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在富含铁的培养基中生长可部分补偿大肠杆菌缺乏锰和铁超氧化物歧化酶的情况。

Growth in iron-enriched medium partially compensates Escherichia coli for the lack of manganese and iron superoxide dismutase.

作者信息

Benov L, Fridovich I

机构信息

Department of Biochemistry, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

J Biol Chem. 1998 Apr 24;273(17):10313-6. doi: 10.1074/jbc.273.17.10313.

Abstract

Enrichment of the growth medium with iron partially relieves the phenotypic deficits imposed on Escherichia coli by lack of both manganese and iron superoxide dismutases. Thus iron supplementation increased the aerobic growth rate, decreased the leakage of sulfite, and diminished sensitivity toward paraquat. Iron supplementation increased the activities of several [4Fe-4S]-containing dehydratases, and this was seen even in the presence of 50 microg/ml of rifampicin, an amount which completely inhibited growth. Assessing the O-2 scavenging activity by means of lucigenin luminescence indicated that the iron-enriched sodAsodB cells had gained some means of eliminating O-2, which was not detectable as superoxide dismutase activity in cell extracts. It is noteworthy that iron-enriched cells were not more sensitive toward the lethality of H2O2 despite having the usual amount of catalase activity. This indicates that iron taken into the cells from the medium is not available for Fenton chemistry, but is available for reconstitution of iron-sulfur clusters. We suppose that oxidation of the [4Fe-4S] clusters of dehydratases by O-2 and their subsequent reductive reconstitution provides a mechanism for scavenging O-2 and that speeding this reductive reconstitution by iron enrichment both spared other targets from O-2 attack and maintained adequate levels of these enzymes to meet the metabolic needs of the cells.

摘要

用铁富集生长培养基可部分缓解因缺乏锰超氧化物歧化酶和铁超氧化物歧化酶而施加给大肠杆菌的表型缺陷。因此,补充铁可提高需氧生长速率,减少亚硫酸盐泄漏,并降低对百草枯的敏感性。补充铁可提高几种含[4Fe-4S]脱水酶的活性,即使在存在50微克/毫升利福平的情况下也是如此,该剂量可完全抑制生长。通过光泽精发光评估超氧阴离子清除活性表明,富含铁的sodAsodB细胞获得了一些清除超氧阴离子的方法,而在细胞提取物中未检测到超氧化物歧化酶活性。值得注意的是,尽管过氧化氢酶活性正常,但富含铁的细胞对过氧化氢的致死性并不更敏感。这表明从培养基进入细胞的铁不能用于芬顿化学反应,但可用于铁硫簇的重构。我们推测,脱水酶的[4Fe-4S]簇被超氧阴离子氧化及其随后的还原重构提供了一种清除超氧阴离子的机制,并且通过铁富集加速这种还原重构既使其他靶点免受超氧阴离子攻击,又维持了这些酶的足够水平以满足细胞的代谢需求。

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