GALANIN BINDING-SITES IN RAT GASTRIC AND JEJUNAL SMOOTH-MUSCLE MEMBRANE PREPARATIONS

被引:68
作者
ROSSOWSKI, WJ [1 ]
ROSSOWSKI, TM [1 ]
ZACHARIA, S [1 ]
ERTAN, A [1 ]
COY, DH [1 ]
机构
[1] TULANE UNIV,SCH MED,GASTROENTEROL SECT,NEW ORLEANS,LA 70112
关键词
Galanin; Galanin binding sites; Galanin fragments; Rat jejunal smooth muscle membranes; Rat stomach smooth muscle membranes;
D O I
10.1016/0196-9781(90)90089-N
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
Receptors for galanin in membranes from the rat gastric and jejunal smooth muscle were studied using [125I] radioiodinated synthetic porcine galanin. Specific binding was time and temperature dependent. At 32°C radioligand was degraded in the presence of smooth muscle membranes in a time-dependent manner. At optimal experimental conditions, the equilibrium binding analyses showed the presence of a single population of high affinity binding sites in both the rat stomach and jejunum (Kd value of 2.77±0.78 nM and 4.93±1.74 nM for stomach and jejunal smooth muscle membranes, respectively). The concentration of the high affinity binding sites was 58.19±11.04 and 32.36±5.68 fmol/mg protein, for gastric and jejunal preparations, respectively. Specific binding was completely inhibited by 10-6 M of nonradioactive galanin; was 75% blocked by 1 μM of galanin(9-29); it was 10% blocked by 1 μM of galanin(15-29). Galanin(1-15) at a concentration of 1 μM was ineffective for inhibiting [125I]galanin binding. Deletion of four C-terminal amino acid residues from galanin(9-29) to give galanin(9-25) also resulted in almost complete loss of affinity. Radioiodinated galanin and N-terminally deleted fragments had receptor binding potency in the following order: galanin(1-29) > galanin(9-29) > galanin(15-29). We conclude that the C-terminal part of the galanin chain is important for the rat gastric and jejunal smooth muscle membrane receptor recognition and binding and that N-terminal amino acid sequences are probably not so important, since galanin(1-15) was not active but galanin(9-29) retained most of the receptor binding activity. © 1990.
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页码:333 / 338
页数:6
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