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成年大鼠原代培养肝细胞中血小板活化因子通过涉及磷脂酶C和烷基单加氧酶的新途径进行代谢。

Metabolism of platelet-activating factor in primary cultured adult rat hepatocytes by a new pathway involving phospholipase C and alkyl monooxygenase.

作者信息

Okayasu T, Hoshii K, Seyama K, Ishibashi T, Imai Y

出版信息

Biochim Biophys Acta. 1986 Mar 21;876(1):58-64.

PMID:3947669
Abstract

The metabolic fate of 1-O-[3H]alkyl-2-acetyl-sn-glycero-3-phosphocholine (PAF-acether) upon interaction with primary cultured adult rat hepatocytes was investigated. [3H]PAF-acether was transformed time-dependently into [3H]lyso-PAF-acether, 1-O-[3H]alkylglycerol and finally converted to 3H-labeled fatty aldehyde. 1-O-[3H]Alkyl-2-acyl-sn-glycero-3-phosphocholine (alkylacyl-GPC) was formed after a long incubation time and with a smaller amount compared with that formed in platelets and neutrophils. When lipids from cells, cell surfaces and incubation medium were analyzed separately, most of the transformed products of [3H]PAF-acether remained in the cells. When 1-O-[3H]alkyl-2-lyso-sn-glycero-3-phosphocholine was incubated with hepatocytes, it was mainly converted into 1-O-[3H]alkylglycerol. 3H-labeled fatty aldehyde and [3H]alkylacyl-GPC were also found. Hepatocytes metabolized slowly from 1-O-[1-14C]hexadecylglycerol to 3H-labeled fatty aldehyde and 3H-labeled phospholipid. These findings suggest that cultured hepatocytes mainly catabolize exogeneous PAF-acether by removing the acetyl residue and the polar head group and, finally, by cleaving an ether bond. The deacetylation-reacylation step, which is important in platelets and neutrophils, was not shown to be a main metabolic pathway of PAF-acether in cultured hepatocytes.

摘要

研究了1-O-[³H]烷基-2-乙酰基-sn-甘油-3-磷酸胆碱(PAF-乙醚)与原代培养的成年大鼠肝细胞相互作用后的代谢命运。[³H]PAF-乙醚随时间依赖性地转化为[³H]溶血-PAF-乙醚、1-O-[³H]烷基甘油,最终转化为³H标记的脂肪醛。长时间孵育后形成了1-O-[³H]烷基-2-酰基-sn-甘油-3-磷酸胆碱(烷基酰基-GPC),但其生成量比在血小板和中性粒细胞中形成的量少。当分别分析细胞、细胞表面和孵育培养基中的脂质时,[³H]PAF-乙醚的大多数转化产物仍留在细胞中。当1-O-[³H]烷基-2-溶血-sn-甘油-3-磷酸胆碱与肝细胞一起孵育时,它主要转化为1-O-[³H]烷基甘油。还发现了³H标记的脂肪醛和[³H]烷基酰基-GPC。肝细胞将1-O-[1-¹⁴C]十六烷基甘油缓慢代谢为³H标记的脂肪醛和³H标记的磷脂。这些发现表明,培养的肝细胞主要通过去除乙酰基残基和极性头部基团,最终通过裂解醚键来分解外源性PAF-乙醚。在血小板和中性粒细胞中重要的脱乙酰化-再酰化步骤,在培养的肝细胞中未显示为PAF-乙醚的主要代谢途径。

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