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- W1968710441 abstract "Ascorbate (20mM) pretreatment of brain membrane suspensions at 37 degrees produced a rapid irreversible loss of specific opioid binding. There was no reduction in specific 3H-halo-peridol binding. Ascorbate induced loss of opioid binding under these experimental conditions was not blocked by low concentrations of EDTA or MN++. In contrast, the slowly developing loss of opioid binding during exposure to 1 mM ascorbate at 23 degrees was completely inhibited by 10(-5)M EDTA or Mn++. At 37 degrees, D-isoascorbate, and several other reducing agents (glutathione, dithiothreitol, cysteine) produced a loss of opioid binding similar to that seen with ascorbate. It is concluded that 1 mM ascorbate at 23 degrees, and 20 mM ascorbate at 37 degrees, destroy opioid binding sites by two independent mechanisms. Lipid peroxidation is implicated at low ascorbate concentrations; a reductive process appears to be responsible for the ascorbate induced loss of binding at higher concentrations." @default.
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- W1968710441 title "The Use of Ascorbate as a Probe of Opioid Receptor Structure: Evidence for two Independent Mechanisms of Receptor Destruction by Ascorbate" @default.
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- W1968710441 doi "https://doi.org/10.3109/10799898009044104" @default.
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