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钴胺素代谢的先天性缺陷:培养中补充钴胺素对正常及突变型人成纤维细胞中甲基丙二酸单酰辅酶A变位酶活性的影响

Inborn errors of cobalamin metabolism: effect of cobalamin supplementation in culture on methylmalonyl CoA mutase activity in normal and mutant human fibroblasts.

作者信息

Willard H F, Rosenberg L E

出版信息

Biochem Genet. 1979 Feb;17(1-2):57-75. doi: 10.1007/BF00484474.

Abstract

We have examined the effect of addition of hydroxocobalamin to growth medium on the activity of the adenosylcobalamin-requiring enzyme methylmalonyl CoA mutase in normal human fibroblasts and in mutant human fibroblasts derived from patients with inherited methylmalonicacidemia. The mutant cell lines were assigned to four distinct genetic complementation groups (cbl A, cbl B, cbl C, and cbl D), each deficient in some step in the synthesis of adenosylcobalamin from hydroxocobalamin. After control cells were grown in cobalamin-supplemented medium, mutase holoenzyme activitiy increased markedly in a time- and concentration-dependent fashion. Growth in cobalamin-supplemented medium had no effect on mutase activity in some mutant lines belonging to the cbl B group, while activity increased severalfold in other cbl B mutants and in all cbl A, cbl C, and cbl D mutants examined, although mutase activity was still less than 10% of control. Comparison of mutase holoenzyme activity and total propionate pathway activity suggests that enhancement of mutase activity in mutant cells after cobalamin supplementation to values 5--10% of control may be sufficient to overcome the inherited metabolic block and to restore total pathway activity to normal.

摘要

我们研究了在生长培养基中添加羟钴胺素对正常人成纤维细胞以及源自遗传性甲基丙二酸血症患者的突变人成纤维细胞中需要腺苷钴胺素的甲基丙二酰辅酶A变位酶活性的影响。这些突变细胞系被分为四个不同的遗传互补组(cbl A、cbl B、cbl C和cbl D),每组在从羟钴胺素合成腺苷钴胺素的某些步骤中存在缺陷。对照细胞在添加钴胺素的培养基中生长后,变位酶全酶活性以时间和浓度依赖性方式显著增加。在添加钴胺素的培养基中生长对属于cbl B组的一些突变株的变位酶活性没有影响,而在其他cbl B突变株以及所有检测的cbl A、cbl C和cbl D突变株中,活性增加了几倍,尽管变位酶活性仍低于对照的10%。变位酶全酶活性与总丙酸途径活性的比较表明,在突变细胞中,添加钴胺素后变位酶活性提高到对照的5%-10%可能足以克服遗传性代谢障碍并使总途径活性恢复正常。

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