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Selective inhibition of cholesterol synthesis by cell-free preparations of rat liver by using inhibitors of cytoplasmic acetoacetyl-coenzyme A thiolase.

机译：通过使用细胞质乙酰乙酰辅酶A硫解酶的抑制剂通过无细胞制备大鼠肝脏来选择性抑制胆固醇的合成。

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摘要

Cytoplasmic acetoacetyl-CoA thiolase (acetyl-CoA C-acetyltransferase, EC 2.3.1.9) was partially purified from rat liver. The enzyme was irreversibly inactivated by 4-bromocrotonyl-CoA, but-3-ynoyl-CoA, pent-3-ynoyl-CoA and dec-3-ynoyl-CoA. In the case of the alk-3-ynoyl-CoA esters the potency as alkylating agents of acetoacetyl-CoA thiolase decreased with increased chain length of the alk-3-ynoyl moiety. Advantage was taken of the specific action of alk-3-ynoyl-CoA esters on acetoacetyl-CoA thiolase to show that in a postmitochondrial fraction from rat liver they are effective inhibitors of cholesterol synthesis from sodium [2-14C]acetate under conditions when mevalonate conversion into cholesterol and fatty acid synthesis are unafffected. Short-chain alk-3-ynoic acids have little effect on sterol synthesis, although dec-3-ynoic acid is an effective inhibitor owing to its conversion into the CoA ester by the microsomal fatty acyl-CoA synthetase.

机译：从大鼠肝脏中部分纯化了细胞质的乙酰乙酰基-CoA硫解酶（乙酰基-CoA C-乙酰基转移酶，EC 2.3.1.9）。该酶被4-溴巴豆酰基-CoA，丁-3-炔酰基-CoA，戊-3-炔酰基-CoA和癸-3-炔酰基-CoA不可逆地灭活。在烷-3-炔酰基-CoA酯的情况下，作为乙酰乙酰基-CoA硫解酶的烷基化剂的效力随着烷-3-炔基部分的链长的增加而降低。利用了烷-3-炔酰基-CoA酯对乙酰乙酰基-CoA硫解酶的特异性作用，显示在大鼠肝脏的线粒体后级分中，它们在甲羟戊酸条件下是有效的抑制剂[2-14C]乙酸钠合成胆固醇转化为胆固醇和脂肪酸合成不受影响。短链烷-3-炔酸对甾醇的合成几乎没有影响，尽管癸-3-炔酸是一种有效的抑制剂，因为它通过微粒体脂肪酰基辅酶A合成酶转化为CoA酯。

著录项

期刊名称 Biochemical Journal
作者
D P Bloxham;
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作者单位

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年(卷),期 1975(147),3
年度 1975
页码 531–539
总页数 9
原文格式 PDF
正文语种
中图分类分子生物学;
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专利

1. Selective inhibition of cholesterol synthesis by cell-free preparations of rat liver by using inhibitors of cytoplasmic acetoacetyl-coenzyme A thiolase. [J] . D P Bloxham The biochemical journal . 1975,第3期

机译：通过使用细胞质乙酰乙酰辅酶A硫解酶的抑制剂，通过无细胞制备大鼠肝脏来选择性抑制胆固醇的合成。
2. A fraction derived from brewer's yeast inhibits cholesterol synthesis by rat liver preparations in vitro [J] . D. V. Kaufman, E. Neville, E. S. Holdsworth The British Journal of Nutrition . 2007,第2期

机译：来自啤酒酵母的级分在体外通过大鼠肝脏制剂抑制胆固醇的合成
3. Mitochondrial toxicity of selective COX-2 inhibitors via inhibition of oxidative phosphorylation (ATP synthesis) in rat liver mitochondria [J] . Syed Muzeeb, Skonberg Christian, Hansen Steen Honore Toxicology in vitro: an international journal published in association with BIBRA . 2016,第Null期

机译：选择性COX-2抑制剂通过抑制大鼠肝线粒体中的氧化磷酸化（ATP合成）的线粒体毒性
4. Evaluation of Cholesterol Absorption Inhibition of Anti NPC1L1 IgY by ~3H-Labeled Cholesterol in Sprague-Dawley Rats [C] . Sang Hyun Park, Hayu Tyas Utami, Jaeyoung Cho, 8th International Conference on Isotopes 2014 . 2014

机译：〜3H标记的胆固醇对Sprague-Dawley大鼠的胆固醇吸收抗NPC1L1 IgY的评估
5. In search of selective and potent Golgi alpha-mannosidase II inhibitors as potential anticancer agents: Synthesis of 3-substituted-swainsonine analogs and preparation of immobilized swainsonine analogs on solid support. [D] . Guo, Luyi. 2003

机译：寻找选择性和有效的高尔基α-甘露糖苷酶II抑制剂作为潜在的抗癌药：3-取代-swainsonine类似物的合成和在固体支持物上固定的swainsonine类似物的制备。
6. The effect of some cofactors on the synthesis of fatty acids and cholesterol in cell-free preparations of rat liver [O] . K. Fletcher, N. B. Myant 1961

机译：某些辅助因子对大鼠肝无细胞制剂中脂肪酸和胆固醇合成的影响
7. Selective inhibition of cholesterol synthesis by cell-free preparations of rat liver by using inhibitors of cytoplasmic acetoacetyl-coenzyme A thiolase. [O] . Bloxham, D P 1975

机译：通过使用细胞质乙酰乙酰辅酶A硫解酶的抑制剂，通过无细胞制备大鼠肝脏来选择性抑制胆固醇的合成。

Selective inhibition of cholesterol synthesis by cell-free preparations of rat liver by using inhibitors of cytoplasmic acetoacetyl-coenzyme A thiolase.

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