ABSTRACT
Neural stem cell (NSC) maintenance and functions are regulated by reactive oxygen species (ROS). However, the mechanisms by which ROS control NSC behavior remain unclear. Here we report that ROS-dependent Igfbp2 signaling controls DNA repair pathways which balance NSC self-renewal and lineage commitment. Ncf1 or Igfbp2 deficiency constrains NSCs to a self-renewing state and prevents neurosphere formation. Ncf1-dependent oxidation of Igfbp2 promotes neurogenesis by NSCs in vitro and in vivo while repressing Brca1 DNA damage response genes and inducing DNA double-strand breaks (DDSBs). By contrast, Ncf1-/- and Igfbp2-/- NSCs favor the formation of oligodendrocytes in vitro and in vivo. Notably, transient repression of Brca1 DNA repair pathway genes induces DDSBs and is sufficient to rescue the ability of Ncf1-/- and Igfbp2-/- NSCs to lineage-commit to form neurospheres and neurons. NSC lineage commitment is dependent on the oxidizable cysteine-43 residue of Igfbp2. Our study highlights the role of DNA damage/repair in orchestrating NSC fate decisions downstream of redox-regulated Igfbp2.
Subject(s)
Neural Stem Cells , Cell Differentiation/genetics , Reactive Oxygen Species/metabolism , Neural Stem Cells/metabolism , Neurogenesis/genetics , Oxidation-Reduction , DNA Damage , Cell ProliferationABSTRACT
Rates of phosphate adsorption to PT-A (a new type of aluminium oxide hydroxide) and ALG (aluminum hydroxide gel) from a pH 3 phosphate solution were measured by a batch method. Phosphate uptake progressed mainly by the adsorption mechanism for PT-A, but dissolution of aluminum and precipitation of aluminum phosphate took place in addition to phosphate adsorption for ALG. The intraparticle diffusivities (Dp'S) of phosphate were evaluated from the time courses of adsorption using the model of pore diffusion with a Freundlich-type adsorption isotherm. The Dp values were approximately 7 x 10(-7) cm2 S-1 for PT-A and 1 x 10(-6) cm2 s(-1) for ALG. The tortuosity factors calculated from a model of parallel plate pore were 5.1 for PT-A and 6.7 for ALG; these values resembled those for porous inorganic ion exchangers. The adsorption rates are high enough for each of the samples to be utilized as a phosphate adsorbent to prevent hyperphosphatemia in patients on chronic dialysis. PT-A is favored as a phosphate adsorbent because of its high chemical stability against acid.
Subject(s)
Aluminum Hydroxide/chemistry , Aluminum Oxide/chemistry , Phosphates/chemistry , Adsorption , Diffusion , Kinetics , Microscopy, Electron, Scanning , X-Ray DiffractionABSTRACT
Hypelcin B is a mixture of antibiotic peptides produced by Hypocrea peltata. Hypelcins B-I, B-II, B-III, B-IV and B-V are components of this mixture purified by reversed-phase high-performance liquid chromatography. The amino acid sequences of these peptides were determined by electrospray mass spectrometry and electrospray mass spectrometry/mass spectrometry. The molecular weights of these peptides were all ca. 2000 and the structures were very similar.
Subject(s)
Alamethicin/analogs & derivatives , Hypocreales/metabolism , Alamethicin/chemistry , Alamethicin/isolation & purification , Amino Acid Sequence , Chromatography, High Pressure Liquid , Esters/chemistry , Mass Spectrometry , Molecular Sequence Data , Molecular WeightABSTRACT
The effects of the local anesthetic bupivacaine on the oxidative phosphorylation in rat liver mitochondria were examined. Bupivacaine caused a maximum of about 7-fold stimulation of state 4 respiration at about 3 mM, released oligomycin-inhibited state 3 respiration, and activated ATPase to a similar extent to that by the weakly acidic uncoupler SF 6847. These effects were greatly enhanced by the addition of certain hydrophobic anions such as 1-anilino-8-naphthalenesulfonate, tetraphenyl borate, and picrate. In the absence of these anions, bupivacaine did not increase the proton conductance in either energized or nonenergized mitochondrial membranes or in artificial bilayer lipid membranes and did not have any effect on the proton motive force. However, it greatly enhanced the proton conductivity of these membrane systems and collapsed the proton motive force in the presence of hydrophobic anions. The results of noise analysis of artificial lipid bilayer membranes indicated that an ion pair complex of bupivacaine with hydrophobic anions formed a leakage-type ion pathway. Thus it is concluded that bupivacaine acts as a decoupler in the absence of added hydrophobic anions but in cooperation with certain anions as an uncoupler of oxidative phosphorylation due to formation of a H(+)-specific pathway in the membranes.