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肾上腺素对人体胰岛素释放抑制作用的受体机制。

A receptor mechanism for the inhibition of insulin release by epinephrine in man.

作者信息

Porte D

出版信息

J Clin Invest. 1967 Jan;46(1):86-94. doi: 10.1172/JCI105514.

Abstract

Normal adult men and women have been infused with epinephrine, 6 mug per minute, during lipolytic blockade with nicotinic acid, beta-adrenergic blockade with propranolol and Butoxamine, and alpha-adrenergic blockade with phentolamine. Epinephrine infusion was associated with low serum levels of immunoreactive insulin (IRI) except when phentolamine was given simultaneously. These findings are compatible with an alpha receptor mechanism for the epinephrine inhibition of insulin release. Phentolamine had no blocking effects on the tachycardia and widened pulse pressure or lipolytic stimulation by epinephrine, whereas both propranolol and Butoxamine blocked lipolysis, tachycardia, and widened pulse pressure. These findings are consistent with an alpha receptor blocking action for phentolamine and beta receptor blocking action for propranolol and Butoxamine. Inhibition of lipolysis by nicotinic acid did not alter IRI or glucose responses to epinephrine. It is concluded that the lipolytic effect of epinephrine is unrelated to its effects on IRI release. Lipolytic blockade by nicotinic acid also did not change IRI or glucose in fasting subjects or their responses to a glucose infusion, 300 mg per minute. These observations appear to conflict with the Randle hypothesis (the glucose-fatty acid cycle) and raise some doubt as to whether plasma FFA concentrations are direct determinants of glucose or IRI concentrations in normal man.

摘要

在使用烟酸进行脂解阻断、使用普萘洛尔和布托沙明进行β-肾上腺素能阻断以及使用酚妥拉明进行α-肾上腺素能阻断的过程中,对正常成年男性和女性以每分钟6微克的速度输注肾上腺素。除了同时给予酚妥拉明的情况外,输注肾上腺素与低血清免疫反应性胰岛素(IRI)水平相关。这些发现与肾上腺素抑制胰岛素释放的α受体机制相符。酚妥拉明对肾上腺素引起的心动过速、脉压增宽或脂解刺激没有阻断作用,而普萘洛尔和布托沙明都能阻断脂解、心动过速和脉压增宽。这些发现与酚妥拉明的α受体阻断作用以及普萘洛尔和布托沙明的β受体阻断作用一致。烟酸对脂解的抑制并未改变IRI或对肾上腺素的葡萄糖反应。得出的结论是,肾上腺素的脂解作用与其对IRI释放的作用无关。烟酸对脂解的阻断在空腹受试者中也未改变IRI或葡萄糖水平,或其对每分钟300毫克葡萄糖输注的反应。这些观察结果似乎与兰德尔假说(葡萄糖-脂肪酸循环)相矛盾,并对血浆游离脂肪酸浓度是否是正常男性中葡萄糖或IRI浓度的直接决定因素提出了一些疑问。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5ed9/297023/ba0aa75376cc/jcinvest00229-0105-a.jpg

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