Brita Hornung scite author profile

The primary objective of this study was to determine the sequence of biochemical signaling events that occur after modulation of the cellular redox state in the B cell lymphoma line, PW, with emphasis on the role of mitochondrial signaling. L-Buthionine sulphoximine (BSO), which inhibits gamma glutamyl cysteine synthetase (gGCS), was used to modulate the cellular redox status. The sequence and role of mitochondrial events and downstream apoptotic signals and mediators was studied. After BSO treatment, there was an early decline in cellular glutathione (GSH), followed by an increase in reactive oxygen species (ROS) production, which induced a variety of apoptotic signals (detectable at different time points) in the absence of any external apoptotic stimuli. The sequence of biochemical events accompanying apoptosis included a 95% decrease in total GSH and a partial (25%) preservation of mitochondrial GSH, without a significant increase in ROS production at 24 h. Early activation and nuclear translocation of the nuclear factor kappa B subunit Rel A was observed at approximately 3 h after BSO treatment. Cytochrome c release into the cytosol was also seen after 24 h of BSO treatment. p53 protein expression was unchanged after redox modulation for up to 72 h, and p21 waf1 independent loss of cellular proliferation was observed. Surprisingly, a truncated form of p53 was expressed in a timedependent manner, beginning at 24 h after BSO incubation. Irreversible commitment to apoptosis occurred between 48 and 72 h after BSO treatment when mitochondrial GSH was depleted, and there was an increase in ROS production. Procaspase 3 protein levels showed a time-dependent reduction following incubation with BSO, notably after 48 h, that corresponded with increasing ROS levels. At 96 h, caspase 3 cleavage products were detectable. The pancaspase inhibitor zVADfmk, partially blocked the induction of apoptosis at 48 h, and was ineffective after 72 h. PW cells could be rescued from apoptosis by removing them from BSO after up to 48, but not 72 h incubation with BSO. Mitochondrial transmembrane potential (DC m ) remained intact in most of the cells during the 72 h observation period, indicating that DC m dissipation is not an early signal for the induction of redox dependent apoptosis in PW cells. These data suggest that a decrease in GSH alone can act as a potent early activator of apoptotic signaling. Increased ROS production following mitochondrial GSH depletion, represents a crucial event, which irreversibly commits PW cells to apoptosis.

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Rotenone-Induced G2/M Cell Cycle Arrest and Apoptosis in a Human B Lymphoma Cell Line PW

Armstrong

Hornung

Lecane

et al. 2001

Biochemical and Biophysical Research Communications

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Room D, 10/17/2000 2: 00 PM - 4: 00 PM (PS) Low Concentrations of Isoflurane Block Long Term Potentiation of Hippocampal Neuron Synapses

Anderson¹,

Hornung²,

Pittson³

et al. 2000

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Brita Hornung

Role of glutathione depletion and reactive oxygen species generation in apoptotic signaling in a human B lymphoma cell line

Rotenone-Induced G2/M Cell Cycle Arrest and Apoptosis in a Human B Lymphoma Cell Line PW

Room D, 10/17/2000 2: 00 PM - 4: 00 PM (PS) Low Concentrations of Isoflurane Block Long Term Potentiation of Hippocampal Neuron Synapses

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