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凝血酶及凝血酶受体的一种14氨基酸肽激动剂对隔区胆碱能神经元的双重作用

Dual effects of thrombin and a 14-amino acid peptide agonist of the thrombin receptor on septal cholinergic neurons.

作者信息

Debeir T, Benavides J, Vigé X

机构信息

CNS Research Department, Synthélabo Recherche, Bagneux, France.

出版信息

Brain Res. 1996 Feb 5;708(1-2):159-66. doi: 10.1016/0006-8993(95)01237-0.

Abstract

We have compared the effects of thrombin and of the 14-amino acid peptide agonist (TRAP-14) of the thrombin protease activated receptor (PAR) on cholinergic neurons in pure cultures of rat septal neurons and in co-cultures of septal neurons and glial cells. In pure septal cultures, low concentrations of thrombin (up to 10 nM) did not affect choline acetyltransferase (ChAT) activity, a marker of cholinergic neurons, or 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide (MTT) reduction, an index of cell viability. However, 100 nM thrombin decreased ChAT activity and MTT reduction by 44 and 17%, respectively. In co-cultures, a low concentration of thrombin (1 nM) increased ChAT activity (+75%), whereas a high concentration (100 nM) decreased it (-83%). At this high concentration, thrombin was neurotoxic, as indicated by a large decrease in MTT reduction (-80%). Thrombin effects on ChAT activity were mimicked by TRAP-14 both in pure septal cultures (no effect at 0.1 microM and -63% at 100 microM) and in co-cultures (+25% at 0.1 microM and -28% at 100 microM). In contrast, this peptide did not affect MTT reduction. These dual effects of thrombin and TRAP-14 on ChAT activity in co-cultures, were also observed on pure cultures of septal cells supplied with NGF. The activation and inhibition by TRAP-14 of the expression of ChAT activity in septal neuron/glial cell cultures were inhibited by a 9-amino acid peptide antagonist of thrombin PAR. Thus, the effects of thrombin on cholinergic neurons seem to be mainly mediated by thrombin PAR and glial cells seem to play a major role in these thrombin actions.

摘要

我们比较了凝血酶和凝血酶蛋白酶激活受体(PAR)的14氨基酸肽激动剂(TRAP-14)对大鼠隔区神经元纯培养物以及隔区神经元与神经胶质细胞共培养物中胆碱能神经元的影响。在隔区神经元纯培养物中,低浓度的凝血酶(高达10 nM)不影响胆碱能神经元标志物胆碱乙酰转移酶(ChAT)的活性,也不影响细胞活力指标3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四氮唑溴盐(MTT)还原率。然而,100 nM凝血酶分别使ChAT活性和MTT还原率降低了44%和17%。在共培养物中,低浓度的凝血酶(1 nM)使ChAT活性增加(+75%),而高浓度(100 nM)则使其降低(-83%)。在这个高浓度下,凝血酶具有神经毒性,MTT还原率大幅下降(-80%)表明了这一点。在隔区神经元纯培养物(0.1 μM时无影响,100 μM时降低63%)和共培养物(0.1 μM时增加25%,100 μM时降低28%)中,TRAP-14均模拟了凝血酶对ChAT活性的影响。相比之下,该肽不影响MTT还原率。凝血酶和TRAP-14对共培养物中ChAT活性的这种双重作用,在补充了神经生长因子(NGF)的隔区细胞纯培养物中也观察到了。TRAP-14对隔区神经元/神经胶质细胞培养物中ChAT活性表达的激活和抑制作用,被凝血酶PAR的一种9氨基酸肽拮抗剂所抑制。因此,凝血酶对胆碱能神经元的作用似乎主要由凝血酶PAR介导,并且神经胶质细胞似乎在这些凝血酶作用中起主要作用。

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