5 research outputs found

    In vitro maintaining of CD4+ central and effector memory cells in normal and inflammatory conditions

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    IL-7 is a key factor for the survival and maintenance of CD4+ central (Tcm) and effector (Tem) memory cells in the whole body. In many autoimmune diseases, an elevated level of IL-7 is detected in blood serum and at the site of inflammation, thus suggesting participation of this homeostatic factor in the survival of memory T cells, including auto-reactive clones, in inflammatory disorders. The aim of the study was to investigate the mechanisms of maintaining CD4+ memory T cells under normal and inflammatory conditions. We developed an in vitro model of inflammation, based on induction of pro-inflammatory cytokines, and then evaluated the effects of IL-7 upon purified sorted populations of CD4+Tcm and Tem under normal conditions and in vitro inflammatory model. IL-7 treatment promoted maintenance of CD4+Tcm phenotype in all variants of cultures. In the absence of contact with adherent cell fraction, the IL-7-induced proliferation of Tcm and Tem was slightly reduced, both under normal and inflammatory conditions, thus suggesting low sensitivity of memory T cells to contacts with MHC, and, probably, a requirement for additional signals to provide complete stimulation with IL-7. The last suggestion is also supported by data about CD127 and CD132 expression, i.e., in the absence of contact with MHC, the proportion of CD127+CD132+ cells was decreased in both subpopulations of CD4+ memory cells. Upon in vitro cultures, IL-7 contributed to decreased expression of CD127, and increased expression of CD132 on CD4+Tcm and Tem. We have evaluated the CD4+Tcm and Tem populations by affinity of T cell receptor (TCR), using the level of CD5 expression. Т cells with high TCR affinity for self-antigens are known to have higher expression of CD5. In comparison to Tem, the Tcm contained more CD5high cells. In cultures, IL-7 promoted a high level of CD5 expression on Tcm, which was comparable to levels observed in peripheral blood cells. High CD5 expression on Tem was observed after stimulation with IL-7 in the in vitro inflammatory model. In the absence of contact with MHC, the number of CD5high cells decreased among CD4+Tem and Tcm. Thus, CD4+Tcm cells with high affinity for autologous antigens are probably dependent on the presence of homeostatic factors, in particular, IL-7, and contacts with antigen-presenting cells (APCs). Under conditions of inflammation, no changes were revealed in the mechanism of maintaining CD4+Tcm, in contrast to CD4+Tem. Being less dependent on IL-7 under normal conditions, CD4+CD5highTem are accumulated in the presence of IL-7 under in vitro inflammatory conditions

    Substantiation of optical criterions of thermal-oxidative stability of lubricating

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    Research results of criteria of thermal-oxidative stability determined by different combinations of coefficient of absorption of light quantity and optical density with coefficient of evaporation and kinematic viscosity of oxygenated oil are presented. It is shown that the amount of optical density and the coefficient of evaporation divided by coefficient of relative viscosity are the most effective criteria of thermal-oxidative stability of lubricating oils described by second order polynomial with a high correlation coefficient. © Published under licence by IOP Publishing Ltd

    Substantiation of optical criterions of thermal-oxidative stability of lubricating oil

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    Research results of criteria of thermal-oxidative stability determined by different combinations of coefficient of absorption of light quantity and optical density with coefficient of evaporation and kinematic viscosity of oxygenated oil are presented. It is shown that the amount of optical density and the coefficient of evaporation divided by coefficient of relative viscosity are the most effective criteria of thermal-oxidative stability of lubricating oils de- scribed by second order polynomial with a high correlation coefficient
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