AI Article Synopsis

  • Mn-salen chloride and Mn-(3,3'-MeO)salen chloride act as mimetics for superoxide dismutase and catalase, protecting against free radical diseases in animals, though Mn-salen can also damage free DNA.
  • Co-administration of glutathione significantly reduces the DNA-damaging effects of Mn-salen, and alpha-lipoic acid, a common antioxidant supplement, also prevents its prooxidant activity.
  • Mn-(3,3'-MeO)salen provides similar protection to fibroblasts against hydrogen peroxide without causing damage to free DNA, with differing levels of DNA binding and cleavage between the two manganese complexes.

Article Abstract

Manganese(III) N,N'-ethylenebis(salicylideneiminato) chloride (Mn-salen chloride) and manganese(III) N,N'-ethylenebis(3-methoxysalicylideneiminato) chloride (Mn-(3,3'-MeO)salen chloride) are in vitro superoxide dismutase and catalase mimetics. They protect against free radical-related disease in animals, but Mn-salen can also be a potent prooxidant, damaging free DNA. Mn-salen protects human fibroblast DNA against hydrogen peroxide damage, however, damage to free DNA was confirmed by the comet assay. The DNA-damaging activity was dramatically reduced by co-administration with glutathione with the combination being less damaging to free DNA than either molecule alone. alpha-Lipoic acid, an antioxidant disulfide commonly used as a dietary supplement, also prevented Mn-salen prooxidant activity. Mn-(3,3'-MeO)salen protected fibroblasts against hydrogen peroxide as efficiently as Mn-salen and showed little damaging activity against free DNA. Protection was invested by both complexes in the presence and in the absence of EDTA, a potential competing chelator. Stabilities of the complexes with respect to decomposition and inactivation were studied by spectroscopic and electrochemical techniques. The complexes' binding to, and cleavage of, DNA was measured using a quartz crystal resonant sensor. Mn-salen was shown to bind strongly to DNA, prior to cleaving it; Mn-(3,3'-MeO)salen bound weakly and left DNA intact. Co-administration of either glutathione or alpha-lipoic acid appears to inhibit binding by Mn-salen thus preventing DNA-cleavage.

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http://dx.doi.org/10.1016/j.jinorgbio.2006.09.023DOI Listing

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