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用于监测人体内异硫氰酸盐水平的新型生物标志物。

New biomarkers for monitoring the levels of isothiocyanates in humans.

机构信息

Department of Environmental Health Sciences, School of Public Health and Tropical Medicine, Tulane University, 1440 Canal Street, Suite 2100 (SL-29), New Orleans, Louisiana 70112, USA.

出版信息

Chem Res Toxicol. 2010 Apr 19;23(4):756-65. doi: 10.1021/tx900393t.

Abstract

Isothiocyanates (ITCs) found in cruciferous vegetables have demonstrated cancer preventive activity in animals, and increased dietary intake of ITCs has been shown to be associated with a reduced cancer risk in humans. ITCs exert their cancer chemopreventive action by multiple mechanisms, for example, by modulating the activities of phase I and phase II drug metabolism enzymes, by inhibiting the cell cycle and histone deacetylase, and by causing apoptotic cell death. In cells, protein adducts account for most of total cellular ITC uptake at 4 h after treatment. The time course of this protein binding correlates well with the inhibition of proliferation and the induction of apoptosis. Animal studies have shown that glutathione conjugates are the major products of ITCs. The major urinary excretion products of ITCs in human are N-acetyl cysteine conjugates. Urinary metabolites might provide the exposure history of the last 24 h, if the urine of the full next day is collected. However, this is not feasible in large epidemiological studies. Furthermore, the mercapturic acids of ITC are not stable. Therefore, stable biomarkers are needed that reflect a larger time span of the ITC exposure history. We developed a method to determine stable (not cysteine adducts) reaction products of ITCs with albumin and hemoglobin in humans and mice. We reacted albumin with the ITCs: benzyl isothiocyanate (BITC), phenylethyl isothiocyanate (PEITC), sulforaphane (SFN), and allyl isothiocyanate (AITC). After enzymatic digestion, we found one major product with lysine using LC-MS/MS. The identity of the adducts was confirmed by comparing the analyses with synthetic standards: N(6)-[(benzylamino)carbonothioyl]lysine (BITC-Lys), N(6)-{[(2-phenylethyl)amino]carbonothioyl}lysine (PEITC-Lys), N(6)-({[3-(methylsulfinyl)propyl]amino}carbonothioyl)lysine (SFN-Lys), and N(6)-[(allylamino]carbonothioyl]lysine (AITC-Lys). The adduct levels were quantified by isotope dilution mass spectrometry using the corresponding new ITC-[(13)C(6)(15)N(2)]lysines as internal standards. The applicability of the method was tested for biological samples obtained from different experiments. In humans consuming garden cress, watercress, and broccoli and/or in mice exposed chronically to N-acetyl-S-{[(2-phenylethyl)amino]carbonothioyl}-l-cysteine, albumin and hemoglobin adducts were found. BITC-Lys, PEITC-Lys, and SFN-Lys released after enzymatic digestion of the proteins were quantified with LC-MS/MS. This new method will enable quantification of ITC adducts in blood proteins from large prospective studies about diet and cancer. Protein adducts are involved in the chemopreventive effects of ITCs. Therefore, blood protein adducts are a potential surrogate marker for the effects of ITCs at the cellular level. This new technique will improve the assessment of ITC exposure and the power of studies on the relationship between ITC intake and cancer.

摘要

异硫氰酸酯(ITC)存在于十字花科蔬菜中,已在动物中证明具有抗癌活性,并且增加 ITC 的饮食摄入已被证明与人类癌症风险降低有关。ITC 通过多种机制发挥其癌症化学预防作用,例如,通过调节 I 相和 II 相药物代谢酶的活性,抑制细胞周期和组蛋白去乙酰化酶,并导致细胞凋亡。在细胞中,蛋白质加合物占处理后 4 小时总细胞 ITC 摄取的大部分。这种蛋白质结合的时间过程与增殖抑制和细胞凋亡诱导密切相关。动物研究表明,谷胱甘肽缀合物是 ITC 的主要产物。ITC 在人类中的主要尿排泄产物是 N-乙酰半胱氨酸缀合物。如果收集第二天的全部尿液,则尿液代谢物可能提供过去 24 小时的暴露史。然而,这在大型流行病学研究中不可行。此外,ITC 的巯基尿酸盐不稳定。因此,需要稳定的生物标志物来反映 ITC 暴露史的更大时间跨度。我们开发了一种方法来确定人类和小鼠中 ITC 与白蛋白和血红蛋白的稳定(非半胱氨酸加合物)反应产物。我们用 ITC 处理白蛋白:苄基异硫氰酸酯(BITC)、苯乙基异硫氰酸酯(PEITC)、萝卜硫素(SFN)和丙烯基异硫氰酸酯(AITC)。用酶消化后,我们使用 LC-MS/MS 发现赖氨酸上有一个主要产物。通过将分析与合成标准品进行比较,确认了加合物的身份:N(6)-[(苄基氨基)羰基硫代]赖氨酸(BITC-Lys)、N(6)-{[(2-苯乙基)氨基]羰基硫代}赖氨酸(PEITC-Lys)、N(6)-{[3-(甲磺酰基)丙基]氨基}羰基硫代}赖氨酸(SFN-Lys)和 N(6)-[(丙烯基氨基]羰基硫代}赖氨酸(AITC-Lys)。通过使用相应的新 ITC-[(13)C(6)(15)N(2)]赖氨酸作为内标物,使用同位素稀释质谱法对加合物水平进行定量。该方法的适用性已在从不同实验中获得的生物样本中进行了测试。在食用豆瓣菜、水田芥和西兰花的人类和/或在慢性暴露于 N-乙酰-S-[(2-苯乙基)氨基]羰基硫代}半胱氨酸的小鼠中发现了白蛋白和血红蛋白加合物。用 LC-MS/MS 定量了蛋白质酶解后释放的 BITC-Lys、PEITC-Lys 和 SFN-Lys。这种新方法将能够在关于饮食和癌症的大型前瞻性研究中定量血液蛋白中的 ITC 加合物。蛋白质加合物参与 ITC 的化学预防作用。因此,血液蛋白加合物是细胞水平上 ITC 作用的潜在替代标志物。这项新技术将提高 ITC 暴露评估和 ITC 摄入与癌症关系研究的能力。

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