Toxicity of arsenic on isolated human lymphocytes: The key role of cytokines and intracellular calcium enhancement in arsenic-induced cell death

IF 1.8 3区化学 Q3 CHEMISTRY, INORGANIC & NUCLEAR

Main Group Metal Chemistry Pub Date : 2019-08-23 DOI:10.1515/mgmc-2019-0014

M. Zarei, J. Pourahmad, Ehsan Nassireslami

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引用次数: 17

Abstract

Abstract Arsenic (As) is a semi-metal which causes health problems in human, and immune system has been documented as one of the main target of arsenic toxicity. Apoptosis has a crucial role in regulation of immune system, but it can also have an important role in As immune suppression. So, we decided to assess the comprehensive mechanism of As cytotoxic effect on lymphocytes isolated from human blood. We determine the direct effect of arsenic on human lymphocytes which have a key role in immune system functionality. To evaluate the mechanism of arsenic toxicity on human lymphocytes, we use accelerated cytotoxicity mechanisms screening (ACMS) technique. Lymphocytes were isolated from blood of healthy persons using Ficoll-paque PLUS standard method. Following treatment of human lymphocytes with 0.05-50 μM of arsenic for 12 h, cell viability was measured. For determination of mechanistic parameters, isolated human lymphocytes incubated with 1/2IC5012h (7.5 μM), IC5012h (15 μM) and 2IC5012h (30 μM) for 2, 4 and 6 h. The results of this study demonstrate arsenic-associated apoptosis in human lymphocytes is mainly through enhancement of intracellular calcium which causes oxidative stress and following adverse effect on lymphocytes organelles (like mitochondria and lysosome). Involvement of cellular proteolysis, activation of caspase-3, lipid peroxidation and stimulation of cytokines (IL2, INF-gamma and TNF-alpha) production were also associated with arsenic induced lymphocyte toxicity.

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砷对离体人淋巴细胞的毒性:细胞因子和细胞内钙增强在砷诱导的细胞死亡中的关键作用

砷是一种危害人体健康的半金属，免疫系统是砷中毒的主要靶点之一。细胞凋亡在免疫系统调控中具有重要作用，但在免疫抑制中也有重要作用。因此，我们决定评估砷对人血淋巴细胞毒性作用的综合机制。我们确定了砷对人体淋巴细胞的直接影响，而淋巴细胞在免疫系统功能中起着关键作用。为了评估砷对人淋巴细胞的毒性作用机制，我们采用了加速细胞毒性机制筛选(ACMS)技术。采用Ficoll-paque PLUS标准方法从健康人血液中分离淋巴细胞。用0.05 ~ 50 μM浓度的砷处理人淋巴细胞12 h后，测定细胞活力。为了确定机制参数，分离的人淋巴细胞在1/2IC5012h (7.5 μM)、IC5012h (15 μM)和2IC5012h (30 μM)下分别培养2、4和6 h。本研究结果表明，砷相关的人淋巴细胞凋亡主要是通过增强细胞内钙引起氧化应激，并对淋巴细胞细胞器(如线粒体和溶酶体)产生不良影响。细胞蛋白水解、caspase-3激活、脂质过氧化和细胞因子(il - 2、inf - γ和tnf - α)产生的刺激也与砷诱导的淋巴细胞毒性有关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Main Group Metal Chemistry CHEMISTRY, INORGANIC & NUCLEAR-CHEMISTRY, ORGANIC

CiteScore

4.10

自引率

27.80%

发文量

审稿时长

4 weeks

期刊介绍： This journal is committed to the publication of short communications, original research, and review articles within the field of main group metal and semi-metal chemistry, Main Group Metal Chemistry is an open-access, peer-reviewed journal that publishes in ongoing way. Papers addressing the theoretical, spectroscopic, mechanistic and synthetic aspects of inorganic, coordination and organometallic main group metal and semi-metal compounds, including zinc, cadmium and mercury are welcome. The journal also publishes studies relating to environmental aspects of these metals, their toxicology, release pathways and fate. Articles on the applications of main group metal chemistry, including in the fields of polymer chemistry, agriculture, electronics and catalysis, are also accepted.