Different oxidative pathways of isonicotinic acid hydrazide and its meta-isomer, nicotinic acid hydrazide

International Journal of Biochemistry Pub Date : 1994-09-01 DOI:10.1016/0020-711X(94)90130-9

Ben J. van der Walt, Johann M. van Zyl, André Kriegler

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引用次数: 4

Abstract

1.
1. Superoxide was generated during the auto-oxidation of the antituberculous drug, isonicotinic acid hydrazide (INH), but not with its meta-isomer, nicotinic acid hydrazide (NH). During Fe²⁺-stimulated oxidation of INH and NH, aromatic hydroxylation occurred which was inhibited by the chelating agent, phytic acid.
2.
2. A mixture of myeloperoxidase (MPO) and a hydrazide induced formation of compound III (oxyperoxidase) and aromatic hydroxylation which was stimulated by phytic acid. INH was considerably more potent than NH.
3.
3. Co-oxidation of a hydrazide and thyroxine (T₄) in the MPO system resulted in the formation of a pink-coloured product (maximum absorbance at 504 nm) which was more stable with NH than with INH.
4.
4. The hydrazides and Cl⁻ acted synergistically on MPO haem modification when co-oxidised in the MPO-H₂O₂ system. INH was more destructive than NH.
5.
5. The different oxidative pathways of the hydrazides are consistent with the fact that an acyl intermediate of INH, unlike that of NH, is resonance stabilized.

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异烟酸肼及其间位异构体烟酸肼的不同氧化途径

1.1. 在抗结核药物异烟酸肼(INH)的自氧化过程中产生超氧化物，但在其间位异构体烟酸肼(NH)的自氧化过程中不产生超氧化物。在Fe2+的刺激下，INH和NH发生了芳香羟基化反应，而这种反应被螯合剂植酸抑制。髓过氧化物酶(MPO)和肼的混合物诱导化合物III(过氧化物酶)的形成和芳香族羟基化，这是由植酸刺激。INH明显强于NH.3.3。在MPO体系中肼和甲状腺素(T4)的共氧化导致形成粉红色的产物(最大吸光度在504 nm)，该产物在NH中比在INH.4.4中更稳定。在MPO- h2o2体系中共氧化时，酰肼和氯离子协同作用于MPO血红素改性。INH比NH.5.5更具破坏性。肼的不同氧化途径与INH的酰基中间体不同于NH是共振稳定的这一事实是一致的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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International Journal of Biochemistry

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