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白三烯在无血清培养中对小鼠转化型睾丸间质细胞增殖的抑制作用。

Inhibition of murine transformed Leydig cell proliferation by leukotrienes in serum-free culture.

作者信息

Nishii K, Nishizawa Y, Nishizawa Y, Matsumoto K, Sato B

机构信息

Third Department of Internal Medicine, Osaka University Hospital, Japan.

出版信息

Cancer Res. 1991 Oct 15;51(20):5573-8.

PMID:1655256
Abstract

We have previously shown that estrogen-dependent growth enhancement of murine transformed Leydig cells (B-1 F) is mediated through inhibition of arachidonic acid metabolite formation. In the present study, the growth-inhibitory ability of leukotrienes (LTs) on B-1 F cells in serum-free culture was directly addressed. All peptidyl LTs (LTC4, LTD4, and LTE4) inhibited B-1 F cell growth in a dose-dependent manner and exhibited maximum inhibition of DNA synthesis (60-80%) compared with that of untreated cells in a range of 10(-9) to 10(-8) M. To examine the mechanism of this LT-dependent inhibition, binding studies of LTD4 toward plasma membrane were conducted. Specific binding sites for LTD4 were identified. Scatchard analyses indicated the presence of a single class of high-affinity sites (Kd = 0.9 +/- 0.2 nM; maximum binding sites, 61 +/- 18 fmol/mg protein). This binding of LTD4 to the high-affinity site was markedly inhibited by ICI 198615, a specific inhibitor for LTD4. These results would suggest that inhibitory effects of LTs, at least LTD4, are elicited as a receptor-mediated event. In addition, this LT-dependent growth inhibition could not be blocked by simultaneous exposure of cells to estrogen, whereas estrogen partially protected arachidonic acid-dependent growth inhibition. Furthermore, treatment of cells with estrogen resulted in marked suppression of 5-lipoxygenase activity. Collectively, the present data clearly show that LTs play an important role as intermediates in an autocrine loop for B-1 F cells to exhibit estrogen-dependent growth.

摘要

我们之前已经表明,雌激素依赖性的小鼠转化型睾丸间质细胞(B-1 F)生长增强是通过抑制花生四烯酸代谢物的形成来介导的。在本研究中,我们直接探讨了白三烯(LTs)在无血清培养中对B-1 F细胞的生长抑制能力。所有肽基白三烯(LTC4、LTD4和LTE4)均以剂量依赖性方式抑制B-1 F细胞生长,与未处理细胞相比,在10^(-9)至10^(-8) M范围内对DNA合成的抑制作用最大(60 - 80%)。为了研究这种LT依赖性抑制的机制,我们进行了LTD4与质膜的结合研究。确定了LTD4的特异性结合位点。Scatchard分析表明存在一类单一的高亲和力位点(Kd = 0.9 ± 0.2 nM;最大结合位点,61 ± 18 fmol/mg蛋白)。LTD4与高亲和力位点的这种结合被LTD4的特异性抑制剂ICI 198615显著抑制。这些结果表明,LTs(至少LTD4)的抑制作用是作为一种受体介导的事件引发的。此外,细胞同时暴露于雌激素并不能阻断这种LT依赖性生长抑制,而雌激素可部分保护细胞免受花生四烯酸依赖性生长抑制。此外,用雌激素处理细胞会导致5-脂氧合酶活性显著抑制。总体而言,目前的数据清楚地表明,LTs在B-1 F细胞表现出雌激素依赖性生长的自分泌环中作为中间产物发挥重要作用。

相似文献

1
Inhibition of murine transformed Leydig cell proliferation by leukotrienes in serum-free culture.白三烯在无血清培养中对小鼠转化型睾丸间质细胞增殖的抑制作用。
Cancer Res. 1991 Oct 15;51(20):5573-8.
2
Competition of leukotrienes and ICI-198,615 for [3H]LTD4 binding sites in guinea pig lung membranes suggests the involvement of two LTD4 receptor subtypes.
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A comparison of leukotriene and prostaglandin binding to human myometrium.白三烯和前列腺素与人体子宫肌层结合的比较。
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Binding of radiolabeled high affinity antagonist to leukotriene D4 receptor in guinea pig lung membranes: interconversion of agonist-receptor binding affinity states.
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Effects of estrogen on cell proliferation and leukotriene formation in transformed mouse Leydig cells cultured under serum-free conditions.雌激素对在无血清条件下培养的转化小鼠睾丸间质细胞中细胞增殖和白三烯生成的影响。
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Guanyl-5'-yl-lmidodiphosphate regulation of ligand binding to LTD4 receptors on guinea pig lung membranes.鸟苷-5'-基-亚氨二磷酸对豚鼠肺膜上白三烯D4受体配体结合的调节作用
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Regulatory role of arachidonic acid-derived metabolites for proliferation of transformed murine Leydig cell in serum-free culture condition.
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Chemotherapy in experimental brain tumor, part 2: pretreatment with leukotriene C4 prolongs survival.实验性脑肿瘤的化疗,第2部分:白三烯C4预处理可延长生存期。
J Neurooncol. 1998 Jan;36(1):7-19. doi: 10.1023/a:1005866207158.