Your search keyword '"Phenformin"' showing total 12 results

1. Ampk regulates IgD expression but not energy stress with B cell activation.

Author

Waters, Lynnea R, Waters, Lynnea R, Ahsan, Fasih M, Ten Hoeve, Johanna, Hong, Jason S, Kim, Diane NH, Minasyan, Aspram, Braas, Daniel, Graeber, Thomas G, Zangle, Thomas A, Teitell, Michael A, Waters, Lynnea R, Waters, Lynnea R, Ahsan, Fasih M, Ten Hoeve, Johanna, Hong, Jason S, Kim, Diane NH, Minasyan, Aspram, Braas, Daniel, Graeber, Thomas G, Zangle, Thomas A, and Teitell, Michael A

Abstract

Ampk is an energy gatekeeper that responds to decreases in ATP by inhibiting energy-consuming anabolic processes and promoting energy-generating catabolic processes. Recently, we showed that Lkb1, an understudied kinase in B lymphocytes and a major upstream kinase for Ampk, had critical and unexpected roles in activating naïve B cells and in germinal center formation. Therefore, we examined whether Lkb1 activities during B cell activation depend on Ampk and report surprising Ampk activation with in vitro B cell stimulation in the absence of energy stress, coupled to rapid biomass accumulation. Despite Ampk activation and a controlling role for Lkb1 in B cell activation, Ampk knockout did not significantly affect B cell activation, differentiation, nutrient dynamics, gene expression, or humoral immune responses. Instead, Ampk loss specifically repressed the transcriptional expression of IgD and its regulator, Zfp318. Results also reveal that early activation of Ampk by phenformin treatment impairs germinal center formation but does not significantly alter antibody responses. Combined, the data show an unexpectedly specific role for Ampk in the regulation of IgD expression during B cell activation.

Published

2019

2. Ampk regulates IgD expression but not energy stress with B cell activation.

Author

Waters, Lynnea R, Waters, Lynnea R, Ahsan, Fasih M, Ten Hoeve, Johanna, Hong, Jason S, Kim, Diane NH, Minasyan, Aspram, Braas, Daniel, Graeber, Thomas G, Zangle, Thomas A, Teitell, Michael A, Waters, Lynnea R, Waters, Lynnea R, Ahsan, Fasih M, Ten Hoeve, Johanna, Hong, Jason S, Kim, Diane NH, Minasyan, Aspram, Braas, Daniel, Graeber, Thomas G, Zangle, Thomas A, and Teitell, Michael A

Abstract

Ampk is an energy gatekeeper that responds to decreases in ATP by inhibiting energy-consuming anabolic processes and promoting energy-generating catabolic processes. Recently, we showed that Lkb1, an understudied kinase in B lymphocytes and a major upstream kinase for Ampk, had critical and unexpected roles in activating naïve B cells and in germinal center formation. Therefore, we examined whether Lkb1 activities during B cell activation depend on Ampk and report surprising Ampk activation with in vitro B cell stimulation in the absence of energy stress, coupled to rapid biomass accumulation. Despite Ampk activation and a controlling role for Lkb1 in B cell activation, Ampk knockout did not significantly affect B cell activation, differentiation, nutrient dynamics, gene expression, or humoral immune responses. Instead, Ampk loss specifically repressed the transcriptional expression of IgD and its regulator, Zfp318. Results also reveal that early activation of Ampk by phenformin treatment impairs germinal center formation but does not significantly alter antibody responses. Combined, the data show an unexpectedly specific role for Ampk in the regulation of IgD expression during B cell activation.

Published

2019

3. Antidiabetika

Author

Bartoš, Martin, Be, Tatiana, Bartoš, Martin, and Be, Tatiana

Abstract

Tato bakalářská práce je tvořena dvěma částmi - teoretickou a experimentální. První část je zaměřena na problematiku antidiabetik, jejich strukturu, popis, výskyt a stanovení v různých matricích. Druhá část se zabývá izotachoforetickým stanovením různých antidiabetik. Byl vybrán optimální elektrolytový system s vedoucím elektrolytem o pH 5 tvořeným 0,01 M octanem draselným a kyselinou octovou k úpravě pH. Jako koncový elektrolyt byla využita 0,01 M kyselina octová. Tento postup stanovení antidiabetik byl použit pro stanovení metforminu v léčivých přípravcích., This bachelor thesis is consisted of two parts - theoretical and experimental. The first part is focused on antidiabetic drugs, their structure, description, occurrence and determination in various matrices. The second part deals with isotachophoretic determination of various antidiabetic drugs. An optimal electrolyte system with 0.01 M potassium acetate and acetic acid (pH 5.0) as leading electrolyte and 0.01 M acetic acid as terminating electrolyte was selected. Validated procedure was used to determine metformin in pharmaceutical products., Fakulta chemicko-technologická, Popis práce, předpověď počtu lidí s diabetem, Dokončená práce s úspěšnou obhajobou

Published

2019

4. Studying the Role of AMPK in Cardiac Hypertrophy and Protein Synthesis.

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, Mailleux, Florence, Beauloye, Christophe, Balligand, Jean-Luc, Horman, Sandrine, Bertrand, Luc, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, Mailleux, Florence, Beauloye, Christophe, Balligand, Jean-Luc, Horman, Sandrine, and Bertrand, Luc

Abstract

Pathological cardiac hypertrophy, which is a compensatory mechanism established to maintain cardiac function in response to neurohormonal or mechanical stresses, becomes maladaptive with time and frequently leads to heart failure. AMP-activated protein kinase (AMPK) has been extensively described in the literature to act as a break in cardiac hypertrophy development. Its anti-hypertrophic action mostly correlates with the inhibition of several important players of cardiac hypertrophy including protein synthesis and pro-hypertrophic gene expression pathways involving the transcription factor nuclear factor of activated T cells (NFAT) and the mitogen-activated protein kinases ERK1/2. In this chapter, we describe methodologies designed to evaluate cardiomyocyte hypertrophy and its major molecular mechanisms in response to AMPK activation. Two different compounds, AICAr and the biguanide phenformin, were used to promote AMPK activation.

Published

2018

5. Studying the Role of AMPK in Cardiac Hypertrophy and Protein Synthesis.

Author

UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service de pathologies cardiovasculaires intensives, UCL - (SLuc) Département cardiovasculaire, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - (SLuc) Département de médecine interne et services associés, Mailleux, Florence, Beauloye, Christophe, Balligand, Jean-Luc, Horman, Sandrine, Bertrand, Luc, UCL - SSS/IREC/CARD - Pôle de recherche cardiovasculaire, UCL - (SLuc) Service de pathologies cardiovasculaires intensives, UCL - (SLuc) Département cardiovasculaire, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - (SLuc) Département de médecine interne et services associés, Mailleux, Florence, Beauloye, Christophe, Balligand, Jean-Luc, Horman, Sandrine, and Bertrand, Luc

Abstract

Pathological cardiac hypertrophy, which is a compensatory mechanism established to maintain cardiac function in response to neurohormonal or mechanical stresses, becomes maladaptive with time and frequently leads to heart failure. AMP-activated protein kinase (AMPK) has been extensively described in the literature to act as a break in cardiac hypertrophy development. Its anti-hypertrophic action mostly correlates with the inhibition of several important players of cardiac hypertrophy including protein synthesis and pro-hypertrophic gene expression pathways involving the transcription factor nuclear factor of activated T cells (NFAT) and the mitogen-activated protein kinases ERK1/2. In this chapter, we describe methodologies designed to evaluate cardiomyocyte hypertrophy and its major molecular mechanisms in response to AMPK activation. Two different compounds, AICAr and the biguanide phenformin, were used to promote AMPK activation.

Published

2018

6. LKB1 promotes metabolic flexibility in response to energy stress.

Author

Parker, Seth J, Parker, Seth J, Svensson, Robert U, Divakaruni, Ajit S, Lefebvre, Austin E, Murphy, Anne N, Shaw, Reuben J, Metallo, Christian M, Parker, Seth J, Parker, Seth J, Svensson, Robert U, Divakaruni, Ajit S, Lefebvre, Austin E, Murphy, Anne N, Shaw, Reuben J, and Metallo, Christian M

Abstract

The Liver Kinase B1 (LKB1) tumor suppressor acts as a metabolic energy sensor to regulate AMP-activated protein kinase (AMPK) signaling and is commonly mutated in various cancers, including non-small cell lung cancer (NSCLC). Tumor cells deficient in LKB1 may be uniquely sensitized to metabolic stresses, which may offer a therapeutic window in oncology. To address this question we have explored how functional LKB1 impacts the metabolism of NSCLC cells using 13C metabolic flux analysis. Isogenic NSCLC cells expressing functional LKB1 exhibited higher flux through oxidative mitochondrial pathways compared to those deficient in LKB1. Re-expression of LKB1 also increased the capacity of cells to oxidize major mitochondrial substrates, including pyruvate, fatty acids, and glutamine. Furthermore, LKB1 expression promoted an adaptive response to energy stress induced by anchorage-independent growth. Finally, this diminished adaptability sensitized LKB1-deficient cells to combinatorial inhibition of mitochondrial complex I and glutaminase. Together, our data implicate LKB1 as a major regulator of adaptive metabolic reprogramming and suggest synergistic pharmacological strategies for mitigating LKB1-deficient NSCLC tumor growth.

Published

2017

7. Immunohistochemical localization of OCT2 in the cochlea of various species

Author

Hellberg, Victoria, Gahm, Caroline, Liu, Wei, Ehrsson, Hans, Rask-Andersen, Helge, Laurell, Göran, Hellberg, Victoria, Gahm, Caroline, Liu, Wei, Ehrsson, Hans, Rask-Andersen, Helge, and Laurell, Göran

Abstract

ObjectiveTo locate the organic cation transporter 2 (OCT2) in the cochlea of three different species and to modulate the ototoxicity of cisplatin in the guinea pig by pretreatment with phenformin, having a known affinity for OCT2. Study DesignImmunohistochemical and in vivo study. MethodsSections from the auditory end organs were subjected to immunohistochemical staining in order to identify OCT2 in cochlea from untreated rats, guinea pigs, and a pig. In the in vivo study, guinea pigs were given phenformin intravenously 30 minutes before cisplatin administration. Electrophysiological hearing thresholds were determined, and hair cells loss was assessed 96 hours later. The total amount of platinum in cochlear tissue was determined using mass spectrometry. ResultsOrganic cation transporter 2 was found in the supporting cells and in type I spiral ganglion cells in the cochlea of all species studied. Pretreatment with phenformin did not reduce the ototoxic side effect of cisplatin. Furthermore, the concentration of platinum in the cochlea was not affected by phenformin. ConclusionsThe localization of OCT2 in the supporting cells and type I spiral ganglion cells suggests that this transport protein is not primarily involved in cisplatin uptake from the systemic circulation. We hypothesize that OCT2 transport intensifies cisplatin ototoxicity via transport mechanisms in alternate compartments of the cochlea. Level of EvidenceN/A. Laryngoscope, 125:E320-E325, 2015

Published

2015

8. Heightening Energetic Stress Selectively Targets LKB1-Deficient Non-Small Cell Lung Cancers.

Author

Momcilovic, Milica, Momcilovic, Milica, McMickle, Robert, Abt, Evan, Seki, Atsuko, Simko, Sarah A, Magyar, Clara, Stout, David B, Fishbein, Michael C, Walser, Tonya C, Dubinett, Steven M, Shackelford, David B, Momcilovic, Milica, Momcilovic, Milica, McMickle, Robert, Abt, Evan, Seki, Atsuko, Simko, Sarah A, Magyar, Clara, Stout, David B, Fishbein, Michael C, Walser, Tonya C, Dubinett, Steven M, and Shackelford, David B

Abstract

Inactivation of the LKB1 tumor suppressor is a frequent event in non-small cell lung carcinoma (NSCLC) leading to the activation of mTOR complex 1 (mTORC1) and sensitivity to the metabolic stress inducer phenformin. In this study, we explored the combinatorial use of phenformin with the mTOR catalytic kinase inhibitor MLN0128 as a treatment strategy for NSCLC bearing comutations in the LKB1 and KRAS genes. NSCLC is a genetically and pathologically heterogeneous disease, giving rise to lung tumors of varying histologies that include adenocarcinomas and squamous cell carcinomas (SCC). We demonstrate that phenformin in combination with MLN0128 induced a significant therapeutic response in KRAS/LKB1-mutant human cell lines and genetically engineered mouse models of NSCLC that develop both adenocarcinomas and SCCs. Specifically, we found that KRAS/LKB1-mutant lung adenocarcinomas responded strongly to phenformin + MLN0128 treatment, but the response of SCCs to single or combined treatment with MLN0128 was more attenuated due to acquired resistance to mTOR inhibition through modulation of the AKT-GSK signaling axis. Combinatorial use of the mTOR inhibitor and AKT inhibitor MK2206 robustly inhibited the growth and viability of squamous lung tumors, thus providing an effective strategy to overcome resistance. Taken together, our findings define new personalized therapeutic strategies that may be rapidly translated into clinical use for the treatment of KRAS/LKB1-mutant adenocarcinomas and squamous cell tumors.

Published

2015

9. Heightening Energetic Stress Selectively Targets LKB1-Deficient Non-Small Cell Lung Cancers.

Author

Momcilovic, Milica, Momcilovic, Milica, McMickle, Robert, Abt, Evan, Seki, Atsuko, Simko, Sarah A, Magyar, Clara, Stout, David B, Fishbein, Michael C, Walser, Tonya C, Dubinett, Steven M, Shackelford, David B, Momcilovic, Milica, Momcilovic, Milica, McMickle, Robert, Abt, Evan, Seki, Atsuko, Simko, Sarah A, Magyar, Clara, Stout, David B, Fishbein, Michael C, Walser, Tonya C, Dubinett, Steven M, and Shackelford, David B

Abstract

Inactivation of the LKB1 tumor suppressor is a frequent event in non-small cell lung carcinoma (NSCLC) leading to the activation of mTOR complex 1 (mTORC1) and sensitivity to the metabolic stress inducer phenformin. In this study, we explored the combinatorial use of phenformin with the mTOR catalytic kinase inhibitor MLN0128 as a treatment strategy for NSCLC bearing comutations in the LKB1 and KRAS genes. NSCLC is a genetically and pathologically heterogeneous disease, giving rise to lung tumors of varying histologies that include adenocarcinomas and squamous cell carcinomas (SCC). We demonstrate that phenformin in combination with MLN0128 induced a significant therapeutic response in KRAS/LKB1-mutant human cell lines and genetically engineered mouse models of NSCLC that develop both adenocarcinomas and SCCs. Specifically, we found that KRAS/LKB1-mutant lung adenocarcinomas responded strongly to phenformin + MLN0128 treatment, but the response of SCCs to single or combined treatment with MLN0128 was more attenuated due to acquired resistance to mTOR inhibition through modulation of the AKT-GSK signaling axis. Combinatorial use of the mTOR inhibitor and AKT inhibitor MK2206 robustly inhibited the growth and viability of squamous lung tumors, thus providing an effective strategy to overcome resistance. Taken together, our findings define new personalized therapeutic strategies that may be rapidly translated into clinical use for the treatment of KRAS/LKB1-mutant adenocarcinomas and squamous cell tumors.

Published

2015

10. Regulation of AMP-activated protein kinase by LKB1 and CaMKK in adipocytes

Author

Gormand, Amélie, Henriksson, Emma, Ström, Kristoffer, Jensen, Thomas Elbenhardt, Sakamoto, Kei, Göransson, Olga, Gormand, Amélie, Henriksson, Emma, Ström, Kristoffer, Jensen, Thomas Elbenhardt, Sakamoto, Kei, and Göransson, Olga

Abstract

AMP-activated protein kinase (AMPK) is a serine/threonine kinase that regulates cellular and whole body energy homeostasis. In adipose tissue, activation of AMPK has been demonstrated in response to a variety of extracellular stimuli. However, the upstream kinase that activates AMPK in adipocytes remains elusive. Previous studies have identified LKB1 as a major AMPK kinase in muscle, liver, and other tissues. In certain cell types, Ca(2+) /calmodulin-dependent protein kinase kinase β (CaMKKβ) has been shown to activate AMPK in response to increases of intracellular Ca(2+) levels. Our aim was to investigate if LKB1 and/or CaMKK function as AMPK kinases in adipocytes. We used adipose tissue and isolated adipocytes from mice in which the expression of LKB1 was reduced to 10-20% of that of wild-type (LKB1 hypomorphic mice). We show that adipocytes from LKB1 hypomorphic mice display a 40% decrease in basal AMPK activity and a decrease of AMPK activity in the presence of the AMPK activator phenformin. We also demonstrate that stimulation of 3T3L1 adipocytes with intracellular [Ca(2+) ]-raising agents results in an activation of the AMPK pathway. The inhibition of CaMKK isoforms, particularly CaMKKβ, by the inhibitor STO-609 or by siRNAs, blocked Ca(2+) -, but not phenformin-, AICAR-, or forskolin-induced activation of AMPK, indicating that CaMKK activated AMPK in response to Ca(2+) . Collectively, we show that LKB1 is required to maintain normal AMPK-signaling in non-stimulated adipocytes and in the presence of phenformin. In addition, we demonstrate the existence of a Ca(2+) /CaMKK signaling pathway that can also regulate the activity of AMPK in adipocytes.

Published

2011

11. Oxygen consumption is depressed in patients with lactic acidosis due to biguanide intoxication

Author

Protti, A, Russo, R, Tagliabue, P, Vecchio, S, Singer, M, Rudiger, A, Foti, G, Rossi, A, Mistraletti, G, Gattinoni, L, FOTI, GIUSEPPE, Gattinoni, L., Protti, A, Russo, R, Tagliabue, P, Vecchio, S, Singer, M, Rudiger, A, Foti, G, Rossi, A, Mistraletti, G, Gattinoni, L, FOTI, GIUSEPPE, and Gattinoni, L.

Abstract

Introduction: Lactic acidosis can develop during biguanide (metformin and phenformin) intoxication, possibly as a consequence of mitochondrial dysfunction. To verify this hypothesis, we investigated whether body oxygen consumption (VO2), that primarily depends on mitochondrial respiration, is depressed in patients with biguanide intoxication.Methods: Multicentre retrospective analysis of data collected from 24 patients with lactic acidosis (pH 6.93 ± 0.20; lactate 18 ± 6 mM at hospital admission) due to metformin (n = 23) or phenformin (n = 1) intoxication. In 11 patients, VO2 was computed as the product of simultaneously recorded arterio-venous difference in O2 content [C(a-v)O2] and cardiac index (CI). In 13 additional cases, C(a-v)O2, but not CI, was available.Results: On day 1, VO2 was markedly depressed (67 ± 28 ml/min/m2) despite a normal CI (3.4 ± 1.2 L/min/m2). C(a-v)O2 was abnormally low in both patients either with (2.0 ± 1.0 ml O2/100 ml) or without (2.5 ± 1.1 ml O2/100 ml) CI (and VO2) monitoring. Clearance of the accumulated drug was associated with the resolution of lactic acidosis and a parallel increase in VO2 (P < 0.001) and C(a-v)O2 (P < 0.05). Plasma lactate and VO2 were inversely correlated (R2 0.43; P < 0.001, n = 32).Conclusions: VO2 is abnormally low in patients with lactic acidosis due to biguanide intoxication. This finding is in line with the hypothesis of inhibited mitochondrial respiration and consequent hyperlactatemia. © 2010 Protti et al.; licensee BioMed Central Ltd.

Published

2010

12. Antidiabetic Biguanides as Anti-Aging Drugs

Author

Anisimov V.N. and Anisimov V.N.

Abstract

Evidence has emerged that metformin and other antidiabetic biguabides are promising candidates for pharmacological interventions leading to slowing down of aging, prolonged life span and preventing or postponing age-associate diseases, including cancer. In this chapter, the available data on effects of biguanides in rodents are summarized and discussed.