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大鼠体内的磷脂酰胆碱合成:甲基化的底物及胆碱的调节作用

Phosphatidylcholine synthesis in the rat: the substrate for methylation and regulation by choline.

作者信息

Datko A H, Aksamit R R, Mudd S H

机构信息

Laboratory of General and Comparative Biochemistry, National Institute of Mental Health, Bethesda, MD 20892.

出版信息

Lipids. 1990 Mar;25(3):135-42. doi: 10.1007/BF02544327.

Abstract

Two lines of evidence led us to reexamine the possibility that methylation of phosphoethanolamine and its partially methylated derivatives, in addition to methylation of the corresponding phosphatidyl derivatives, plays a role in mammalian phosphatidylcholine biosynthesis: (a) Results obtained by Salerno and Beeler with rat [Salerno, D.M. and Beeler, D.A. (1973) Biochim. Biophys. Acta 326, 325-338] appear to strongly support such a role for methylation of phosphobases; (b) Such reactions have recently been shown to play major roles in phosphatidylcholine synthesis by higher plants [see Datko, A.H. and Mudd, S.H. (1988) Plant Physiol. 88, 854-861 and references therein]. We found that, following continuous labeling of rat liver with L-[methyl-3H]methionine for 10.4 min (intraperitoneal administration) or for 0.75 min (intraportal administration), virtually no 3H was detected in methylated derivatives of phosphoethanolamine, but readily detectable amounts of 3H were present in the base moiety of each methylated derivative of phosphatidylethanolamine. Thus, there was no indication that phospho-base methylation makes a significant contribution. Studies of cultured rat hepatoma cells showed definitively for the first time in a mammalian system that choline deprivation up-regulates the rate of flow of methyl groups originating in methionine into phosphatidylethanolamine and derivatives. Even under these conditions, methylation of phosphoethanolamine bases appeared to play a negligible role.

摘要

两条证据线索促使我们重新审视磷酸乙醇胺及其部分甲基化衍生物的甲基化,除了相应磷脂酰衍生物的甲基化外,在哺乳动物磷脂酰胆碱生物合成中发挥作用的可能性:(a) 萨勒诺和比勒对大鼠的研究结果 [萨勒诺,D.M. 和比勒,D.A. (1973) 《生物化学与生物物理学学报》326, 325 - 338] 似乎有力地支持了磷酸碱基甲基化具有这样的作用;(b) 最近已表明此类反应在高等植物的磷脂酰胆碱合成中起主要作用 [见达特科,A.H. 和马德,S.H. (1988) 《植物生理学》88, 854 - 861 及其参考文献]。我们发现,用 L-[甲基 - ³H]甲硫氨酸连续标记大鼠肝脏 10.4 分钟(腹腔注射)或 0.75 分钟(门静脉注射)后,在磷酸乙醇胺的甲基化衍生物中几乎检测不到 ³H,但在磷脂酰乙醇胺的每种甲基化衍生物的碱基部分存在易于检测到的 ³H 量。因此,没有迹象表明磷酸碱基甲基化有显著贡献。对培养的大鼠肝癌细胞的研究首次在哺乳动物系统中明确表明,胆碱缺乏会上调源自甲硫氨酸的甲基流入磷脂酰乙醇胺及其衍生物的速率。即使在这些条件下,磷酸乙醇胺碱基的甲基化似乎也起微不足道的作用。

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