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萝卜硫素调节转化和未转化的人T淋巴细胞中的细胞周期和细胞凋亡。

Sulforaphane modulates cell cycle and apoptosis in transformed and non-transformed human T lymphocytes.

作者信息

Fimognari Carmela, Nüsse Michael, Berti Fausto, Iori Renato, Cantelli-Forti Giorgio, Hrelia Patrizia

机构信息

Department of Pharmacology, University of Bologna, 40126 Bologna, Italy.

出版信息

Ann N Y Acad Sci. 2003 Dec;1010:393-8. doi: 10.1196/annals.1299.072.

DOI:10.1196/annals.1299.072
PMID:15033759
Abstract

Isothiocyanates exert chemopreventive effects against chemically induced tumors in animals, modulating enzymes required for carcinogens' activation/detoxification and/or the induction of cell-cycle arrest and apoptosis in tumor cell lines. To investigate the chemopreventive potential of isothiocyanates, we studied proliferation, apoptosis induction and p53, bcl-2 and bax protein expression in Jurkat T-leukemia cells by the isothiocyanate sulforaphane. Sulforaphane caused G(2)/M-phase delay and increase of apoptotic cell fraction in a time- and dose-dependent manner. Necrosis was observed after prolonged exposure to elevated sulforaphane doses. Moreover, it markedly increased p53 and bax protein expression, and slightly affected bcl-2 expression. Since selective targeting and low toxicity for normal host tissues are fundamental requisites for proposed chemopreventive agents such as sulforaphane, we tested sulforaphane on non-transformed phytohemagglutinin-stimulated human T-lymphocytes. We demonstrated that sulforaphane arrested cell-cycle progression in G1 phase by a significant down-modulation of cyclin D3. Moreover, sulforaphane induced apoptosis (and also necrosis), mediated by an increase in the expression of p53, whereas it exerted little effect on bcl-2 and bax levels. These findings indicate that sulforaphane can exert protective effects inhibiting leukemic cell growth. Moreover, sulforaphane is active not only in transformed lymphocytes but also in their normal counterpart. Although in vitro studies do not necessarily predict in vivo outcomes, our findings raise important questions regarding the suitability of sulforaphane for cancer chemoprevention.

摘要

异硫氰酸盐对动物化学诱导的肿瘤具有化学预防作用,可调节致癌物激活/解毒所需的酶和/或诱导肿瘤细胞系中的细胞周期停滞和凋亡。为了研究异硫氰酸盐的化学预防潜力,我们通过异硫氰酸盐萝卜硫素研究了Jurkat T白血病细胞中的增殖、凋亡诱导以及p53、bcl-2和bax蛋白表达。萝卜硫素以时间和剂量依赖性方式导致G(2)/M期延迟并增加凋亡细胞比例。长时间暴露于高剂量萝卜硫素后观察到坏死。此外,它显著增加p53和bax蛋白表达,并轻微影响bcl-2表达。由于对正常宿主组织的选择性靶向和低毒性是萝卜硫素等拟议化学预防剂的基本要求,我们在未转化的植物血凝素刺激的人T淋巴细胞上测试了萝卜硫素。我们证明萝卜硫素通过显著下调细胞周期蛋白D3使细胞周期进程停滞在G1期。此外,萝卜硫素诱导凋亡(以及坏死),由p53表达增加介导,而它对bcl-2和bax水平影响很小。这些发现表明萝卜硫素可以发挥抑制白血病细胞生长的保护作用。此外,萝卜硫素不仅在转化的淋巴细胞中具有活性,在其正常对应物中也具有活性。虽然体外研究不一定能预测体内结果,但我们的发现提出了关于萝卜硫素用于癌症化学预防适用性的重要问题。

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