Compartmental Analysis Suggests Macropinocytosis at the Onset of Diatom Valve Formation

During valve formation of the siliceous frustules of diatoms, bulk uptake of silicic acid and its subsequent transport through the cell is required before it can be deposited in the silica deposition vesicle (SDV). It has been assumed that transport takes place via silicon transporters (SITs), but if that were the case a control mechanism would have to exist for stabilization of the large amounts of reactive silicon species during their passage through the cell on the way to the SDV. There is, however, no reason to assume that classical silica chemistry does not apply at elevated levels of silicic acid, and therefore autopolymerization could reasonably be expected to occur. In order to find alternative ways of Si transport that correspond with the high speed of valve formation at the earliest stages of cell division we followed 31Si(OH)4 uptake in synchronously dividing cells of the diatoms Coscinodiscus wailesii, Navicula pelliculosa, N. salinarum, and Pleurosira laevis. The results were related to systematically derived mathematical models for a compartmental analysis of 5 possible uptake/transport pathways, including one involving SITs and one involving (macro)pinocytosis-mediated uptake from the extracellular environment. Our study indicates that the uptake of radioactive silicic acid matches best with the model that describes macropinocytosis-mediated silicon uptake. This process is well in line with the observed ‘surge uptake’ at the start of valve formation when the demand for silicon is high; it infers that in diatoms a pathway of uptake and transport exists in which SITs are not involved.Radiation, Radionuclides and ReactorsApplied Science

The role of GABAA receptors in the acute and chronic effects of ethanol: a decade of progress

The past decade has brought many advances in our understanding of GABA(A) receptor-mediated ethanol action in the central nervous system. We now know that specific GABA(A) receptor subtypes are sensitive to ethanol at doses attained during social drinking while other subtypes respond to ethanol at doses attained by severe intoxication. Furthermore, ethanol increases GABAergic neurotransmission through indirect effects, including the elevation of endogenous GABAergic neuroactive steroids, presynaptic release of GABA, and dephosphorylation of GABA(A) receptors promoting increases in GABA sensitivity. Ethanol’s effects on intracellular signaling also influence GABAergic transmission in multiple ways that vary across brain regions and cell types. The effects of chronic ethanol administration are influenced by adaptations in GABA(A) receptor function, expression, trafficking, and subcellular localization that contribute to ethanol tolerance, dependence, and withdrawal hyperexcitability. Adolescents exhibit altered sensitivity to ethanol actions, the tendency for higher drinking and longer lasting GABAergic adaptations to chronic ethanol administration. The elucidation of the mechanisms that underlie adaptations to ethanol exposure are leading to a better understanding of the regulation of inhibitory transmission and new targets for therapies to support recovery from ethanol withdrawal and alcoholism