Your search keyword '"Mehrdad Ghashghaeinia"' showing total 18 results

1. Human erythrocytes, nuclear factor kappaB (NFκB) and hydrogen sulfide (H2S) – from non-genomic to genomic research

Author

Mehrdad Ghashghaeinia and Ulrich Mrowietz

Subjects

insulin, obesity, Programmed cell death, Erythrocytes, P50, Hydrogen sulfide, hydrogen sulfide, Inflammation, Review, Biology, Kidney, chemistry.chemical_compound, medicine, Humans, Glycolysis, glutathione, methemoglobin, Molecular Biology, Kinase, Human erythrocytes, NF-kappa B, psoriasis, Cell Biology, Glutathione, glycolysis, equipment and supplies, Cell biology, chemistry, inflammation, medicine.symptom, NFĸB, Signal Transduction, Developmental Biology

Abstract

Enucleated mature human erythrocytes possess NFĸBs and their upstream kinases. There is a negative correlation between eryptosis (cell death of erythrocytes) and the amount of NFĸB subunits p50 and Rel A (p65). This finding is based on the fact that young erythrocytes have the highest levels of NFĸBs and the lowest eryptosis rate, while in old erythrocytes the opposite ratio prevails. Human erythrocytes (hRBCs) effectively control the homeostasis of the cell membrane permeable anti-inflammatory signal molecule hydrogen sulfide (H2S). They endogenously produce H2S via both non-enzymic (glutathione-dependent) and enzymic processes (mercaptopyruvate sulfur transferase-dependent). They uptake H2S from diverse tissues and very effectively degrade H2S via methemoglobin (Hb-Fe3+)-catalyzed oxidation. Interestingly, a reciprocal correlation exists between the intensity of inflammatory diseases and endogenous levels of H2S. H2S deficiency has been observed in patients with diabetes, psoriasis, obesity, and chronic kidney disease (CKD). Furthermore, endogenous H2S deficiency results in impaired renal erythropoietin (EPO) production and EPO-dependent erythropoiesis. In general we can say: dynamic reciprocal interaction between tumor suppressor and oncoproteins, orchestrated and sequential activation of pro-inflammatory NFĸB heterodimers (RelA-p50) and the anti-inflammatory NFĸB-p50 homodimers for optimal inflammation response, appropriate generation, subsequent degradation of H2S etc., are prerequisites for a functioning cell and organism. Diseases arise when the fragile balance between different signaling pathways that keep each other in check is permanently disturbed. This work deals with the intact anti-inflammatory hRBCs and their role as guarantors to maintain the redox status in the physiological range, a basis for general health and well-being.

Published

2021

2. Coronavirus disease 2019 (COVID-19), human erythrocytes and the PKC-alpha/-beta inhibitor chelerythrine –possible therapeutic implication

Author

Mehrdad Ghashghaeinia, Thomas Wieder, Peter Dreischer, and Martin Köberle

Subjects

0301 basic medicine, Drug, Erythrocytes, Protein Kinase C-alpha, media_common.quotation_subject, protein kinase C-alpha (PKC-α), Respiratory Tract Diseases, Protein Kinase C beta, Apoptosis, mTORC1, Review, Mechanistic Target of Rapamycin Complex 2, Pharmacology, Biology, Mechanistic Target of Rapamycin Complex 1, PKC alpha, Antiviral Agents, Virus, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Humans, RNA Viruses, Beta (finance), Molecular Biology, chelerythrine, Protein Kinase Inhibitors, media_common, Benzophenanthridines, SARS-CoV-2, RNA polymerases, COVID-19, Cell Biology, DNA-Directed RNA Polymerases, COVID-19 Drug Treatment, 030104 developmental biology, Chelerythrine, chemistry, 030220 oncology & carcinogenesis, Protein Biosynthesis, mammalian target of rapamycin complex 1 & 2 (mTORC1/-2), Developmental Biology

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) causes COVID-19. Until now, diverse drugs have been used for the treatment of COVID-19. These drugs are associated with severe side effects, e.g. induction of erythrocyte death, named eryptosis. This massively affects the oxygen (O2) supply of the organism. Therefore, three elementary aspects should be considered simultaneously: (1) a potential drug should directly attack the virus, (2) eliminate virus-infected host cells and (3) preserve erythrocyte survival and functionality. It is known that PKC-α inhibition enhances the vitality of human erythrocytes, while it dose-dependently activates the apoptosis machinery in nucleated cells. Thus, the use of chelerythrine as a specific PKC-alpha and -beta (PKC-α/-β) inhibitor should be a promising approach to treat people infected with SARS-CoV-2.

Published

2020

3. Association between nuclear factor of kappa B (NFκB) deficiency and induction of eryptosis in mouse erythrocytes

Author

Ulrich Mrowietz, Mehrdad Ghashghaeinia, Peter Dreischer, and Martin Köberle

Subjects

Mice, Knockout, Pharmacology, Cancer Research, Erythrocytes, business.industry, Biochemistry (medical), Clinical Biochemistry, Eryptosis, NF-kappa B p50 Subunit, Pharmaceutical Science, Cell Biology, ddc, Mice, Inbred C57BL, Mice, Apoptosis, Cancer research, Animals, Humans, Medicine, Female, business, Letter to the Editor, Cells, Cultured, Spleen, Kappa

Published

2020

4. Proliferating tumor cells mimick glucose metabolism of mature human erythrocytes

Author

Ingolf Bernhardt, Mehrdad Ghashghaeinia, Ulrich Mrowietz, and Martin Köberle

Subjects

0301 basic medicine, Erythrocytes, Carcinogenesis, pentose phosphate pathway, Review, Pentose phosphate pathway, Nicotinamide adenine dinucleotide, Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Humans, Glycolysis, Phosphoglycerate kinase 1, education, Molecular Biology, Cell Proliferation, Hexokinase, education.field_of_study, ion channels, Cell Biology, glycolysis, tumor acidic microenvironment, Citric acid cycle, Glucose, 030104 developmental biology, chemistry, Biochemistry, Proliferating tumor cells, 030220 oncology & carcinogenesis, NAD+ kinase, Nicotinamide adenine dinucleotide phosphate, Developmental Biology

Abstract

Mature human erythrocytes are dependent on anerobic glycolysis, i.e. catabolism (oxidation) of one glucose molecule to produce two ATP and two lactate molecules. Proliferating tumor cells mimick mature human erythrocytes to glycolytically generate two ATP molecules. They deliberately avoid or switch off their respiration, i.e. tricarboxylic acid (TCA) cycle and oxidative phosphorylation (OXPHOS) machinery and consequently dispense with the production of additional 36 ATP molecules from one glucose molecule. This phenomenon is named aerobic glycolysis or Warburg effect. The present review deals with the fate of a glucose molecule after entering a mature human erythrocyte or a proliferating tumor cell and describes why it is useful for a proliferating tumor cell to imitate a mature erythrocyte. Blood consisting of plasma and cellular components (99% of the cells are erythrocytes) may be regarded as a mobile organ, constantly exercising a direct interaction with other organs. Therefore, the use of drugs, which influences the biological activity of erythrocytes, has an immediate effect on the entire organism. Abbreviations: TCA: tricarboxylic acid cycle; OXPHOS: oxidative phosphorylation; GSH: reduced state of glutathione; NFκB: Nuclear factor of kappa B; PKB (Akt): protein kinase B; NOS: nitric oxide synthase; IgG: immune globulin G; H2S: hydrogen sulfide; slanDCs: Human 6-sulfo LacNAc-expressing dendritic cells; IL-8: interleukin-8; LPS: lipopolysaccharide; ROS: reactive oxygen species; PPP: pentose phosphate pathway; NADPH: nicotinamide adenine dinucleotide phosphate hydrogen; R5P: ribose-5-phophate; NAD: nicotinamide adenine dinucleotide; FAD: flavin adenine dinucleotide; O2●−: superoxide anion; G6P: glucose 6-phosphate; HbO2: Oxyhemoglobin; GAPDH: glyceraldehyde-3-phosphate dehydrogenase; GAP: glyceraldehyde-3-phosphate; 1,3-BPG: 1,3-bis-phosphoglycerate; 2,3-BPG: 2,3-bisphosphoglycerte; PGAM1: phosphoglycerate mutase 1; 3-PG: 3-phosphoglycerate; 2-PG: 2-phosphoglycerate; MIPP1: Multiple inositol polyphosphate phosphatase; mTORC1: mammalian target of rapamycin complex 1; Ru5P: ribulose 5-phosphate; ox-PPP: oxidative branch of pentose phosphate pathway; PGK: phosphoglycerate kinase; IFN-γ: interferon-γ; LDH: lactate dehydrogenase; STAT3: signal transducer and activator of transcription 3; Rheb: Ras homolog enriched in Brain; H2O2: hydrogen peroxide; ROOH: lipid peroxide; SOD: superoxide dismutase; MRC: mitochondrial respiratory chain; MbFe2+-O2: methmyoglobin; RNR: ribonucleotide reductase; PRPP: phosphoribosylpyrophosphate; PPi: pyrophosphate; GSSG: oxidized state of glutathione; non-ox-PPP: non-oxidative branch of pentose phosphate pathway; RPI: ribose-5-phosphate isomerase; RPE: ribulose 5-phosphate 3-epimerase; X5P: xylulose 5-phosphate; TK: transketolase; TA: transaldolase; F6P: fructose-6-phosphate; AR2: aldose reductase 2; SD: sorbitol dehydrogenase; HK: hexokinase; MG: mehtylglyoxal; DHAP: dihydroxyacetone phosphate; TILs: tumor-infiltrating lymphocytes; MCTs: monocarboxylate transporters; pHi: intracellular pH; Hif-1α: hypoxia-induced factor 1; NHE1: sodium/H+ (Na+/H+) antiporter 1; V-ATPase: vacuolar-type proton ATPase; CAIX: carbonic anhydrase; CO2: carbon dioxide; HCO3−: bicarbonate; NBC: sodium/bicarbonate (Na+/HCO3−) symporter; pHe: extracellular pH; GLUT-1: glucose transporter 1; PGK-1: phosphoglycerate kinase 1, Graphical Abstract

Published

2019

5. The specific PKC-α inhibitor chelerythrine blunts costunolide-induced eryptosis

Author

Martin Köberle, Martin Schaller, Vladimir Divoky, Mehrdad Ghashghaeinia, Ranieri Rossi, Daniela Giustarini, Birgit Fehrenbacher, Pavla Koralkova, Florian Lang, Renata Mojzikova, Ulrich Mrowietz, Thomas Wieder, Antonio Martínez-Ruiz, and Peter Dreischer

Subjects

0301 basic medicine, Cancer Research, Erythrocytes, Protein Kinase C-alpha, Clinical Biochemistry, Eryptosis, Pharmaceutical Science, Apoptosis, Glucose-6-phosphate dehydrogenase (G6PDH), Pharmacology, Glucosephosphate Dehydrogenase, medicine.disease_cause, Neuroprotection, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Costunolide, medicine, Humans, Chelerythrine, Glutathione, Phosphatidylserine exposure, Enzyme Inhibitors, Protein kinase C, Benzophenanthridines, Chemistry, Biochemistry (medical), Cell Biology, ddc, Oxidative Stress, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Calcium, Reactive Oxygen Species, Sesquiterpenes, Oxidative stress

Abstract

Costunolide, a natural sesquiterpene lactone, has multiple pharmacological activities such as neuroprotection or induction of apoptosis and eryptosis. However, the effects of costunolide on pro-survival factors and enzymes in human erythrocytes, e.g. glutathione and glucose-6-phosphate dehydrogenase (G6PDH) respectively, have not been studied yet. Our aim was to determine the mechanisms underlying costunolide-induced eryptosis and to reverse this process. Phosphatidylserine exposure was estimated from annexin-V-binding, cell volume from forward scatter in flow cytometry, and intracellular glutathione [GSH]ifrom high performance liquid chromatography. The oxidized status of intracellular glutathione and enzyme activities were measured by spectrophotometry. Treatment of erythrocytes with costunolide dose-dependently enhanced the percentage of annexin-V-binding cells, decreased the cell volume, depleted [GSH]iand completely inhibited G6PDH activity. The effects of costunolide on annexin-V-binding and cell volume were significantly reversed by pre-treatment of erythrocytes with the specific PKC-α inhibitor chelerythrine. The latter, however, had no effect on costunolide-induced GSH depletion. Costunolide induces eryptosis, depletes [GSH]iand inactivates G6PDH activity. Furthermore, our study reveals an inhibitory effect of chelerythrine on costunolide-induced eryptosis, indicating a relationship between costunolide and PKC-α. In addition, chelerythrine acts independently of the GSH depletion. Understanding the mechanisms of G6PDH inhibition accompanied by GSH depletion should be useful for development of anti-malarial therapeutic strategies or for synthetic lethality-based approaches to escalate oxidative stress in cancer cells for their sensitization to chemotherapy and radiotherapy.

Published

2020

6. Trifluoperazine-Induced Suicidal Erythrocyte Death and S-Nitrosylation Inhibition, Reversed by the Nitric Oxide Donor Sodium Nitroprusside

Author

Mehrdad Ghashghaeinia, Zohreh Hosseinzadeh, Sabrina Waibel, Kossai Alzoubi, Polina Petkova-Kirova, Mauro C. Wesseling, Martin Köberle, Ingolf Bernhardt, Thomas Wieder, Rosi Bissinger, Azam Shahvaroughi-Farahani, Baerbel Edelmann, Elena Ramos, Lars Kaestner, Ulrich Mrowietz, Florian Lang, Elisabeth Lang, Antonio Martínez-Ruiz, and Peter Dreischer

Subjects

0301 basic medicine, Nitroprusside, Erythrocytes, Patch-Clamp Techniques, Physiology, Eryptosis, chemistry.chemical_element, Action Potentials, Trifluoperazine, Phosphatidylserines, Calcium, Pharmacology, Hemolysis, lcsh:Physiology, Nitric oxide, lcsh:Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Potency, Humans, Nitric Oxide Donors, lcsh:QD415-436, Phosphatidylserine, Cell Size, lcsh:QP1-981, Ionomycin, Erythrocyte Membrane, S-Nitrosylation, 030104 developmental biology, chemistry, Biochemistry, Microscopy, Fluorescence, Trifuoperazine, 030220 oncology & carcinogenesis, Sodium nitroprusside, Protein Processing, Post-Translational, medicine.drug

Abstract

Background and Purpose: The high potency antipsychotic drug trifluoperazine (10-[3-(4-methyl-1-piperazinyl)-propyl]-2-(trifluoromethyl)-(10)H-phenothiazine dihydrochloride; TFP) may either counteract or promote suicidal cell death or apoptosis. Similar to apoptosis, erythrocytes may enter eryptosis, characterized by phosphatidylserine exposure at the cell surface and cell shrinkage. Eryptosis can be stimulated by an increase in cytoplasmic Ca2+ concentration ([Ca2+]i) and inhibited by nitric oxide (NO). We explored whether TFP treatment of erythrocytes induces phosphatidylserine exposure, cell shrinkage, and calcium influx, whether it impairs S-nitrosylation and whether these effects are inhibited by NO. Methods: Phosphatidylserine exposure at the cell surface was estimated from annexin-V-binding, cell volume from forward scatter, [Ca2+]i from Fluo3-fluorescence, and protein nitrosylation from fluorescence switch of the Bodipy-TMR/Sypro Ruby signal. Results: Exposure of human erythrocytes to TFP significantly enhanced the percentage of annexin-V-binding cells, raised [Ca2+]i, and decreased S-nitrosylation. The effect of TFP on annexin-V-binding was not affected by removal of extracellular Ca2+ alone, but was significantly inhibited by pre-treatment with sodium nitroprusside (SNP), an effect significantly augmented by additional removal of extracellular Ca2+. A 3 hours treatment with 0.1 µM Ca2+ ionophore ionomycin triggered annexin-V-binding and cell shrinkage, effects fully reversed by removal of extracellular Ca2+. Conclusions: TFP induces eryptosis and decreases protein S-nitrosylation, effects blunted by nitroprusside. The effect of nitroprusside is attenuated in the presence of extracellular Ca2+.

Published

2017

7. Genetic deficiency of the tumor suppressor protein p53 influences erythrocyte survival

Author

Leticia Quintanilla-Martinez, Yogesh Singh, Elisabeth Lang, Hajar Fakhri, Martin Schaller, Mehrdad Ghashghaeinia, Florian Lang, Irene Gonzalez-Menendez, Rosi Bissinger, Lisann Pelzl, Abdulla Al Mamun Bhuyan, Birgit Fehrenbacher, Basma Sukkar, Syed M. Qadri, Madhuri S. Salker, and Anja T. Umbach

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Erythrocytes, Genotype, Reticulocytosis, Clinical Biochemistry, Cell, Eryptosis, Pharmaceutical Science, Mice, Transgenic, Phosphatidylserines, Mitochondrion, Erythrocyte homeostasis, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Internal medicine, medicine, Animals, Erythropoiesis, Erythroid Precursor Cells, Pharmacology, Chemistry, Biochemistry (medical), Cell Biology, Phosphatidylserine, Erythrocyte Aging, Blood Cell Count, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Glucose, Apoptosis, 030220 oncology & carcinogenesis, Calcium, medicine.symptom, Tumor Suppressor Protein p53

Abstract

The transcription factor p53 suppresses tumor growth by inducing nucleated cell apoptosis and cycle arrest. Because of its influence on primitive erythroid cell differentiation and survival, p53 is an important determinant of erythropoiesis. However, the impact of p53 on the fate of erythrocytes, cells lacking nucleus and mitochondria, during their post-maturation phase in the circulation remained elusive. Erythrocyte survival may be compromised by suicidal erythrocyte death or eryptosis, which is hallmarked by phosphatidylserine translocation and stimulated by increase of cytosolic Ca2+ concentration. Here, we comparatively examined erythrocyte homeostasis in p53-mutant mice (Trp53tm1Tyj/J) and in corresponding WT mice (C57BL/6J) by analyzing eryptosis and erythropoiesis. To this end, spontaneous cell membrane phosphatidylserine exposure and cytosolic Ca2+ concentration were higher in erythrocytes drawn from Trp53tm1Tyj/J mice than from WT mice. Eryptosis induced by glucose deprivation, a pathophysiological cell stressor, was slightly, but significantly more prominent in erythrocytes drawn from Trp53tm1Tyj/J mice as compared to WT mice. The loss of erythrocytes by eryptosis was fully compensated by enhanced erythropoiesis in Trp53tm1Tyj/J mice, as reflected by increased reticulocytosis and abundance of erythroid precursor cells in the bone marrow. Accordingly, erythrocyte number, packed cell volume and hemoglobin were similar in Trp53tm1Tyj/J and WT mice. Taken together, functional p53 deficiency enhances the turnover of circulating erythrocytes by parallel increase of eryptosis and stimulated compensatory erythropoiesis.

Published

2018

8. Impact of Cyclin-Dependent Kinase CDK4 Inhibition on Eryptosis

Author

Mehrdad Ghashghaeinia, Adrian Lupescu, Anand Rotte, Rosi Bissinger, Florian Lang, Christine Zelenak, Elisabeth Lang, Matthias Eberhard, and Syed M. Qadri

Subjects

Programmed cell death, Erythrocytes, CDK4, Cell Survival, Physiology, Cell, Eryptosis, Apoptosis, Phosphatidylserines, Biology, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, lcsh:Physiology, Cell membrane, lcsh:Biochemistry, chemistry.chemical_compound, tert-Butylhydroperoxide, Cyclin-dependent kinase, medicine, Cell shrinkage, Humans, lcsh:QD415-436, Protein Kinase Inhibitors, lcsh:QP1-981, Cell growth, Cyclin-dependent kinase 4, Cyclin-Dependent Kinase 4, Phosphatidylserine, Molecular biology, Cell biology, medicine.anatomical_structure, chemistry, biology.protein, Calcium

Abstract

Background/Aims: The cyclin-dependent kinase 4 (CDK4) participates in the regulation of apoptosis of nucleated cells by altering transcriptional regulation of genes governing cell proliferation and cell death. Similar to apoptosis of nucleated cells, erythrocytes may enter eryptosis, which is characterized by cell shrinkage and cell membrane scrambling with phosphatidylserine (PS) exposure at the cell surface. As mature erythrocytes lack nuclei, acute stimulation of eryptosis cannot result from altered gene expression. Eryptosis is triggered by isotonic cell shrinkage following Cl- removal (replacement with the impermeant organic anion gluconate) or by oxidative stress (exposure to 0.3 mM tertbutyl-hydroperoxide [tBOOH]). The present study explored whether CDK4 is expressed in erythrocytes and whether the CDK4 inhibitors II (NSC625987) and III (ryuvidine) influence eryptosis. Methods: Western blotting was utilized for determination of the presence of CDK4 protein in human erythrocytes, and FACS analysis to determine Fluo3 fluorescence (reflecting cytosolic Ca2+), annexin-V-binding (reflecting PS-exposure) and forward scatter (reflecting cell volume). Results: CDK4 protein was present in human erythrocytes. Cl- removal was followed by decrease of forward scatter and increase of both annexin-V-binding and Fluo3 fluorescence, an effect significantly curtailed by CDK4 inhibitors II and III. Furthermore, CDK4 inhibition blunted enhanced PS-exposure elicited by tBOOH treatment. Conclusions: The present observations disclose the presence of CDK4 protein in human erythrocytes and the suppression of suicidal erythrocyte death by pharmacological inhibition of CDK4.

Published

2015

9. Age Sensitivity of NFκB Abundance and Programmed Cell Death in Erythrocytes Induced by NFκB Inhibitors

Author

Mehrdad Ghashghaeinia, Judith C. Cluitmans, Mahmoud Toulany, Mohammad Saki, Martin Köberle, Elisabeth Lang, Peter Dreischer, Tilo Biedermann, Michael Duszenko, Florian Lang, Giel J. Bosman, and Thomas Wieder

Subjects

Parthenolide, lcsh:Biochemistry, Bay 11-7082, lcsh:QP1-981, Cell volume, Eryptosis, lcsh:QD415-436, Phosphatidylserine, lcsh:Physiology

Abstract

Background/Aims: Erythrocytes may enter eryptosis, a suicidal death characterized by cell shrinkage and phosphatidylserine exposure at the erythrocyte outer membrane. Susceptibility to eryptosis is enhanced in aged erythrocytes and stimulated by NFκB-inhibitors Bay 11-7082 and parthenolide. Here we explored whether expression of NFκB and susceptibility to inhibitor-induced eryptosis is sensitive to erythrocyte age. Methods: Human erythrocytes were separated into five fractions, based on age-associated characteristics cell density and volume. NFκB compared to ß-actin protein abundance was estimated by Western blotting and cell volume from forward scatter. Phosphatidylserine exposure was identified using annexin-V binding. Results: NFκB was most abundant in young erythrocytes but virtually absent in aged erythrocytes. A 24h or 48h exposure to Ringer resulted in spontaneous decrease of forward scatter and increase of annexin V binding, effects more pronounced in aged than in young erythrocytes. Both, Bay 11-7082 (20 µM) and parthenolide (100 µM) triggered eryptosis, effects again most pronounced in aged erythrocytes. Conclusion: NFκB protein abundance is lowest and spontaneous eryptosis as well as susceptibility to Bay 11-7082 and parthenolide highest in aged erythrocytes. Thus, inhibition of NFκB signalling alone is not responsible for the stimulation of eryptosis by parthenolide or Bay 11-7082.

Published

2013

10. Pharmacological targeting of glucose-6-phosphate dehydrogenase in human erythrocytes by Bay 11-7082, parthenolide and dimethyl fumarate

Author

Daniela Giustarini, Ranieri Rossi, Renata Mojzikova, Ulrich Mrowietz, Mehrdad Ghashghaeinia, Kousi Alzoubi, Martin Köberle, Rosi Bissinger, Pavla Koralkova, Zohreh Hosseinzadeh, Ingolf Bernhardt, Thomas Wieder, Mahmoud Toulany, Peter Dreischer, and Florian Lang

Subjects

0301 basic medicine, Erythrocytes, Dimethyl Fumarate, Glutathione reductase, Eryptosis, Dehydrogenase, Biology, Glucosephosphate Dehydrogenase, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Nitriles, Glucose-6-phosphate dehydrogenase, Humans, Parthenolide, Sulfones, chemistry.chemical_classification, Multidisciplinary, Dimethyl fumarate, Glutathione, 030104 developmental biology, Enzyme, chemistry, Biochemistry, 030220 oncology & carcinogenesis, Glutathione disulfide, Sesquiterpenes

Abstract

In mature erythrocytes, glucose-6-phosphate dehydrogenase (G6PDH) and 6-phosphogluconate dehydrogenase (6PGDH) yield NADPH, a crucial cofactor of the enzyme glutathione reductase (GR) converting glutathione disulfide (GSSG) into its reduced state (GSH). GSH is essential for detoxification processes in and survival of erythrocytes. We explored whether the anti-inflammatory compounds Bay 11–7082, parthenolide and dimethyl fumarate (DMF) were able to completely deplete a common target (GSH), and to impair the function of upstream enzymes of GSH recycling and replenishment. Treatment of erythrocytes with Bay 11–7082, parthenolide or DMF led to concentration-dependent eryptosis resulting from complete depletion of GSH. GSH depletion was due to strong inhibition of G6PDH activity. Bay 11–7082 and DMF, but not parthenolide, were able to inhibit the GR activity. This approach “Inhibitors, Detection of their common target that is completely depleted or inactivated when pharmacologically relevant concentrations of each single inhibitor are applied, Subsequent functional analysis of upstream enzymes for this target” (IDS), can be applied to a broad range of inhibitors and cell types according to the selected target. The specific G6PDH inhibitory effect of these compounds may be exploited for the treatment of human diseases with high NADPH and GSH consumption rates, including malaria, trypanosomiasis, cancer or obesity.

Published

2016

11. Blunted apoptosis of erythrocytes in mice deficient in the heterotrimeric G-protein subunit Gαi2

Author

Sabina Honisch, Lutz Birnbaumer, Syed M. Qadri, Christine Zelenak, Guilai Liu, Adrian Lupescu, Birgit Fehrenbacher, Anja T. Umbach, Florian Lang, Hong Chen, Andreas F. Mack, Rexhep Rexhepaj, Guoxing Liu, Rosi Bissinger, Yogesh Singh, Elisabeth Lang, Martin Schaller, Mehrdad Ghashghaeinia, and Hajar Fakhri

Subjects

Erythrocyte Indices, 0301 basic medicine, G Protein, Programmed cell death, Ceramide, CIENCIAS MÉDICAS Y DE LA SALUD, Erythrocytes, genetic structures, Cell Survival, G protein, Inmunología, Eryptosis, BIOLOGIA CELULAR, Apoptosis, Phosphatidylserines, Biology, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Animals, Humans, Gi2alpha, PROTEINA, Erythocyte, Mice, Knockout, Multidisciplinary, Phosphatidylserine, purl.org/becyt/ford/3.1 [https], Molecular biology, 3. Good health, Cell biology, Medicina Básica, Cytosol, 030104 developmental biology, Erythrocyte maturation, chemistry, CELULAS DE LA SANGRE, 030220 oncology & carcinogenesis, purl.org/becyt/ford/3 [https], GTP-Binding Protein alpha Subunit, Gi2, Sphingomyelin

Abstract

Fil: Bissinger, Rosi. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Lang, Elisabeth. University of Duesseldorf. Hepatology and Infectious Diseases. Department of Gastroenterology; Alemania Fil: Ghashghaeinia, Mehrdad. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Zelenak, Christine. Charité Medical University. Department of Internal Medicine; Alemania Fil: Fehrenbacher, Birgit. University of Tuebingen. Department of Dermatology; Alemania Fil: Honisch, Sabina. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Chen, Hong. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Fakhri, Hajar. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Umbach, Anja T. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Liu, Guilai. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Rexhepaj, Rexhep. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Rexhepaj, Rexhep. University of Bonn. Institute of Biochemistry and Molecular Biology; Alemania Fil: Liu, Guoxing. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Schaller, Martin. University of Tuebingen. Department of Dermatology; Alemania Fil: Mack, Andreas F. University of Tuebingen. Institute of Anatomy; Alemania Fil: Lupescu, Adrian. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Birnbaumer, Lutz. Pontificia Universidad Católica Argentina. Facultad de Ciencias Médicas. Instituto de Investigaciones Biomédicas; Argentina Fil: Birnbaumer, Lutz. National Institute of Health. Neurobiology Laboratory; Estados Unidos Fil: Lang, Florian. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Qadri, Syed M. University of Tuebingen. Vascular Medicine and Physiology. Institute of Cardiology; Alemania Fil: Qadri, Syed M. McMaster University. Department of Pathology and Molecular Medicine; Canadá Abstract: Putative functions of the heterotrimeric G-protein subunit Gαi2-dependent signaling include ion channel regulation, cell differentiation, proliferation and apoptosis. Erythrocytes may, similar to apoptosis of nucleated cells, undergo eryptosis, characterized by cell shrinkage and cell membrane scrambling with phosphatidylserine (PS) exposure. Eryptosis may be triggered by increased cytosolic Ca(2+) activity and ceramide. In the present study, we show that Gαi2 is expressed in both murine and human erythrocytes and further examined the survival of erythrocytes drawn from Gαi2-deficient mice (Gαi2(-/-)) and corresponding wild-type mice (Gαi2(+/+)). Our data show that plasma erythropoietin levels, erythrocyte maturation markers, erythrocyte counts, hematocrit and hemoglobin concentration were similar in Gαi2(-/-) and Gαi2(+/+) mice but the mean corpuscular volume was significantly larger in Gαi2(-/-) mice. Spontaneous PS exposure of circulating Gαi2(-/-) erythrocytes was significantly lower than that of circulating Gαi2(+/+) erythrocytes. PS exposure was significantly lower in Gαi2(-/-) than in Gαi2(+/+) erythrocytes following ex vivo exposure to hyperosmotic shock, bacterial sphingomyelinase or C6 ceramide. Erythrocyte Gαi2 deficiency further attenuated hyperosmotic shock-induced increase of cytosolic Ca(2+) activity and cell shrinkage. Moreover, Gαi2(-/-) erythrocytes were more resistant to osmosensitive hemolysis as compared to Gαi2(+/+) erythrocytes. In conclusion, Gαi2 deficiency in erythrocytes confers partial protection against suicidal cell death.

Published

2016

12. Roles of the NFκB and glutathione pathways in mature human erythrocytes

Author

Mehrdad Ghashghaeinia, Mohammad Saki, Florian Lang, Ulrich Mrowietz, Thomas Wieder, H. Peter Rodemann, and Mahmoud Toulany

Subjects

Programmed cell death, Erythrocytes, Mini Review, Cell, Eryptosis, Biology, Biochemistry, Nuclear factor kappa B, Parthenolide, chemistry.chemical_compound, Bay 11-7082, Phospholipid scrambling, NF-KappaB Inhibitor alpha, medicine, Humans, Molecular Biology, Transcription factor, NF-kappa B, IκB-α, Cell Biology, Phosphatidylserine, NFKB1, Glutathione, Cell biology, medicine.anatomical_structure, IKK-α, chemistry, I-kappa B Proteins, Signal transduction, NFκB, Signal Transduction

Abstract

Anucleated erythrocytes were long considered as oxygen-transporting cells with limited regulatory functions. Components of different nuclear signaling pathways have not been investigated in those cells, yet. Surprisingly, we repeatedly found significant amounts of transcription factors in purified erythrocyte preparations, i.e. nuclear factor κB (NFκB), and major components of the canonical NFκB signaling pathway. To investigate the functional role of NFκB signaling, the effects of the preclinical compounds Bay 11-7082 and parthenolide on the survival of highly purified erythrocytes were investigated. Interestingly, both inhibitors of the NFκB pathway triggered erythrocyte programmed cell death as demonstrated by enhanced phospholipid scrambling (phosphatidylserine exposure) and cell shrinkage. Anucleated erythrocytes are an ideal cellular model allowing the study of nongenomic mechanisms contributing to suicidal cell death. As NFκB inhibitors might also interfere with the anti-oxidative defense systems of the cell, we measured the levels of reduced glutathione (GSH) after challenge with the inhibitors. Indeed, incubation of erythrocytes with Bay 11-7082 clearly decreased erythrocyte GSH levels. In conclusion, the pharmacological inhibitors of the NFκB pathway Bay 11-7082 and parthenolide interfere with the survival of erythrocytes involving mechanisms other than disruption of NFκB-dependent gene expression. Besides affecting erythrocyte survival, NFκB inhibition and induction of erythrocyte phosphatidylserine exposure may influence blood clotting. Future studies will be aimed at discriminating between NFκB-dependent and NFκB-independent GSH-mediated effects of Bay 11-7082 and parthenolide on erythrocyte death.

Published

2011

13. The NFĸB Pathway Inhibitors Bay 11-7082 and Parthenolide Induce Programmed Cell Death in Anucleated Erythrocytes

Author

Martin Röcken, Martin Schaller, Kamran Ghoreschi, Mehrdad Ghashghaeinia, Birgit Fehrenbacher, Florian Lang, H. Peter Rodemann, Thomas Wieder, Mahmoud Toulany, Rudolf A. Rupec, Mohammad Saki, and Diwakar Bobbala

Subjects

Programmed cell death, Erythrocytes, Physiology, Apoptosis, Phosphatidylserines, Biology, Cell membrane, chemistry.chemical_compound, Annexin, Nitriles, medicine, Humans, Parthenolide, Sulfones, Annexin A5, Cell Size, Aniline Compounds, Anti-Inflammatory Agents, Non-Steroidal, NF-kappa B, Glutathione, Molecular biology, I-kappa B Kinase, Cell biology, medicine.anatomical_structure, Xanthenes, chemistry, Calcium, Signal transduction, Sesquiterpenes, Protein Binding, Signal Transduction

Abstract

The preclinical compounds Bay 11-7082 and parthenolide trigger apoptosis, an effect contributing to their antiinflammatory action. The substances interfere with the activation and nuclear translocation of nuclear factor NFκB, by inhibiting NFκB directly (parthenolide) or by interfering with the inactivation of the NFκB inhibitory protein IκB-α (Bay 11-7082). Beyond that, the substances may be effective in part by nongenomic effects. Similar to apoptosis of nucleated cells, erythrocytes may undergo apoptosis-like cell death (eryptosis) characterized by cell membrane scrambling with phosphatidylserine exposure, and cell shrinkage. Thus, erythrocytes allow the study of nongenomic mechanisms contributing to suicidal cell death, e.g. Ca(2+) leakage or glutathione depletion. The present study utilized Western blotting to search for NFκB and IκB-α expression in erythrocytes, FACS analysis to determine cytosolic Ca(2+) (Fluo3 fluorescence), phosphatidylserine exposure (annexin V binding), and cell volume (forward scatter), as well as an enzymatic method to determine glutathione levels. As a result, both NFκB and IκB-α are expressed in erythrocytes. Targeting the NFκB pathway by Bay 11-7082 (IC(50) ≈ 10 μM) and parthenolide (IC(50) ≈ 30 μM) triggered suicidal erythrocyte death as shown by annexin V binding and decrease of forward scatter. Bay 11-7082 treatment further increased intracellular Ca(2+) and led to depletion of reduced glutathione. The effects of Bay 11-7082 and parthenolide on annexin V binding could be fully reversed by the antioxidant N-acetylcysteine. In conclusion, the pharmacological inhibitors of NFκB, Bay 11-7082 and parthenolide, interfere with the survival of erythrocytes involving mechanisms other than disruption of NFκB-dependent gene expression.

Published

2011

14. Targeting glutathione by dimethylfumarate protects against experimental malaria by enhancing erythrocyte cell membrane scrambling

Author

Kamran Ghoreschi, Martin Röcken, Florian Lang, Birgit Fehrenbacher, Martin Schaller, Saisudha Koka, Diwakar Bobbala, Mehrdad Ghashghaeinia, Jiirgen Brück, and Thomas Wieder

Subjects

Glutathione metabolism, Plasmodium, Erythrocytes, Physiology, Dimethyl Fumarate, Phosphatidylserines, Biology, medicine.disease_cause, Antioxidants, Cell membrane, Mice, chemistry.chemical_compound, Fumarates, parasitic diseases, medicine, Animals, Humans, Cell survival, Dimethyl fumarate, Erythrocyte Membrane, Cell Biology, Phosphatidylserine, Glutathione, medicine.disease, Malaria, Cell biology, medicine.anatomical_structure, chemistry, Biochemistry, Immunosuppressive Agents, Oxidative stress

Abstract

The balance between GSH-levels and oxidative stress is critical for cell survival. The GSH-levels of erythrocytes are dramatically decreased during infection with Plasmodium spp. We therefore investigated the consequences of targeting GSH for erythrocyte and Plasmodium survival in vitro and in vivo using dimethylfumarate (DMF) at therapeutically established dosage. We first show that noninfected red blood cells (RBC) exposed to DMF undergo changes typical of apoptosis or eryptosis, such as cell shrinkage and cell membrane scrambling with subsequent phosphatidylserine (PS) exposure. DMF did not induce appreciable hemolysis. DMF-triggered PS exposure was mediated by intracellular GSH depletion and reversed by the antioxidative N-acetyl-l-cysteine. DMF treatment controlled intraerythrocyte DNA amplification and in vitro parasitemia of Plasmodium falciparum -infected RBC. In vivo, DMF treatment had no effect on RBC count or GSH levels in noninfected mice. Consistent with its effects on infected RBC, DMF treatment abrogated parasitemia and enhanced the survival of mice infected with Plasmodium berghei from 0% to 60%. In conclusion, DMF sensitizes the erythrocytes to the effect of Plasmodium infection on PS exposure, thus accelerating the clearance of infected erythrocytes. Accordingly, DMF treatment favorably influences the clinical course of malaria. As DMF targets mechanisms within the host cell, it is not likely to generate resistance of the pathogen.

Published

2010

15. Inhibition of suicidal erythrocyte death by nitric oxide

Author

Jan P. Nicolay, Judith Haendeler, Mehrdad Ghashghaeinia, Olivier M. Niemoeller, Florian Lang, Gerd Liebig, Thomas Wieder, Rudi Busse, and Saisudha Koka

Subjects

Nitroprusside, medicine.medical_specialty, Programmed cell death, Erythrocytes, Annexins, Physiology, Clinical Biochemistry, Succinimides, Apoptosis, Phosphatidylserines, Biology, Ceramides, Nitric Oxide, Calcium in biology, Nitric oxide, Mice, chemistry.chemical_compound, Annexin, Physiology (medical), Internal medicine, medicine, Animals, Humans, Cyclic GMP, Fluorescent Dyes, Mice, Knockout, Ionophores, Protein nitrosylation, Ionomycin, Erythrocyte Membrane, Fluoresceins, Cell biology, Endocrinology, chemistry, Calcium, cGMP-dependent protein kinase

Abstract

Nitric oxide (NO) is known to counteract apoptosis by S-nitrosylation of protein thiol groups. NO is generated and stored in erythrocytes, which may undergo eryptosis, a suicidal cell death similar to apoptosis of nucleated cells. Eryptosis is triggered by increased cytosolic Ca2+ activity and/or ceramide and characterized by cell shrinkage and phosphatidylserine exposure at the cell surface. The present study explored whether nitric oxide could interfere with the machinery underlying eryptosis. To this end, erythrocyte phosphatidylserine exposure (annexin V-binding) and cell volume (forward scatter) were determined by flow cytometry. The Ca2+ ionophore ionomycin (0.1 microM) increased cytosolic Ca2+ activity, triggered annexin binding, and decreased forward scatter. The annexin binding and decrease of forward scatter but not the increase of cytosolic Ca2+ activity were reversed by the NO-donor nitroprusside (1 microM) and papanonoate (100 microM). Higher concentrations of nitroprusside (0.1 and 1 mM) stimulated eryptosis. Glucose depletion, exposure to C6-ceramide (3 microM), hypertonic (addition of 550 mM sucrose), and isotonic (replacement of Cl- with gluconate) cell shrinkage all triggered annexin V binding, effects all reversed by nitroprusside (1 microM). Dibutyryl-cGMP (1 mM) blunted the ionomycin- but not the ceramide-induced annexin V binding. Ionomycin decreased protein nitrosylation and thioredoxin activity, effects reversed by the NO-donor papanonoate. Clearance of erythrocytes from circulating blood was significantly faster in eNOS knockout mice than in their wild-type littermates. In conclusion, nitric oxide participates in the regulation of erythrocyte survival, an effect partially mimicked by cGMP and paralleled by alterations of protein nitrosylation and thioredoxin activity.

Published

2007

16. Accelerated apoptotic death and in vivo turnover of erythrocytes in mice lacking functional mitogen- and stress-activated kinase MSK1/2

Author

Shuchen Gu, J. Simon C. Arthur, Michael Föller, Teresa F. Ackermann, Madhuri S. Salker, Syed M. Qadri, Kathleen M. S. E. Reyskens, Kashif Jilani, Christine Zelenak, Rosi Bissinger, Yogesh Singh, Elisabeth Lang, Florian Lang, Adrian Lupescu, Erwin Schleicher, Abul Fajol, William P. Sheffield, and Mehrdad Ghashghaeinia

Subjects

Erythrocyte Indices, Male, Erythrocytes, Primary Cell Culture, Gene Expression, Apoptosis, Phosphatidylserines, Biology, Hematocrit, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, Hemolysis, Ribosomal Protein S6 Kinases, 90-kDa, Article, Hemoglobins, Mice, chemistry.chemical_compound, Reticulocyte Count, Osmotic Pressure, In vivo, Extracellular, medicine, Animals, Humans, Mice, Knockout, Multidisciplinary, Osmotic concentration, medicine.diagnostic_test, Erythrocyte fragility, Phosphatidylserine, Molecular biology, Cell biology, body regions, Osmotic Fragility, chemistry, Female, Ex vivo

Abstract

The mitogen- and stress-activated kinase MSK1/2 plays a decisive role in apoptosis. In analogy to apoptosis of nucleated cells, suicidal erythrocyte death called eryptosis is characterized by cell shrinkage and cell membrane scrambling leading to phosphatidylserine (PS) externalization. Here, we explored whether MSK1/2 participates in the regulation of eryptosis. To this end, erythrocytes were isolated from mice lacking functional MSK1/2 (msk−/−) and corresponding wild-type mice (msk+/+). Blood count, hematocrit, hemoglobin concentration and mean erythrocyte volume were similar in both msk−/− and msk+/+ mice, but reticulocyte count was significantly increased in msk−/− mice. Cell membrane PS exposure was similar in untreated msk−/− and msk+/+ erythrocytes, but was enhanced by pathophysiological cell stressors ex vivo such as hyperosmotic shock or energy depletion to significantly higher levels in msk−/− erythrocytes than in msk+/+ erythrocytes. Cell shrinkage following hyperosmotic shock and energy depletion, as well as hemolysis following decrease of extracellular osmolarity was more pronounced in msk−/− erythrocytes. The in vivo clearance of autologously-infused CFSE-labeled erythrocytes from circulating blood was faster in msk−/− mice. The spleens from msk−/− mice contained a significantly greater number of PS-exposing erythrocytes than spleens from msk+/+ mice. The present observations point to accelerated eryptosis and subsequent clearance of erythrocytes leading to enhanced erythrocyte turnover in MSK1/2-deficient mice.

Published

2015

17. Age sensitivity of NFkappaB abundance and programmed cell death in erythrocytes induced by NFkappaB inhibitors

Author

Martin Köberle, Mehrdad Ghashghaeinia, Peter Dreischer, Tilo Biedermann, Florian Lang, Giel J. C. G. M. Bosman, Michael Duszenko, Judith C. A. Cluitmans, Thomas Wieder, Mohammad Saki, Elisabeth Lang, and Mahmoud Toulany

Subjects

Chemical and physical biology [NCMLS 7], Aging, Programmed cell death, Erythrocytes, Time Factors, Physiology, Cell, Apoptosis, Stimulation, Biology, chemistry.chemical_compound, Phospholipid scrambling, Annexin, Immune Regulation [NCMLS 2], Nitriles, medicine, Humans, Parthenolide, Sulfones, Cells, Cultured, NF-kappa B, Phosphatidylserine, Molecular biology, Blot, medicine.anatomical_structure, Biochemistry, chemistry, Sesquiterpenes

Abstract

Contains fulltext : 125210.pdf (Publisher’s version ) (Open Access) BACKGROUND/AIMS: Erythrocytes may enter eryptosis, a suicidal death characterized by cell shrinkage and phosphatidylserine exposure at the erythrocyte outer membrane. Susceptibility to eryptosis is enhanced in aged erythrocytes and stimulated by NFkappaB-inhibitors Bay 11-7082 and parthenolide. Here we explored whether expression of NFkappaB and susceptibility to inhibitor-induced eryptosis is sensitive to erythrocyte age. METHODS: Human erythrocytes were separated into five fractions, based on age-associated characteristics cell density and volume. NFkappaB compared to ss-actin protein abundance was estimated by Western blotting and cell volume from forward scatter. Phosphatidylserine exposure was identified using annexin-V binding. RESULTS: NFkappaB was most abundant in young erythrocytes but virtually absent in aged erythrocytes. A 24h or 48h exposure to Ringer resulted in spontaneous decrease of forward scatter and increase of annexin V binding, effects more pronounced in aged than in young erythrocytes. Both, Bay 11-7082 (20 microM) and parthenolide (100 microM) triggered eryptosis, effects again most pronounced in aged erythrocytes. CONCLUSION: NFkappaB protein abundance is lowest and spontaneous eryptosis as well as susceptibility to Bay 11-7082 and parthenolide highest in aged erythrocytes. Thus, inhibition of NFkappaB signalling alone is not responsible for the stimulation of eryptosis by parthenolide or Bay 11-7082.

Published

2013

18. Retraction Statement. Paper by Li J, Yu J, Zhang H, Wang B, GuoH, Bai J, Wang J, Dong Y, Zhao Y., Wang Y., entitled ‘Exosomes-Derived MiR-302b Suppresses Lung Cancer Cell Proliferation and Migration via TGFβRII Inhibition‘ Cell Physiol Biochem 2016;38(5):1715-1726. doi:10.1159/000443111

Author

Ping Lin, Na Cui, Chao-Peng Li, Huanhai Liu, Emi Kurosawa, Yaping Xu, Di Wu, Yin Cheng, Xiaohui Xu, Qingwei Wen, Fandong Meng, Baoxi Zhang, Richard D. Magie, Yueqing Jiang, Luo Xu, Bo Zhai, Sarah J. Matches, Xiaolong Kong, Kazuhisa Ouhara, Peng Zhou, Xiaorong Hu, Huixia Wang, Tao Jiang, Shenyi Jiang, Lijun Hao, Xiu-Ming Liu, Chao Liu, Masahiro Tanaka, Salome Asanidze, Jianbo Wu, Xin Tian, Zohreh Hosseinzadeh, Jens Zierle, Lei Cai, Aimin Yang, Rui Liu, Fangxing Ye, Junhui He, Bu-Chun Zhang, Lars Kaestner, Jianxin Ye, Sara Y. Brucker, Qinyi Liu, Xuefei Wang, Lei Yang, Hidemi Kurihara, Yoshiko Onozawa, Yuki Hirota-Takahata, Futian Ma, W. Paul Bowman, Chaonan Li, Guimin Hao, Zhansong Zhou, Ying Li, Renbin Huang, Yu Ding, Thithaihoa Pham, Ting Deng, Wenhao Shen, Tong-Da Xu, Yi Xiong, Nusrath Habiba, Feifei Xuan, Qiong Deng, Peng He, Yuandong Zhu, Huan Du, Xiaodong Li, Jian Jiang, Yaozong Yuan, Yong Shang, Zhuojun Zheng, Yingzhi Liu, Xiaobao Xie, Xue Cao, Dawei Ge, Hongyi Liu, Liyu Chen, Florian Lang, Nagla Mohamed, Jun Que, Katsuhiro Takeda, Lei Jiang, Yogesh Singh, Susan Franks, De-Feng Pan, Zoe Webster, Fabrizio Carta, Gerolf Gros, Zhiwen Chen, Pengyuan Zheng, Boya Zhang, Miranda Menniti, Zuolei Chen, Jan Hegermann, Juntian Lang, Lianjiang Zhang, Yifan Li, Qiang Huang, Yurong Tan, Jun Wen, Wei Zheng, Jie Xu, Jan J. Brosens, Shugang Yang, Zhaoyu Zhong, Lucia D'Antona, Shuang Ding, Jinzhou Wang, Hongli Jiang, Jiayuan Kou, Xu Wang, Xinyu Xu, Haibin Liu, Baohua Cheng, Haibo Wang, Qiuqiao Xie, Meitong Liu, Francesco Ortuso, Xuesong Li, Yehua Wang, Yongjian Huang, Dong-Ye Li, Xuewei Zhang, Dongmei Yu, Jing Sun, Jennifer H. Steel, Jun Chiba, Riyaz Basha, Qianqian Sun, Judy Mutua, Yonglong Zhang, Hongming Guo, Tetsuya Yoshimoto, Shiguo Liu, Jichun Wang, Zhong Yin, Benjamin Hanf, Xueqi Li, Donat R. Spahn, Qiuying Li, Zhongkai Liu, Liye Fu, Changhong Li, Mariela Arias-Hidalgo, Jian Yuan, Jiabao Zhang, Hideki Kobayashi, Yujie Chen, Claudiu T. Supuran, Xiaoli Wu, Duc Bach Nguyen, Chengyu Wang, Aiqin Li, Shundong Dai, Mikihito Kajiya, Mehrdad Ghashghaeinia, Etheresia Pretorius, Stefano Alcaro, Ni Qin, Wei Wang, Yueming Xu, Shijun Zhang, Vincenzo Dattilo, Hu Peng, Cheng Liu, Ruisong Ma, Chunfeng Yi, Xiaojun Tang, Xianfeng Yu, Rosario Amato, Cong-Wei Zhang, Xuefei Li, Yi Ba, Lingfang Li, Junxuan Chang, Chunxia Chen, Lei Chen, Ji Zheng, Hongyuan Xia, Shane Fernando, Bao-ping Yu, Madhuri S. Salker, Yong Liu, Jingping Fan, Guojun Wu, Yating Tang, Bao Nguyen, Weipan Xu, Cheng Wang, Jianchun Liao, Sai Luo, Liming Yang, Yanfeng Liu, Cataldo Bianco, Chenyu Zhang, Yan Gao, Akihiro Tamura, Qi Fan, Wansu Huang, Mauro C. Wesseling, Yan Yang, Xiao Li, Kimberly G. Fulda, Hao Jiang, Yang Wang, Jie Zhang, Juman Li, Shu-Guang Song, Huiyu Liu, Jeanette N. du Plooy, Ban Liu, Zhijun Sun, Le Tao, Silvia Schenone, Deep Shah, Bo Fu, Volker Endeward, Wei Zhang, Xiaojian Cao, Huijie Gao, Hong Jiang, Ingolf Bernhardt, Yi Lu, Xiaozhou Zhou, Georgios Tsiavaliaris, Dan Li, Yingbin Ge, Youhong Jiang, Ning Chen, Bing Wang, Weiyan Yao, Janette Bester, Lisa Wagner-Britz, Chunfeng He, Guangwei Zhu, Jinfu Zhuang, Deyong Zhao, Shinji Matsuda, Cristina Talarico, Zhen-peng Huang, Dongying Xue, Gensheng Lu, Nicola Perrotti, Tsuyoshi Fujita, Jinhong Pan, Chengguang Sui, Yan Li, Jia Su, Toru Hasegawa, Xiaojie Wei, Rosi Bissinger, Zhennan Zhao, Xiaoqing Zhao, Hu Qiu, Haichen Chu, Lingling Wu, Jianchun Huang, Jin Hua, Shuiping Liu, Longbin Zheng, Weiying Gu, Xiangmei Chen, Jaya Nautiyal, Jingting Jiang, Wenting Ma, Xuefeng Sun, Chunni Zhang, Yoko Ishimoto, Yi Zhi, Guoqiang Zhao, Xuefeng Feng, Ye Tian, Ruirui Han, Jian Tang, Yang Lu, Ziyu Dai, Tao Sui, Yuko Iwadate, Haruka Imai, Wen-Qi Wang, Zhongni Liu, Jin Yang, Lili Wang, and Na Liu

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Lung cancer cell, Physiology, Chemistry, 030220 oncology & carcinogenesis, Cell, medicine, Molecular biology, Microvesicles

Published

2016