Ascorbate in pharmacologic concentrations selectively generates ascorbate radical and hydrogen peroxide in extracellular fluid in vivo

细胞外液 化学 体内 过氧化氢 抗坏血酸 药理学 前药 毒性 生物化学 细胞外 医学 生物 食品科学 生物技术 有机化学
作者
Qi Chen,Michael Graham Espey,Andrew Y. Sun,Je‐Hyuk Lee,Murali C. Krishna,Emily Shacter,Peter L. Choyke,Chaya Pooput,Kenneth L. Kirk,Garry R. Buettner,Mark Levine
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:104 (21): 8749-8754 被引量:615
标识
DOI:10.1073/pnas.0702854104
摘要

Ascorbate (ascorbic acid, vitamin C), in pharmacologic concentrations easily achieved in humans by i.v. administration, selectively kills some cancer cells but not normal cells. We proposed that pharmacologic ascorbate is a prodrug for preferential steady-state formation of ascorbate radical (Asc •− ) and H 2 O 2 in the extracellular space compared with blood. Here we test this hypothesis in vivo . Rats were administered parenteral (i.v. or i.p.) or oral ascorbate in typical human pharmacologic doses (≈0.25–0.5 mg per gram of body weight). After i.v. injection, ascorbate baseline concentrations of 50–100 μM in blood and extracellular fluid increased to peaks of >8 mM. After i.p. injection, peaks approached 3 mM in both fluids. By gavage, the same doses produced ascorbate concentrations of <150 μM in both fluids. In blood, Asc •− concentrations measured by EPR were undetectable with oral administration and always <50 nM with parenteral administration, even when corresponding ascorbate concentrations were >8 mM. After parenteral dosing, Asc •− concentrations in extracellular fluid were 4- to 12-fold higher than those in blood, were as high as 250 nM, and were a function of ascorbate concentrations. By using the synthesized probe peroxyxanthone, H 2 O 2 in extracellular fluid was detected only after parenteral administration of ascorbate and when Asc •− concentrations in extracellular fluid exceeded 100 nM. The data show that pharmacologic ascorbate is a prodrug for preferential steady-state formation of Asc •− and H 2 O 2 in the extracellular space but not blood. These data provide a foundation for pursuing pharmacologic ascorbate as a prooxidant therapeutic agent in cancer and infections.
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