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纳洛酮可消除生长抑素对人体胰岛素诱导的低血糖所引发的催产素释放的抑制作用。

Naloxone abolishes the inhibiting effect of somatostatin on the release of oxytocin evoked by insulin-induced hypoglycemia in humans.

作者信息

Chiodera P, Gnudi A, Bianconi L, Capretti L, Fagnoni F, Volpi R, Coiro V

机构信息

Cattedra di Endocrinologia e Patologia Costituzionale, Università di Parma, Italy.

出版信息

Metabolism. 1989 Aug;38(8):709-11. doi: 10.1016/0026-0495(89)90053-x.

Abstract

The effect of somatostatin (SRIH) on the release of oxytocin (OT) in response to hypoglycemia during insulin tolerance test (ITT) was studied in seven normal men. Subjects were injected intravenously with 0.15 U/kg insulin alone (control test) or together with SRIH (4.1 micrograms/min x 90 min), naloxone (10 mg in an IV bolus), or the combination of the two substances. Plasma OT concentrations rose significantly during ITT; the OT response was significantly reduced by the treatment with SRIH and increased in the presence of naloxone. When both SRIH and naloxone were given, the OT response to hypoglycemia did not differ from that observed in the control test. These findings provide evidence that the effect of hypoglycemia on plasma OT levels is sensitive to the inhibition by SRIH and by naloxone-sensitive endogenous opioids. Because naloxone reversed the inhibiting effects of SRIH, an involvement of opioid peptides in SRIH action might be supposed. Alternatively, SRIH and naloxone-sensitive opioids might produce their inhibiting effects on OT rise in response to hypoglycemia through independent pathways.

摘要

在七名正常男性中研究了生长抑素(SRIH)对胰岛素耐量试验(ITT)期间低血糖反应中催产素(OT)释放的影响。受试者静脉注射单独的0.15 U/kg胰岛素(对照试验)或与SRIH(4.1微克/分钟×90分钟)、纳洛酮(静脉推注10毫克)或这两种物质的组合。ITT期间血浆OT浓度显著升高;SRIH治疗显著降低了OT反应,而在纳洛酮存在下OT反应增加。当同时给予SRIH和纳洛酮时,OT对低血糖的反应与对照试验中观察到的反应无差异。这些发现提供了证据,表明低血糖对血浆OT水平的影响对SRIH和纳洛酮敏感的内源性阿片类物质的抑制敏感。由于纳洛酮逆转了SRIH的抑制作用,可能推测阿片肽参与了SRIH的作用。或者,SRIH和纳洛酮敏感的阿片类物质可能通过独立途径对低血糖反应中OT升高产生抑制作用。

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