42 research outputs found

    Book review: India and the Islamic heartlands: an Eighteenth-Century world of circulation and exchange by Gagan D.S. Sood

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    Drawing on the chance discovery of a number of letters exchanged during the period, in India and the Islamic Heartlands: An Eighteenth-Century World of Circulation and Exchange author Gagan D.S. Sood attempts to capture the lives of ordinary people to reconstruct the connective tissues of a world lived beyond the purview of the sovereign. While the nature of the source material occasionally limits the book’s scope of analysis, this work successfully weaves together an insightful narrative to draw attention to a neglected arena and period, finds Mithilesh Kumar Jha

    Book review: Benign violence: education in and beyond the age of reason by Ansgar Allen

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    In Benign Violence: Education In and Beyond the Age of Reason, Ansgar Allen challenges the view that education is, at its core, an incontestable social good by outlining how its structures are underpinned by systemic violence. While Allen’s argument may not entirely sway readers away from the overarchingly positive value typically attributed to education, it nonetheless asks serious questions about the role that the education system and examinations have played in shaping us and our world, writes Mithilesh Kumar Jha

    Book review: performing politics: media interviews, debates and press conferences by Geoffrey Craig

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    In Performing Politics: Media Interviews, Debates and Press Conferences, Geoffrey Craig examines media interactions between politicians and journalists as power struggles that have come to be seen as crucial in indicating the potential success and competence of political leaders. While the book understands politics through largely conventional terms that bypass the emergence of newer political movements, it nonetheless serves to promote greater literacy and understanding of contemporary political communication and the battlegrounds therein, writes Mithilesh Kumar Jha

    Formulation of SrO-MBCUS Agglomerates for Esterification and Transesterification of High FFA Vegetable Oil

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    Musa Balbisiana Colla Underground Stem (MBCUS) catalyst was treated thermally mixing with 5:1 w/w of Strontium Oxide (SrO) and the dynamic sites were reformed. The MBCUS-SrO showed sharper crystalline phases as evidence from XRD and TEM analysis. The composition and morphology were characterized from BET, SEM, EDX thermo-gravimetric analysis (TGA) and XRF analysis. The optimization process for biodiesel production from Jatropha curcas L oil (JCO) having high percentage of free fatty acids was carried out using orthogonal arrays adopting the Taguchi method. The linear equation was obtained from the analysis and subsequent biodiesel production (96% FAME) was taken away from the JCO under optimal reaction conditions. The biodiesel so prepared had identical characteristics to that with MBCUS alone, but at a lower temperature (200ËšC) and internal vapour pressure. Metal leaching was much lower while reusability of the catalyst was enhanced. It was also confirmed that the particle size has little impact upon the conversion efficacy, but the basic active sites are more important.

    Pyruvate Dehydrogenase Kinase-mediated Glycolytic Metabolic Shift in the Dorsal Root Ganglion Drives Painful Diabetic Neuropathy

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    The dorsal root ganglion (DRG) is a highly vulnerable site in diabetic neuropathy. Under diabetic conditions, the DRG is subjected to tissue ischemia or lower ambient oxygen tension that leads to aberrant metabolic functions. Metabolic dysfunctions have been documented to play a crucial role in the pathogenesis of diverse pain hypersensitivities. However, the contribution of diabetes-induced metabolic dysfunctions in the DRG to the pathogenesis of painful diabetic neuropathy remains ill-explored. In this study, we report that pyruvate dehydrogenase kinases (PDK2 and PDK4), key regulatory enzymes in glucose metabolism, mediate glycolytic metabolic shift in the DRG leading to painful diabetic neuropathy. Streptozotocin-induced diabetes substantially enhanced the expression and activity of the PDKs in the DRG, and the genetic ablation of Pdk2 and Pdk4 attenuated the hyperglycemia-induced pain hypersensitivity. Mechanistically, Pdk2/4 deficiency inhibited the diabetes-induced lactate surge, expression of pain-related ion channels, activation of satellite glial cells, and infiltration of macrophages in the DRG, in addition to reducing central sensitization and neuroinflammation hallmarks in the spinal cord, which probably accounts for the attenuated pain hypersensitivity. Pdk2/4-deficient mice were partly resistant to the diabetes-induced loss of peripheral nerve structure and function. Furthermore, in the experiments using DRG neuron cultures, lactic acid treatment enhanced the expression of the ion channels and compromised cell viability. Finally, the pharmacological inhibition of DRG PDKs or lactic acid production substantially attenuated diabetes-induced pain hypersensitivity. Taken together, PDK2/4 induction and the subsequent lactate surge induce the metabolic shift in the diabetic DRG, thereby contributing to the pathogenesis of painful diabetic neuropathy

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    Die durch Agentien wie IL-1α, Prostaglandine oder Forskolin induzierte Erhöhung von intrazellulärem zyklischem Adenosin-Monophosphat (cAMP) in T-Lymphozyten inhibiert die Synthese Th1-typischer Zytokine und stimuliert die Synthese Th2-typischer Zytokine. Die fĂĽr die cAMP-vermittelte Induktion von Th2-Zytokinen verantwortlichen Signaltransduktionskaskaden sind bisher nur unvollständig aufgeklärt. Deshalb konzentrierte sich meine Dissertation auf die Erforschung des cAMP-Signalweges in primären T-Helferzellen. Während die Induktion muriner EL-4 T-Zellen mit Forskolin sowohl zur Aktivierung Th2-typischer als auch zur Inhibierung Th1-typischer Lymphokine fĂĽhrt, kann die ektopische Expression einer katalytisch aktiven Proteinkinase A (PKA) zwar die Synthese von Th2-typischen Lymphokinen stimulieren, nicht jeder die Expression Th1-typischer Lymphokine inhibieren. Dies bedeutet, dass die Aktivierung von PKA selektiv an der Stimulation der Th2-Lymphokinexpression beteiligt ist, während andere, cAMP-abhängige Signaltransduktionswege zur Inhibierung Th1-typischer Lymphokine fĂĽhren. Durch vergleichende Analysen verschiedener Th-Zellen konnte im Rahmen dieser Arbeit gezeigt werden, dass durch aktive PKA in Th0- und Th2, nicht jeder in Th1-Zellen die Expression von IL-5 erhöht wird. Dieses Phänomen ist wahrscheinlich auf die unterschiedliche Konzentration des Transkriptionsfaktors GATA-3 zurĂĽckzufĂĽhren. So kommt GATA-3 in Th2-Zellen in hoher, in Th0-Zellen in geringerer und in Th1-Zellen in sehr geringer Konzentration vor. Die ektopische Expression von GATA-3 in Th1-Zellen induziert die Synthese Th2- typischer Lymphokine, die durch erhöhte cAMP-Konzentration oder durch aktive PKA noch verstärkt werden kann. Untersuchungen bezĂĽglich des Einflusses erhöhter cAMP-Spiegel auf Th2- Lymphokine in der Th2-Zelllinie D10 zeigten, dass erhöhte cAMP-Konzentrationen nicht die PKA-Aktivität, sondern vielmehr die Aktivität der p38-Kinase stimuliert. Diese Aktivierung fĂĽhrt zur Phosphorylierung von GATA-3 und dadurch zur Induktion der IL-5- und IL-13-Expression (Chen et al., 2000). In primären T-Helferzellen, die im Mittelpunkt der hier vorgelegten Arbeit standen, konnte beobachtet werden, dass bereits die Expression der katalytischen Untereinheit α der PKA ausreichend fĂĽr eine optimale IL-5-Expression in Th0-Zellen ist. Die Beobachtung, dass primäre Th2-Zellen sowohl auf die Behandlung mit dem spezifischen PKA-Inhibitor H-89 als auch auf die ektopische Expression der negativ wirkenden Untereinheit 1 der PKA mit signifikant verminderter IL-5-Produktion reagierten, unterstreicht die wichtige Rolle aktiver PKA bei der Regulation des IL-5 Gens. Zusammenfassend konnte in dieser Arbeit durch die Untersuchung verschiedener primärer CD4+ T-Lymphozyten, einschlieĂźlich der auch in vivo IL-5 produzierenden Th2-Zellen, gezeigt werden, dass der Adenylzyklase/cAMP/PKASignaltransduktionsweg bedeutend fĂĽr die IL-5 Genexpression in primären Th2-Zellen und somit auch wichtig fĂĽr deren Effektorfunktion ist.Elevation of intracellular cAMP in T lymphocytes, induced by agents such as IL-1α, prostaglandins or forskolin, inhibits Th1-type cytokine production but stimulates Th2-type cytokine production. The signaling pathway engaged in cAMP-mediated induction of Th2 lymphokines remains obscure and therefore my doctoral work was focused on the elucidation of cAMP pathway in primary Th lymphocytes. While forskolin treatment of EL-4 cells led both to an activation of Th2 lymphokines and inhibition of Th1 lymphokines, ectopic expression of catalytically active PKA stimulated Th2 lymphokines but failed to inhibit Th1 lymphokine expression. Thus, the PKA activity is selectively involved in the stimulation of Th2 lymphokine expression whereas other cAMP-dependent pathway(s) appears to downregulate Th1 lymphokines. By investigating different types of primary murine Th cells, it was found that active PKA enhanced IL-5 expression only in Th0 and Th2 but not in Th1 cells. This is likely due to the different levels of GATA-3 whose expression is high in Th2, moderate in Th0 and very low in Th1 cells. Ectopic expression of GATA-3 in Th1 cells induced Th2 lymphokine expression which could be further enhanced by increased cAMP levels or PKA activity. Investigations on the role of increased cAMP levels on Th2 lymphokines in D10 cells, a Th2-type cell line, led to the conclusion that elevated cAMP concentrations do not stimulate PKA but p38 activity which, through phosphorylation of GATA-3, appeared to induce IL-5 and IL-13 expression (Chen et al., 2000). While focusing on primary Th lymphocytes, it was observed that expression of the catalytic subunit α of PKA is sufficient for optimal IL-5 expression in primary Th0 cells. In addition, downregulation of IL-5 production in primary Th2 cells by the treatment with low concentrations of H-89, a PKA specific inhibitor, as well as by the ectopic expression of a negatively acting version of regulatory PKA subunit I demonstrates that active PKA plays an important role in IL-5 gene regulation. These findings using different types of primary CD4+ T lymphocytes, including Th2 cells, the one likely to represent the native IL-5 producers in vivo, demonstrates that the adenylyl cyclase/cAMP/PKA signaling pathway plays an important role in IL-5 gene expression in primary Th2 cells. Thus the importance of cAMP/PKA signaling pathway in Th2 effector function was established during this doctoral research work

    Some constructions of balanced ternary residual treatment effects designs

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    In balanced ternary residual treatment effects designs, a treatment occurs in a given sequence at most twice but the same treatment does not appear in two consecutive periods. This paper gives some methods of construction of new families of balanced ternary residual treatment effects designs. © 2010 Taylor & Francis Group, LLC. All rights reserved

    Constructions of residual treatment effects designs for comparing test treatments with a control

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    This article deals with residual treatment effects designs for the purpose of comparing v test treatments with a control treatment when the number of periods is no larger than v + 1. Control balanced residual treatment effects designs, which are Schur-optimal, are considered. Some methods of their construction are given
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