学术探索
学术期刊
新闻热点
数据分析
智能评审

BINDING-SITES FOR ISLET AMYLOID POLYPEPTIDE IN MAMMALIAN LUNG - SPECIES VARIATION AND EFFECTS ON ADENYLYL-CYCLASE

被引:8
作者
BHOGAL, R [1 ]
SMITH, DM [1 ]
OWJI, AA [1 ]
BLOOM, SR [1 ]
机构
[1] HAMMERSMITH HOSP,ROYAL POSTGRAD MED SCH,DEPT MED,ENDOCRINE UNIT,LONDON W12 0NN,ENGLAND
来源
CANADIAN JOURNAL OF PHYSIOLOGY AND PHARMACOLOGY | 1995年 / 73卷 / 07期
关键词
ISLET AMYLOID POLYPEPTIDE; AMYLIN; CALCITONIN GENE RELATED PEPTIDE; LUNG; RECEPTORS;
D O I
10.1139/y95-145
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Islet amyloid polypeptide (IAPP) and calcitonin gene related peptide (CGRP) share a 47% sequence homology. LAPP can interact with adenylyl cyclase coupled CGRP receptors. We have examined [I-125]IAPP binding in mouse, pig, and guinea pig lung membranes in competition with IAPP, CORP, and CGRP(8-37). Three types of site were shown by order of potency: (i) mouse, IAPP > CGRP(8-37) much greater than CGRP; (ii) pig, CGRP > IAPP > CGRP(8-37); and (iii) guinea pig, CORP = IAPP = CGRP(8-37). Chemical cross-linking of [I-125]IAPP and [I-125]CGRP binding sites in lung demonstrated that both sites had similar molecular weights in any one species but differed across species, i.e., mouse M(r) = 70 000 and 98 000; pig M(r) = 68 000, 56 000, and 47 000; and guinea pig M(r) = 106 000 and 56 000. Adenylyl cyclase activity was stimulated by forskolin and A1Cl(3)-NaF in rat, mouse, pig, and guinea pig membranes. Only in mouse and pig were CORP and IAPP able to stimulate adenylyl cyclase activity. In mouse lung CGRP and LAPP stimulated adenylyl cyclase activity with EC(50) values of 642 +/- 222 nM (n = 4) and 325 +/- 115 nM (n = 4), respectively. In pig lung membranes EC(50) values were 5.7 +/- 0.3 nM (n = 4) for CGRP and 1230 +/- 1130 nM (n = 4) far IAPP. Thus IAPP either did not stimulate adenylyl cyclase activity in these lung membranes or did so with a low potency.
引用
收藏
页码:1030 / 1036
页数:7
相关论文
共 30 条
[21]   CALCITONIN GENE-RELATED PEPTIDE - MULTIPLE ACTIONS, MULTIPLE RECEPTORS [J].
POYNER, DR .
PHARMACOLOGY & THERAPEUTICS, 1992, 56 (01) :23-51
[22]   HIGHLY SENSITIVE ADENYLATE CYCLASE ASSAY [J].
SALOMON, Y ;
LONDOS, C ;
RODBELL, M .
ANALYTICAL BIOCHEMISTRY, 1974, 58 (02) :541-548
[23]   CALCITONIN GENE-RELATED PEPTIDE-BINDING SITES OF PORCINE CARDIAC MUSCLES AND CORONARY-ARTERIES - SOLUBILIZATION AND CHARACTERIZATION [J].
SANO, Y ;
HIROSHIMA, O ;
YUZURIHA, T ;
YAMATO, C ;
SAITO, A ;
KIMURA, S ;
HIRABAYASHI, T ;
GOTO, K .
JOURNAL OF NEUROCHEMISTRY, 1989, 52 (06) :1919-1924
[24]   CHARACTERIZATION OF AMYLIN BINDING-SITES IN A HUMAN HEPATOBLASTOMA CELL-LINE [J].
SHERIFF, S ;
FISCHER, JE ;
BALASUBRAMANIAM, A .
PEPTIDES, 1992, 13 (06) :1193-1199
[25]   REVERSAL OF THE INHIBITORY EFFECTS OF CALCITONIN-GENE-RELATED PEPTIDE (CGRP) AND AMYLIN ON INSULIN-SECRETION BY THE 8-37-FRAGMENT OF HUMAN CGRP [J].
SILVESTRE, RA ;
SALAS, M ;
DEGANO, P ;
PEIRO, E ;
MARCO, J .
BIOCHEMICAL PHARMACOLOGY, 1993, 45 (11) :2343-2347
[26]   PHOTOAFFINITY-LABELING OF RAT CALCITONIN GENE-RELATED PEPTIDE RECEPTORS AND ADENYLATE-CYCLASE ACTIVATION - IDENTIFICATION OF RECEPTOR SUBTYPES [J].
STANGL, D ;
MUFF, R ;
SCHMOLCK, C ;
FISCHER, JA .
ENDOCRINOLOGY, 1993, 132 (02) :744-750
[27]   CHARACTERIZATION AND PHOTOAFFINITY-LABELING OF A CALCITONIN GENE-RELATED PEPTIDE RECEPTOR SOLUBILIZED FROM HUMAN CEREBELLUM [J].
STANGL, D ;
BORN, W ;
FISCHER, JA .
BIOCHEMISTRY, 1991, 30 (35) :8605-8611
[28]   WHOLE-BODY AUTORADIOGRAPHY OF I-123 LABELED ISLET AMYLOID POLYPEPTIDE (IAPP) - ACCUMULATION IN THE LUNG PARENCHYMA AND IN THE VILLI OF THE INTESTINAL-MUCOSA IN RATS [J].
STRIDSBERG, M ;
TJALVE, H ;
WILANDER, E .
ACTA ONCOLOGICA, 1993, 32 (02) :155-159
[29]   COMPARATIVE-STUDY OF DISTRIBUTION AND BIOCHEMICAL-CHARACTERIZATION OF BRAIN CALCITONIN GENE-RELATED PEPTIDE RECEPTORS IN 5 DIFFERENT SPECIES [J].
WIMALAWANSA, SJ ;
ELKHOLY, AA .
NEUROSCIENCE, 1993, 54 (02) :513-519
[30]   AMYLIN INCREASES CYCLIC-AMP FORMATION IN L6 MYOCYTES THROUGH CALCITONIN GENE-RELATED PEPTIDE RECEPTORS [J].
ZHU, GC ;
DUDLEY, DT ;
SALTIEL, AR .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1991, 177 (02) :771-776
123