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长期α1-肾上腺素能阻断可减轻大鼠饮食诱导的血脂异常和高胰岛素血症。

Long-term alpha1-adrenergic blockade attenuates diet-induced dyslipidemia and hyperinsulinemia in the rat.

作者信息

Fajardo N, Deshaies Y

机构信息

Department of Physiology, School of Medicine, Laval University, Québec, Québec, Canada.

出版信息

J Cardiovasc Pharmacol. 1998 Dec;32(6):913-9. doi: 10.1097/00005344-199812000-00007.

Abstract

This study evaluated the ability of alpha1-adrenergic blockade to interfere with the development of diet-induced hyperlipidemia and deterioration of insulin action. Diets having extremely divergent effects on glucose and lipid metabolism were contrasted. Rats were fed for 4 weeks either a nonpurified diet (chow) or a hyperlipidemic (HL) purified diet containing 40% energy as sucrose, 40% as fat, and 20% as casein. Half of each dietary cohort was given the alpha1-adrenergic antagonist prazosin (3 mg/kg/day in the food). Blood was collected in the fasted state (10 h after food removal) and 2 h after the intake of a meal. In the fasted state, plasma triacylglycerols (TGs) were higher in rats fed the HL diet than in those given chow and were not affected by long-term treatment with prazosin. Postprandially, plasma TG increased twofold in the chow-fed group, with or without long-term prazosin. In contrast, prazosin reduced by more than half the eightfold increase in TG that followed intake of the high-fat meal (Diet x Blocker interaction; p < 0.002) in the HL cohort. The HL-fed animals also displayed fasting hypercholesterolemia (+30%; p < 0.0001), which was prevented by long-term treatment with prazosin. Likewise, the 50% increase in plasma cholesterol that followed meal ingestion only in the HL cohort was blunted by the alpha1-blocker (Diet x Blocker interaction; p < 0.001). Long-term prazosin also abolished fasting hyperinsulinemia in the HL cohort, whereas it did not alter fasting insulin in chow-fed animals (Diet x Blocker interaction; p < 0.005). Measurement of postprandial lipoprotein lipase activity in several tissues did not suggest the involvement of changes in the absolute availability of the enzyme as a determinant of the hypotriacylglycerolemic action of the alpha1-blocker. Thus long-term alpha1-adrenergic blockade, with minimal effects in rats fed a hypolipidemic diet, strongly attenuates several of the fasting and postprandial alterations in plasma variables of lipid and glucose metabolism induced by an extremely lipogenic diet.

摘要

本研究评估了α1-肾上腺素能阻滞剂干扰饮食诱导的高脂血症发展及胰岛素作用恶化的能力。对比了对葡萄糖和脂质代谢有极大不同影响的饮食。将大鼠分为两组,分别喂食4周非纯化饮食(普通饲料)或高脂(HL)纯化饮食,其中HL纯化饮食含40%能量的蔗糖、40%能量的脂肪和20%能量的酪蛋白。每组中的一半大鼠给予α1-肾上腺素能拮抗剂哌唑嗪(食物中3毫克/千克/天)。在禁食状态(去除食物后10小时)和进食后2小时采集血液。在禁食状态下,喂食HL饮食的大鼠血浆三酰甘油(TGs)高于喂食普通饲料的大鼠,且长期给予哌唑嗪对其无影响。餐后,无论是否长期给予哌唑嗪,普通饲料喂养组的血浆TG均增加两倍。相比之下,哌唑嗪使HL组大鼠摄入高脂餐后TG增加的八倍减少了一半以上(饮食×阻滞剂相互作用;p < 0.002)。喂食HL饮食的动物还表现出空腹高胆固醇血症(+30%;p < 0.0001),长期给予哌唑嗪可预防。同样,仅在HL组中进食后血浆胆固醇增加50%的情况也被α1-阻滞剂减弱(饮食×阻滞剂相互作用;p < 0.001)。长期给予哌唑嗪还消除了HL组的空腹高胰岛素血症,而对喂食普通饲料的动物的空腹胰岛素无影响(饮食×阻滞剂相互作用;p < 0.005)。对多个组织餐后脂蛋白脂肪酶活性的测量表明,酶的绝对可用性变化并非α1-阻滞剂降三酰甘油作用的决定因素。因此,长期的α1-肾上腺素能阻滞对喂食低脂饮食的大鼠影响极小,但能显著减轻由极高脂肪生成饮食诱导的脂质和葡萄糖代谢血浆变量的几种空腹和餐后改变。

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