Your search keyword '"Kath JC"' showing total 260 results

151. Phosphorylation of IRS1 at Serine 307 in Response to Insulin in Human Adipocytes Is Not Likely to be Catalyzed by p70 Ribosomal S6 Kinase.

Author

Rajan, Meenu Rohini, Fagerholm, Siri, Jönsson, Cecilia, Kjølhede, Preben, Turkina, Maria V., and Strålfors, Peter

Subjects

TREATMENT of diabetes, SERINE, FAT cells, PROTEIN kinases, INSULIN receptors, INSULIN resistance, MTOR protein, CELLULAR signal transduction, FEEDBACK control systems

Abstract

The insulin receptor substrate-1 (IRS1) is phosphorylated on serine 307 (human sequence, corresponding to murine serine 302) in response to insulin as part of a feedback loop that controls IRS1 phosphorylation on tyrosine residues by the insulin receptor. This in turn directly affects downstream signaling and is in human adipocytes implicated in the pathogenesis of insulin resistance and type 2 diabetes. The phosphorylation is inhibited by rapamycin, a specific inhibitor of mammalian target of rapamycin (mTOR) in complex with raptor (mTORC1). The mTORC1-downstream p70 ribosomal protein S6 kinase (S6K1), which is activated by insulin, can phosphorylate IRS1 at serine 307 in vitro and is considered the physiological protein kinase. Because the IRS1 serine 307-kinase catalyzes a critical step in the control of insulin signaling and constitutes a potential target for treatment of insulin resistance, it is important to know whether S6K1 is the physiological serine 307-kinase or not. We report that, by several criteria, S6K1 does not phosphorylate IRS1 at serine 307 in response to insulin in intact human primary adipocytes: (i) The time-courses for phosphorylation of S6K1 and its phosphorylation of S6 are not compatible with the phosphorylation of IRS1 at serine 307; (ii) A dominant-negative construct of S6K1 inhibits the phosphorylation of S6, without effect on the phosphorylation of IRS1 at serine 307; (iii) The specific inhibitor of S6K1 PF-4708671 inhibits the phosphorylation of S6, without effect on phosphorylation of IRS1 at serine 307. mTOR-immunoprecipitates from insulin-stimulated adipocytes contains an unidentified protein kinase specific for phosphorylation of IRS1 at serine 307, but it is not mTOR or S6K1. [ABSTRACT FROM AUTHOR]

Published

2013

152. Akt Regulates TNFα Synthesis Downstream of RIP1 Kinase Activation during Necroptosis.

Author

McNamara, Colleen R., Ahuja, Ruchita, Osafo-Addo, Awo D., Barrows, Douglas, Kettenbach, Arminja, Skidan, Igor, Teng, Xin, Cuny, Gregory D., Gerber, Scott, and Degterev, Alexei

Subjects

PROTEIN kinase B, TUMOR necrosis factors, RECEPTOR-interacting proteins, CELL death, NECROSIS, INFLAMMATORY bowel diseases, PHOSPHORYLATION, CELLULAR signal transduction, RAPAMYCIN, MACROPHAGES

Abstract

Necroptosis is a regulated form of necrotic cell death that has been implicated in the pathogenesis of various diseases including intestinal inflammation and systemic inflammatory response syndrome (SIRS). In this work, we investigated the signaling mechanisms controlled by the necroptosis mediator receptor interacting protein-1 (RIP1) kinase. We show that Akt kinase activity is critical for necroptosis in L929 cells and plays a key role in TNFα production. During necroptosis, Akt is activated in a RIP1 dependent fashion through its phosphorylation on Thr308. In L929 cells, this activation requires independent signaling inputs from both growth factors and RIP1. Akt controls necroptosis through downstream targeting of mammalian Target of Rapamycin complex 1 (mTORC1). Akt activity, mediated in part through mTORC1, links RIP1 to JNK activation and autocrine production of TNFα. In other cell types, such as mouse lung fibroblasts and macrophages, Akt exhibited control over necroptosis-associated TNFα production without contributing to cell death. Overall, our results provide new insights into the mechanism of necroptosis and the role of Akt kinase in both cell death and inflammatory regulation. [ABSTRACT FROM AUTHOR]

Published

2013

153. Microdomain heterogeneity in 3D affects the mechanics of neonatal cardiac myocyte contraction.

Author

Curtis, Matthew, Budyn, Elisa, Desai, Tejal, Samarel, Allen, and Russell, Brenda

Subjects

MUSCLE cells, HEART cells, CELL culture, CONFOCAL microscopy, PROTEIN kinase C

Abstract

Cardiac muscle cells are known to adapt to their physical surroundings, optimizing intracellular organization and contractile function for a given culture environment. A previously developed in vitro model system has shown that the inclusion of discrete microscale domains (or microrods) in three dimensions (3D) can alter long-term growth responses of neonatal ventricular myocytes. The aim of this work was to understand how cellular contact with such a domain affects various mechanical changes involved in cardiac muscle cell remodeling. Myocytes were maintained in 3D gels over 5 days in the presence or absence of 100−μm-long microrods, and the effect of this local heterogeneity on cell behavior was analyzed via several imaging techniques. Microrod abutment resulted in approximately twofold increases in the maximum displacement of spontaneously beating myocytes, as based on confocal microscopy scans of the gel xy-plane or the myocyte long axis. In addition, microrods caused significant increases in the proportion of aligned myofibrils (≤20° deviation from long axis) in fixed myocytes. Microrod-related differences in axial contraction could be abrogated by long-term interruption of certain signals of the RhoA-/Rho-associated kinase (ROCK) or protein kinase C (PKC) pathway. Furthermore, microrod-induced increases in myocyte size and protein content were prevented by ROCK inhibition. In all, the data suggest that microdomain heterogeneity in 3D appears to promote the development of axially aligned contractile machinery in muscle cells, an observation that may have relevance to a number of cardiac tissue engineering interventions. [ABSTRACT FROM AUTHOR]

Published

2013

154. Supplementation of carnitine leads to an activation of the IGF-1/PI3K/Akt signalling pathway and down regulates the E3 ligase MuRF1 in skeletal muscle of rats.

Author

Keller, Janine, Couturier, Aline, Haferkamp, Melanie, Most, Erika, and Eder, Klaus

Subjects

IMMUNOBLOTTING, MASS spectrometry methodology, ANIMAL experimentation, CARNITINE, CELLULAR signal transduction, DIETARY supplements, ENZYME-linked immunosorbent assay, GENES, GROWTH factors, POLYMERASE chain reaction, RATS, DATA analysis software, SKELETAL muscle, DESCRIPTIVE statistics

Abstract

Background: Recently, it has been shown that carnitine down-regulates genes involved in the ubiquitin-proteasome system (UPS) in muscle of pigs and rats. The mechanisms underlying this observation are yet unknown. Based on the previous finding that carnitine increases plasma IGF-1 concentration, we investigated the hypothesis that carnitine down-regulates genes of the UPS by modulation of the of the IGF-1/PI3K/Akt signalling pathway which is an important regulator of UPS activity in muscle. Methods: Male Sprague-Dawley rats, aged four weeks, were fed either a control diet with a low native carnitine concentration or the same diet supplemented with carnitine (1250 mg/kg diet) for four weeks. Components of the UPS and IGF-1/PI3K/Akt signalling pathway in skeletal muscle were examined. Results: Rats fed the diet supplemented with carnitine had lower mRNA and protein levels of MuRF1, the most important E3 ubiquitin ligase in muscle, decreased concentrations of ubiquitin-protein conjugates in skeletal muscle and higher IGF-1 concentration in plasma than control rats (P < 0.05). Moreover, in skeletal muscle of rats fed the diet supplemented with carnitine there was an activation of the PI3K/Akt signalling pathway, as indicated by increased protein levels of phosphorylated (activated) Akt1 (P < 0.05). Conclusion: The present study shows that supplementation of carnitine markedly decreases the expression of MuRF1 and concentrations of ubiquitinated proteins in skeletal muscle of rats, indicating a diminished degradation of myofibrillar proteins by the UPS. The study moreover shows that supplementation of carnitine leads to an activation of the IGF-1/PI3K/Akt signalling pathway which in turn might contribute to the observed down-regulation of MuRF1 and muscle protein ubiquitination. [ABSTRACT FROM AUTHOR]

Published

2013

155. The role of focal adhesion kinase catalytic activity on the proliferation and migration of squamous cell carcinoma cells.

Author

Serrels, Alan, McLeod, Kenneth, Canel, Marta, Kinnaird, Andrew, Graham, Kathryn, Frame, Margaret C, and Brunton, Valerie G

Abstract

Focal adhesion kinase (FAK) is upregulated in several epithelial tumours and there has been considerable interest in developing small molecule kinase inhibitors of FAK. However, FAK also has important adaptor functions within the cell, integrating signals from both integrins and growth factors. To investigate the role of FAKs kinase domain, we generated fak-deficient squamous cell carcinoma (SCC) cell lines. Re-expression of a wild type or kinase dead FAK allowed us to delineate its kinase dependent functions. In addition, we used the novel FAK kinase inhibitor PF-562,271. The kinase activity of FAK was important for tumour cell migration and polarity but more striking was its requirement for the anchorage independent 3 dimensional (3D) proliferation of SCC cells and their growth as xenografts in mice. Inhibition of FAK activity and prevention of growth in 3D correlated with Src inhibition. We further identified a mechanism whereby FAK regulates proliferation in 3D via regulation of the kinase activity of Src. This was dependent on the kinase activity of FAK and its resulting phosphorylation on Y397 that provides a high affinity binding site for Src. These data support the further development of FAK kinase inhibitors as agents that have the potential to inhibit both tumour cell migration and proliferation. [ABSTRACT FROM AUTHOR]

Published

2012

156. p70 S6K1 nuclear localization depends on its mTOR-mediated phosphorylation at T389, but not on its kinase activity towards S6.

Author

Rosner, M., Schipany, K., and Hengstschläger, M.

Subjects

PROTEIN kinases, PHOSPHORYLATION, CYTOKINES, GROWTH factors, RAPAMYCIN, TARGETED drug delivery, CYTOPLASM

Abstract

The protein kinase p70 S6K1 is regulated in response to cytokines, nutrients and growth factors, and plays an important role in the development of a variety of human diseases. Mammalian target of rapamycin (mTOR) is known to phosphorylate and thereby activate p70 S6K1. p70 S6K1 phosphorylates different cytoplasmic and nuclear substrates involved in the regulation of protein synthesis, cell cycle, cell growth and survival. Recently, we have shown that mTOR-mediated phosphorylation of p70 S6K1 at T389 also regulates its nucleocytoplasmic localization. Since this phosphorylation is associated with its kinase activity the question whether p70 S6K1 phosphorylation or kinase activity is essential for its proper localization remained elusive. Recently, the chemical compound PF-4708671 has been demonstrated to block p70 S6K1 kinase activity while inducing its phosphorylation at T389. This potential of PF-4708671 to separate p70 S6K1 activity from its T389 phosphorylation allowed us to demonstrate that the proper nucleocytoplasmic localization of this kinase depends on its mTOR-mediated phosphorylation but not on its kinase activity. These findings provide important insights into the regulation of p70 S6K1 and allow a more detailed understanding of subcellular enzyme localization processes. [ABSTRACT FROM AUTHOR]

Published

2012

157. Use of a Mouse Model of Pancreatic Neuroendocrine Tumors to Find Pericyte Biomarkers of Resistance to Anti-angiogenic Therapy.

Author

Franco, M., Pàez-Ribes, M., Cortez, E., Casanovas, O., and Pietras, K.

Subjects

NEUROENDOCRINE tumors, VASCULAR endothelial growth factors, BIOMARKERS, ACTIN, ANIMAL models in research, RETROSPECTIVE studies

Abstract

The successful introduction of rationally targeted agents into standard cancer care is a testimony of the vast knowledge base in tumor biology. However, in order to provide individually tailored therapy to patients and to identify small subsets of patients with a high likelihood to benefit from treatment, the identification of biomarkers for response or resistance to a particular therapeutic regimen is imperative. Herein, by the use of a genetically engineered mouse model of pancreatic neuroendocrine tumors, we have assessed the utility of pericyte characteristics in terms of differential marker expression to serve as surrogate markers for response or evasive resistance to anti-angiogenic therapy. We found that tumors refractory to therapy following long-term treatment with a vascular endothelial growth factor receptor-2 blocking antibody contained blood vessels with a prolific investment of pericytes expressing α-smooth muscle actin. Further analysis by simultaneous immunostaining for different pericyte markers led to the conclusion that the increased abundance of this particular subtype of blood vessels most likely occurred by co-option of vessels from the surrounding exocrine pancreas. Our findings may form the basis for retrospective analysis of pancreatic neuroendocrine tumors from patients having undergone treatment with anti-angiogenic agents in order to validate the occurrence of pericytes expressing α-smooth muscle actin as a biomarker for tumors refractory to therapy. [ABSTRACT FROM AUTHOR]

Published

2011

158. The lymphocyte potassium channels Kv1.3 and KCa3.1 as targets for immunosuppression.

Author

Lam, Jenny and Wulff, Heike

Published

2011

159. Abrogation of Cbl-PI3K interaction increases bone formation and osteoblast proliferation.

Author

Brennan, Tracy, Adapala, Naga, Barbe, Mary, Yingling, Vanessa, Sanjay, Archana, Adapala, Naga Suresh, and Barbe, Mary F

Subjects

OSTEOCLASTS, BONE growth, CELL proliferation, MESENCHYMAL stem cells, BINDING sites, GENE expression, HOMEOSTASIS

Abstract

Cbl is an adaptor protein and E3 ligase that plays both positive and negative roles in several signaling pathways that affect various cellular functions. Tyrosine 737 is unique to Cbl and phosphorylated by Src family kinases. Phosphorylated CblY737 creates a binding site for the p85 regulatory subunit of phosphatidylinositol 3 kinase (PI3K) that also plays an important role in the regulation of bone homeostasis. To investigate the role of Cbl-PI3K interaction in bone homeostasis, we examined knock-in mice in which the PI3K binding site on Cbl was ablated due to the substitution of tyrosine 737 to phenylalanine (Cbl(YF/YF), YF mice). We previously reported that bone volume in these mice is increased due to decreased osteoclast function (Adapala et al., J Biol Chem 285:36745-36758, 19). Here, we report that YF mice also have increased bone formation and osteoblast numbers. In ex vivo cultures bone marrow-derived YF osteoblasts showed increased Col1A expression and their proliferation was also significantly augmented. Moreover, proliferation of MC3T3-E1 cells was increased after treatment with conditioned medium generated by culturing YF bone marrow stromal cells. Expression of stromal derived factor-1 (SDF-1) was increased in YF bone marrow stromal cells compared to wild type. Increased immunostaining of SDF-1 and CXCR4 was observed in YF bone marrow stromal cells compared to wild type. Treatment of YF condition medium with neutralizing anti-SDF-1 and anti-CXCR4 antibodies attenuated MC3T3-E1 cell proliferation. Cumulatively, these results show that abrogation of Cbl-PI3K interaction perturbs bone homeostasis, affecting both osteoclast function and osteoblast proliferation. [ABSTRACT FROM AUTHOR]

Published

2011

160. β1 integrin mediates an alternative survival pathway in breast cancer cells resistant to lapatinib.

Subjects

EPIDERMAL growth factor, BREAST cancer, TRASTUZUMAB, APOPTOSIS, CELL proliferation

Abstract

The article focuses on the research of human epidermal growth factor receptor (HER)-2 in human breast cancer. It mentions that (HER)-2 is related to the usage of HER2-targeted therapies including trastuzumab (T) and lapatinib (L). It mentions that apoptosis (TUNEL assay) and proliferation were assayed in eight-well chamberslide.

Published

2011

161. Osteoblasts in osteoporosis: past, emerging, and future anabolic targets.

Author

Pierre J Marie

Subjects

OSTEOPOROSIS, AGE factors in disease, BONE diseases, BONE resorption, PARATHYROID hormone, CELL physiology

Abstract

OBJECTIVE: Age-related bone loss is associated with significant changes in bone remodeling characterized by decreased trabecular and periosteal bone formation relative to bone resorption, resulting in bone fragility and increased risk of fractures. Prevention or reversal of age-related decrease in bone mass and increase in bone fragility has been based on inhibition of bone resorption using anticatabolic drugs. The current challenge is to promote osteoblastogenesis and bone formation to prevent age-related bone deterioration. METHODS: A limited number of approved therapeutic molecules are available to activate bone formation. Therefore, there is a need for anabolic drugs that promote bone matrix apposition at the endosteal, endocortical, and periosteal envelopes by increasing the number of osteoblast precursor cells and/or the function of mature osteoblasts. In this study, we review current therapeutics promoting bone formation and anabolic molecules targeting signaling pathways involved in osteoblastogenesis, based on selected full-text articles searched on Medline search from 1990 to 2010. RESULTS AND DISCUSSION: We present current therapeutic approaches focused on intermittent parathyroid hormone and Wnt signaling agonists/antagonists. We also discuss novel approaches for prevention and treatment of defective bone formation and bone loss associated with aging and osteoporosis. These strategies targeting osteoblastic cell functions may prove to be useful in promoting bone formation and improving bone strength in the aging population. [ABSTRACT FROM AUTHOR]

Published

2011

162. Mitotic lymphoma cells are characterized by high expression of phosphorylated ribosomal S6 protein.

Author

Egervári, Gábor, Márk, Ágnes, Hajdu, Melinda, Barna, Gábor, Sápi, Zoltán, Krenács, Tibor, Kopper, László, and Sebestyén, Anna

Subjects

LYMPHOMAS, GROWTH factors, MITOGENS, PHOSPHORYLATION, PROTEIN synthesis, CELL proliferation, HOMEOSTASIS, CELL cycle

Abstract

Growth factors and mitogens influence signaling pathways and often induce the activity of p70S6 kinase (p70S6K), which in turn phosphorylates the ribosomal S6 protein (S6). Although recent data are rather conflicting, the overall view suggests that phosphorylated S6 is a regulator of global protein synthesis, cell proliferation, cell size and glucose homeostasis. In the present work, emphasis was given to cell cycle-dependent activation of S6 focusing mainly on human lymphoid and lymphoma cells. Paraffin-embedded human tissue blocks from lymph node and different tumor biopsies as well as in vitro cell lines were investigated by immunohistochemistry, immunocytochemistry, flow cytometry and Western blotting using antibodies directed against phospho-S6, phospho-mTOR, phospho-p70S6K and phospho-Histone H3. To enrich the cell number in different phases of the cell cycle, nocodazole, staurosporine or rapamycin were used in cell cultures. We observed strong phospho-S6 positivity by immunostainings in the dividing lymphoid cells of reactive lymph nodes and in lymphoma cells cultured in vitro. Phospho-S6 protein levels were shown to be elevated throughout mitosis in lymphoma cells; however, the high expression of phospho-S6 in mitotic cells was not a general hallmark of tumor cell types studied so far: phospho-S6-negative mitotic cells were detected in several carcinoma and sarcoma biopsies. These observations may have practical implications as they raise the possibility to consider p70S6K and/or S6 as a potential therapeutic target-besides mTOR-in certain lymphomas and perhaps in clinical immunosuppression. [ABSTRACT FROM AUTHOR]

Published

2011

163. Inhibition of focal adhesion kinase suppresses the adverse phenotype of endocrine-resistant breast cancer cells and improves endocrine response in endocrine-sensitive cells.

Author

Hiscox, Stephen, Barnfather, Peter, Hayes, Edd, Bramble, Pamela, Christensen, James, Nicholson, Robert, and Barrett-Lee, Peter

Abstract

quired resistance to endocrine therapy in breast cancer is a major clinical problem. Previous reports have demonstrated that cell models of acquired endocrine resistance have altered cell-matrix adhesion and a highly migratory phenotype, features which may impact on tumour spread in vivo. Focal adhesion kinase (FAK) is an intracellular kinase that regulates signalling pathways central to cell adhesion, migration and survival and its expression is frequently deregulated in breast cancer. In this study, we have used the novel FAK inhibitor PF573228 to address the role of FAK in the development of endocrine resistance. Whilst total-FAK expression was similar between endocrine-sensitive and endocrine-resistant MCF7 cells, FAK phosphorylation status (Y397 or Y861) was altered in resistance. PF573228 promoted a dose-dependent inhibition of FAK phosphorylation at Y397 but did not affect other FAK activation sites (pY407, pY576 and pY861). Endocrine-resistant cells were more sensitive to these inhibitory effects versus MCF7 (mean IC for FAK pY397 inhibition: 0.43 μM, 0.05 μM and 0.13 μM for MCF7, TamR and FasR cells, respectively). Inhibition of FAK pY397 was associated with a reduction in TamR and FasR adhesion to, and migration over, matrix components. PF573228 as a single agent (0-1 μM) did not affect the growth of MCF7 cells or their endocrine-resistant counterparts. However, treatment of endocrine-sensitive cells with PF573228 and tamoxifen combined resulted in greater suppression of proliferation versus single agent treatment. Together these data suggest the importance of FAK in the process of endocrine resistance, particularly in the development of an aggressive, migratory cell phenotype and demonstrate the potential to improve endocrine response through combination treatment. [ABSTRACT FROM AUTHOR]

Published

2011

164. Corticotropin Releasing Factor-Induced CREB Activation in Striatal Neurons Occurs via a Novel Gbc Signaling Pathway.

Author

Stern, Christopher M., Luoma, Jessie I., Meitzen, John, and Mermelstein, Paul G.

Subjects

CORTICOTROPIN releasing hormone, NEURONS, CHEMICAL reactions, SIGNALS & signaling, ADENYLATE cyclase, PHOSPHORYLATION

Abstract

The peptide corticotropin-releasing factor (CRF) was initially identified as a critical component of the stress response. CRF exerts its cellular effects by binding to one of two cognate G-protein coupled receptors (GPCRs), CRF receptor 1 (CRFR1) or 2 (CRFR2). While these GPCRs were originally characterized as being coupled to Gas, leading to downstream activation of adenylyl cyclase (AC) and subsequent increases in cAMP, it has since become clear that CRFRs couple to and activate numerous other downstream signaling cascades. In addition, CRF signaling influences the activity of many diverse brain regions, affecting a variety of behaviors. One of these regions is the striatum, including the nucleus accumbens (NAc). CRF exerts profound effects on striatal-dependent behaviors such as drug addiction, pair-bonding, and natural reward. Recent data indicate that at least some of these behaviors regulated by CRF are mediated through CRF activation of the transcription factor CREB. Thus, we aimed to elucidate the signaling pathway by which CRF activates CREB in striatal neurons. Here we describe a novel neuronal signaling pathway whereby CRF leads to a rapid Gβγ- and MEK-dependent increase in CREB phosphorylation. These data are the first descriptions of CRF leading to activation of a Gβγ-dependent signaling pathway in neurons, as well as the first description of Gbc activation leading to downstream CREB phosphorylation in any cellular system. Additionally, these data provide additional insight into the mechanisms by which CRF can regulate neuronal function. [ABSTRACT FROM AUTHOR]

Published

2011

165. Phase Ib study of CP-868,596, a PDGFR inhibitor, combined with docetaxel with or without axitinib, a VEGFR inhibitor.

Author

Michael, M., Vlahovic, G., Khamly, K., Pierce, K. J., Guo, F., and Olszanski, A. J.

Subjects

HYPERTENSION, ENDOTHELIAL growth factors, DRUG therapy, DOCETAXEL, CONSTIPATION

Abstract

Background: Tumoural interstitial hypertension, possibly modulated by platelet-derived and vascular endothelial growth factor receptors (PDGFR and VEGFR), may mediate resistance to chemotherapy.Methods: Forty-eight patients with advanced solid tumours received oral PDGFR inhibitor CP-868,596 (60-100 mg twice daily (BID)) and docetaxel (75-100 mg m⁻²), or CP-868,596 (60 mg BID), docetaxel (75 mg m⁻²), and VEGFR inhibitor axitinib (5 mg BID).Results: The CP-868,596/docetaxel was escalated as above. The CP-868,596/docetaxel/axitinib was not dose escalated because of increased incidence of mucositis-like adverse events (AEs) with concurrent neutropenia relative to that expected for docetaxel. All tested regimens were tolerable, including 100 mg BID CP-868,596 (recommended phase II dose) plus 100 mg m⁻² docetaxel (maximum approved dose). Most treatment-emergent AEs were mild-moderate and reversible, commonly including nausea, diarrhoea, vomiting, constipation, fatigue, and anaemia (CP-868,596/docetaxel), and hypertension, lethargy, diarrhoea, and fatigue (CP-868,596/docetaxel/axitnib). Pharmacokinetics were unaffected by co-administration. Twenty-one patients achieved stable disease, including all seven evaluable on CP-868,596/docetaxel/axitinib. All nine CP-868,596/docetaxel/axitinib patients received therapy for a median of six (range, 3-16) cycles.Conclusions: The CP-868,596/docetaxel was well tolerated, but increased efficacy was not observed. Addition of axitinib delivered greater benefits than expected in the number of patients achieving prolonged stable disease with a moderate increase in AEs. [ABSTRACT FROM AUTHOR]

Published

2010

166. Extracellular Matrix Produced by Osteoblasts Cultured Under Low-Magnitude, High-Frequency Stimulation is Favourable to Osteogenic Differentiation of Mesenchymal Stem Cells.

Author

Dumas, Virginie, Ducharne, Benjamin, Perrier, Anthony, Fournier, Carole, Guignandon, Alain, Thomas, Mireille, Peyroche, Sylvie, Guyomar, Daniel, Vico, Laurence, and Rattner, Aline

Subjects

EXTRACELLULAR matrix, STEM cells, PHOSPHOPROTEINS, CYTOSKELETON, FIBRONECTINS

Abstract

The effects of low-magnitude, high-frequency (LMHF) mechanical stimulation on osteoblastic cells are poorly understood. We have developed a system that generates very small (15-40 με), high-frequency (400 Hz, sine) deformations on osteoblast cultures (MC3T3-E1). We investigated the effects of these LMHF stimulations mainly on extracellular matrix (ECM) synthesis. The functional properties of this ECM after decellularization were evaluated on C3H10T1/2 mesenchymal stem cells (MSCs). LMHF stimulations were applied 20 min once daily for 1, 3, or 7 days in MC3T3-E1 culture (1, 3, or 7 dLMHF). Cell number and viability were not affected after 3 or 7 dLMHF. Osteoblast response to LMHF was assessed by an increase in nitric oxide secretion, alteration of the cytoskeleton, and focal contacts. mRNA expression for fibronectin, osteopontin, bone sialoprotein, and type I collagen in LMHF cultures were 1.8-, 1.6-, 1.5-, and 1.7-fold higher than controls, respectively ( P < 0.05). In terms of protein, osteopontin levels were increased after 3 dLMHF and ECM organization was altered as shown by fibronectin topology after 7 dLMHF. After decellularization, 7 dLMHF-ECM or control ECM was reseeded with MSCs. Seven dLMHF-ECM improved early events such as cell attachment (2 h) and focal contact adhesion (6 h) and, later (16 h), modified MSC morphological parameters. After 5 days in multipotential medium, gene-expression changes indicated that 7 dLMHF-ECM promoted the expression of osteoblast markers at the expense of adipogenic marker. LMHF stimulations of osteoblasts are therefore efficient and sufficient to generate osteogenic matrix. [ABSTRACT FROM AUTHOR]

Published

2010

167. Calcium-activated and voltage-gated potassium channels of the pancreatic islet impart distinct and complementary roles during secretagogue induced electrical responses.

Author

Jacobson, David A., Mendez, Felipe, Thompson, Michael, Torres, Jacqueline, Cochet, Olivia, and Philipson, Louis H.

Abstract

Glucose-induced β-cell action potential (AP) repolarization is regulated by potassium efflux through voltage gated (Kv) and calcium activated (KCa) potassium channels. Thus, ablation of the primary Kv channel of the β-cell, Kv2.1, causes increased AP duration. However, Kv2.1−/− islet electrical activity still remains sensitive to the potassium channel inhibitor tetraethylammonium. Therefore, we utilized Kv2.1−/− islets to characterize Kv and KCa channels and their respective roles in modulating the β-cell AP. The remaining Kv current present in Kv2.1−/−β-cells is inhibited with 5 μm CP 339818. Inhibition of the remaining Kv current in Kv2.1−/− mouse β-cells increased AP firing frequency by 39.6% but did not significantly enhance glucose stimulated insulin secretion (GSIS). The modest regulation of islet AP frequency by CP 339818 implicates other K+ channels, possibly KCa channels, in regulating AP repolarization. Blockade of the KCa channel BK with slotoxin increased β-cell AP amplitude by 28.2%, whereas activation of BK channels with isopimaric acid decreased β-cell AP amplitude by 30.6%. Interestingly, the KCa channel SK significantly contributes to Kv2.1−/− mouse islet AP repolarization. Inhibition of SK channels decreased AP firing frequency by 66% and increased AP duration by 67% only when Kv2.1 is ablated or inhibited and enhanced GSIS by 2.7-fold. Human islets also express SK3 channels and their β-cell AP frequency is significantly accelerated by 4.8-fold with apamin. These results uncover important repolarizing roles for both Kv and KCa channels and identify distinct roles for SK channel activity in regulating calcium- versus sodium-dependent AP firing. [ABSTRACT FROM AUTHOR]

Published

2010

168. MLN3 897 Plus Methotrexate in Patients With Rheumatoid Arthritis.

Author

Vergunst, Clarissa E., Gerlag, Danielle M., von Moltke, Lisa, Karol, Michael, Tim Wyant, Xuedong Chi, Matzkin, Ellen, Leach, Timothy, and Tak, Paul P.

Subjects

RHEUMATOID arthritis, INFLAMMATORY mediators, IMMUNOLOGY of inflammation, CHEMOKINES, METHOTREXATE, LEUCOCYTE motility

Abstract

The article presents a study on the efficacy of MLN3897, a CC chemokine receptor (CCR1) antagonist, in rheumatoid arthritis (RA) patients receiving methotrexate (MTX). It is stated in the study that chemokines are involved in the migration of leukocytes, causing inflammation. It notes that patients who met the American College of Rheumatology (ACR) criteria participated in the study. It also mentions that MLN3897 had no evident activity and CCR1 antagonism is not a good strategy for treatment.

Published

2009

169. Chemokines as Possible Targets in Modulation of the Secondary Damage After Acute Spinal Cord Injury: A Review.

Author

Petra Kravčuková and Darina Kluchová

Subjects

CHEMOKINES, SPINAL cord injuries, THERAPEUTICS, TARGETED drug delivery, CELL death, MEDICAL statistics, THERAPEUTIC use of glucocorticoids, AXONS, NEURON development

Abstract

Abstract  In spite of many promising experimental studies, an effective treatment dramatically eliminating the secondary damage after spinal cord injury (SCI) is still missing. Since clinical data on the therapeutical effect after methylprednisolone treatment are not conclusive, new therapeutical modalities targeting specific components of secondary spinal cord damage needs to be developed. It is known that immune cells are recruited to injury sites by chemokines, which are small, structurally similar proteins released locally at the site of inflammation. Hence, this review was aimed to summarize possible roles of chemokines in the inflammation following SCI as well as to identify possible new therapeutical targets which can potentially be effective in ameliorating individual components of this inflammatory response. Data concerning inflammation reduction together with techniques improving axonal growth, cell replacement and remyelinization, may be crucial to move a small step forward in an attempt to make paraplegic and quadriplegic patients to walk. [ABSTRACT FROM AUTHOR]

Published

2009

170. Assignment of the absolute configuration of zwitterionic and neutral macropodumines by means of TDDFT CD calculations.

Author

Guo, Yue-Wei, Kurtán, Tibor, Krohn, Karsten, Pescitelli, Gennaro, and Zhang, Wen

Published

2009

171. Clofazimine Inhibits Human Kv1.3 Potassium Channel by Perturbing Calcium Oscillation in T Lymphocytes.

Author

Yunzhao R. Ren, Fan Pan, Parvez, Suhel, Fleig, Andrea, Chong, Curtis R., Jing Xu, Yongjun Dang, Jin Zhang, Hongsi Jiang, Penner, Reinhold, and Liu, Jun O.

Subjects

POTASSIUM channels, T cells, AUTOIMMUNE diseases, MOLECULES, MULTIPLE sclerosis, PSORIASIS, PERTURBATION theory, INTERLEUKIN-2, MYCOBACTERIAL disease treatment

Abstract

The Kv1.3 potassium channel plays an essential role in effector memory T cells and has been implicated in several important autoimmune diseases including multiple sclerosis, psoriasis and type 1 diabetes. A number of potent small molecule inhibitors of Kv1.3 channel have been reported, some of which were found to be effective in various animal models of autoimmune diseases. We report herein the identification of clofazimine, a known anti-mycobacterial drug, as a novel inhibitor of human Kv1.3. Clofazimine was initially identified as an inhibitor of intracellular T cell receptor-mediated signaling leading to the transcriptional activation of human interleukin-2 gene in T cells from a screen of the Johns Hopkins Drug Library. A systematic mechanistic deconvolution revealed that clofazimine selectively blocked the Kv1.3 channel activity, perturbing the oscillation frequency of the calcium-release activated calcium channel, which in turn led to the inhibition of the calcineurin-NFAT signaling pathway. These effects of clofazimine provide the first line of experimental evidence in support of a causal relationship between Kv1.3 and calcium oscillation in human T cells. Furthermore, clofazimine was found to be effective in blocking human T cell-mediated skin graft rejection in an animal model in vivo. Together, these results suggest that clofazimine is a promising immunomodulatory drug candidate for treating a variety of autoimmune disorders. [ABSTRACT FROM AUTHOR]

Published

2008

172. The differential expression of low-threshold K+ currents generates distinct firing patterns in different subtypes of adult mouse trigeminal ganglion neurones.

Author

Catacuzzeno, Luigi, Fioretti, Bernard, Pietrobon, Daniela, and Franciolini, Fabio

Abstract

In adult mouse trigeminal ganglion (TG) neurones we identified three neuronal subpopulations, defined in terms of their firing response to protracted depolarizations, namely MF neurones, characterized by a multiple tonic firing; DMF neurones, characterized by a delay before the beginning of repetitive firing; and SS neurones, characterized by a strongly adapting response. The three subpopulations also differed in several other properties important for defining their functional role in vivo, namely soma size, action potential (AP) shape and capsaicin sensitivity. MF neurones had small soma, markedly long AP and mostly responded to capsaicin, properties typical of a subgroup of C-type nociceptors. SS neurones had large soma, short AP duration and were mostly capsaicin insensitive, suggesting that most of them have functions other than nociception. DMF neurones were all capsaicin insensitive, had a small soma size and intermediate AP duration, making them functionally distinct from both MF and SS neurones. We investigated the ionic basis underlying the delay to the generation of the first AP of DMF neurones, and the strong adaptation of SS neurones. We found that the expression of a fast-inactivating, 4-AP- and CP-339,818-sensitive K+ current ( IA) in DMF neurones plays a critical role in the generation of the delay, whereas a DTX-sensitive K+ current ( IDTX) selectively expressed in SS neurones appeared to be determinant for their strong firing adaptation. A minimal theoretical model of TG neuronal excitability confirmed that IA and IDTX have properties congruent with their suggested role. [ABSTRACT FROM AUTHOR]

Published

2008

173. Inhibition of epidermal growth factor receptor signaling pathway by delphinidin, an anthocyanidin in pigmented fruits and vegetables.

Author

Afaq, Farrukh, Zaman, Najia, Khan, Naghma, Syed, Deeba N., Sarfaraz, Sami, Zaid, Mohammad Abu, and Mukhtar, Hasan

Published

2008

174. Regeneration of human epidermis on acellular dermis is impeded by small-molecule inhibitors of EGF receptor tyrosine kinase.

Author

Forsberg, Sofi, Östman, Arne, and Rollman, Ola

Subjects

PROTEIN-tyrosine kinases, EPIDERMIS, KERATINOCYTES, SKIN diseases, IMMUNOHISTOCHEMISTRY

Abstract

The family of human epidermal growth factor receptors (EGFR, HER2–4) exerts key functions in normal and malignant epithelial cells. Both EGFR and HER2 are valuable targets for anti-cancer drugs by interfering with ligand binding, receptor dimerization, or tyrosine kinase activity. A similar therapeutic strategy has been advocated for chronic psoriasis since plaque lesions overexpress EGFR and its ligands. Our aim was to characterize EGFR/HER2 protein expression in skin cultures and to evaluate the effects of tyrosine kinase inhibitors on epidermal outgrowth, morphology, and EGFR activation. Human skin explants were established on cell-free dermis and cultured at the air–liquid interface. The impact of small-molecule HER inhibitors on outgrowth was assayed by fluorescence-based image analysis and histometry. Effects of a dual EGFR/HER2 kinase inhibitor, PKI166, on neoepidermis were studied by immunohistochemistry and Western blot. Receptor immunostaining showed in vivo-like distributions with highest EGFR intensity in the proliferative layers whereas HER2 was mainly expressed by suprabasal keratinocytes. Reepithelialization was associated with EGFR autophosphorylation irrespective of exogenous ligand stimulation. PKI166 inhibited neoepidermal EGFR activation, keratinocyte proliferation, and outgrowth from normal and psoriatic skin explants. The rate of epidermalization in presence of other HER inhibitors varied suggesting that drug specificity, potency, and reversibility determine the dynamic outcome. Overall, agents predominantly targeting EGFR kinase were more efficient inhibitors of epidermal regeneration than an HER2-selective drug. The study illustrates the usefulness of a dynamic skin model and emphasizes the potential of HER-directed approaches to control epidermal growth in hyperproliferative skin disorders. [ABSTRACT FROM AUTHOR]

Published

2008

175. Effects of changes in extracellular pH and potassium concentration on Kv1.3 inactivation.

Author

Somodi, S´ndor, Hajdu, Péter, Gáspár, Rezső, Panyi, György, and Varga, Zoltán

Subjects

POTASSIUM channels, BARIUM, BINDING sites, ION channels, ACTIVE biological transport

Abstract

The Kv1.3 channel inactivates via the P/C-type mechanism, which is influenced by a histidine residue in the pore region (H399, equivalent of Shaker 449). Previously we showed that the electric field of the protonated histidines at low extracellular pH (pHe) creates a potential barrier for K+ ions just outside the pore that hinders their exit from the binding site controlling inactivation (control site) thereby slowing inactivation kinetics. Here we examined the effects of extracellular potassium [K+]e and pHe on the rate of inactivation of Kv1.3 using whole-cell patch-clamp. We found that in 150 mM [K+]e inactivation was accelerated upon switching to pHe 5.5 as opposed to the slowing at 5 mM [K+]e. The transition from slowing to acceleration occurred at 40 mM [K+]e, whereas this “turning point” was at 20 mM [K+]e for inward currents. The rate of entry of Ba2+ ions from the extracellular space to the control site was significantly slowed by low pHe in wild-type hKv1.3, but it was insensitive to pHe in H399K and H399L mutants. Based on these observations we expanded our model and propose that the potential barrier created by the protonated histidines impedes the passage of K+ ions between the extracellular medium and the control site in both directions and the effect on inactivation rate (acceleration or slowing) depends on the relative contribution of filling from the extracellular and intracellular sides. [ABSTRACT FROM AUTHOR]

Published

2008

176. ErbB2 Induces Notch1 Activity and Function in Breast Cancer Cells.

Author

Lindsay, Jaime, Xuanmao Jiao, Sakamaki, Toshiyuki, Casimiro, Mathew C., Shirley, Lawrence A., Tran, Thai H., Xiaoming Ju, Liu, Manran, Zhiping Li, Chenguang Wang, Katiyar, Sanjay, Rao, Mahadev, Allen, Kathleen G., Glazer, Robert I., Changhui Ge, Stanley, Pamela, Lisanti, Michael P., Rui, Hallgeir, and Pestell, Richard G.

Subjects

BREAST cancer, ONCOGENIC viruses, CANCER genes, ONCOGENES, CARCINOGENS, ONCOGENIC DNA viruses, BRCA genes, CANCER cell growth, TUMOR growth

Abstract

The ErbB2 (Her2/neu epidermal growth receptor family) oncogene is overexpressed in 30% to 40% of human breast cancers. Cyclin D1 is the regulatory subunit of the holoenzyme that phosphorylates and inactivates the retinoblastoma (pRb) tumor suppressor and is an essential downstream target of ErbB2-induced tumor growth. Herein, we demonstrate that ErbB2 induces the activity of the Notch signaling pathway. ErbB2 induction of DNA synthesis, contact-independent growth, and mammosphere induction required Notch1. ErbB2-induced cyclin D1 and cyclin D1 expression was suficient to induce Notch1 activity, and conversely, genetic deletion of Notch1 in mammary epithelial cells using foxed Notch ( Notchfl/fl) mice demonstrated that cyclin D1 is induced by Notch1. Genetic deletion of cyclin D1 or small interfering RNA (siRNA) to cyclin D1-reduced Notch1 activity and reintroduction of cyclin D1 into cyclin D1-deficient cells restored Notch1 activity through the inhibition of Numb, an endogenous inhibitor of Notch1 activity. Thus, cyclin D1 functions downstream as a genetic target of Notch1, amplifies Notch1 activity by repressing Numb, and identifies a novel pathway by which ErbB2 induces Notch1 activity via the induction of cyclin D1. [ABSTRACT FROM AUTHOR]

Published

2008

177. FERM control of FAK function.

Author

Ssang-Taek Lim, Mikolon, David, Stupack, Dwayne G., and Schlaepfe, David D.

Published

2008

178. Cell–matrix adhesion.

Author

Berrier, Allison L. and Yamada, Kenneth M.

Subjects

MEMBRANE fusion, CELL membranes, CELL adhesion, CONNECTIVE tissues, EXTRACELLULAR matrix, PHYSIOLOGICAL control systems

Abstract

The complex interactions of cells with extracellular matrix (ECM) play crucial roles in mediating and regulating many processes, including cell adhesion, migration, and signaling during morphogenesis, tissue homeostasis, wound healing, and tumorigenesis. Many of these interactions involve transmembrane integrin receptors. Integrins cluster in specific cell–matrix adhesions to provide dynamic links between extracellular and intracellular environments by bi-directional signaling and by organizing the ECM and intracellular cytoskeletal and signaling molecules. This mini review discusses these interconnections, including the roles of matrix properties such as composition, three-dimensionality, and porosity, the bi-directional functions of cellular contractility and matrix rigidity, and cell signaling. The review concludes by speculating on the application of this knowledge of cell–matrix interactions in the formation of cell adhesions, assembly of matrix, migration, and tumorigenesis to potential future therapeutic approaches. J. Cell. Physiol. 213:565–573. © 2007 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2007

179. Targeting EGFR and HER-2 receptor tyrosine kinases for cancer drug discovery and development.

Author

Kamath, Shantaram and Buolamwini, John K.

Abstract

Conventional anticancer therapy using cytotoxic drugs lacks selectivity and is prone to toxicity and drug resistance. Anticancer therapies targeting aberrant growth factor receptor signaling are gaining interest. The erbB receptor family belongs to the type I, the receptor tyrosine kinases class, and comprises EGFR, HER-2, HER-3, and HER-4. It has been targeted for solid tumor therapy, including breast, ovarian, colon, head-and-neck, and non-small-cell lung cancers. This review summarizes structural aspects of this class of growth factor receptors, their oncogenic expression, and various pharmacological interventions including biological products and small molecules that inhibit these enzymes. We have also discussed various mutations that occur in EGFR and their consequences on anticancer therapy. © 2006 Wiley Periodicals, Inc. Med Res Rev, 26, No. 5, 569-594, 2006 [ABSTRACT FROM AUTHOR]

Published

2006

180. Drug Discovery in the Kinase Inhibitory Field Using theNested Chemical Library™ Technology.

Author

György Kéri, Zsolt Székelyhidi, Péter Bánhegyi, Zoltán Varga, Bálint Hegymegi-Barakonyi, Csaba Szántai-Kis, Doris Hafenbradl, Bert Klebl, Gerhard Muller, Axel Ullrich, Dániel Erös, Zoltán Horváth, Zoltán Greff, Jenö Marosfalvi, János Pató, István Szabadkai, Ildikó Szilágyi, Zsolt Szegedi, István Varga, and Frigyes Wáczek

Published

2005

181. Angiogenesis in Gliomas: Imaging and Experimental Therapeutics.

Author

Gagner, Jean-Pierre, Law, Meng, Fischer, Ingeborg, Newcomb, Elizabeth W., and Zagzag, David

Published

2005

182. Anti-erbB-2 antibody trastuzumab in the treatment of HER2-amplified breast cancer.

Author

Christina H. Yeon and Mark D. Pegram

Abstract

Abstract Human epidermal growth factor receptor-2 (HER2/erbB-2) is a member of a family of four transmembrane receptor tyrosine kinases that regulate cell growth, survival and differentiation via multiple signal transduction pathways. Amplification of the HER2 gene occurs in 20–25% of human breast cancers. This amplification event is an independent adverse prognostic factor as well as a predictive factor for increased response to doxorubicin-based combination chemotherapy, response to trastuzumab and decreased response to hormonal therapy. Methods for detecting protein overexpression or gene amplification in clinical tumor specimens include immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH) techniques, with the latter considered by some to be more accurate. Trastuzumab (Herceptin) is a recombinant humanized monoclonal antibody which targets an epitope in the extracellular domain of the HER2 protein. Preclinical models demonstrated that this antibody has significant anti-tumor activity as a single agent and has synergy with certain chemotherapeutic drugs. Phase II and III clinical trials performed in women with metastatic breast cancer that overexpress HER2 have shown that trastuzumab has clinical activity when used as first-, second- or third-line monotherapy, and improves survival when used as first-line therapy in combination with chemotherapy. Newer combinations with numerous chemotherapeutic drugs have also shown significant clinical activity in phase II studies. In all of these trials, trastuzumab was generally well-tolerated, but cardiac toxicity (particularly when the antibody was combined with anthracyclines) was an unexpected adverse effect. Although trastuzumab is currently usually administered on a weekly intravenous schedule, evidence suggests that a triple dose of the drug given once every three weeks has a pharmacokinetic profile expected to be equally efficacious. Neither the optimal schedule nor the optimal duration of trastuzumab therapy has yet been clearly defined in controlled clinical trials. Current clinical investigations of trastuzumab include its use in both the adjuvant and neoadjuvant settings as well as in combination with other chemotherapy drugs or new biologic targeted agents. [ABSTRACT FROM AUTHOR]

Published

2005

183. PH-dependent modulation of Kv1.3 inactivation: role of His399.

Author

Somodi, Sándor, Varga, Zoltán, Hajdu, Péter, Starkus, John G., Levy, Daniel I., Gáspár, Rezsö, and Panyi, György

Subjects

POTASSIUM channels, TYROSINE, AMINO acids, ION channels, SOLUTION (Chemistry), INTERMEDIATES (Chemistry)

Abstract

The Kv1.3 K+ channel lacks N-type inactivation, but during prolonged depolarized periods it inactivates via the slow (P/C type) mechanism. It bears a titratable histidine residue in position 399 (equivalent of Shaker 449), a site known to influence the rate of slow inactivation. As opposed to several other voltage-gated K+ channels, slow inactivation of Kv1.3 is slowed when extracellular pH (pHo) is lowered under physiological conditions. Our findings are as follows. First, when His399 was mutated to a lysine, arginine, leucine, valine or tyrosine, extracellular acidification (pH 5.5) accelerated inactivation reminiscent of other Kv channels. Second, inactivation of the wild-type channel was accelerated by low pHo when the ionic strength of the external solution was raised. Inactivation of the H399K mutant was also accelerated by high ionic strength at pH 7.35 but not the inactivation of H399L. Third, after the external application of blocking barium ions, recovery of the wildtype current during washout was slower in low pHo. Fourth, the dissociation rate of Ba2+ was pH insensitive for both H399K and H399L. Furthermore, Ba2+ dissociation rates were equal for H399K and the wild type at pH 5.5 and were equal for H399L and the wild type at pH 7.35. These observations support a model in which the electric field of the protonated histidines creates a potential barrier for potassium ions just outside the external mouth of the pore that hinders their exit from the binding site controlling inactivation. In Kv1.3, this effect overrides the generally observed speeding of slow inactivation when pHo is reduced. [ABSTRACT FROM AUTHOR]

Published

2004

184. Chemokines in joint disease: the key to inflammation?

Author

Haringman, J. J., Ludikhuize, J., and Tak, P. P.

Published

2004

185. Flux Assays in High Throughput Screening of Ion Channels in Drug Discovery.

Author

Sikander Gill, Raj Gill, Soo Sen Lee, J. Christian Hesketh, David Fedida, Saman Rezazadeh, Larisa Stankovich, and Dong Liang

Published

2003

186. Kinetics and mechanism of formation and decomposition of substituted 1-phenylpyrrolidin-2-ones in basic medium.

Author

Sedlák, Milos̆, Hejtmánková, Ludmila, Kas̆parová, Pavla, and Kaválek, Jaromír

Published

2002

187. Altered outward-rectifying K+ current reveals microglial activation induced by HIV-1 Tat protein.

Author

Visentin, Sergio, Renzi, Massimiliano, and Levi, Giulio

Published

2001

188. Influence of permeating ions on Kv1.5 channel block by nifedipine.

Author

Lin, S. and Wang, Z.

Subjects

IONS, NIFEDIPINE, POTASSIUM channels

Abstract

Provides information on a study which demonstrated that the nature of the permeant ion does affect the dose dependence and kinetics of nifedipine block of Kv1.5, a cardiac potassium channel. Materials and methods used in the study; Results and discussion.

Published

2001

189. Chemokine Receptor Antagonists.

Author

Horuk, Richard and Ng, Howard P.

Published

2000

190. Allosteric effects of mutations in the extracellular S5-P loop on the gating and ion permeation properties of the hERG potassium channel.

Author

Dun, W., Jiang, M., and Tseng, G.-N.

Subjects

AMINO acids, GENETICS, PHENOTYPES, ACIDS, PEPTIDES, POTASSIUM

Abstract

The hERG channel has an unusually long (39 amino acids) extracellular loop between the transmembrane S5 segment and the pore region that may play a role in channel function. We explored this possibility by mutating two histidine residues in this region (H578 and H587, referred to as H1 and H2) to various residues and examined the resulting changes in channel function. Both positions could tolerate drastic changes in side-chain properties (proline, cysteine, glutamate and lysine), indicating that they are solvent exposed. None of the H1 mutations affected hERG channel function. On the other hand, although replacing H2 with glutamate had little or no effect on hERG properties, putting a proline or lysine at this position disrupted the C-type inactivation process and the pore's K selectivity. There was also a hyperpolarizing shift in the voltage dependence of activation. The phenotype of the H2C mutant was similar to that of H2P or H2K. However, dithiothreitol (DTT, a thiol-reducing agent) treatment converted the H2C phenotype to that of the wild-type channel. These observations suggest that the peptide backbone conformation around position 587 in the extracellular S5-P loop of hERG channel can affect the channel's gating and ion selectivity functions. [ABSTRACT FROM AUTHOR]

Published

2000

191. Daphniphyllum Alkaloids: Recent Findings on Chemistry and Pharmacology.

Author

Haifeng Wu, Xiaopo Zhang, Lisheng Ding, Shilin Chen, Junshan Yang, and Xudong Xu

Subjects

ALKALOIDS, ALTERNATIVE medicine, ANTINEOPLASTIC agents, ANTIOXIDANTS, VASODILATION, PHYSICAL & theoretical chemistry, MEDICINAL plants, PHARMACEUTICAL chemistry, PLANT extracts, PLATELET aggregation inhibitors

Abstract

The unique polycyclic fused ring systems of Daphniphyllum alkaloids, along with their extensive bioactivities, make this family of alkaloids especially attractive targets for total synthesis and biogenetic studies. Successive discoveries of new alkaloids with unprecedented skeletons have made a great contribution to structural diversities of alkaloids elaborated by plants of the genus Daphniphyllum. By the end of 2008, more than 200 alkaloids belonging to 14 different skeletal types have been isolated from different parts of plants of thirteen Daphniphyllum species. These alkaloids show cytotoxic, antioxidant, vasorelaxant, and antiplatelet activating factor effects. The plausible biosynthetic pathways for Daphniphyllum alkaloids have been proposed and biomimetic total syntheses of some alkaloids completed. To provide an update of the previous reviews published in 2009, new structures, synthesis, and bioactivity of Daphniphyllum alkaloids reported in recent years are presented in this article. In the meantime, an additional 54 novel alkaloids have been isolated and identified. Among them, some possess unprecedented frameworks. Several inspired organic syntheses were completed. [ABSTRACT FROM AUTHOR]

Published

2013

192. Inactivation of Voltage-Gated Cardiac K+ Channels.

Author

Rasmusson, Randall L., Morales, Michael J., Wang, Shimin, Liu, Shuguang, Campbell, Donald L., Brahmajothi, Mulugu V., and Strauss, Harold C.

Published

1998

193. Enhanced differentiation of human pluripotent stem cells into pancreatic endocrine cells in 3D culture by inhibition of focal adhesion kinase.

Author

Liu, Xiaofang, Qin, Jinhua, Chang, Mingyang, Wang, Shuyong, Li, Yali, Pei, Xuetao, and Wang, Yunfang

Subjects

FOCAL adhesion kinase, ENTEROENDOCRINE cells, HUMAN stem cells, PLURIPOTENT stem cells, HUMAN embryonic stem cells, CELL culture, GTPASE-activating protein

Abstract

Background: Generation of insulin-producing cells from human pluripotent stem cells (hPSCs) in vitro would be useful for drug discovery and cell therapy in diabetes. Three-dimensional (3D) culture is important for the acquisition of mature insulin-producing cells from hPSCs, but the mechanism by which it promotes β cell maturation is poorly understood. Methods: We established a stepwise method to induce high-efficiency differentiation of human embryonic stem cells (hESCs) into mature monohormonal pancreatic endocrine cells (PECs), with the last maturation stage in 3D culture. To comprehensively compare two-dimensional (2D) and 3D cultures, we examined gene expression, pancreas-specific markers, and functional characteristics in 2D culture-induced PECs and 3D culture-induced PECs. The mechanisms were considered from the perspectives of cell–cell and cell–extracellular matrix interactions which are fundamentally different between 2D and 3D cultures. Results: The expression of the pancreatic endocrine-specific transcription factors PDX1, NKX6.1, NGN3, ISL1, and PAX6 and the hormones INS, GCG, and SST was significantly increased in 3D culture-induced PECs. 3D culture yielded monohormonal endocrine cells, while 2D culture-induced PECs co-expressed INS and GCG or INS and SST or even expressed all three hormones. We found that focal adhesion kinase (FAK) phosphorylation was significantly downregulated in 3D culture-induced PECs, and treatment with the selective FAK inhibitor PF-228 improved the expression of β cell-specific transcription factors in 2D culture-induced PECs. We further demonstrated that 3D culture may promote endocrine commitment by limiting FAK-dependent activation of the SMAD2/3 pathway. Moreover, the expression of the gap junction protein Connexin 36 was much higher in 3D culture-induced PECs than in 2D culture-induced PECs, and inhibition of the FAK pathway in 2D culture increased Connexin 36 expression. Conclusion: We developed a strategy to induce differentiation of monohormonal mature PECs from hPSCs and found limited FAK-dependent activation of the SMAD2/3 pathway and unregulated expression of Connexin 36 in 3D culture-induced PECs. This study has important implications for the generation of mature, functional β cells for drug discovery and cell transplantation therapy for diabetes and sheds new light on the signaling events that regulate endocrine specification. [ABSTRACT FROM AUTHOR]

Published

2020

194. Identification and characterization of the Cucurbitacins, a novel class of small-molecule inhibitors of Tropomyosin receptor kinase a.

Author

Zhong, Yueling, Xu, Hong, Zhong, Yi, Zhang, Xuemiao, Zeng, Ting, Li, Limei, Xu, Gaojie, Li, Minhui, Liu, Jin, and Yang, Tai

Subjects

CELL culture, CELL receptors, ITCHING, CHINESE medicine, MOLECULAR structure, PHOSPHORYLATION, PROTEIN-tyrosine kinases, SKIN, TERPENES, TRANSFERASES, PLANT extracts, IN vitro studies

Abstract

Background: NGF-TrkA is well known to play a key role in propagating and sustaining pruritogenic signals, which form the pathology of chronic pruritus. Inhibition of NGF-TrkA is a known strategy for the treatment of pruritus. In the present paper, we describe the identification, in vitro characterization, structure–activity analysis, and inhibitory evaluation of a novel TrkA inhibitory scaffold exemplified by Cucurbitacins (Cus). Methods: Cus were identified as TrkA inhibitors in a large-scale kinase library screen. To obtain structural models of Cus as TrkA inhibitors, AutoDock was used to explore their binding to TrkA. Furthermore, PC12 cell culture systems have been used to study the effects of Cus and traditional Chinese medicinal plants (Tian Gua Di and bitter gourd leaf) extracts on the kinase activity of TrkA. Results: Cus block the phosphorylation of TrkA on several tyrosine sites, including Tyr490, Tyr674/675, and Tyr785, and inhibit downstream Akt and MAPK phosphorylation in response to NGF in PC12 cell model systems. Furthermore, traditional Chinese medicinal plants (Tian Gua Di and bitter gourd leaf) containing Cu extracts were shown to inhibit the phosphorylation of TrkA and Akt. These data reveal mechanisms, at least partly, of the anti-pruritus bioactivity of Cus. Conclusion: Taken together, with the recent discovery of the important role of TrkA as a therapeutic target, Cus could be the basis for the design of improved TrkA kinase inhibitors, which could someday help treat pruritus. [ABSTRACT FROM AUTHOR]

Published

2019

195. Identification of a novel S6K1 inhibitor, rosmarinic acid methyl ester, for treating cisplatin-resistant cervical cancer.

Author

Nam, Ki Hong, Yi, Sang Ah, Nam, Gibeom, Noh, Jae Sung, Park, Jong Woo, Lee, Min Gyu, Park, Jee Hun, Oh, Hwamok, Lee, Jieun, Lee, Kang Ro, Park, Hyun-Ju, Lee, Jaecheol, and Han, Jeung-Whan

Subjects

CISPLATIN, CERVICAL cancer, METHYL formate

Abstract

Background: The mTOR/S6K1 signaling pathway is often activated in cervical cancer, and thus considered a molecular target for cervical cancer therapies. Inhibiting mTOR is cytotoxic to cervical cancer cells and creates a synergistic anti-tumor effect with conventional chemotherapy agents. In this study, we identified a novel S6K1 inhibitor, rosmarinic acid methyl ester (RAME) for the use of therapeutic agent against cervical cancer.Methods: Combined structure- and ligand-based virtual screening was employed to identify novel S6K1 inhibitors among the in house natural product library. In vitro kinase assay and immunoblot assay was used to examine the effects of RAME on S6K1 signaling pathway. Lipidation of LC3 and mRNA levels of ATG genes were observed to investigate RAME-mediated autophagy. PARP cleavage, mRNA levels of apoptotic genes, and cell survival was measured to examine RAME-mediated apoptosis.Results: RAME was identified as a novel S6K1 inhibitor through the virtual screening. RAME, not rosmarinic acid, effectively reduced mTOR-mediated S6K1 activation and the kinase activity of S6K1 by blocking the interaction between S6K1 and mTOR. Treatment of cervical cancer cells with RAME promoted autophagy and apoptosis, decreasing cell survival rate. Furthermore, we observed that combination treatment with RAME and cisplatin greatly enhanced the anti-tumor effect in cisplatin-resistant cervical cancer cells, which was likely due to mTOR/S6K1 inhibition-mediated autophagy and apoptosis.Conclusions: Our findings suggest that inhibition of S6K1 by RAME can induce autophagy and apoptosis in cervical cancer cells, and provide a potential option for cervical cancer treatment, particularly when combined with cisplatin. [ABSTRACT FROM AUTHOR]

Published

2019

196. TRAP1 downregulation in human ovarian cancer enhances invasion and epithelial-mesenchymal transition.

Author

Amoroso, Maria R, Matassa, Danilo S, Agliarulo, Ilenia, Avolio, Rosario, Lu, Haonan, Sisinni, Lorenza, Lettini, Giacomo, Gabra, Hani, Landriscina, Matteo, and Esposito, Franca

Published

2016

197. β1 integrin mediates an alternative survival pathway in breast cancer cells resistant to lapatinib.

Author

Huang, Catherine, Park, Catherine C, Hilsenbeck, Susan G, Ward, Robin, Rimawi, Mothaffar F, Wang, Yen-Chao, Shou, Jiang, Bissell, Mina J, Osborne, C Kent, and Schiff, Rachel

Abstract

Introduction: The overexpression of human epidermal growth factor receptor (HER)-2 in 20% of human breast cancers and its association with aggressive growth has led to widespread use of HER2-targeted therapies, such as trastuzumab (T) and lapatinib (L). Despite the success of these drugs, their efficacy is limited in patients whose tumors demonstrate de novo or acquired resistance to treatment. The β1 integrin resides on the membrane of the breast cancer cell, activating several elements of breast tumor progression including proliferation and survival.Methods: We developed a panel of HER2-overexpressing cell lines resistant to L, T, and the potent LT combination through long-term exposure and validated these models in 3D culture. Parental and L/T/LT-resistant cells were subject to HER2 and β1 integrin inhibitors in 3D and monitored for 12 days, followed by quantification of colony number. Parallel experiments were conducted where cells were either stained for Ki-67 and Terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL) or harvested for protein and analyzed by immunoblot. Results were subjected to statistical testing using analysis of variance and linear contrasts, followed by adjustment with the Sidak method.Results: Using multiple cell lines including BT474 and HCC1954, we reveal that in L and LT resistance, where phosphorylation of EGFR/HER1, HER2, and HER3 are strongly inhibited, kinases downstream of β1 integrin--including focal adhesion kinase (FAK) and Src--are up-regulated. Blockade of β1 by the antibody AIIB2 abrogates this up-regulation and functionally achieves significant growth inhibition of L and LT resistant cells in 3D, without dramatically affecting the parental cells. SiRNA against β1 as well as pharmacologic inhibition of FAK achieve the same growth inhibitory effect. In contrast, trastuzumab-resistant cells, which retain high levels of phosphorylated EGFR/HER1, HER2, and HER3, are only modestly growth-inhibited by AIIB2.Conclusions: Our data suggest that HER2 activity, which is suppressed in resistance involving L but not T alone, dictates whether β1 mediates an alternative pathway driving resistance. Our findings justify clinical studies investigating the inhibition of β1 or its downstream signaling moieties as strategies to overcome acquired L and LT resistance. [ABSTRACT FROM AUTHOR]

Published

2011

198. Recent nanotechnological aspects and molecular targeting strategies for lung cancer therapy

Author

Mishra, Lopamudra, Kumari, Lakshmi, Sharma, Yash, Chahar, Kanak, Kumar, Mritunjay, Patel, Preeti, Das Gupta, Ghanshyam, and Das Kurmi, Balak

Published

2024

199. Drug Design and Discovery : Inhibitors of Mitogen-Activated Protein Kinases

Author

Surya K. De and Surya K. De

Subjects

Drug delivery systems, Pharmacology, Pharmacy

Abstract

This book covers the important role small molecules can play in the modulation of stress-activated protein kinase (SAPK), also called the mitogen-activated protein kinase (MAPK) pathway, and the potential this may offer in enabling the development of future medicine therapies. It is clear that MAP kinase pathway therapies could continue to drive increasing interest in the field, both within academic laboratories and also in the biotechnology and pharmaceutical sectors. This book provides an overview of protein kinase inhibitors, the biological roles of MAP kinases, ATP-competitive and non-competitive inhibitors, covalent inhibitors, and more. This book is intended for professors in academia, researchers in pharmaceutical and biotechnology sectors working on protein kinases, and graduate students in pharmacy/chemistry.

Published

2024

200. Advanced Materials for Multidisciplinary Applications

Author

Marinda Wu, Wei Gao, Lei Li, Yingchun Lu, Jingbo Louise Liu, Marinda Wu, Wei Gao, Lei Li, Yingchun Lu, and Jingbo Louise Liu

Subjects

Materials, Catalysis, Force and energy, Biomaterials, Nanotechnology, Renewable energy sources, Chemistry

Abstract

This book provides an overview of recent research in the area of advanced materials for improving human healthcare, protecting the environment and alternative energy resources. The authors analyze and deliver viable technical solutions, demonstrating how chemistry and engineering can collectively solve technical and societal challenges. The book explores innovative technology for the synthesis of complex carbohydrates & glycoproteins, new drug development & delivery, theragnostics of infectious disease and cancer. It also provides insights into the nature of energy extraction, management and usage related to fossil fuels and sustainable energy. The book brings together a group of dynamic and productive scientists, engineers, and other professionals in celebration of the 40th Anniversary of Chinese American Chemical Society. It is a valuable resource for all readers interested in the study of materials to address society's increasing need forelectrical and chemical energy.

Published

2023