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精胺对蛋白激酶C的膜相关形式和膜插入形式的影响。

Effect of spermine on membrane-associated and membrane-inserted forms of protein kinase C.

作者信息

Moruzzi M S, Marverti G, Piccinini G, Frassineti C, Monti M G

机构信息

Istituto di Chimica Biologica, Università di Modena, Italy.

出版信息

Mol Cell Biochem. 1993 Jul 7;124(1):1-9. doi: 10.1007/BF01096375.

Abstract

Protein kinase C is reported to exist in two membrane-bound states: a reversible one which can be dissociated by calcium chelators (membrane-associated form) and an irreversible one which is chelator stable (membrane-inserted form). In the present work the effects of a naturally occurring polyamine (spermine) on the membrane-associated and membrane-inserted forms of protein kinase C were investigated using a reconstituted system consisting of partially purified protein kinase C from rat brain and phospholipid vesicles of defined composition. The active membrane-bound complex was conveniently determined by its ability to bind radioactive phorbol ester with an exact 1:1 stoichiometry. Our experimental data show that, in the absence of calcium ions, the amount of enzyme bound to phospholipids vesicles was dramatically reduced by the presence of spermine whereas the PDBu binding affinity was not significantly affected. The addition of the divalent cation increased the affinity of phorbol ester for the active complex but had no effect on Nmax; spermine added in this experimental conditions was no longer able to decrease the total number of enzyme molecules bound to liposomes. Moreover gel filtration experiments of the protein kinase C-phospholipids complex formed in the presence of calcium, indicated that polyamine added during the association process was able to reduce the extent of enzyme insertion into liposomes. Since the increase in phospholipid concentration resulted in a higher level of non-dissociable protein kinase C-liposomes complex we propose that spermine, complexing to membrane binding sites both in the absence and in the presence of Ca++, could promote binding conditions that oppose to the formation of the inserted form of the enzyme. As a consequence the distribution between the reversible and the irreversible membrane-bound forms of protein kinase C is affected.

摘要

据报道,蛋白激酶C以两种膜结合状态存在:一种是可逆的,可被钙螯合剂解离(膜相关形式);另一种是不可逆的,对螯合剂稳定(膜插入形式)。在本研究中,使用由大鼠脑部分纯化的蛋白激酶C和特定组成的磷脂囊泡组成的重组系统,研究了天然存在的多胺(精胺)对蛋白激酶C的膜相关形式和膜插入形式的影响。通过其以精确的1:1化学计量比结合放射性佛波酯的能力,方便地测定活性膜结合复合物。我们的实验数据表明,在没有钙离子的情况下,精胺的存在会显著降低与磷脂囊泡结合的酶量,而佛波酯的结合亲和力没有受到显著影响。二价阳离子的加入增加了佛波酯对活性复合物的亲和力,但对Nmax没有影响;在该实验条件下加入的精胺不再能够减少与脂质体结合的酶分子总数。此外,在钙存在下形成的蛋白激酶C - 磷脂复合物的凝胶过滤实验表明,在结合过程中加入的多胺能够降低酶插入脂质体的程度。由于磷脂浓度的增加导致了更高水平的不可解离的蛋白激酶C - 脂质体复合物,我们提出精胺在有无Ca++的情况下都与膜结合位点结合,可能促进与酶插入形式形成相反的结合条件。因此,蛋白激酶C的可逆和不可逆膜结合形式之间的分布受到影响。

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