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Developmental changes in the activity of phosphatidylethanolamine N-methyltransferases in rat brain.

机译:大鼠脑磷脂酰乙醇胺N-甲基转移酶活性的发育变化。

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摘要

The activity of phosphatidylethanolamine N-methyltransferase (PeMT), an enzymic system that catalyses the synthesis of phosphatidylcholine (PtdCho) via sequential methylation of phosphatidylethanolamine (PtdEtn) using S-adenosylmethionine (AdoMet) as a methyl donor, was examined in brain homogenates from rats of various ages. The data thus obtained were consistent with the existence of two distinct enzyme activities within this enzyme system, i.e. one catalysing the methylation of PtdEtn [to form phosphatidyl-N-monomethylethanolamine (PtdMeEtn)], and the other catalysing the methylations of PtdMeEtn and phosphatidyl-NN-dimethylethanolamine (PtdMe2Etn) (to form PtdMe2Etn and PtdCho, respectively). PeMT (PtdEtn-methylating) activity per g of brain was 4-fold higher in neonatal than in adult brains. The enzyme activity in adult brains exhibited Michaelis-Menten kinetics for AdoMet, and its affinity for AdoMet was high (apparent Km 1.6 microM). In neonatal brain the relationships between AdoMet concentrations and PtdMeEtn formation were more complex: a sigmoidal component (with a Hill coefficient of 2.7), requiring 90 microM-AdoMet for half-saturation predominated over the high-affinity component (similar to that of the adult brain). PeMT (PtdMe2Etn-methylating) activity per g of brain increased 2-fold between the 5th and the 20th postnatal days and remained constant thereafter; it was higher than that of PeMT (PtdEtn-methylating) activity at all ages studied, and its affinity for AdoMet was low (apparent Km 99 microM). No sexual dimorphism in brain PeMT activity was observed at any age. We conclude that PeMT (PtdEtn-methylating) catalyses the rate-limiting step in PtdCho synthesis in rat brain, and that PtdCho formation via this pathway may be greatest during the neonatal period.
机译:在大鼠脑匀浆中检查了磷脂酰乙醇胺N-甲基转移酶(PeMT)的活性,该酶系统通过使用S-腺苷甲硫氨酸(AdoMet)作为甲基供体,通过磷脂酰乙醇胺(PtdEtn)的顺序甲基化来催化磷脂酰胆碱(PtdEtn)的合成。各个年龄段。如此获得的数据与该酶系统中存在两种不同的酶活性一致,即一种催化PtdEtn的甲基化[形成磷脂酰-N-单甲基乙醇胺(PtdMeEtn)],另一种催化PtdMeEtn的甲基化和磷脂酰-甲基化。 NN-二甲基乙醇胺(PtdMe2Etn)(分别形成PtdMe2Etn和PtdCho)。在新生儿中,每克大脑的PeMT(PtdEtn-甲基化)活性比成年大脑高4倍。成年大脑中的酶活性表现出AdoMet的Michaelis-Menten动力学,并且它对AdoMet的亲和力很高(​​表观Km为1.6 microM)。在新生儿大脑中,AdoMet浓度与PtdMeEtn形成之间的关系更为复杂:S形分量(希尔系数为2.7),需要90 microM-AdoMet的半饱和度高于高亲和力分量(与成人相似)脑)。每克大脑的PeMT(PtdMe2Etn-甲基化)活性在出生后第5天至第20天增加了2倍,此后保持不变;在所有研究的年龄中,它都比PeMT(PtdEtn-甲基化)活性高,并且它对AdoMet的亲和力很低(表观Km 99 microM)。在任何年龄段均未观察到大脑PeMT活动的性二态性。我们得出的结论是,PeMT(PtdEtn甲基化)催化大鼠脑PtdCho合成中的限速步骤,并且在新生儿期通过该途径形成的PtdCho可能最大。

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