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磷脂酶A2下调[3H]AMPA与大鼠皮质膜结合的亲和力。

Phospholipase A2 down-regulates the affinity of [3H]AMPA binding to rat cortical membranes.

作者信息

Dev K K, Honoré T, Henley J M

机构信息

Department of Anatomy, University of Bristol, Medical School, England, UK.

出版信息

J Neurochem. 1995 Jul;65(1):184-91. doi: 10.1046/j.1471-4159.1995.65010184.x.

Abstract

The effects of exogenous phospholipase A2 on the binding of alpha-[3H]amino-3-hydroxy-5-methylisoxazole-4-propionate ([3H]AMPA) to rat cortical membranes in the presence of the chaotrope potassium thiocyanate were assessed. Pretreatment of membranes with secretory phospholipase A2 (sPLA2) elicited a concentration-dependent decrease in specific [3H]AMPA binding due mainly to a decrease in affinity (KD). This observation, together with protease inhibitor and western blot evidence, suggest that the sPLA2 effect is not due to proteolysis. The sPLA2-evoked decrease was temperature and calcium dependent. Inclusion of the specific inhibitor oleoyloxyethyl phosphocholine or preincubation of the enzyme with reducing agents to degrade its secondary structure significantly reduced the sPLA2 inhibition. These results suggest that the effects of sPLA2 arise from an enzymatic action rather than a competitive interaction at the AMPA binding site. However, arachidonic acid, a major metabolite of sPLA2 action, did not cause a similar decrease in the affinity of [3H]AMPA binding. In contrast to the effects on [3H]AMPA binding, sPLA2 caused an increase in [3H]CNQX binding, which is in accordance with the functionality of the AMPA receptor complex. These results suggest that sPLA2 may play a role in the physiological and pathophysiological regulation of AMPA receptors.

摘要

评估了在外源性硫氰酸钾存在的情况下,外源性磷脂酶A2对α-[3H]氨基-3-羟基-5-甲基异恶唑-4-丙酸([3H]AMPA)与大鼠皮层膜结合的影响。用分泌型磷脂酶A2(sPLA2)预处理膜会引起特异性[3H]AMPA结合呈浓度依赖性降低,这主要是由于亲和力(KD)降低所致。这一观察结果,连同蛋白酶抑制剂和蛋白质印迹证据,表明sPLA2的作用不是由于蛋白水解。sPLA2引起的降低是温度和钙依赖性的。加入特异性抑制剂油酰氧基乙基磷酸胆碱或用还原剂对酶进行预孵育以降解其二级结构,可显著降低sPLA2的抑制作用。这些结果表明,sPLA2的作用源于酶促作用,而非在AMPA结合位点的竞争性相互作用。然而,花生四烯酸,sPLA2作用的主要代谢产物,并未导致[3H]AMPA结合亲和力出现类似降低。与对[3H]AMPA结合的影响相反,sPLA2导致[3H]CNQX结合增加,这与AMPA受体复合物的功能一致。这些结果表明,sPLA2可能在AMPA受体的生理和病理生理调节中发挥作用。

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