SOMATOSTATIN RECEPTORS ON THYROTROPIN-SECRETING PITUITARY-ADENOMAS - COMPARISON WITH THE INHIBITORY EFFECTS OF OCTREOTIDE UPON INVIVO AND INVITRO HORMONAL SECRETIONS

被引:82
作者
BERTHERAT, J
BRUE, T
ENJALBERT, A
GUNZ, G
RASOLONJANAHARY, R
WARNET, A
JAQUET, P
EPELBAUM, J
机构
[1] CTR P BROCA, INSERM, U159, 2 TER RUE ALESIA, F-75014 PARIS, FRANCE
[2] UER MED NORD, INSERM U297, MARSEILLE, FRANCE
[3] HOP LARIBOISIERE, F-75475 PARIS 10, FRANCE
关键词
D O I
10.1210/jc.75.2.540
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The in vivo and in vitro inhibitory effects of a somatostatin (SRIH) analog, octreotide, upon TSH, alpha-subunit, GH, and PRL have been studied, as well as SRIH receptors and their coupling to adenylate cyclase, in nine TSH-secreting pituitary adenomas. From in vivo and cell culture studies, the TSH- and alpha-subunit-secreting adenomas appeared heterogeneous, with four out of the nine tumors cosecreting GH and/or PRL. A single sc injection of octreotide (100-mu-g) lowered plasma concentration of TSH by 40 +/- 5% (mean +/- SE of 5), of alpha-subunit by 27 +/- 9% (n = 5), of GH by 60 +/- 5% (n = 4), and of PRL by 27 +/- 9% (n = 4). In cells cultures, octreotide (10(-8) mol/L) inhibited equally TSH, alpha-subunit, and GH release. I-125-Tyr0-DTrp8-SRIH binding sites were measurable in the nine TSH-secreting adenomas either on membrane preparations (n = 6; B(max): 152 +/- 73 fmol/mg protein) or on frozen sections by radioautography (n = 3). Their density was variable among TSH adenomas and was lower than that measured in GH-secreting adenomas but higher than in nonfunctioning tumors. Two out of three TSH-secreting adenoma displayed an heterogeneous distribution of I-125-Tyr0-DTrp8-SRIH binding sites. I-125-Tyro-DTrp8-SRIH specific binding was inhibited by guanosine triphosphate (GTP: 10(-4) mol/L). SRIH inhibited adenylate cyclase in 5/5 TSH-secreting adenomas and a good correlation (r = 0.92, P < 0.02) was found between I-125-Tyr0-DTrp8-SRIH binding capacity (B(max)) and maximal adenylate cyclase inhibition by SRIH. These results demonstrate in vivo and in vitro inhibition of TSH, alpha-subunit, PRL, and GH secretion by octreotide in TSH-secreting pituitary adenomas. Functional SRIH receptors are present on these tumors and the effect of SRIH on hormonal secretion could be mediated, at least in part, by inhibition of adenylate cyclase. These findings support the medical treatment of this rare type of tumors by SRIH analogs.
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页码:540 / 546
页数:7
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