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豆甾醇可降低大鼠血浆胆固醇水平,并抑制其肝脏合成及肠道吸收。

Stigmasterol reduces plasma cholesterol levels and inhibits hepatic synthesis and intestinal absorption in the rat.

作者信息

Batta Ashok K, Xu Guorong, Honda Akira, Miyazaki Teruo, Salen Gerald

机构信息

Department of Medicine, UMDNJ-NJ Medical School, Newark, NJ 07103, USA.

出版信息

Metabolism. 2006 Mar;55(3):292-9. doi: 10.1016/j.metabol.2005.08.024.

Abstract

Plant sterols compete with cholesterol (cholest-5-en-3beta-ol) for intestinal absorption to limit absorption and lower plasma concentrations of cholesterol. Stigmasterol (24-ethyl-cholesta-5,22-dien-3beta-ol; Delta(22) derivative of sitosterol [24-ethyl-cholest-5-en-3beta-ol]), but not campesterol (24-methyl-cholest-5-en-3beta-ol) and sitosterol, is reported to inhibit cholesterol biosynthesis via inhibition of sterol Delta(24)-reductase in human Caco-2 and HL-60 cell lines. We studied the effect of feeding 0.5% stigmasterol on plasma and liver sterols and intestinal cholesterol and sitosterol absorption in 12 wild-type Kyoto (WKY) and 12 Wistar rats. After 3 weeks of feeding, cholesterol and sitosterol absorption was determined in 6 rats from each group by plasma dual-isotope ratio method. After 3 more weeks, plasma and hepatic sterols and hepatic enzyme activities were determined in all rats. After feeding stigmasterol, baseline plasma cholesterol was 1.3 times and plant sterols 3 times greater in WKY compared with Wistar rats. Stigmasterol feeding lowered plasma cholesterol by approximately 11%, whereas plasma campesterol and sitosterol levels were virtually unchanged in both rat strains, and stigmasterol constituted 3.2% of plasma sterols in WKY rats and 1% in Wistar rats. After 6 weeks of feeding, cholesterol and sitosterol absorption decreased 23% and 30%, respectively, in WKY, and 22% and 16%, respectively, in the Wistar rats as compared with untreated rats. The intestinal bacteria in both rat strains metabolized stigmasterol to mainly the 5beta-H stanol (>40%), with only small amounts of 5alpha-H derivative (approximately 1.5%), whereas the C-22 double bond was resistant to bacterial metabolism. Hepatic stigmasterol levels increased from 11 microg/g liver tissue to 104 mug/g in WKY rats and from 5 microg/g liver tissue to 21 microg/g in Wistar rats. 3-Hydroxy-3-methylglutaryl coenzyme A reductase activity was suppressed 4-fold in the WKY and almost 1.8-fold in Wistar rats, cholesterol 7alpha-hydroxylase activity was suppressed 1.6-fold in the WKY and 3.5-fold in Wistar rats, whereas cholesterol 27-hydroxylase activity was unchanged after feeding. In conclusion, stigmasterol, when fed, lowers plasma cholesterol levels, inhibits intestinal cholesterol and plant sterol absorption, and suppresses hepatic cholesterol and classic bile acid synthesis in Wistar as well as WKY rats. However, plasma and hepatic incorporation of stigmasterol is low.

摘要

植物甾醇与胆固醇(胆甾 - 5 - 烯 - 3β - 醇)竞争肠道吸收,以限制胆固醇的吸收并降低血浆胆固醇浓度。据报道,豆甾醇(24 - 乙基 - 胆甾 - 5,22 - 二烯 - 3β - 醇;谷甾醇[24 - 乙基 - 胆甾 - 5 - 烯 - 3β - 醇]的Δ(22)衍生物),而非菜油甾醇(24 - 甲基 - 胆甾 - 5 - 烯 - 3β - 醇)和谷甾醇,可通过抑制人Caco - 2和HL - 60细胞系中的甾醇Δ(24) - 还原酶来抑制胆固醇生物合成。我们研究了给12只野生型京都(WKY)大鼠和12只Wistar大鼠喂食0.5%豆甾醇对血浆和肝脏甾醇以及肠道胆固醇和谷甾醇吸收的影响。喂食3周后,通过血浆双同位素比率法测定每组6只大鼠的胆固醇和谷甾醇吸收情况。再过3周后,测定所有大鼠的血浆和肝脏甾醇以及肝脏酶活性。喂食豆甾醇后,WKY大鼠的基线血浆胆固醇是Wistar大鼠的1.3倍,植物甾醇是3倍。喂食豆甾醇可使血浆胆固醇降低约11%,而两种大鼠品系的血浆菜油甾醇和谷甾醇水平基本不变,在WKY大鼠中豆甾醇占血浆甾醇的3.2%,在Wistar大鼠中占1%。喂食6周后,与未处理的大鼠相比,WKY大鼠的胆固醇和谷甾醇吸收分别降低了23%和30%,Wistar大鼠分别降低了22%和16%。两种大鼠品系的肠道细菌将豆甾醇主要代谢为5β - H甾烷醇(>40%),只有少量的5α - H衍生物(约1.5%),而C - 22双键对细菌代谢具有抗性。WKY大鼠肝脏中的豆甾醇水平从11微克/克肝组织增加到104微克/克,Wistar大鼠从5微克/克肝组织增加到21微克/克。3 - 羟基 - 3 - 甲基戊二酰辅酶A还原酶活性在WKY大鼠中被抑制了4倍,在Wistar大鼠中几乎被抑制了1.8倍,胆固醇7α - 羟化酶活性在WKY大鼠中被抑制了1.6倍,在Wistar大鼠中被抑制了3.5倍,而喂食后胆固醇27 - 羟化酶活性未改变。总之,喂食豆甾醇可降低Wistar大鼠和WKY大鼠的血浆胆固醇水平,抑制肠道胆固醇和植物甾醇吸收,并抑制肝脏胆固醇和经典胆汁酸合成。然而,豆甾醇在血浆和肝脏中的掺入量较低。

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