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单(S)-羟基脂肪酸:胞质肌动蛋白的新型配体。

Mono (S) hydroxy fatty acids: novel ligands for cytosolic actin.

作者信息

Kang L T, Vanderhoek J Y

机构信息

Department of Biochemistry and Molecular Biology, The George Washington University Medical Center, Washington, DC 20037, USA.

出版信息

J Lipid Res. 1998 Jul;39(7):1476-82.

PMID:9684751
Abstract

The ubiquitous hydroxylated fatty acids derived from arachidonic acid (HETEs) or linoleic acid (HODEs) exhibit diverse biological effects including chemotaxis, cell proliferation, and modulation of several enzymatic pathways, including the 5-lipoxygenase leading to the inflammatory leukotrienes. It was observed that 12(S)- and 15(S)-HETE and 13(S)-HODE (12- and 15-lipoxygenase-derived metabolites, respectively) inhibited the 5-lipoxygenase present in rat basophilic leukemia (RBL-1) cell homogenates whereas the 15(R) chiral enantiomer and the nonhydroxylated linoleic, oleic, and stearic acids were either less potent or ineffective. In examining the mechanism of this inhibition, the relative effectiveness of several fatty acids in displacing [3H]15-HETE bound to cytosol preparations were compared and the results indicated that these (S) hydroxy fatty acids and 5(S)-HETE were significantly more potent than either the 15(R) enantiomer, 15(S)-HETE methyl ester, arachidonic acid, or prostaglandin F2alpha. In order to identify the protein(s) that specifically binds HETEs, 15(S)-HETE biotin hydrazide was used as a probe to detect any HETE-protein complexes as this compound both inhibited the 5-lipoxygenase and interfered with the binding of [3H]15-HETE to cytosol preparations. SDS-PAGE analysis and chemiluminescent detection revealed that the major cytosolic proteins that bound this biotinylated probe had molecular masses of 43 and 51 kD. Fatty acid competition experiments indicated that the order of effectiveness in displacing this probe from these proteins was 13(S)-HODE > 5(S)-HETE approximately equal to 15(S)-HETE > > stearic acid approximately equal to arachidonic acid approximately equal to 15(R)-HETE. Amino acid sequence analysis showed that the 43 kD protein was actin. These findings suggest the possibility that actin may play a major role in the biological effects of monohydroxylated metabolites derived from cellular 5-, 12-, and 15-lipoxygenases.

摘要

源自花生四烯酸的普遍存在的羟基化脂肪酸(HETEs)或亚油酸(HODEs)具有多种生物学效应,包括趋化性、细胞增殖以及对多种酶促途径的调节,其中包括导致炎性白三烯的5-脂氧合酶途径。据观察,12(S)-和15(S)-HETE以及13(S)-HODE(分别为12-和15-脂氧合酶衍生的代谢产物)抑制大鼠嗜碱性白血病(RBL-1)细胞匀浆中的5-脂氧合酶,而15(R)手性对映体以及未羟基化的亚油酸、油酸和硬脂酸的抑制作用较弱或无抑制作用。在研究这种抑制机制时,比较了几种脂肪酸置换与胞质溶胶制剂结合的[3H]15-HETE的相对效力,结果表明这些(S)羟基脂肪酸和5(S)-HETE比15(R)对映体、15(S)-HETE甲酯、花生四烯酸或前列腺素F2α的效力显著更高。为了鉴定特异性结合HETEs的蛋白质,使用15(S)-HETE生物素酰肼作为探针来检测任何HETE-蛋白质复合物,因为该化合物既抑制5-脂氧合酶,又干扰[3H]15-HETE与胞质溶胶制剂的结合。SDS-PAGE分析和化学发光检测显示,结合该生物素化探针的主要胞质蛋白的分子量为43和51 kD。脂肪酸竞争实验表明,将该探针从这些蛋白质上置换下来的效力顺序为13(S)-HODE > 5(S)-HETE ≈ 15(S)-HETE >> 硬脂酸 ≈ 花生四烯酸 ≈ 15(R)-HETE。氨基酸序列分析表明,43 kD的蛋白质是肌动蛋白。这些发现提示肌动蛋白可能在细胞5-、12-和15-脂氧合酶衍生的单羟基化代谢产物的生物学效应中起主要作用。

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