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小鼠神经母细胞瘤N18TG2细胞中油酸衍生的代谢产物。

Oleic acid derived metabolites in mouse neuroblastoma N18TG2 cells.

作者信息

Merkler David J, Chew Geoffrey H, Gee Andrew J, Merkler Kathleen A, Sorondo Jean-Paul O, Johnson Mitchell E

机构信息

Department of Chemistry, University of South Florida, Tampa, Florida 33620, USA.

出版信息

Biochemistry. 2004 Oct 5;43(39):12667-74. doi: 10.1021/bi049529p.

Abstract

Oleamide is an endogenous sleep-inducing lipid that has been isolated from the cerebrospinal fluid of sleep-deprived mammals. Oleamide is the best-understood member of the primary fatty acid amide family. One key unanswered question regarding oleamide and all other primary acid amides is the pathway by which these molecules are produced. One proposed pathway involves oleoyl-CoA and N-oleoylglycine as intermediates: oleic acid --> oleoyl-CoA --> N-oleoylglycine --> oleamide. The first and third reactions are known reactions, catalyzed by acyl-CoA synthetase and peptidylglycine alpha-amidating monooxygenase (PAM). Oleoyl-CoA formation from oleic acid has been demonstrated in vitro and in vivo while, to date, N-oleoylglycine cleavage to oleamide has been established only in vitro. PAM catalyzes the final step in alpha-amidated peptide biosynthesis, and its proposed role in primary fatty acid amide biosynthesis has been controversial. Mouse neuroblastoma N(18)TG(2) cells are an excellent model system for the study of oleamide biosynthesis because these cells convert [(14)C]-oleic acid to [(14)C]-oleamide and express PAM in a regulated fashion. We report herein that growth of the N(18)TG(2) cells in the presence of [(14)C]-oleic acid under conditions known to stimulate PAM expression generates an increase in [(14)C]-oleamide or in the presence of a PAM inhibitor generates [(14)C]-N-oleoylglycine. This represents the first identification of N-oleoylglycine from a biological source. In addition, N(18)TG(2) cell growth in the presence of N-oleoylglycine yields oleamide. These results strongly indicate that N-oleoylglycine is an intermediate in oleamide biosynthesis and provide further evidence that PAM does have a role in primary fatty acid amide production in vivo.

摘要

油酰胺是一种内源性诱导睡眠的脂质,已从睡眠剥夺的哺乳动物的脑脊液中分离出来。油酰胺是初级脂肪酸酰胺家族中研究得最透彻的成员。关于油酰胺和所有其他初级酸酰胺,一个关键的未解决问题是这些分子的产生途径。一种提出的途径涉及油酰辅酶A和N - 油酰甘氨酸作为中间体:油酸→油酰辅酶A→N - 油酰甘氨酸→油酰胺。第一个和第三个反应是已知反应,分别由酰基辅酶A合成酶和肽基甘氨酸α - 酰胺化单加氧酶(PAM)催化。油酸形成油酰辅酶A已在体外和体内得到证实,而迄今为止,N - 油酰甘氨酸裂解为油酰胺仅在体外得到证实。PAM催化α - 酰胺化肽生物合成的最后一步,其在初级脂肪酸酰胺生物合成中的作用一直存在争议。小鼠神经母细胞瘤N(18)TG(2)细胞是研究油酰胺生物合成的优秀模型系统,因为这些细胞能将[(14)C] - 油酸转化为[(14)C] - 油酰胺,并以一种受调控的方式表达PAM。我们在此报告,在已知能刺激PAM表达的条件下,N(18)TG(2)细胞在[(14)C] - 油酸存在下生长会导致[(14)C] - 油酰胺增加,或者在存在PAM抑制剂的情况下会产生[(14)C] - N - 油酰甘氨酸。这是首次从生物来源鉴定出N - 油酰甘氨酸。此外,N(18)TG(2)细胞在N - 油酰甘氨酸存在下生长会产生油酰胺。这些结果有力地表明N - 油酰甘氨酸是油酰胺生物合成的中间体,并进一步证明PAM在体内初级脂肪酸酰胺产生中确实起作用。

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