Hou W, Tsuda T, Jensen R T
Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892, USA.
Biochim Biophys Acta. 1998 Apr 22;1391(3):337-50. doi: 10.1016/s0005-2760(98)00014-9.
The actions of neuromedin B (NMB), a recently discovered mammalian bombesin-related peptide, are mediated by interacting with a distinct receptor; however, little is known about its cellular basis of action. Recent studies show activation of phospholipase D (PLD) is an important transduction cascade for a number of GI hormones, especially for stimulation of growth and protein sorting. The purpose of the present study was to determine whether activation of the NMB receptor causes activation of PLD and to explore whether this activation was coupled to PLC activation. Rat C6 glioblastoma cells (C6 cells), which contain a low density of native NMB receptors and BALB 3T3 cells stably transfected with rat NMB receptors, were used. NMB caused a 3-fold increase in C6 cells and an 11-fold increase in rNMB-R transfected cells in PLD activity. Increases in PLD activity were rapid and NMB was 100-fold more potent than gastrin-releasing peptide (GRP). NMB caused a half-maximal increase in [Ca2+]i at 0.2 nM, in [3H]IP and PLD at 1 nM, and half-maximal receptor occupation at 1.2 nM. TPA increased PLD dose-dependently with a half-maximal effect at 60 nM. The calcium ionophore A23187 (1 microM) alone did not increase PLD activity but potentiated the effect of TPA. The Ca2+-ATPase inhibitor, thapsigargin, did not affect NMB- or TPA-stimulated PLD activities, although it blocked completely the NMB-induced increase in [Ca2+]i. The PKC inhibitor GF109203X completely abolished TPA-induced PLD activity, however, it only inhibited NMB-induced PLD activity by 20%. The combination of thapsigargin and GF109203X had the same effect as GF109203X alone. These data indicate that NMB receptor activation is coupled to both PLC and PLD. In contrast to a number of other phospholipase C-coupled receptors, NMB receptor stimulated changes in [Ca2+]i do not contribute to PLD activation. Both PKC-dependent and PKC-independent mechanisms are involved in the NMB-stimulated PLD activation with the PKC-independent pathway predominating.
神经介素B(NMB)是一种最近发现的与哺乳动物蛙皮素相关的肽,其作用是通过与一种独特的受体相互作用来介导的;然而,对其细胞作用基础却知之甚少。最近的研究表明,磷脂酶D(PLD)的激活是许多胃肠激素的重要转导级联反应,特别是对于生长刺激和蛋白质分选而言。本研究的目的是确定NMB受体的激活是否会导致PLD的激活,并探讨这种激活是否与PLC激活相关联。使用了大鼠C6胶质母细胞瘤细胞(C6细胞),其含有低密度的天然NMB受体,以及稳定转染了大鼠NMB受体的BALB 3T3细胞。NMB使C6细胞中的PLD活性增加了3倍,使转染了rNMB-R的细胞中的PLD活性增加了11倍。PLD活性的增加迅速,且NMB的效力比胃泌素释放肽(GRP)高100倍。NMB在0.2 nM时使[Ca2+]i增加至最大值的一半,在1 nM时使[3H]IP和PLD增加至最大值的一半,在1.2 nM时使受体占有率达到最大值的一半。佛波酯(TPA)以剂量依赖性方式增加PLD活性,在60 nM时达到最大效应的一半。钙离子载体A23187(1 microM)单独使用时不会增加PLD活性,但会增强TPA的作用。Ca2+-ATP酶抑制剂毒胡萝卜素并不影响NMB或TPA刺激的PLD活性,尽管它完全阻断了NMB诱导的[Ca2+]i增加。蛋白激酶C(PKC)抑制剂GF109203X完全消除了TPA诱导的PLD活性,然而,它仅将NMB诱导的PLD活性抑制了20%。毒胡萝卜素和GF109203X的组合与单独使用GF109203X具有相同的效果。这些数据表明,NMB受体激活与PLC和PLD均相关联。与许多其他磷脂酶C偶联受体不同,NMB受体刺激引起的[Ca2+]i变化对PLD激活没有贡献。NMB刺激的PLD激活涉及PKC依赖性和PKC非依赖性机制,其中PKC非依赖性途径占主导地位。
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