GRB-IR splice variant (a human GRB10 homolog) with the insulin and insulin-like growth factor I receptors. Evidence for a role in mitogenic signaling.

Author

O'Neill TJ, Rose DW, Pillay TS, Hotta K, Olefsky JM, and Gustafson TA

Subjects

Adipose Tissue chemistry, Alternative Splicing, Amino Acid Sequence, Animals, Base Sequence, Cell Division drug effects, Fibroblasts drug effects, GRB10 Adaptor Protein, Haplorhini, HeLa Cells, Humans, Mice, Microinjections, Molecular Sequence Data, Phosphotyrosine metabolism, Proteins genetics, RNA, Messenger metabolism, Rats, Yeasts, Insulin metabolism, Proteins metabolism, Receptor, IGF Type 1 metabolism, Receptor, Insulin metabolism, Signal Transduction

Abstract

We have utilized the yeast two-hybrid system to identify proteins that interact with the cytoplasmic domain of the insulin receptor. We identified a human cDNA that is a splice variant of the human GRB10 homolog GRB-IR, which we term GRB10/IR-SV1 (for GRB10/GRB-IR splice variant 1). The protein encoded by the GRB10/IR-SV1 cDNA contains an SH2 domain and a pleckstrin homology domain. Cloning of a full-length human cDNA revealed a predicted coding sequence that was similar to the mouse GRB10 protein, although GRB10/IR-SV1 contained an 80-amino acid deletion. The GRB10/IR-SV1 cDNA is a splice variant of the GRB-IR cDNA such that GRB10/IR-SV1 contains an intact pleckstrin homology domain and a distinct amino terminus. The interaction of GRB10/IR-SV1 with the insulin receptor and the insulin-like growth factor I (IGF-I) receptor is mediated by the SH2 domain, and we show that glutathione S-transferase-SH2 domain fusion proteins interact specifically in vitro with the insulin receptor derived from mammalian cells. The GRB10/IR-SV1 SH2 domain also interacted with an approximately 135-kDa phosphoprotein from unstimulated cell lysates, an interaction that decreased after insulin stimulation. We present evidence that the GRB10/IR-SV1 protein plays a functional role in insulin and IGF-I signaling by showing that microinjection of an SH2 domain fusion protein inhibited insulin- and IGF-I-stimulated mitogenesis in fibroblasts, yet had no effect on mitogenesis induced by epidermal growth factor. Our findings suggest that GRB10/IR-SV1 may serve to positively link the insulin and IGF-I receptors to an uncharacterized mitogenic signaling pathway.

Published

1996

33. Protein-tyrosine phosphatase 1B is a negative regulator of insulin- and insulin-like growth factor-I-stimulated signaling.

Author

Kenner KA, Anyanwu E, Olefsky JM, and Kusari J

Subjects

Amino Acid Sequence, Animals, CHO Cells, Cell Line, Cricetinae, Glucose metabolism, Glycogen metabolism, Molecular Sequence Data, Phosphotyrosine metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Rats, Receptor, Insulin physiology, Recombinant Proteins, Signal Transduction, Insulin physiology, Insulin-Like Growth Factor I physiology, Protein Tyrosine Phosphatases metabolism

Abstract

To understand the physiological role of protein-tyrosine phosphatase 1B (PTPase 1B) in insulin and insulin-like growth factor-I (IGF-I) signaling, we established clonal cell lines overexpressing wild type or inactive mutant (C215S) PTPase 1B in cells overexpressing insulin (Hirc) or IGF-I (CIGFR) receptors. PTPase 1B overexpression in transfected cells was verified by immunoblot analysis with a monoclonal PTPase 1B antibody. Subfractionation of parental cells demonstrated that greater than 90% of PTPase activity was localized in the Triton X-100-soluble particulate (P1) cell fraction. PTPase activity in the P1 fraction of cells overexpressing wild type PTPase 1B was 3-6-fold higher than parental cells but was unaltered in all fractions from C215S PTPase 1B-containing cells. The overexpression of wild type and C215S PTPase 1B had no effects on intrinsic receptor kinase activity, growth rate, or general cell morphology. The effects of PTPase 1B overexpression on cellular protein tyrosine phosphorylation were examined by anti-phosphotyrosine immunoblot analysis. No differences were apparent under basal conditions, but hormone-stimulated receptor autophosphorylation and/or insulin receptor substrate tyrosine phosphorylation were inhibited in cells overexpressing wild type PTPase 1B and increased in cells expressing mutant PTPase 1B, in comparison with parental cells. Metabolic signaling, assessed by ligand-stimulated [14C]glucose incorporation into glycogen, was also inhibited in cells overexpressing active PTPase 1B and enhanced in cells containing C215S PTPase 1B. These data strongly suggest that PTPase 1B acts as a negative regulator of insulin and IGF-I signaling.

Published

1996

34. Activated phosphatidylinositol 3-kinase is sufficient to mediate actin rearrangement and GLUT4 translocation in 3T3-L1 adipocytes.

Author

Martin SS, Haruta T, Morris AJ, Klippel A, Williams LT, and Olefsky JM

Subjects

3T3 Cells, Animals, Biological Transport, Cell Compartmentation, Cell Membrane metabolism, Cell Membrane ultrastructure, Enzyme Activation, Genetic Vectors, Glucose Transporter Type 4, Mice, Microinjections, Microscopy, Fluorescence, Phosphatidylinositol 3-Kinases, Phosphotransferases (Alcohol Group Acceptor) genetics, Recombinant Proteins metabolism, Actins metabolism, Adipocytes metabolism, Monosaccharide Transport Proteins metabolism, Muscle Proteins, Phosphotransferases (Alcohol Group Acceptor) metabolism

Abstract

Insulin stimulation of 3T3-L1 adipocytes causes rapid translocation of actin and the GLUT4 glucose transporter to the plasma membrane. Both processes depend on the activity of phosphatidylinositol 3-kinase. Using single cell microinjection, we have transiently expressed a constitutively activated mutant of phosphatidylinositol 3-kinase, p110*, in 3T3-L1 adipocytes. Fluorescent detection of GLUT4 protein and actin within these cells demonstrates that expression of p110* is sufficient to cause translocation of GLUT4 to the plasma membrane and the formation of actin membrane ruffles. These effects are inhibited by wortmannin in the p110*-expressing cells, indicating that the phosphatidylinositol 3-kinase activity of the protein is required. Overexpression of an identical protein containing a point mutation in the kinase domain, p110*Deltakin, was incapable of mediating either action, confirming that neither the microinjection process nor a nonspecific effect of the protein was responsible for the observed effects. These data suggest that although insulin is capable of inducing numerous signaling pathways, the isolated activation of phosphatidylinositol 3-kinase can initiate the signaling cascade leading to both actin rearrangement and GLUT4 translocation in the absence of insulin stimulation.

Published

1996

35. Expression of dominant negative mutant SHPTP2 attenuates phosphatidylinositol 3'-kinase activity via modulation of phosphorylation of insulin receptor substrate-1.

Author

Ugi S, Maegawa H, Kashiwagi A, Adachi M, Olefsky JM, and Kikkawa R

Subjects

Animals, CHO Cells, Cell Line, Cricetinae, Glutathione Transferase genetics, Glutathione Transferase metabolism, Humans, Insulin Receptor Substrate Proteins, Intracellular Signaling Peptides and Proteins, Phosphatidylinositol 3-Kinases, Phosphorylation, Protein Kinases metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 11, Protein Tyrosine Phosphatase, Non-Receptor Type 6, Protein Tyrosine Phosphatases genetics, Rats, Recombinant Fusion Proteins metabolism, Tyrosine metabolism, Insulin metabolism, Phosphoproteins metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism, Protein Tyrosine Phosphatases metabolism

Abstract

To clarify the role of protein-tyrosine phosphatase (PTPase) containing Src homology 2 regions (SHPTP2) in insulin signaling, either wild-type or mutant SHPTP2 (delta PTP; lacking full PTPase domain) was expressed in Rat 1 fibroblasts overexpressing human insulin receptors. In response to insulin, phosphorylation of insulin receptor substrate 1 (IRS-1), IRS-1-associated PTPase activities and phosphatidylinositol (PI) 3'-kinase activities were slightly enhanced in wild-type cells when compared with those in the parent cells transfected with hygromycin-resistant gene alone. In contrast, introduction of delta PTP inhibited insulin-induced association of IRS-1 with endogenous SHPTP2 and impaired both insulin-stimulated phosphorylation of IRS-1 and activation of PI 3'-kinase. Furthermore, decreased content of p85 subunit of PI 3'-kinase was also found in mutant cells. Consistently, the insulin-stimulated mitogen-activated protein kinase activities and DNA synthesis were also enhanced in wild-type cells, but impaired in mutant cells. Thus, the interaction of SHPTP2 with IRS-1 may be associated with modulation of phosphorylation levels of IRS-1, resulting in the changes of PI 3'-kinase and mitogen-activated protein kinase activity. Furthermore, an impaired insulin signaling in mutant cells may be partly reflected in a decreased content of p85 protein of PI 3'-kinase.

Published

1996

36. Involvement of ErbB2 in the signaling pathway leading to cell cycle progression from a truncated epidermal growth factor receptor lacking the C-terminal autophosphorylation sites.

Author

Sasaoka T, Langlois WJ, Bai F, Rose DW, Leitner JW, Decker SJ, Saltiel A, Gill GN, Kobayashi M, Draznin B, and Olefsky JM

Subjects

Animals, Cell Line, Cell Membrane metabolism, Epidermal Growth Factor physiology, GRB2 Adaptor Protein, Guanine Nucleotide Exchange Factors, Guanosine Diphosphate metabolism, Humans, Macromolecular Substances, Membrane Proteins metabolism, Mice, Phosphorylation, Phosphotyrosine metabolism, Proteins metabolism, Proto-Oncogene Proteins p21(ras) physiology, Shc Signaling Adaptor Proteins, Signal Transduction, Son of Sevenless Proteins, Src Homology 2 Domain-Containing, Transforming Protein 1, Structure-Activity Relationship, ras Guanine Nucleotide Exchange Factors, Adaptor Proteins, Signal Transducing, Adaptor Proteins, Vesicular Transport, Cell Cycle, ErbB Receptors physiology, Receptor, ErbB-2 physiology

Abstract

To investigate the mechanisms underlying the enhanced mitogenic activity of the truncated epidermal growth factor receptor (EGFR) lacking the C-terminal autophosphorylation sites (Delta973-EGFR), we studied the intracellular signaling pathways in NR6 cells expressing human wild type EGFR and Delta973-EGFR. Microinjection of dominant/negative p21ras(N17) completely inhibited EGF-induced DNA synthesis in both cell types. EGF stimulated Shc phosphorylation as well as the formation of wild type EGFR.Shc complexes. In contrast, EGF stimulated Shc phosphorylation without formation of Delta973-EGFR.Shc complexes. Tyrosine-phosphorylated Shc formed complexes with Grb2.Sos, and microinjection of anti-Shc antibody and Shc-SH2 GST fusion protein inhibited EGF stimulation of DNA synthesis in both cell lines. EGF markedly increased ErbB2 tyrosine phosphorylation in wild type EGFR cells. In Delta973-EGFR cells, ErbB2 was tyrosine phosphorylated in the basal state and EGFR stimulated further phosphorylation of ErbB2. In addition to ErbB2, additional proteins were tyrosine phosphorylated in Delta973-EGFR cells, mostly in the molecular mass range of 120 170 kDa. Taken together with our findings indicating coupling of ErbB2 to Shc, these data suggest the importance of an alternative signaling pathway in Delta973-EGFR cells mediated by the formation of heterodimeric structures between the truncated EGFR and ErbB2, followed by coupling through Shc to Grb2.Sos and the p21ras pathway, ultimately leading to mitogenesis.

Published

1996

37. Insulin-stimulated GLUT4 translocation is mediated by a divergent intracellular signaling pathway.

Author

Haruta T, Morris AJ, Rose DW, Nelson JG, Mueckler M, and Olefsky JM

Subjects

1-Methyl-3-isobutylxanthine pharmacology, 3T3 Cells, Adipocytes cytology, Adipocytes drug effects, Animals, Cell Differentiation, Cell Line, Cell Membrane metabolism, Dexamethasone pharmacology, Fibroblasts, Genes, ras, Glucose Transporter Type 4, Humans, Kinetics, Mice, Proto-Oncogene Proteins p21(ras) biosynthesis, Proto-Oncogene Proteins p21(ras) metabolism, Rats, Receptor, Insulin biosynthesis, Receptor, Insulin drug effects, Swine, Transfection, Adipocytes metabolism, Insulin pharmacology, Monosaccharide Transport Proteins metabolism, Muscle Proteins, Receptor, Insulin physiology, Signal Transduction drug effects

Abstract

Insulin stimulates glucose transport largely by mediating translocation of the insulin-sensitive glucose transporter (GLUT4) from an intracellular compartment to the plasma membrane. Using single cell microinjection of 3T3-L1 adipocytes, coupled with immunofluorescence detection of GLUT4 proteins, we have determined that inhibition of endogenous p21ras or injection of oncogenic p21ras has no effect on insulin-stimulated GLUT4 translocation. On the other hand, microinjection of anti-phosphotyrosine antibodies or inhibition of endogenous phosphatidylinositol 3-kinase by microinjection of a GST-p85 SH2 fusion protein markedly inhibits this biologic effect of insulin. These data suggest that the p21ras/mitogen-activated protein kinase pathway is not involved in this metabolic effect of insulin, whereas tyrosine phosphorylation and stimulation of phosphatidylinositol 3-kinase activity are critical components of this signaling pathway.

Published

1995

38. Negative feedback regulation and desensitization of insulin- and epidermal growth factor-stimulated p21ras activation.

Author

Langlois WJ, Sasaoka T, Saltiel AR, and Olefsky JM

Subjects

Animals, Blotting, Western, Calcium-Calmodulin-Dependent Protein Kinases metabolism, GRB2 Adaptor Protein, Guanine Nucleotide Exchange Factors, Guanosine Diphosphate analysis, Guanosine Triphosphate analysis, Humans, Precipitin Tests, Proto-Oncogene Proteins p21(ras) chemistry, Rats, ras Guanine Nucleotide Exchange Factors, Adaptor Proteins, Signal Transducing, Down-Regulation, Epidermal Growth Factor pharmacology, Insulin pharmacology, Proteins metabolism, Proto-Oncogene Proteins p21(ras) metabolism, Signal Transduction

Abstract

Insulin and epidermal growth factor receptors transmit signals for cell proliferation and gene regulation through formation of active GTP-bound p21ras mediated by the guanine nucleotide exchange factor Sos. Sos is constitutively bound to the adaptor protein Grb2 and growth factor stimulation induces association of the Grb2/Sos complex with Shc and movement of Sos to the plasma membrane location of p21ras. Insulin or epidermal growth factor stimulation induces a rapid increase in p21ras levels, but after several minutes levels decline toward basal despite ongoing hormone stimulation. Here we show that deactivation of p21ras correlates closely with phosphorylation of Sos and dissociation of Sos from Grb2, and that inhibition of mitogen-activated protein (MAP) kinase kinase (also known as extracellular signal-related kinase (ERK) kinase, or MEK) blocks both events, resulting in prolonged p21ras activation. These data suggest that a negative feedback loop exists whereby activation of the Raf/MEK/MAP kinase cascade by p21ras causes Sos phosphorylation and, therefore, Sos/Grb2 dissociation, limiting the duration of p21ras activation by growth factors. A serine/threonine kinase downstream of MEK (probably MAP kinase) mediates this desensitization feedback pathway.

Published

1995

39. Localization of the insulin-like growth factor I receptor binding sites for the SH2 domain proteins p85, Syp, and GTPase activating protein.

Author

Seely BL, Reichart DR, Staubs PA, Jhun BH, Hsu D, Maegawa H, Milarski KL, Saltiel AR, and Olefsky JM

Subjects

Amino Acid Sequence, Animals, Arsenicals pharmacology, Binding Sites, CHO Cells, Cricetinae, GTPase-Activating Proteins, Insulin-Like Growth Factor I pharmacology, Intracellular Signaling Peptides and Proteins, Molecular Sequence Data, Phosphatidylinositol 3-Kinases, Phosphorylation, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Protein Tyrosine Phosphatase, Non-Receptor Type 11, Protein Tyrosine Phosphatase, Non-Receptor Type 6, SH2 Domain-Containing Protein Tyrosine Phosphatases, Type C Phospholipases metabolism, Tyrosine metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism, Protein Tyrosine Phosphatases metabolism, Proteins metabolism, Receptor, IGF Type 1 metabolism

Abstract

Potential signaling substrates for the insulin-like growth factor I (IGF-I) receptor are SH2 domain proteins including the p85 subunit of phosphatidylinositol 3-kinase, the tyrosine phosphatase Syp, GTPase activating protein (GAP), and phospholipase C-gamma (PLC-gamma). In this study, we demonstrate an association between the IGF-I receptor and p85, Syp, and GAP, but not with PLC-gamma in lysates of cells overexpressing the human IGF-I receptor. We further investigated these interactions using glutathione S-transferase (GST) fusion proteins containing the amino-terminal SH2 domains of p85 or GAP, or both SH2 domains of Syp or PLC-gamma to precipitate the IGF-I receptor from purified receptor preparations and from whole cell lysates. p85-, Syp-, and GAP-GSTs precipitated the IGF-I receptor, whereas the PLC-gamma-GST did not. Using phosphopeptides corresponding to IGF-I receptor phosphorylation sites, we determined that the p85- and Syp-GST association with the IGF-I receptor could be inhibited by a carboxyl-terminal peptide containing pY1316 and that the GAP-GST association could be inhibited by a NPXY domain peptide. The GAP-GST binding site was confirmed by showing that a mutant IGF-I receptor with a deletion of the NPXY domain including tyrosine 950 was poorly precipitated by the GAP-GST. We conclude that p85 and Syp may bind directly to the IGF-I receptor at tyrosine 1316, and that GAP may bind to the IGF-I receptor at and PLC-gamma was not evident. p85, Syp, and GAP are potential modulators of IGF-I receptor signal transduction.

Published

1995

40. Mechanisms of enhanced transmembrane signaling by an insulin receptor lacking a cytoplasmic beta-subunit domain.

Author

Sasaoka T, Langlois WJ, Rose DW, and Olefsky JM

Subjects

Animals, Cell Line, DNA biosynthesis, Gene Expression, Genes, fos, Glycogen metabolism, In Vitro Techniques, Insulin pharmacology, Insulin Receptor Substrate Proteins, Insulin-Like Growth Factor I physiology, Phosphatidylinositol 3-Kinases, Phosphoproteins metabolism, Phosphorylation, Phosphotransferases (Alcohol Group Acceptor) metabolism, Proto-Oncogene Proteins c-fos genetics, RNA, Messenger genetics, Rats, Receptor, Insulin physiology, Sequence Deletion, Structure-Activity Relationship, Receptor, Insulin chemistry, Signal Transduction

Abstract

We have recently characterized a mutant insulin receptor (HIR delta 978) in which the insulin receptor beta-subunit was truncated at amino acid residue 978. Compared with parental Rat1 cells, the cells expressing the truncated receptor exhibited enhanced sensitivity to insulin's biologic actions. All of these effects are now extended to transcriptional events, since we now show enhanced sensitivity to insulin stimulation of c-fos mRNA expression. These effects were insulin-specific, since insulin-like growth factor-1 stimulation of glucose incorporation into glycogen, alpha-aminoisobutyric acid uptake, and thymidine incorporation into DNA were normal. In addition, the truncated receptor exhibited enhanced sensitivity only in vivo, but not in vitro, since the kinase activity of wheat germ agglutinin-purified receptor preparations was comparable between HIR delta 978 and parental Rat1 insulin receptors. Parental rat endogenous insulin-like growth factor-1 receptors and transfected human insulin receptors form hybrid receptors as well as homologous tetrameric receptors. The normal heterotetrameric receptors possess kinase activity in vivo leading to tyrosine phosphorylation of insulin receptor substrate-1 (IRS-1) and its association with the p85 regulatory subunit of phosphatidyl inositol 3-kinase. Interestingly, preincubation with human-specific anti-insulin receptor antibody abolished the increased insulin sensitivity in glucose incorporation into glycogen in HIR delta 978 cells. Furthermore, microinjection of anti-IRS-1 antibody into HIR delta 978 cells inhibited insulin stimulation of DNA synthesis. In summary: 1) truncated receptors on the cell surface confer enhanced insulin sensitivity in vivo; 2) the normal heterotetrameric receptors are functionally active and couple to IRS-1 efficiently; and 3) IRS-1 is an important molecule transmitting insulin's biological signals in HIR delta 978 cells.

Published

1995

41. Insulin stimulates the tyrosine dephosphorylation of pp125 focal adhesion kinase.

Author

Pillay TS, Sasaoka T, and Olefsky JM

Subjects

Animals, Cells, Cultured, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, Phosphorylation, Rats, Receptor, Insulin metabolism, Cell Adhesion Molecules metabolism, Insulin pharmacology, Protein-Tyrosine Kinases metabolism, Tyrosine metabolism

Abstract

The phosphorylation state of pp125 focal adhesion kinase in response to insulin was examined in parental and transfected Rat-1 fibroblasts expressing both wild-type (HIRc cells) and mutant human insulin receptor cDNAs lacking the C-terminal twin tyrosine phosphorylation sites (YF2 cells) or a deletion mutant lacking the distal 43 amino acids of the beta-subunit (delta CT cells). In HIRc cells insulin stimulated the tyrosine dephosphorylation of pp125fak, whereas IGF-I did not. In contrast, the tyrosine phosphorylation state of pp125fak was unchanged in the parental Rat-1 fibroblasts and the YF2 or delta CT mutant cell lines in response to insulin. Analysis of the supernatants revealed that pp125fak was only one component of the major M(r), 120-130-kDa phosphotyrosine band seen in HIRc cells. We conclude that: 1) in contrast to other growth factors, insulin stimulates the dephosphorylation of pp125fak; 2) the presence of the insulin receptor C-terminal tyrosines 1328 and 1334 is required for the insulin-stimulated tyrosine dephosphorylation of pp125fak, suggesting a possible SH2 domain-dependent interaction; 3) insulin may modulate integrin-mediated signaling through pp125fak by altering the phosphorylation state of pp125fak.

Published

1995

42. The signaling pathway coupling epidermal growth factor receptors to activation of p21ras.

Author

Sasaoka T, Langlois WJ, Leitner JW, Draznin B, and Olefsky JM

Subjects

Animals, Cell Line, Epidermal Growth Factor pharmacology, GRB2 Adaptor Protein, Phosphorylation, Proteins metabolism, Rats, Tyrosine metabolism, Adaptor Proteins, Signal Transducing, ErbB Receptors metabolism, Oncogene Protein p21(ras) metabolism, Signal Transduction

Abstract

Epidermal growth factor (EGF) treatment causes autophosphorylation of the epidermal growth factor receptor (EGFR) leading to increased guanine nucleotide exchange factor (GEF; Sos) activity and enhanced formation of p21ras-GTP. The connection of the EGFR to p21ras activation can occur through binding of Grb2.Sos complexes to the EGFR or through the adaptor protein Shc via EGFR.Shc.Grb2.Sos multimeric complexes. Therefore, we investigated the importance of Shc in coupling the EGFR to activation of ras GEF (Sos). EGF treatment led to rapid tyrosine phosphorylation of Shc. Although phosphorylated EGFR can bind to both Shc and Grb2, the predominant linkage was observed between EGFR and Shc. Similarly, more Grb2 was associated with Shc than with EGFR after EGF stimulation. Immunoprecipitation of Shc from EGF-stimulated cells removed almost all EGFR-associated Grb2. Furthermore, immunodepletion of Shc proteins from membrane fractions of EGF-stimulated cells removed 93% of the ras GEF activity, whereas, precipitation of EGFR had only a small effect on ras GEF activity. These data indicate that coupling to Shc provides the major pathway linking activated EGFRs to Grb2.Sos and stimulation of the p21ras pathway.

Published

1994

43. Localization of the insulin receptor binding sites for the SH2 domain proteins p85, Syp, and GAP.

Author

Staubs PA, Reichart DR, Saltiel AR, Milarski KL, Maegawa H, Berhanu P, Olefsky JM, and Seely BL

Subjects

Amino Acid Sequence, Animals, Binding Sites, GTPase-Activating Proteins, In Vitro Techniques, Intracellular Signaling Peptides and Proteins, Molecular Sequence Data, Phosphatidylinositol 3-Kinases, Phosphotyrosine, Protein Tyrosine Phosphatase, Non-Receptor Type 11, Protein Tyrosine Phosphatase, Non-Receptor Type 6, Rats, SH2 Domain-Containing Protein Tyrosine Phosphatases, Tyrosine analogs & derivatives, Tyrosine metabolism, Phosphopeptides metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism, Protein Tyrosine Phosphatases metabolism, Proteins metabolism, Receptor, Insulin metabolism

Abstract

The insulin receptor is known to interact with the SH2 domain proteins p85 (the regulatory subunit of phosphatidylinositol 3-kinase), Syp (a tyrosine phosphatase), and GAP (GTPase-activating protein). In this study, we mapped the insulin receptor binding sites for each of these proteins by examining the ability of phosphopeptides, corresponding to insulin receptor phosphorylation sites, and mutant insulin receptors to inhibit an insulin receptor-SH2 domain interaction. Precipitation of partially purified insulin receptors by glutathione S-transferase fusion proteins containing the N-terminal SH2 domains of p85 and GAP and both SH2 domains of Syp was demonstrated. The effect of the addition of each phosphopeptide on insulin receptor precipitation was tested. pY1322, the C-terminal insulin receptor peptide, inhibited insulin receptor precipitation by both p85- and Syp-GST. The NPXY internalization domain peptide inhibited insulin receptor precipitation by GAP-GST. These data were confirmed by mutant insulin receptor experiments. The insulin receptor C-terminal mutants, delta CT and Y/F2, were not precipitated by p85- or Syp-GST and the NPXY mutant insulin receptors, delta Ex16 and HI delta NPEY, were not precipitated by GAP-GST. Therefore, we conclude that p85 and Syp bind to the insulin receptor C terminus at tyrosine 1322 and GAP binds to the insulin receptor NPXY domain at tyrosine 960.

Published

1994

44. Syp (SH-PTP2) is a positive mediator of growth factor-stimulated mitogenic signal transduction.

Author

Xiao S, Rose DW, Sasaoka T, Maegawa H, Burke TR Jr, Roller PP, Shoelson SE, and Olefsky JM

Subjects

Amino Acid Sequence, Animals, Cell Division, Cells, Cultured, Glutathione Transferase metabolism, Immunoglobulin G, Intracellular Signaling Peptides and Proteins, Microinjections, Molecular Sequence Data, Phosphorylation, Protein Tyrosine Phosphatase, Non-Receptor Type 11, Protein Tyrosine Phosphatase, Non-Receptor Type 6, Rats, Recombinant Fusion Proteins metabolism, Tyrosine metabolism, Growth Substances metabolism, Protein Tyrosine Phosphatases metabolism, Signal Transduction

Abstract

Syp (SH-PTP2) was recently identified as a phosphotyrosine phosphatase containing two SH2 domains within its primary structure. In response to appropriate growth factor stimulation, Syp becomes phosphorylated on tyrosine residues and associates with insulin receptor substrate 1 (IRS-1) and/or the corresponding growth factor receptor via its SH2 domains, leading to increased Syp activity. To assess the importance of Syp in mitogenic signaling, we microinjected mammalian fibroblasts with several reagents designed to interfere with Syp SH2/phosphotyrosine interaction in vivo. Insulin-, insulin-like growth factor-1-, and epidermal growth factor-stimulated DNA synthesis, indicated by bromodeoxyuridine (BrdUrd) incorporation, was dramatically decreased following microinjection of a Syp antibody (Ab) (65-85%) or a Syp GST-SH2 fusion protein (approximately 90%) in comparison with cells microinjected with control IgG or glutathione S-transferase (GST), respectively. In addition, microinjection of an IRS-1-derived phosphonopeptide, which inhibits in vitro binding of Syp-SH2 to IRS-1 with an ED50 value of approximately 23 microM, also decreased BrdUrd incorporation in vivo by approximately 50-75%. Microinjection of the Syp Ab, Syp GST-SH2 fusion protein, or the phosphonopeptide had no effect on serum-stimulated BrdUrd incorporation. In conclusion, disruption of Syp function in living cells inhibited cell cycle progression in response to growth factor stimulation, indicating that Syp is a critical positive regulator of mitogenic signal transduction.

Published

1994

45. Evidence for a functional role of Shc proteins in mitogenic signaling induced by insulin, insulin-like growth factor-1, and epidermal growth factor.

Author

Sasaoka T, Rose DW, Jhun BH, Saltiel AR, Draznin B, and Olefsky JM

Subjects

Animals, Cell Line, Humans, Phosphorylation, Proteins chemistry, Rats, Receptor, Insulin genetics, Transfection, Epidermal Growth Factor pharmacology, Insulin pharmacology, Insulin-Like Growth Factor I pharmacology, Mitogens pharmacology, Proteins physiology, Proto-Oncogene Proteins pp60(c-src), Signal Transduction

Abstract

Shc proteins contain a single SH2 domain, lack catalytic activity, and are substrates for activated receptors for insulin, insulin-like growth factor-1 (IGF-1), and epidermal growth factor (EGF). Treatment with these growth factors induced rapid tyrosine phosphorylation of Shc. We investigated the potential role of Shc in mitogenic signaling. Affinity-purified antibodies were microinjected into living Rat1 fibroblasts overexpressing human insulin receptors. Bromodeoxyuridine incorporation into newly synthesized DNA was subsequently studied to assess the importance of Shc. Cellular microinjection of anti-Shc antibody inhibited BrdU incorporation induced by insulin, IGF-1, and EGF, but did not affect cells stimulated by fetal calf serum. Microinjection of an oncogenic p21ras protein (T24) into quiescent cells produced constitutively active mitogenic signaling, and comicroinjection of T24 with the anti-Shc antibody restored insulin and EGF stimulation of DNA synthesis. Immunoprecipitates of Shc from lysates of insulin-stimulated cells removed 70-80% of guanine nucleotide-releasing factor activity. These results indicate that Shc is an important component in a mitogenic signal transduction pathway that is shared by insulin, IGF-1, and EGF. The functional locus of Shc is either upstream of p21ras or lies on a distinct branch of the pathway leading to cell cycle progression.

Published

1994

46. Shc is the predominant signaling molecule coupling insulin receptors to activation of guanine nucleotide releasing factor and p21ras-GTP formation.

Author

Sasaoka T, Draznin B, Leitner JW, Langlois WJ, and Olefsky JM

Subjects

Animals, Cells, Cultured, GRB2 Adaptor Protein, Guanine Nucleotide Exchange Factors, Insulin Receptor Substrate Proteins, Kinetics, Phosphoproteins metabolism, Rats, Shc Signaling Adaptor Proteins, Src Homology 2 Domain-Containing, Transforming Protein 1, ras Guanine Nucleotide Exchange Factors, Adaptor Proteins, Signal Transducing, Adaptor Proteins, Vesicular Transport, Guanosine Triphosphate metabolism, Oncogene Protein p21(ras) metabolism, Proteins metabolism, Receptor, Insulin metabolism, Signal Transduction

Abstract

Insulin stimulates tyrosine phosphorylation of insulin receptor substrate-1 (IRS-1) and She in Rat1 fibroblasts overexpressing wild type insulin receptors. We investigated the relative role of IRS-1 and She in insulin activation of guanine nucleotide releasing factor (GNRF) and p21ras-GTP formation. The time course of insulin-stimulated tyrosine phosphorylation of IRS-1 was rapid, whereas Shc phosphorylation was relatively slow. Growth factor receptor bound protein-2 (Grb2) associated with IRS-1 rapidly and gradually dissociated after 5 min, whereas Grb2 association with Shc was slower and reached a maximum at 10 min after insulin stimulation. Thus, the kinetics of Grb2 association with IRS-1 and She corresponded closely to the time course of tyrosine phosphorylation of IRS-1 and Shc, respectively. Importantly, 3-13-fold more Grb2 was associated with Shc than with IRS-1. In addition, the kinetics of insulin-stimulated GNRF activity and p21ras-GTP formation corresponded more closely to the time course of Shc phosphorylation than to the kinetics of IRS-1 phosphorylation. Furthermore, immunoprecipitation of Shc proteins from cell lysates of insulin-stimulated cells removed 67% of the GNRF activity, whereas precipitation of IRS-1 had a negligible effect on GNRF activity. Thus, although both IRS-1 and Shc associate with Grb2, the current results indicate that Shc plays a more important role than IRS-1 in insulin stimulation of GNRF activity and subsequent p21ras-GTP formation.

Published

1994

47. Mutation of the two carboxyl-terminal tyrosines in the insulin receptor results in enhanced activation of mitogen-activated protein kinase.

Author

Pang L, Milarski KL, Ohmichi M, Takata Y, Olefsky JM, and Saltiel AR

Subjects

Animals, Cells, Cultured, Enzyme Activation, Glutathione Transferase metabolism, Insulin Receptor Substrate Proteins, Mitogen-Activated Protein Kinase 1, Phosphatidylinositol 3-Kinases, Phosphoproteins metabolism, Phosphorylation, Phosphotransferases (Alcohol Group Acceptor) metabolism, Rats, Recombinant Fusion Proteins metabolism, Mutation, Protein Serine-Threonine Kinases metabolism, Protein-Tyrosine Kinases metabolism, Receptor, Insulin genetics, Tyrosine genetics

Abstract

Activation of mitogen-activated protein (MAP) kinase represents an important mechanism in hormonal regulation. To clarify the role of MAP kinase activation in insulin action, we compared the activation of the enzyme in Rat-1 cells transfected with wild-type (Hirc) and mutant insulin receptors in which the 2 carboxyl-terminal tyrosines were substituted with phenylalanine (Y/F2). Expression of the Y/F2 mutant receptor enhanced the responsiveness of MAP kinase to insulin. Moreover, the insulin responsiveness of the activator of this enzyme, MAP kinase kinase, was also increased in these cells. To explore the early signaling events that might account for this increase in responsiveness, we evaluated the tyrosine phosphorylation of the insulin receptor substrate, IRS-1, and its subsequent association with phosphatidylinositol (PI)-3 kinase. In both cell types, insulin led to a dose-dependent increase in the association of tyrosine phosphorylated IRS-1 with the SH2 domain of the p85 regulatory subunit of PI-3 kinase, and also increased the amount of PI kinase activity detected in anti-IRS-1 immunoprecipitates. The effect of insulin was significantly greater in Y/F2 cells, as determined in both assays. In previous studies, cells bearing this receptor mutant exhibited an identical metabolic response but enhanced mitogenic response to insulin when compared with wild-type receptor. These data provide further evidence for divergence of the mitogenic and metabolic signaling pathways at or near the insulin receptor.

Published

1994

48. Insulin and insulin-like growth factor-I signal transduction requires p21ras.

Author

Jhun BH, Meinkoth JL, Leitner JW, Draznin B, and Olefsky JM

Subjects

Animals, Antibodies pharmacology, Cell Line, DNA biosynthesis, Guanosine Triphosphate metabolism, Humans, Microinjections, Oncogene Protein p21(ras) immunology, Proto-Oncogene Proteins c-fos biosynthesis, Rats, Insulin metabolism, Insulin-Like Growth Factor I metabolism, Oncogene Protein p21(ras) physiology, Signal Transduction

Abstract

We have investigated the role of cellular p21ras protein in insulin and insulin-like growth factor-I (IGF-I) signaling pathways. Insulin stimulation increased Ras-GTP formation in Rat-1 fibroblasts overexpressing normal human insulin receptors (HIRc-B), far greater than in parental Rat-1 fibroblasts, indicating that competent insulin receptors mediate this response. Cellular microinjection of a dominant-negative mutant p21ras protein (N17 ras) or anti-p21ras monoclonal antibody (Y13-259) into HIRc-B cells reduced insulin- and IGF-I-stimulated DNA synthesis by 75-90%. Insulin-induced c-fos protein expression was also inhibited by 74%. Microinjection of oncogenic p21ras (T-24 ras) into HIRc-B cells activated the mitogenic pathway, and coinjection of N17 ras and T-24 ras showed that oncogenic p21ras rescued the cells from the N17 ras blockade. This later finding indicates that T-24 ras acts downstream of N17 ras. In conclusion, 1) microinjection of a dominant interferring ras mutant into quiescent cells abrogated subsequent insulin and IGF-I mitogenic signaling; 2) oncogenic ras protein rescued cells from the N17 ras blockade, indicating that T24 ras action is downstream of the site of N17 inhibition; and 3) p21ras is an intermediate signaling molecule in the insulin/IGF-I signal transduction pathway and is required for gene expression and DNA synthesis.

Published

1994

49. Regulation of protein tyrosine phosphatases by insulin and insulin-like growth factor I.

Author

Kenner KA, Hill DE, Olefsky JM, and Kusari J

Subjects

Amino Acid Sequence, Animals, Cell Line, Dose-Response Relationship, Drug, Gene Expression Regulation, Enzymologic drug effects, Immunoblotting, Insulin metabolism, Kinetics, Molecular Sequence Data, Muscles drug effects, Peptides metabolism, Protein Tyrosine Phosphatases biosynthesis, Protein Tyrosine Phosphatases isolation & purification, RNA, Messenger biosynthesis, Rats, Receptor, Insulin metabolism, Subcellular Fractions enzymology, Transcription, Genetic drug effects, Insulin pharmacology, Insulin-Like Growth Factor I pharmacology, Muscles enzymology, Protein Tyrosine Phosphatases metabolism

Abstract

In this study, we have examined the effects of insulin and insulin-like growth factor (IGF)-I on protein tyrosine phosphatase (PTPase) activity in rat L6 skeletal muscle cells. Under basal conditions, about 85% of total cellular PTPase activity was associated with the particulate (Triton X-100-soluble) fraction. Incubation of the cells with 100 nM insulin or IGF-I significantly increased particulate PTPase activity (p < 0.005) without altering activity in the supernatant or Triton X-100-insoluble fractions. Dose responses studies suggested that the effect of each hormone was mediated through its own receptor. PTPase activity was regulated by both acute and chronic insulin and IGF-I treatment. Maximal stimulation by both ligands occurred at 32 h and then declined. By using an antibody and a cDNA specific for PTPase1B, we found that the chronic stimulation of PTPase activity was accompanied by enhanced expression of PTPase1B mRNA and protein. Maximal induction of PTPase1B mRNA and protein by insulin and IGF-I occurred at 12 and 24 h, respectively. Based on these data, it can be suggested that ligand-stimulated PTPase activity might oppose tyrosine kinase-mediated insulin or IGF-I signal transmission and thus desensitize cells to long-term action by insulin and IGF-I. However, it is also possible that PTPase act as positive mediators of insulin and IGF-I action.

Published

1993

50. Insulin activates p21Ras and guanine nucleotide releasing factor in cells expressing wild type and mutant insulin receptors.

Author

Draznin B, Chang L, Leitner JW, Takata Y, and Olefsky JM

Subjects

Animals, Cell Line, GTPase-Activating Proteins, Guanine Nucleotide Exchange Factors, Guanosine Diphosphate metabolism, Guanosine Triphosphate metabolism, Kinetics, Mutagenesis, Site-Directed, Phenols pharmacology, Protein-Tyrosine Kinases antagonists & inhibitors, Proteins isolation & purification, Proto-Oncogene Proteins p21(ras) isolation & purification, Rats, Receptor, Insulin biosynthesis, Receptor, Insulin genetics, Recombinant Proteins biosynthesis, Recombinant Proteins metabolism, Transfection, ras GTPase-Activating Proteins, ras Guanine Nucleotide Exchange Factors, ras-GRF1, Insulin pharmacology, Inulin pharmacology, Proteins metabolism, Proto-Oncogene Proteins p21(ras) metabolism, Receptor, Insulin metabolism

Abstract

Insulin stimulates the formation of p21RasGTP in Rat-1 fibroblasts overexpressing wild type (HIRc) or mutant (delta CT and Y/F2) insulin receptors. Maximal insulin effect was observed at 7 min in Y/F2 cells, at 10 min in delta CT cells, and at 15 min in HIRc cells. Mutant insulin receptors which display enhanced mitogenic signaling properties stimulated p21Ras.GTP formation to a greater extent than wild type receptors. The amount of p21Ras was not affected by insulin (Western blotting). Tyrosine kinase inhibitor, Lavendustin A (10 nM), completely prevented insulin-induced activation of p21Ras in all cell lines. Insulin did not lead to GAP phosphorylation, or a change in cellular GAP activity, but did result in marked stimulation of Ras guanine nucleotide releasing factor (GRF) activity (by 48% in HIRc, 71% in delta CT, and 120% in Y/F2 cells). These results indicated that p21Ras.GTP is an important signaling molecule in insulin's mitogenic pathway, but may not participate in metabolic signaling and that insulin's stimulatory effects on p21Ras.GTP formation are mediated through Ras GRF.

Published

1993