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人脑中溶血磷脂代谢酶的特性研究

Characterization of lysophospholipid metabolizing enzymes in human brain.

作者信息

Ross B M, Kish S J

机构信息

Human Neurochemical Pathology Laboratory, Clarke Institute of Psychiatry, Toronto, Ontario, Canada.

出版信息

J Neurochem. 1994 Nov;63(5):1839-48. doi: 10.1046/j.1471-4159.1994.63051839.x.

Abstract

Lysophospholipids are generated during the turnover and breakdown of membrane phospholipids. We have identified and partially characterized three enzymes involved in the metabolism of lysophospholipids in human brain, namely, lysophospholipase, lysophospholipid:acyl-CoA acyltransferase (acyltransferase), and lysophospholipid:lysophospholipid transacylase (transacylase). Each enzyme displayed comparable levels of activity in biopsied and autopsied human brain, although in all cases the activity was somewhat lower in human than that in rat brain. All three enzymes were localized predominantly in the particulate fraction, with lysophospholipase possessing the greatest activity followed by acyltransferase and transacylase. Lysophosphatidylcholine possessed a Km in the micromolar range for lysophospholipase and transacylase, and in the millimolar range for acyltransferase, whereas arachidonyl-CoA displayed a Km in the micromolar range for acyltransferase. The three enzymes differed in their pH optima, with lysophospholipase being most active at pH 8.0, transacylase at pH 7.5, and acyltransferase at pH 6.0. Both bromophenacyl bromide and N-ethylmaleimide inhibited lysophospholipase activity and, to a lesser extent, that of acyltransferase and transacylase. None of the enzyme activities were affected by the presence of dithiothreitol or EDTA, although particulate lysophospholipase was activated approximately two-fold by the addition of 5 mM MgCl2 or CaCl2 but not KCl. Transacylating activity was stimulated by CoA, the EC50 of activation being 6.8 microM. Acyltransferase displayed an approximately threefold preference for arachidonyl-CoA over palmitoyl-CoA, whereas the acylation rate of different lysophospholipids was in the order lysophosphatidylinositol > 1-palmitoyl lysophosphatidylcholine > 1-oleoyl lysophosphatidylcholine >> lysophosphatidylserine > lysophosphatidylethanolamine. This, and the preference of human brain phospholipase A2 for phosphatidylinositol, suggests that this phospholipid may possess a higher turnover rate than the other phospholipid classes examined. Human brain homogenates also possessed the ability to transfer fatty acid from lysophosphatidylcholine to lysophosphatidylethanolamine. In addition, we also present evidence that diacylglycerophospholipids can act as acyl donors for the transacylation of lysophospholipids. We have therefore demonstrated the presence of, and partially characterized, three enzymes that are involved in the metabolism of lysophospholipids in human brain. Our results suggest that lysophospholipase may be the major route by which lysophospholipids are removed from the cell membrane in human brain. However, all three enzymes likely play an important role in the remodeling of membrane composition and thereby contribute to the overall functioning of membrane-associated processes.

摘要

溶血磷脂是在膜磷脂的周转和分解过程中产生的。我们已经鉴定并部分表征了三种参与人脑中溶血磷脂代谢的酶,即溶血磷脂酶、溶血磷脂:酰基辅酶A酰基转移酶(酰基转移酶)和溶血磷脂:溶血磷脂转酰基酶(转酰基酶)。在活检和尸检的人脑中,每种酶都表现出相当的活性水平,尽管在所有情况下,人脑中的活性都略低于大鼠脑。所有这三种酶主要定位于颗粒部分,其中溶血磷脂酶活性最高,其次是酰基转移酶和转酰基酶。溶血磷脂酰胆碱对溶血磷脂酶和转酰基酶的Km值在微摩尔范围内,对酰基转移酶的Km值在毫摩尔范围内,而花生四烯酰辅酶A对酰基转移酶的Km值在微摩尔范围内。这三种酶的最适pH值不同,溶血磷脂酶在pH 8.0时活性最高,转酰基酶在pH 7.5时活性最高,酰基转移酶在pH 6.0时活性最高。溴苯甲酰溴和N-乙基马来酰亚胺均抑制溶血磷脂酶活性,对酰基转移酶和转酰基酶活性的抑制作用较小。二硫苏糖醇或EDTA的存在不影响任何一种酶的活性,尽管添加5 mM MgCl2或CaCl2可使颗粒状溶血磷脂酶的活性提高约两倍,但添加KCl则无此作用。转酰基活性受到辅酶A的刺激,激活的EC50为6.8 microM。酰基转移酶对花生四烯酰辅酶A的偏好比对棕榈酰辅酶A高约三倍,而不同溶血磷脂的酰化速率顺序为溶血磷脂酰肌醇>1-棕榈酰溶血磷脂酰胆碱>1-油酰溶血磷脂酰胆碱>>溶血磷脂酰丝氨酸>溶血磷脂酰乙醇胺。这一点,以及人脑中磷脂酶A2对磷脂酰肌醇的偏好,表明这种磷脂的周转率可能高于所检测的其他磷脂类别。人脑匀浆还具有将脂肪酸从溶血磷脂酰胆碱转移到溶血磷脂酰乙醇胺的能力。此外,我们还提供证据表明,二酰基甘油磷脂可以作为溶血磷脂转酰基作用的酰基供体。因此,我们已经证明了人脑中参与溶血磷脂代谢的三种酶的存在并对其进行了部分表征。我们的结果表明,溶血磷脂酶可能是人脑中溶血磷脂从细胞膜中去除的主要途径。然而,所有这三种酶可能在膜成分的重塑中发挥重要作用,从而有助于与膜相关过程的整体功能。

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