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啮齿动物的肝脏生物转化及天然α-羟基胆汁酸23(R)-羟基鹅去氧胆酸的物理化学性质

Hepatic biotransformation in rodents and physicochemical properties of 23(R)-hydroxychenodeoxycholic acid, a natural alpha-hydroxy bile acid.

作者信息

Merrill J R, Schteingart C D, Hagey L R, Peng Y, Ton-Nu H T, Frick E, Jirsa M, Hofmann A F

机构信息

Division of Gastroenterology, University of California, San Diego, La Jolla 92093-0813, USA.

出版信息

J Lipid Res. 1996 Jan;37(1):98-112.

PMID:8820106
Abstract

The hepatic biotransformation in the rat and hamster of 23(R)-hydroxychenodeoxycholic acid (23(R)OH-CDCA), the alpha-hydroxy derivative of CDCA, was defined; some physiological and physicochemical properties were also assessed. 23(R)OH-CDCA was isolated from duck bile; [24-14C]23(R)OH-CDCA was synthesized. The compound was administered intravenously to anesthetized biliary fistula rats at doses of 1, 3, or 5 mu mol/kg-min and to hamsters at 3 mu mol/min-kg. Biliary bile acids and radioactivity were analyzed by thin-layer chromatography (TLC), high pressure liquid chromatography (HPLC), and gas chromatography-mass spectrometry (GC-MS). Recovery of radioactivity in bile was incomplete (50-70% of infused dose); some was also recovered as breath 14CO2. Radioactivity in bile was present as unchanged compound (25-50%, dose-dependent) and its conjugates (with taurine, with glycine, or with glucuronate). Nor-CDCA (C23) was present in bile (in both unconjugated and conjugated form), indicating that 23(R)OH-CDCA had undergone oxidative decarboxylation (alpha-oxidation) with loss of the C-24 carboxyl group. The alpha-oxidation was 20 +/- 5% (mean +/- SD) of administered dose in the rat and was not dose-dependent; in hamsters, alpha-oxidation was 35 +/- 8%. In rats, the S isomer of 23OH-CDCA also underwent alpha-oxidation (10 +/- 2%). Nor-CDCA also underwent 6beta-hydroxylation to form nor-alpha-muricholic acid, as well as reduction of its C-23 carboxyl group to form the C23 alcohol. The taurine conjugate of 23(R)OH-CDCA [23(R)OH-CDC-tau] was prepared synthetically and characterized by 1H-NMR. By surface tension measurements, it had a critical micellization concentration (CMC) of 3.5 mM (in 0.15 M Na+), as compared to 1.8 mM for CDC-taurine. Aqueous solubility of 23(R)OH-CDCA increased markedly above pH 5, compared to pH 7 for CDCA. When incubated with cholylglycine hydrolase, 23(R)OH-CDC-tau was deconjugated at a rate one-fourth that of CDC-tau. It is concluded that the presence of a 23(R)-hydroxyl group in a 3alpha, 7alpha-dihydroxy bile acid alters its metabolism in the rodent hepatocyte, as evidenced by inefficient conjugation with taurine or glycine, alpha-oxidation to nor (C23) bile acid, and reduction of the nor bile acid to the primary alcohol. The taurine conjugate of 23(R)OH-CDCA, a major biliary bile acid of marine mammals and wading birds, is a biological detergent with properties superior to those of the taurine conjugate of CDCA. Natural C23 nor-bile acids may be formed by alpha-oxidation of alpha-hydroxy C24 bile acids.

摘要

对鹅去氧胆酸(CDCA)的α-羟基衍生物23(R)-羟基鹅去氧胆酸(23(R)OH-CDCA)在大鼠和仓鼠体内的肝脏生物转化进行了研究;还评估了其一些生理和物理化学性质。23(R)OH-CDCA从鸭胆汁中分离得到;[24-¹⁴C]23(R)OH-CDCA经合成制得。该化合物以1、3或5 μmol/kg·min的剂量静脉注射给麻醉的胆瘘大鼠,以3 μmol/min·kg的剂量注射给仓鼠。通过薄层色谱法(TLC)、高压液相色谱法(HPLC)和气相色谱-质谱联用法(GC-MS)分析胆汁中的胆汁酸和放射性。胆汁中放射性的回收率不完全(注入剂量的50-70%);部分放射性也以呼出的¹⁴CO₂形式回收。胆汁中的放射性以未变化的化合物(25-50%,剂量依赖性)及其结合物(与牛磺酸、与甘氨酸或与葡萄糖醛酸结合)形式存在。去氧胆酸(Nor-CDCA,C23)存在于胆汁中(以未结合和结合形式),表明23(R)OH-CDCA发生了氧化脱羧(α-氧化),失去了C-24羧基。大鼠体内的α-氧化为给药剂量的20±5%(平均值±标准差),且不依赖于剂量;仓鼠体内的α-氧化为35±8%。在大鼠中,23OH-CDCA的S异构体也发生了α-氧化(10±2%)。Nor-CDCA还发生了6β-羟基化形成去氧-α-鼠胆酸,以及其C-23羧基还原形成C23醇。23(R)OH-CDCA的牛磺酸结合物[23(R)OH-CDC-牛磺酸]经合成制备并通过¹H-NMR进行了表征。通过表面张力测量,其临界胶束浓度(CMC)为3.5 mM(在0.15 M Na⁺中),而CDCA-牛磺酸为1.8 mM。与CDCA在pH 7时相比,23(R)OH-CDCA在pH 5以上时水溶性显著增加。当与胆酰甘氨酸水解酶一起孵育时,23(R)OH-CDC-牛磺酸的去结合速率是CDCA-牛磺酸的四分之一。得出的结论是,3α,7α-二羟基胆汁酸中23(R)-羟基的存在改变了其在啮齿动物肝细胞中的代谢,这表现为与牛磺酸或甘氨酸的结合效率低下、α-氧化为去氧(C23)胆汁酸以及去氧胆汁酸还原为伯醇。23(R)OH-CDCA的牛磺酸结合物是海洋哺乳动物和涉禽的主要胆汁胆汁酸,是一种性能优于CDCA牛磺酸结合物的生物洗涤剂。天然的C23去氧胆汁酸可能由α-羟基C24胆汁酸的α-氧化形成。

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