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Data contain source data for Figure 5c from Schilling et al., 2009. Cell fate decisions are regulated by the coordinated activation of signalling pathways such as the extracellular signal-regulated kinase (ERK) cascade, but contributions of individual kinase isoforms are mostly unknown. The authors combined quantitative data from erythropoietin-induced pathway activation in primary erythroid progenitor (colony-forming unit erythroid stage, CFU-E) cells with mathematical modelling, in order to predict and experimentally confirmed a distributive ERK phosphorylation mechanism in CFU-E cells. The authors found evidences that double-phosphorylated ERK1 attenuates proliferation beyond a certain activation level, whereas activated ERK2 enhances proliferation with saturation kinetics. Retrovirally transduced CFU-E cells were incubated with increasing Epo concentrations for 14 h and proliferation was measured by [3H]-thymidine incorporation.

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Twenty-five samples from selected cored intervals of problematic Triassic-Jurassic age from Sites 545, 546, and Hole 547B have been analyzed palynologically to aid age determination. Section 545-73-1 yielded a marine palynoflora of Sinemurian-Bajocian age. A palynoflora of nonmarine origin and assigned a Rhaetian-Hettangian age was recovered from halite in Section 546-18-2. Marine palynofloras of Hettangian-early Pliensbachian age were recovered from Sample 547B-24-CC to Section 547B-14-2. Sections 547B-28-1 to 547B-25-3 yielded impoverished nonmarine palynofloras to which only a general Rhaetian-Hettangian age could be given.