Cabot M C, Welsh C J, Cao H T, Chabbott H
W. Alton Jones Cell Science Center, Lake Placid, NY 12946.
FEBS Lett. 1988 Jun 6;233(1):153-7. doi: 10.1016/0014-5793(88)81374-7.
Agonist-induced degradation of phosphatidylcholine (PC) is of interest as this pathway of diacylglycerol (DG) generation may provide added opportunities for the regulation of protein kinase C (PKC). In REF52 cells [3H]myristic acid is preferentially incorporated into PC; this, coupled with the use of [3H]choline, allows for quantitation of both the water-soluble and the lipid products generated when PC is degraded. In cells prelabeled with [3H]choline, TPA stimulated a time-dependent release, into the medium, of choline and not phosphocholine or glycerophosphocholine. Treatment of [3H]myristic acid-labeled cells with either phorbol diesters, sn-1,2-dioctanoylglycerol, or vasopressin elicited the formation of labeled phosphatidate (PA) and DG. The temporal pattern of PC hydrolysis in cells treated with TPA is indicative of a precursor (PA)-product (DG) relationship for an enzymatic sequence initiated by phospholipase D. Adding propranolol, a phosphatidate phosphohydrolase inhibitor, eliminated TPA-induced DG formation, whereas PA generation was unaffected. From these data we conclude that TPA elicits DG formation from PC by the sequential actions of phospholipase D and phosphatidate phosphohydrolase.
激动剂诱导的磷脂酰胆碱(PC)降解备受关注,因为这种二酰基甘油(DG)生成途径可能为蛋白激酶C(PKC)的调节提供更多机会。在REF52细胞中,[3H]肉豆蔻酸优先掺入PC;这与[3H]胆碱的使用相结合,使得在PC降解时能够对水溶性产物和脂质产物进行定量分析。在用[3H]胆碱预标记的细胞中,佛波酯(TPA)刺激胆碱随时间依赖性释放到培养基中,而不是磷酸胆碱或甘油磷酸胆碱。用佛波醇酯、sn-1,2-二辛酰甘油或血管加压素处理[3H]肉豆蔻酸标记的细胞,会引发标记磷脂酸(PA)和DG的形成。用TPA处理的细胞中PC水解的时间模式表明,由磷脂酶D启动的酶促序列存在前体(PA)-产物(DG)关系。添加磷脂酸磷酸水解酶抑制剂普萘洛尔可消除TPA诱导的DG形成,而PA生成不受影响。从这些数据我们得出结论,TPA通过磷脂酶D和磷脂酸磷酸水解酶的相继作用,从PC引发DG的形成。
