EFFECT OF PHOSPHOLIPASES AND PROTEASES ON THE [H-3] N6-(R)-PHENYLISOPROPYLADENOSINE ([H-3]R-PIA) BINDING TO ADENOSINE-A1-RECEPTORS FROM PIG CEREBRAL-CORTEX

被引：8

作者：

CASADO, V ^{[1
]}

MALLOL, J ^{[1
]}

LLUIS, C ^{[1
]}

CANELA, EI ^{[1
]}

FRANCO, R ^{[1
]}

机构：

[1] UNIV BARCELONA,SCH CHEM,DEPT BIOCHEM & PHYSIOL,MARTI & FRANQUES 1,E-08071 BARCELONA,SPAIN

来源：

JOURNAL OF CELLULAR BIOCHEMISTRY | 1991年 / 47卷 / 03期

关键词：

BRAIN CORTICAL MEMBRANES; RECEPTOR MODULATION; TRYPSIN; BINDING CAPACITY; CO-SOLUBILIZATION;

D O I：

10.1002/jcb.240470314

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The effect of phospholipases and proteases on the membrane-bound and solubilized A1 adenosine receptor has been studied. Phospholipids modulate the [H-3]N6-(R)-phenylisopropyladenosine binding to A1 adenosine receptors in crude membranes and in soluble preparations, because changes in the phospholipid environment decrease both the binding capacity and the affinity for the ligand. It has become clear that 1) there is co-solubilization of receptor and phospholipids; 2) the phospholipid requirements are different for the coupled and the uncoupled receptor; 3) a net charge in the polar head produced by phospholipase D prevents the agonist binding to the receptor-G protein complex; alternatively, when the whole polar head is removed by phospholipase C the uncoupled receptor is altered; and 4) the protease action upon the receptor suggests that receptor coupled to G protein is more protected by the membrane than the uncoupled receptor. In kinetic experiments performed on membranes it was demonstrated that phospholipase C and trypsin increased the K(d) value of the high-affinity state by modifying both k1 and k-1. In contrast they only modified the dissociation constant of the low-affinity state. In conclusion it should be noted that phospholipids play a key role for the binding of R-PIA to A1 adenosine receptor. Also, a different disposition within the membrane of the coupled and uncoupled receptor is encountered.

引用

页码：278 / 288

页数：11

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