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1
Blocking activator protein-1 activity, but not activating retinoic acid response element, is required for the antitumor promotion effect of retinoic acid.维甲酸的抗肿瘤促进作用需要阻断激活蛋白-1的活性,而不是激活维甲酸反应元件。
Proc Natl Acad Sci U S A. 1997 May 27;94(11):5826-30. doi: 10.1073/pnas.94.11.5826.
2
Inhibition of tumor promoter-induced transformation by retinoids that transrepress AP-1 without transactivating retinoic acid response element.通过反式抑制AP-1而不反式激活视黄酸反应元件的类视黄醇对肿瘤启动子诱导的转化的抑制作用。
Cancer Res. 1996 Feb 1;56(3):483-9.
3
Retinoic acid (RA) receptor transcriptional activation correlates with inhibition of 12-O-tetradecanoylphorbol-13-acetate-induced ornithine decarboxylase (ODC) activity by retinoids: a potential role for trans-RA-induced ZBP-89 in ODC inhibition.维甲酸(RA)受体转录激活与类视黄醇抑制12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯诱导的鸟氨酸脱羧酶(ODC)活性相关:反式维甲酸诱导的ZBP - 89在ODC抑制中的潜在作用。
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4
Lack of effect of retinoic acid and fluocinolone acetonide on mirex tumor promotion indicates a novel mirex mechanism.视黄酸和丙酮缩氟氢羟龙对灭蚁灵肿瘤促进作用无效表明存在一种新的灭蚁灵作用机制。
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5
Inhibition of 7-bromomethylbenz[a]anthracene-promoted mouse skin tumor formation by retinoic acid and dexamethasone.维甲酸和地塞米松对7-溴甲基苯并[a]蒽促进的小鼠皮肤肿瘤形成的抑制作用。
Cancer Res. 1983 Jul;43(7):3045-9.
6
Two-stage tumor promotion in mouse skin: an alternative interpretation.小鼠皮肤中的两阶段肿瘤促进作用:一种不同的解释。
J Natl Cancer Inst. 1985 Apr;74(4):735-40.
7
In vivo long-term effects of retinoic acid exposure in utero on induced tumours in adult mouse skin.孕期暴露于视黄酸对成年小鼠皮肤诱导肿瘤的体内长期影响。
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8
Retinoic acid receptor- and retinoid X receptor-selective retinoids activate signaling pathways that converge on AP-1 and inhibit squamous differentiation in human bronchial epithelial cells.维甲酸受体和类视黄醇X受体选择性类视黄醇激活汇聚于AP-1的信号通路,并抑制人支气管上皮细胞的鳞状分化。
Cell Growth Differ. 1996 Aug;7(8):997-1004.
9
Identification of a novel class of retinoic acid receptor beta-selective retinoid antagonists and their inhibitory effects on AP-1 activity and retinoic acid-induced apoptosis in human breast cancer cells.一类新型视黄酸受体β选择性类视黄醇拮抗剂的鉴定及其对人乳腺癌细胞中AP-1活性和视黄酸诱导凋亡的抑制作用。
J Biol Chem. 1999 May 28;274(22):15360-6. doi: 10.1074/jbc.274.22.15360.
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Inhibitors of both nuclear factor-kappaB and activator protein-1 activation block the neoplastic transformation response.核因子-κB和活化蛋白-1激活的抑制剂均可阻断肿瘤转化反应。
Cancer Res. 1997 Aug 15;57(16):3569-76.

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本文引用的文献

1
Progressive elevation of ap-1 activity during preneoplastic-to-neoplastic progression as modeled in mouse jb6 cell variants.在小鼠JB6细胞变体模型中,从癌前病变到肿瘤形成过程中ap-1活性的逐步升高。
Int J Oncol. 1995 Aug;7(2):359-64. doi: 10.3892/ijo.7.2.359.
2
Inhibitory effects of ascorbic acid on AP-1 activity and transformation of JB6 cells.抗坏血酸对AP-1活性及JB6细胞转化的抑制作用。
Int J Oncol. 1996 Feb;8(2):389-93. doi: 10.3892/ijo.8.2.389.
3
Intestinal tumorigenesis is suppressed in mice lacking the metalloproteinase matrilysin.在缺乏金属蛋白酶基质溶素的小鼠中,肠道肿瘤发生受到抑制。
Proc Natl Acad Sci U S A. 1997 Feb 18;94(4):1402-7. doi: 10.1073/pnas.94.4.1402.
4
Requirement for phosphatidylinositol 3-kinase in epidermal growth factor-induced AP-1 transactivation and transformation in JB6 P+ cells.磷脂酰肌醇3激酶在表皮生长因子诱导的JB6 P+细胞中AP-1反式激活及转化中的作用
Mol Cell Biol. 1996 Nov;16(11):6427-35. doi: 10.1128/MCB.16.11.6427.
5
Inhibition of tumor promoter-induced transformation by retinoids that transrepress AP-1 without transactivating retinoic acid response element.通过反式抑制AP-1而不反式激活视黄酸反应元件的类视黄醇对肿瘤启动子诱导的转化的抑制作用。
Cancer Res. 1996 Feb 1;56(3):483-9.
6
Blocking of tumor promoter-induced AP-1 activity inhibits induced transformation in JB6 mouse epidermal cells.阻断肿瘤启动子诱导的AP-1活性可抑制JB6小鼠表皮细胞的诱导转化。
Proc Natl Acad Sci U S A. 1994 Jan 18;91(2):609-13. doi: 10.1073/pnas.91.2.609.
7
Constitutive AP-1 DNA binding and transactivating ability of malignant but not benign mouse epidermal cells.恶性而非良性小鼠表皮细胞的组成型AP-1 DNA结合及反式激活能力。
Mol Carcinog. 1994 Feb;9(2):61-6. doi: 10.1002/mc.2940090202.
8
Stable expression of a c-JUN deletion mutant in two malignant mouse epidermal cell lines blocks tumor formation in nude mice.c-JUN缺失突变体在两种恶性小鼠表皮细胞系中的稳定表达可阻断裸鼠体内肿瘤的形成。
Cell Growth Differ. 1994 Jan;5(1):9-16.
9
The retinoid signaling pathway: molecular and genetic analyses.维甲酸信号通路:分子与遗传学分析
Semin Cell Biol. 1994 Apr;5(2):115-25. doi: 10.1006/scel.1994.1015.
10
Binding of promoter-associated AP-1 is not altered during induction and subsequent repression of the c-jun promoter by TPA and UV irradiation.在佛波酯(TPA)和紫外线照射诱导并随后抑制c-jun启动子时,启动子相关的激活蛋白-1(AP-1)的结合未发生改变。
Carcinogenesis. 1994 Jun;15(6):1105-13. doi: 10.1093/carcin/15.6.1105.

维甲酸的抗肿瘤促进作用需要阻断激活蛋白-1的活性,而不是激活维甲酸反应元件。

Blocking activator protein-1 activity, but not activating retinoic acid response element, is required for the antitumor promotion effect of retinoic acid.

作者信息

Huang C, Ma W Y, Dawson M I, Rincon M, Flavell R A, Dong Z

机构信息

The Hormel Institute, University of Minnesota, 801 16th Avenue, N.E., Austin, MN 55912, USA.

出版信息

Proc Natl Acad Sci U S A. 1997 May 27;94(11):5826-30. doi: 10.1073/pnas.94.11.5826.

DOI:10.1073/pnas.94.11.5826
PMID:9159159
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC20865/
Abstract

Retinoic acid is one of the most promising drugs for chemotherapy and chemoprevention of cancer. Either blocking activator protein-1 (AP-1) activity or activating retinoic acid response element (RARE) have been proposed to be responsible for its antitumor activity. However, evidence for this hypothesis is lacking in vivo studies. To address this issue, we used an AP-1-luciferase transgenic mouse as a carcinogenesis model and new synthetic retinoids that are either selective inhibitors of AP-1 activation or selective activators of the RARE. The results showed that the SR11302, an AP-1 inhibition-specific retinoid, and other AP-1 inhibitors such as trans-retinoic acid and fluocinolone acetonide, markedly inhibit both 12-O-tetradecanoylphorbol-13-acetate-induced papilloma formation and AP-1 activation in 7,12-dimethyl benz(a)anthracene-initiated mouse skin (P < 0.05). In contrast, repeated applications of SR11235, a retinoid with RARE transactivating activity, but devoid of AP-1 inhibiting effect, did not cause significant inhibition of papilloma formation and AP-1 activation (P > 0.05). These results provide the first in vivo evidence that the antitumor effect of retinoids is mediated by blocking AP-1 activity, but not by activation of RARE.

摘要

维甲酸是用于癌症化疗和化学预防最有前景的药物之一。阻断激活蛋白-1(AP-1)活性或激活维甲酸反应元件(RARE)被认为与其抗肿瘤活性有关。然而,体内研究缺乏支持这一假说的证据。为解决这一问题,我们使用AP-1荧光素酶转基因小鼠作为致癌模型,并使用了新型合成维甲酸,它们要么是AP-1激活的选择性抑制剂,要么是RARE的选择性激活剂。结果显示,AP-1抑制特异性维甲酸SR11302以及其他AP-1抑制剂,如全反式维甲酸和醋酸氟轻松,在7,12-二甲基苯并(a)蒽引发的小鼠皮肤中,显著抑制了12-O-十四烷酰佛波醇-13-乙酸酯诱导的乳头瘤形成和AP-1激活(P<0.05)。相反,重复应用具有RARE反式激活活性但无AP-1抑制作用的维甲酸SR11235,并未显著抑制乳头瘤形成和AP-1激活(P>0.05)。这些结果首次提供了体内证据,表明维甲酸的抗肿瘤作用是通过阻断AP-1活性介导的,而非通过激活RARE介导。