Inhibition of Succinate-cytochrome C Reductase by a Ferromacrocyclic Complex

M. Balbaa, M. Khalifa, M. El-Sabaway, Kamal Kandeelaf
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引用次数: 5

Abstract

Succinate-cytochrome c reductase (SCR) from mouse liver was inhibited strongly and reversibly by an iron (II) macrocyclic complex 3. The inhibition was observed for the enzyme toward the reduction of both 2,6-dichlorophenol indophenol (DCIP) and cytochrome c (cyt c). The inhibition was a mixed type and noncompetitive with respect to the reduction of DCIP and cyt c, respectively. Values of the inhibition constant ranged from 6.6 to 8.3 μM. The IC50 for the complex 3 was found to be 16.6 × 0.8 and 12.1 × 0.5 μM for the enzyme toward DCIP and cyt c, respectively. The reduced form of complex 3 also exhibited enzyme inhibition but to a less extent. Complex 3, at a lower level, equal to 25% of its LD50 showed about 50% inhibition of the enzyme through in vivo dose-dependent effect. These findings suggested that the structure of the equatorial benzoquinoid macrocyclic ligand of the Fe(II) complex is involved in the enzyme inhibition.
大环铁络合物对琥珀酸-细胞色素C还原酶的抑制作用
小鼠肝脏琥珀酸-细胞色素c还原酶(SCR)被铁(II)大环复合物3强烈可逆地抑制。该酶对2,6-二氯酚吲哚酚(DCIP)和细胞色素c (cyt c)的还原均有抑制作用,抑制作用为混合型,对DCIP和cyt c的还原均为非竞争性。抑制常数范围为6.6 ~ 8.3 μM。该酶对DCIP和cytc的IC50分别为16.6 × 0.8 μM和12.1 × 0.5 μM。复合体3的还原形式也表现出酶抑制,但程度较轻。复合物3在较低水平时,相当于其LD50的25%,通过体内剂量依赖效应对酶的抑制作用约为50%。这些发现表明Fe(II)配合物的赤道型苯并醌类大环配体的结构参与了酶的抑制作用。
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