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跨细胞生物合成有助于体内炎症反应期间白三烯的产生。

Transcellular biosynthesis contributes to the production of leukotrienes during inflammatory responses in vivo.

作者信息

Fabre Jean-Etienne, Goulet Jennifer L, Riche Estelle, Nguyen MyTrang, Coggins Kenneth, Offenbacher Steven, Koller Beverly H

机构信息

Department of Genetics, University of North Carolina Chapel Hill, 27599, USA.

出版信息

J Clin Invest. 2002 May;109(10):1373-80. doi: 10.1172/JCI14869.

Abstract

Leukotrienes are lipid mediators that evoke primarily proinflammatory responses by activating receptors present on virtually all cells. The production of leukotrienes is tightly regulated, and expression of 5-lipoxygenase, the enzyme required for the first step in leukotriene synthesis, is generally restricted to leukocytes. Arachidonic acid released from the cell membrane of activated leukocytes is rapidly converted to LTA(4) by 5-lipoxygenase. LTA(4) is further metabolized to either LTC(4) or LTB(4) by the enzyme LTC(4) synthase or LTA(4) hydrolase, respectively. Unlike 5-lipoxygenase, these enzymes are expressed in most tissues. This observation previously has led to the suggestion that LTA(4) produced by leukocytes may, in some cases, be delivered to other cell types before being converted into LTC(4) or LTB(4). While in vitro studies indicate that this process, termed transcellular biosynthesis, can lead to the production of leukotrienes, it has not been possible to determine the significance of this pathway in vivo. Using a series of bone marrow chimeras generated from 5-lipoxygenase- and LTA(4) hydrolase-deficient mice, we show here that transcellular biosynthesis contributes to the production of leukotrienes in vivo and that leukotrienes produced by this pathway are sufficient to contribute significantly to the physiological changes that characterize an ongoing inflammatory response.

摘要

白三烯是脂质介质,主要通过激活几乎所有细胞上存在的受体引发促炎反应。白三烯的产生受到严格调控,白三烯合成第一步所需的酶5-脂氧合酶的表达通常仅限于白细胞。从活化白细胞细胞膜释放的花生四烯酸被5-脂氧合酶迅速转化为LTA(4)。LTA(4)分别通过LTC(4)合酶或LTA(4)水解酶进一步代谢为LTC(4)或LTB(4)。与5-脂氧合酶不同,这些酶在大多数组织中都有表达。这一观察结果此前曾引发一种观点,即白细胞产生的LTA(4)在某些情况下可能在转化为LTC(4)或LTB(4)之前被传递给其他细胞类型。虽然体外研究表明这一过程(称为跨细胞生物合成)可导致白三烯的产生,但尚未确定该途径在体内的重要性。利用从5-脂氧合酶和LTA(4)水解酶缺陷小鼠产生的一系列骨髓嵌合体,我们在此表明跨细胞生物合成在体内对白三烯的产生有贡献,并且通过该途径产生的白三烯足以对正在进行的炎症反应所特有的生理变化做出显著贡献。

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